LYMPHOMAS
WITH PRIMARY CUTANEOUS MANIFESTATIONS (so-called CUTANEOUS
LYMPHOMAS)
Table of contents :
A variety of T- and B-cell neoplasms can involve the skin, either primarily
or secondarily. The term "primary cutaneous lymphoma" refers to cutaneous
T-cell lymphomas (CTCLs) and cutaneous B-cell lymphomas (CBCLs) that present
in the skin with no evidence of extracutaneous disease at the time of diagnosis.
After the gastrointestinal tract, the skin is the second most common site
of extranodal non-Hodgkin lymphoma, with an estimated annual incidence
of 1:100,000ref.
Primary cutaneous lymphomas often have a completely different clinical
behavior and prognosis from histologically similar systemic lymphomas,
which may involve the skin secondarily, and therefore require different
types of treatment. For that reason, recent classification systems for
non-Hodgkin lymphomas such as the European Organization for Research and
Treatment of Cancer (EORTC) classification for primary cutaneous lymphomas
and the World Health Organization (WHO) classification for tumors of hematopoietic
and lymphoid tissues included primary cutaneous lymphomas as separate entitiesref
(Jaffe ES, Harris NL, Stein H, Vardiman JW (Eds). World Health Organization
Classification of Tumors: Pathology and Genetics of Tumours of Hematopoietic
and Lymphoid Tissues. Lyon, France: IARC Press;2001). In the EORTC classification,
distinction was made between primary cutaneous lymphomas with an indolent,
intermediate, or aggressive clinical behavior. The clinical validity of
this classification has been validated by several large studies, including
follow-up data of > 1300 patients with a primary cutaneous lymphomaref1,
ref2,
ref3.
Although there was consensus between the EORTC and WHO classifications
on the classification of most types of CTCLs, remaining differences between
the 2 classification systems, in particular the controversy on the definition
and terminology of the different types of CBCLs, has resulted in considerable
debate and confusionref1,
ref2,
ref3,
ref4.
During consensus meetings in Lyon, France (September 2003) and Zurich,
Switzerland (January 2004), these differences were resolved by representatives
of both classification systems, and a consensus classification was developed.
This focuses on primary cutaneous lymphomas and a few other conditions
that frequently first present in the skin, such as CD4+/CD56+
hematodermic neoplasm (formerly also known as blastic natural killer cell
lymphoma) and adult T-cell leukemia/lymphoma. Other neoplasms that may
also first present in the skin in a minority of cases, such as precursor
B-lymphoblastic leukemia/lymphoma and acute myeloid leukemia, and secondary
cutaneous manifestations of systemic lymphomas, are not discussed,
but will be included in the monograph to be published in the WHO Blue Book
series in 2005. Relative frequency and disease-specific 5-year survival
of 1905 primary cutaneous lymphomas classified according to the WHO-EORTC
classification :
-
classification of CTCLs other than mycosis fungoides, Sézary syndrome,
and primary cutaneous CD30+ lymphoproliferations : the classification
of this remaining group of CTCLs is difficult and confusing, which is not
surprising given the heterogeneity and rarity of these tumors. Together,
they constitute less than 10% of all CTCLsref1,
ref2,
ref3
(Jaffe ES, Harris NL, Stein H, Vardiman JW (Eds). World Health Organization
Classification of Tumors: Pathology and Genetics of Tumours of Hematopoietic
and Lymphoid Tissues. Lyon, France: IARC Press;2001) With few exceptions,
these lymphomas are clinically aggressive and in most cases systemic chemotherapy
is required. In the EORTC classification, most of these lymphomas were
grouped as primary cutaneous CD30- large T-cell lymphoma or
in the provisional group of primary cutaneous small/medium-sized pleomorphic
CTCLs. Distinction between these 2 categories, which is based on the presence
of > or < 30% large neoplastic T cells, was considered useful because
several studies demonstrated a significant difference in survival between
these 2 groupsref1,
ref2,
ref3,
ref4.
Recent studies suggest, however, that this favorable prognosis is restricted
to small/medium-sized pleomorphic CTCLs with a CD4+ T-cell phenotype,
in particular those that present with localized disease, in contrast to
those with a CD8+ T-cell phenotyperef.
Moreover, the EORTC category of CD30- large-cell CTCLs has become
quite heterogeneous through the recognition of new diagnostic categories,
such as subcutaneous panniculitis-like T-cell lymphoma (SPTL)ref1,
ref2,
ref3,
ref4,
ref5,
ref6,
extranodal NK/T-cell lymphoma, nasal typeref1,
ref2,
ref3,
CD4+/CD56+
hematodermic neoplasm (blastic NK-cell lymphoma)
ref1,
ref2,
ref3,
ref4,
aggressive epidermotropic CD8+ CTCLref1,
ref2,
ref3,
and cutaneous g/d T-cell lymphomaref1,
ref2,
ref3,
ref4,
ref5.
In the WHO classification, SPTL, nasal-type NK/T-cell lymphoma, and blastic
NK-cell lymphoma were included as separate entities, whereas the other
entities were part of the broad category of peripheral T-cell lymphoma
(PTL), unspecified. In the WHO-EORTC classification, extranodal NK/T-cell
lymphoma, nasal type, and CD4+/CD56+ hematodermic
neoplasm (blastic NK-cell lymphoma), are defined as separate entities.
Recent studies showed both clinical, histologic, and immunophenotypical
differences between cases of SPTL with an a/b
T-cell phenotype and those with a g/d T-cell
phenotype, suggesting that these may represent different entities. Whereas
SPTLs with an / T-cell phenotype are homogeneous with a rather indolent
clinical behavior in many patients, SPTLs with a g/d
T-cell phenotype overlap with other types of g/d+
T/NK-cell lymphoma and invariably run a very aggressive clinical courseref1,
ref2,
ref3,
ref4,
ref5.
We therefore suggest that the term "SPTL" be restricted for SPTLs with
an a/b T-cell phenotyperef.
Recent studies have suggested that some disorders can be separated out
as provisional entities from the broad group of "PTL, unspecified," in
the WHO classification. These include aggressive epidermotropic CD8+
CTCL, cutaneous g/d T-cell lymphoma (including
cases formerly diagnosed as SPTL with a g/d
phenotype), and primary cutaneous small-medium CD4+ T-cell lymphoma.
In the WHO-EORTC classification the term "PTL, unspecified," is maintained
for remaining cases that do not fit into either of these provisional entities.
-
Primary cutaneous follicle-center cell lymphoma and primary cutaneous diffuse
large B-cell lymphoma : in recent years, the EORTC categories of primary
cutaneous follicle center cell lymphoma (PCFCCL) and primary cutaneous
large B-cell lymphoma of the leg (PCLBCL-leg) have been the subject of
much debate. The term PCFCCL was introduced in 1987 as a term encompassing
cutaneous lymphomas that were composed of cells with the morphology of
follicle center cells (ie, centroblasts and [large] centrocytes), and that
were classified as either centroblastic/centrocytic or centroblastic lymphoma
according to criteria of the Kiel classificationref.
Whereas small and early lesions may show both small and large neoplastic
B cells and many admixed T cells, and may have a partly follicular growth
pattern, tumorous lesions generally show a predominance of large B cells,
particularly large cleaved or multilobated cells, and less frequently a
predominance of typical centroblasts and immunoblastsref1,
ref2,
ref3.
In contrast to nodal follicular lymphomas, PCFCCLs do generally not express
bcl-2 and are not typically associated with the t(14;18) translocationref1,
ref2.
Clinically, most patients present with localized skin lesions on the head
or trunk and, regardless of the histologic subclassification on the basis
of growth pattern or number of blast cells, are highly responsive to radiotherapy
and have an excellent prognosisref1,
ref2,
ref3,
ref4,
ref5,
ref6,
ref7.
The WHO classification approached these lesions from a different perspective.
PCFCCLs with a partly follicular growth pattern were included as a variant
of follicular lymphoma and designated cutaneous follicle center lymphoma,
while cases with a diffuse growth pattern and a predominance of large centrocytes
or centroblasts were generally classified as diffuse large B-cell lymphoma.
The designation of this latter group as diffuse large B-cell lymphoma was
controversial, since it could lead to overtreatment with multiagent chemotherapy
rather than radiotherapy.
PCLBCL-leg was initially recognized as a subgroup of PCFCCL with a somewhat
different histology and a more unfavorable prognosisref.
In the EORTC classification it was included as a separate subgroup. PCLBCL-leg
particularly affects elderly people and has a higher relapse rate and a
more unfavorable prognosis than PCFCCL with a diffuse large B-cell morphologyref.
Histologically, they have a predominance of centroblasts and immunoblasts
rather than large centrocytes, and consistently strongly express bcl-2
proteinref.
Although delineation of this subgroup based on site has been criticizedref1,
ref2,
recent clinicopathologic and genetic studies further support that PCFCCL
and PCLBCL-leg are distinct groups of CBCLref1,
ref2,
ref3,
ref4,
ref5.
During the consensus meeting in Zurich, histologic slides of a large number
of PCFCCLs and PCLBCL-leg's were reviewed, together with the immunophenotype
and clinical data. It was recognized that PCFCCLs as defined in the EORTC
classification indeed form a spectrum of disease that includes cases with
a follicular, a follicular and diffuse, and a diffuse growth pattern, and
a range of cellular composition from predominantly small centrocytes to
a predominance of large centrocytes with variable numbers of admixed centroblasts
and immunoblasts. This entity will further be referred to as "primary cutaneous
follicle center lymphoma" (PCFCL). The group of PCLBCL-leg was also recognized
as a separate entity. According to the results of a recent multicenter
study, it is also clear that cases with a similar morphology (predominance
or cohesive sheets of centroblasts and immunoblasts), immunophenotype (strong
expression of bcl-2 and Mum-1/IRF4), and prognosis may arise at sites other
than the legref.
In the WHO-EORTC classification the term "PCLBCL, leg type" is proposed
for both lesions on the legs and similar lesions at other skin sites. In
addition, the term "PCLBCL, other" is introduced for rare cases of PCLBCL
not belonging to the group of PCLBCL, leg type, or PCFCL with a diffuse
infiltration of large centrocytes.
Cutaneous T-cell lymphomas(indolent)
: a group of lymphomas including a spectrum of disorders, all of which
exhibit (1) antigen-independent clonal expansion of malignant T lymphocytes
arrested at varying stages of differentiation of cells committed to the
series of Th2 lymphocytes,
and (2) malignant infiltration of the skin, which may be the chief or only
manifestation of diseaseref.
-
mycosis
fungoides (MF) or granuloma fungoides is a commonly
epidermotropic CTCL (the name is a misnomer because it was formerly thought
to be of fungal origin) characterized by a proliferation of small-to medium-sized
T lymphocytes with cerebriform nuclei. The term MF should be used only
for the classical "Alibert-Bazin" type characterized by the evolution
of patches, plaques, and tumors, or for variants showing a similar clinical
course
Epidemiology : MF typically affects older
adults (median age at diagnosis: 55-60 years; male-to-female ratio: 1.6-2.0:1),
but may occur in children and adolescentsref1,
ref2,
ref3,
ref4.
MF is the most common type of CTCL and accounts for almost 50% of all primary
cutaneous lymphomas.
Aetiology :
-
HTLV-1
?
-
Borrelia burgdorferi
: in an endemic area, PCR for the flagellin gene of Bb was used to study
formalin-fixed paraffin-embedded lesional skin biopsies from 83 patients
with
MF and 83 sex- and age-matched healthy controls with homolocalised cutaneous
nevi. Borrelia burgdorferi-specific sequence was detected in 15
out of 83 skin samples of patients with MF (18.1%), but in 0 out of 83
matched healthy controls (P<0.0001)ref
Pathogenesis : neoplastic T cells in mycosis
fungoides (MF) are resistant to apoptotic agents, including galectin-1
that is abundant in skin. While MF cells are typically CD7-,
and thus galectin-1 resistant, CD7+ HH cells, derived from an
MF patient, were also resistant to galectin-1. HH cells demonstrate altered
cell surface glycosylation, with loss of core 2 O-glycan ligands
for galectin-1 created by core 2 b1,6-N-acetylglucosaminyltransferase
(C2GnT-I). Loss of core 2 O-glycans on tumor cells was also seen
in primary CD7+ MF lesions. Surprisingly, HH cells are heterozygous
for a C2GnT-I point mutation, yet this mutation resulted in a dramatic
reduction in cellular glycosyltransferase activity. Expression of wildtype
C2GnT-I in human HH cells, or murine lymphoma cells that lack C2GnT-I,
restored core 2 O-glycan expression and susceptibility to galectin-1,
while mutant enzyme lacked activity and did not restore core 2 O-glycan
expression or susceptibility to galectin-1. Mutant enzyme did not have
a dominant negative effect by affecting dimerization or activity of wildtype
enzyme; rather, C2GnT-I haploinsufficiency is sufficient for loss of core
2 O-glycan expression and galectin-1 resistance. Thus, glycosyltransferase
haploinsufficiency results in altered cellular glycosylation and resistance
to cell death, identifying a new survival mechanism for T lymphoma cellsref.
Symptoms & signs : MF has an indolent
clinical course with slow progression over years or sometimes decades,
from patches to more infiltrated plaques and eventually to tumors. In some
patients, lymph nodes and visceral organs may become involved in the
later stages of the disease. The initial skin lesions have a predilection
for the buttocks and other sun-protected areas. Patients with tumor-stage
MF characteristically show a combination of patches, plaques, and tumors,
which often show ulceration. If only tumors are present, without preceding
or concurrent patches or plaques, a diagnosis of MF is highly unlikely
and another type of CTCL should be considered. In some cases it evolves
into generalized lymphoma with a tendency for nodal, hematogenous, and
visceral involvement. Stages :
-
premycotic stage : intensely pruritic erythematous, eczematous,
or psoriasiform eruptions on the buttock
-
mycotic stage / stage of infiltrated plaques : presence of Sézary
cells
-
tumor stage : mushroom-like tumors that often ulcerate
In a variant type of tumor stage (mycosis fungoides d'emblée),
tumors may develop without preceding lesions or prodromal symptoms
Laboratory examinations :
-
histopathology : early patch lesions in MF show superficial bandlike or
lichenoid infiltrates, mainly consisting of lymphocytes and histiocytes.
Atypical cells with small-to medium-sized, highly indented (cerebriform),
and sometimes hyperchromatic nuclei are few, and mostly confined to the
epidermis (epidermotropism). They characteristically colonize the basal
layer of the epidermis either as single, often haloed cells, or in a linear
configurationref.
In typical plaques, epidermotropism is generally more pronounced than in
the patches. The presence of intraepidermal collections of atypical cells
(Pautrier microabscesses) is a highly characteristic feature, but is observed
in only a minority of casesref.
With progression to tumor stage, the dermal infiltrates become more diffuse
and epidermotropism may be lost. The tumor cells increase in number and
size, showing variable proportions of small, medium-sized, to large cerebriform
cells, blast cells with prominent nuclei, and intermediate forms. Transformation
to a diffuse large-cell lymphoma that may be either CD30- or
CD30+ may occur and is often associated with a poor prognosisref.
Mycosis fungoides. (A) Typical patches and plaques on the trunk. (B) Infiltration
of atypical T cells into the epidermis with formation of Pautrier microabscess
(hematoxylin and eosin [H&E] staining; original magnification, x 200).
The image in panel B was obtained through a Leica DM6000B microscope (Leica,
Rijswijk, the Netherlands). Image acquisition was performed with a ProgResC10
camera and software (JenaOptik, Jena, Germany). An HC Plan APO 40x/0.85
objective was used.
-
immunophenotype : the neoplastic cells in MF have a mature CD2+3+4+5+7+/-8-45RO+
memory
T-cell phenotype. In rare cases of otherwise classical, MF a CD4-,
CD8+ mature T-cell phenotype may be seenref1,
ref2,
ref3,
ref4.
Such cases have the same clinical behavior and prognosis as CD4+
cases, and should not be considered separately. Demonstration of an aberrant
phenotype (eg, loss of pan–T-cell antigens such as CD2, CD3, and CD5) is
often seen and is an important adjunct in the diagnosis of MFref.
Expression of cytotoxic proteins (T-cell intracellular antigen-1 [TIA-1],
granzyme B) by the neoplastic CD4+ T-cells has been detected
in 10% of MF plaques, but is much more common in tumors showing blastic
transformationref.
-
cytogenetics : clonal TcR gene rearrangements are detected in most casesref.
Many structural and numerical chromosomal abnormalities have been described,
in particular in the advanced stages of MF, but recurrent, MF-specific
chromosomal translocations have not been identifiedref1,
ref2.
Chromosomal loss at 10q and abnormalities in p15, p16, and p53 tumor suppressor
genes are commonly found in patients with MFref.
Prognosis : dependent on stage, and in particular
the type and extent of skin lesions and the presence of extracutaneous
diseaseref1,
ref2,
ref3.
Patients with limited patch/plaque-stage MF have a similar life expectancy
to an age-, sex-, and race-matched control population. In recent studies,
10-year disease-specific survivals were 97-98% for patients with limited
patch/plaque disease (covering < 10% of the skin surface), 83% for patients
with generalized patch/plaque disease (covering > 10% of the skin surface),
42% for patients with tumor stage disease, and about 20% for patients with
histologically documented lymph node involvementref1,
ref2,
ref3.
Patients with effaced lymph nodes, visceral involvement, and transformation
into a large T-cell lymphoma have an aggressive clinical course. Patients
usually die of systemic involvement or infections. In its earliest stage,
IA (patches and/or plaques involving < 10% of body surface area), MF
has a survival that does not impact the expected normal life span (Zackheim
HS, Amin S, Kashani-Sabet M, et al. Prognosis in cutaneous T-cell lymphoma
by skin stage: Long-term survival in 489 patients. J Am Acad Dematol. 1999;40:418–425)ref.
Alternatively, patients with extracutaneous disease, or stage IV, have
median survivals < 2 yearsref
Therapy :
-
limited stage diseaseref
: skin-targeted therapies as photo (chemo)–therapy (eg, psoralen
plus ultraviolet A [PUVA]),
topical application of nitrogen mustard or
carmustine
(BCNU),
or radiotherapy,
including total skin electron beam irradiation (TSEBI), are preferredref1,
ref2,
ref3.
In patients with limited patch-stage disease topical corticosteroids
or bexarotene
gel can be used. However, the exact place of these new treatments, either
as single-agent therapy or in combination with other therapies (eg, PUVA)
in the treatment of MF remains to be established. Multiagent chemotherapy
is generally used in case of unequivocal lymph node or systemic involvement,
or in cases with widespread tumor-stage MF refractory to skin-targeted
therapies, but should not be considered in early patch/plaque stage diseaseref.
-
more advanced disease : systemic therapy includes photopheresis, IFN-a
and other cytokines (eg, IL-12),
steroids, and chemotherapy. New agents that have been developed for progressive
and/or stage IV disease includeref1,
ref2,
ref3,
ref4,
ref5
:
-
bexarotene
(Targretin, LGD 1069) is an oral agent, a rexinoid or RXR-selective retinoid
agonist, approved in 2000 in the US for patients with MF who are refractory
to at least one prior systemic therapy. In patients with relapsed MF who
were heavily pretreated, response rates of 45% and 55% were observed among
patients receiving 300 mg/m2/d or higher doses, respectivelyref.
The median time to response was 180 days (range, 14 to 197) for patients
receiving 300 mg/m2/d and 59 days (range, 22 to 169) for the
higher dosesref.
Approximately 33% of patients progressed at a median time of 1 year. The
most common adverse events were hypertriglyceridemia (82%), hypercholesterolemia
(30%), hypothyroidism (29%), elevated liver functions (20%), headache (20%),
asthenia (16%), pruritus (13%), leukopenia (11%), and rash (11%)ref.
Lipid lowering agents and thyroid replacement for central hypothyroidism
are recommended. In a pilot project 10 patients with advanced CTCLs, who
had received a variety of previous treatments, were treated with bexarotene
300 mg/m2 body surface daily at the departments of dermatology
in Munster, Minden and Charite Berlin, Germanyref
-
DAB389IL-2; denileukin
diftitox,
also approved in the US in 2000, is a recombinant fusion protein consisting
of peptide sequences for the enzymatically active and membrane translocation
domains of diphtheria toxin with rIL-2. CD25, an IL-2 receptor marker,
has been utilized for determining eligibility for denileukin difitox; however,
studies are investigating whether the marker is required for response.
In a trial of 2 dose levels of denileukin difitox, 9 or 18 µg/kg/d
x 5 days every 3 weeks, 30% of 71 patients with MF had an objective response
(20% PR, 10% CR)ref.
The median time to first response was 6 weeks (range 3-27), and 95% of
patients who had a response had at least a 25% decrease in disease by week
9.60 The median duration of response was 6.9 months (range, 2.7-46.1+).
Adverse events included acute infusion-related events in 60% of patients
[dyspnea (20%), back pain (17%), hypotension (17%), and chest pain/tightness
(13%)], flu-like symptoms in 85% of patients, and a vascular leak syndrome
(hypoalbuminemia, edema and/or hypotensin) in 25% of patients. Hypoalbuminemia
occurred in 79% (15% grade 3 or 4) and elevated hepatic transaminases were
observed in 61% (17% grade 3 or 4) of patientsref
-
nucleoside analogs, 2'-deoxycoformycin
(dCF; pentostatin),
2
chlorodeoxyadenosine (CdA),
and fludarabine (F-ara-A AMP)
are purine antimetabolites that inhibit adensosine deaminase, an enzyme
with high concentrations in lymphoid cells, particularly T cells. The phosphorylated
derivatives of the analogs induce apoptosis through down regulation of
ribonucleotide reductase and inhibition of DNA replication and repair.
Most of the clinical trials of these agents in T cell lymphomas have been
in patients with MF, but some of the studies have included PTCL, usually
with cutaneous involvementref1,
ref2,
ref3,
ref4,
ref5,
ref6
(Kurzrock R. Pentostatin (Nipent) in T-cell lymphomas. Semin Oncol. 2000;27(suppl
5):64–66). Gemcitabine (2',2-difluorodeoxy-cytidine) is a pyrimidine antimetabolite
that has also shown activity in MF and PTCLref.
The results of some of the largest series of patients primarily with advanced
stage MF who received single agent nucleoside analogs. The response rates
vary from a low of 19% for fludarabine to 70% and 71% for gemcitabine and
dCF, respectively; the latter two series included patients with PTCL whose
response was similar to MF. The median duration of response is usually
< 6 months. The addition of interferon to dCF in MF did not appear to
increase the response rate (41%) but did improve the progression-free survival
in responders to over a year (13.1 mo)ref
|
drug/author
|
|
no. of patients
|
regimen
|
response rate (%)
|
CR (%)
|
comments
|
| fludarabine |
Von Hoffref |
31 |
25 mg/m2/d x 5 |
19 |
3 |
SWOG: 30% response in good risk |
| 2'-deoxycoformycin |
Horef |
44 |
4 mg/m2 q week x 3, then q 2 wk x 3, q mo x4 |
36 |
2 |
EORTC: median response 4.5 mo for SS and 8.3 mo for MF |
| Kurzrock R. Pentostatin (Nipent) in T-cell lymphomas. Semin Oncol.
2000;27(suppl 5):64–66 |
24 |
3.75-5.0 mg/m2/d q d X 3d q 3 wks |
71 |
25 |
median response was 2 mo in tumor stage mycosis fungoides and 3.5 mo
in Sezary syndrome. 3 pts with PTCL responded. |
| 2-CdA |
Savenref |
15 |
0.05-0.15 mg/kg/d x 7 d |
47 |
20 |
median response of 5 mo |
| Kuzelref |
21 |
0.1 mg/kg/d x 7 d or x 5 d |
28 |
14 |
median response 4.5 mo for CR, 2 mo for PR |
| gemcitabine |
Zinzaniref |
44 |
1.2 gm/m2 d 1,8,15 q mo x 3 cycles |
70 |
11.5 |
no difference in response between PTCL (N=14) and MF; median response
15 mo for CR, 10 mo for PR |
-
variants and
subtypes of mycosis fungoides : apart from the classical Alibert-Bazin
type of MF, many clinical and/or histologic variants have been reported.
Clinical variants, such as bullous and hyper- or hypopigmented MF, have
a clinical behavior similar to that of classical MF, and therefore are
not considered separately. In contrast, folliculotropic MF (MF-associated
follicular mucinosis), pagetoid reticulosis, and granulomatous slack skin
have distinctive clinicopathologic features, and are therefore considered
separately.
-
folliculotropic MF is a variant
of MF characterized by the presence of folliculotropic infiltrates, often
with sparing of the epidermis, and preferential involvement of the head
and neck area. Most cases show mucinous degeneration of the hair follicles
(follicular mucinosis) and are traditionally designated as MF-associated
follicular mucinosis. Similar cases, but without follicular mucinosis,
have been reported as folliculocentric or pilotropic MFref.
Recent studies showed no differences in clinical presentation and clinical
behavior between cases of folliculotropic MF with or without associated
follicular mucinosis, and suggested that cases with a preferential infiltration
of hair follicles with or without the presence of mucin should be termed
"follicular MF" or "folliculotropic MF"ref1,
ref2,
ref3.
In the WHO-EORTC classification, folliculotropic MF is preferred as the
most appropriate term. From a biologic point of view, the most relevant
feature in both cases with and without associated follicular mucinosis
is the deep, follicular, and perifollicular localization of the neoplastic
infiltrates, which makes them less accessible to skin-targeted therapies.
Epidemiology : occurs mostly in adults,
but may occasionally affect children and adolescents. Males are more often
affected than females
Symptoms & signs : patients may present
with grouped follicular papules, acneiform lesions, indurated plaques,
and sometimes tumors, which preferentially involve and are most pronounced
in the head and neck arearef.
The skin lesions are often associated with alopecia, and sometimes with
mucinorrhea. Infiltrated plaques in the eyebrows with concurrent alopecia
are a common and highly characteristic finding. Unlike in classical MF,
pruritus is often severe, and may represent a good parameter of disease
progression. Secondary bacterial infections are frequently observed.
Laboratory examinations :
-
histopathology. Characteristic findings include the primarily perivascular
and periadnexal localization of the dermal infiltrates with variable infiltration
of the follicular epithelium by small, medium-sized, or sometimes large
hyperchromatic cells with cerebriform nuclei, and sparing of the epidermis
(folliculotropism instead of epidermotropism). Most cases show mucinous
degeneration of the follicular epithelium (follicular mucinosis), as assessed
with Alcian blue staining. There is often a considerable admixture of eosinophils
and sometimes plasma cells. In most cases the neoplastic T cells have a
CD3+, CD4+, CD8- phenotype as in classical
MF. An admixture of CD30+ blast cells is common. (A) Infiltrated
plaques on the forehead and right eyebrow showing hair loss. (B) Diffuse
dermal infiltrate surrounding follicular structures. Note infiltrate-free
zone beneath epidermis (no epidermotropism) (H&E staining; original
magnification, x 25). Image acquisition was performed as described for
Figure 1B. An HC FLUOTAR 2.5x/0.07 objective was used.
In some cases, prominent infiltration of both follicular epithelium
and eccrine sweat glands may be observedref.
Similar cases with prominent infiltration of eccrine sweat glands, often
associated with alopecia, have been designated as syringotropic MFref1,
ref2
Prognosis : recent studies described a disease-specific
5-year survival of approximately 70-80% in patients with folliculotropic
MF, which is similar to that of classical tumor-stage MF, but significantly
worse than that of patients with classical plaque stage MFref1,
ref2
Treatment : because of the perifollicular
localization of the dermal infiltrates, folliculotropic MF is often less
responsive to skin-targeted therapies, such as PUVA and topical nitrogen
mustard, than classical plaque-stage MF. In such cases total skin electron
beam irradiation is an effective treatment, but sustained complete remissions
are rarely achievedref.
Alternatively, PUVA combined with retinoids or interferon alpha may be
considered, whereas persistent tumors can be effectively treated with local
radiotherapy.
-
pagetoid reticulosis is a variant
of MF characterized by the presence of localized patches or plaques with
an intraepidermal proliferation of neoplastic T cells. The term pagetoid
reticulosis should only be used for the localized type (Woringer-Kolopp
type) and not for the disseminated type (Ketron-Goodman type).
Generalized cases would currently likely be classified as aggressive
epidermotropic CD8+ CTCL, cutaneous
g/d+
T-cell lymphoma, or tumor
Symptoms & signs : patients present
with a solitary psoriasiform or hyperkeratotic patch or plaque, which is
usually localized on the extremities
Laboratory examinations :
-
histopathology. The typical histologic picture shows a hyperplastic epidermis
with marked infiltration by atypical pagetoid cells, singly or arranged
in nests. The atypical cells have medium-sized or large, sometimes hyperchromatic
and cerebriform nuclei, and abundant, vacuolated cytoplasm. The upper dermis
may show a mixed infiltrate of lymphocytes or histiocytes, but does not
contain neoplastic T cells.
-
immunophenotype : the neoplastic T cells may have either a CD3+,
CD4+, CD8- or a CD3+, CD4-,
CD8+ phenotype. CD30 is often expressedref1,
ref2
Prognosis : slowly progressive. In contrast
to classical MF, extracutaneous dissemination or disease-related deaths
have never been reported
Treatment : the preferred mode is radiotherapy
or surgical excision. In some instances topical nitrogen mustard or topical
corticosteroids
may be an acceptable alternative.
-
granulomatous slack skin
(GSS) is an extremely rare subtype of CTCL characterized by the slow
development of folds of lax skin in the major skin folds and histologically
by a granulomatous infiltrate with clonal T cellsref
Symptoms & signs : circumscribed areas
of pendulous lax skin with a predilection for the axillae and groins. In
approximately one-third of the reported patients, an association with Hodgkin
lymphoma was observed, and association with classical MF has also been
reportedref1,
ref2,
ref3.
Most patients have an indolent clinical course
Laboratory examinations :
-
histopathology. Fully developed lesions show dense granulomatous dermal
infiltrates containing atypical T cells with slightly indented to cerebriform
nuclei, macrophages and often many multinucleated giant cells, and destruction
of elastic tissue. The epidermis may show focal infiltration by small atypical
T cells
-
immunophenotype : the atypical T cells have a CD3+, CD4+,
CD8- phenotype.
Therapy : radiotherapy
may be effective, but experience is limited. Rapid recurrences after surgical
excision have been reported.
-
Sézary syndrome (SS) or
erythroderma (Sézary A & Bouvrain Y. Erythrodermie avec
présence de cellules monstrueuses dans le derme et sang circulant.
Bull.Soc.Franç Derm.Syph. 45:254-260 (1938)) is defined historically
by the triad of erythroderma, generalized lymphadenopathy, and the presence
of neoplastic T cells (Sézary cells) in skin, lymph nodes, and peripheral
bloodref.
In a recent report of the International Society for Cutaneous Lymphomas
(ISCL), criteria recommended for the diagnosis of SS include one or more
of the following:
-
an absolute Sézary cell count > 1000 cells/mm3
-
demonstration of immunophenotypical abnormalities (an expanded CD4+
T-cell population resulting in a CD4/CD8 ratio > 10, loss of any or all
of the T-cell antigens CD2, CD3, CD4, and CD5, or both)
-
demonstration of a T-cell clone in the peripheral blood by molecular or
cytogenetic methodsref
It is acknowledged that SS is part of a broader spectrum of erythrodermic
CTCL, and that alternative staging systems for assessment of the degree
of peripheral blood involvement in these erythrodermic CTCLs have been
proposedref1,
ref2.
However, until the results of an ISCL study investigating the clinical
validity of these proposals are available, demonstration of a T-cell clone
(preferably of the same T-cell clone in skin and peripheral blood) in combination
with one of the above-mentioned cytomorphologic or immunophenotypic criteria
are suggested as minimal criteria for the diagnosis of SS to exclude patients
with benign inflammatory conditions simulating SS.
Epidemiology : SS is a rare disease and
occurs exclusively in adults. It is characterized by erythroderma, which
may be associated with marked exfoliation, edema, and lichenification,
and which is intensely pruritic. Lymphadenopathy, alopecia, onychodystrophy,
and palmoplantar hyperkeratosis are common findingsref
Aetiology : HTLV-1
?
Symptoms & signs : exfoliative erythroderma,
intense
pruritus,
peripheral lymphadenopathy, Pautrier's microabscess or abscess (one
of the well-defined collections of mycosis cells located within nonspongiotic
intraepidermal vesicles in CTCL)
Laboratory examinations :
-
Sézary cell (an abnormal mononuclear cell (medium to large
lymphocyte) with a hyperchromic infolded cribriform nucleus (said to resemble
a monocyte nucleus) and a narrow rim of cytoplasm that may contain vacuoles,
occurring in small and large cell variants)
-
histopathology : the histological features in SS may be similar to those
in MF. However, the cellular infiltrates in SS are more often monotonous,
and epidermotropism may sometimes be absent. In up to one-third of biopsies
from patients with otherwise classical SS the histologic picture may be
nonspecificref1,
ref2.
Involved lymph nodes characteristically show a dense, monotonous infiltrate
of Sézary cells with effacement of the normal lymph node architectureref.
Bone marrow may be involved, but the infiltrates are often sparse and mainly
interstitialref
-
immunophenotype : the neoplastic T cells have a CD1a++2++3++4++5++7++8-10-11b-16-19-25-38-71-158k
/ KIR3DL2+TdT-, sIg-, HLA-DR-
phenotype. In cases with a predominant CD3+, CD4-,
CD8+ T-cell population in the skin and peripheral blood, the
diagnosis of actinic reticuloid should be consideredref.
Circulating Sézary cells often show loss of CD7 and CD26ref
-
cytogenetics : TcR genes are clonally rearranged. Demonstration of clonal
T cells in the peripheral blood is considered as an important diagnostic
criterion allowing differentiation between SS and benign forms of erythrodermaref1,
ref2,
ref3.
Recurrent chromosomal translocations have not been detected in SS, but
complex karyotypes are commonref1,
ref2.
Several studies have identified a consistent pattern of identical chromosomal
abnormalities in SS, which was almost identical to that in MF, suggesting
that both conditions represent parts of the same spectrum of disease with
a similar pathogenesisref1,
ref2.
Chromosomal amplification of the JUNB gene, a member of the activator protein-1
(AP-1) transcription factor complex involved in cell proliferation and
T helper 2 (Th2) cytokine expression by T cells, has been identified
in SSref1,
ref2
-
circulating malignant and nonmalignant clones vimentinhiCD158k-ref
-
T-cell receptor (TCR) clonality studies
-
TCR Vb monoclonal antibody (mAb) analysis alone
is not enough
Prognosis : generally poor, with a median
survival between 2 and 4 years, depending on the exact definition usedref1,
ref2.
The disease-specific 5-year survival of 52 SS patients included in the
Dutch and Austrian registries was 24%. Most patients die of opportunistic
infections that are due to immunosuppression.
Therapy : extracorporeal photopheresis
(ECP), either alone or in combination with other treatment modalities (eg,
IFN-a),
has been reported as an effective treatment in SS and erythrodermic MF,
with overall response rates of 30%-80%, and complete response rates of
14-25%ref1,
ref2.
This great variation in response rates may reflect differences in patient
selection and/or concurrent therapies. The suggested superiority of ECP
over the traditional low-dose chemotherapy regimens has not yet been substantiated
by controlled randomized trialsref.
Beneficial results have also reported of IFN-a,
either alone or in combination with PUVA therapy, prolonged treatment with
a combination of low-dose chlorambucil
(2-4 mg/d) and prednisone
(10-20 mg/d) or with methotrexate
(5-25 mg/wk), but complete responses are uncommon. Skin-directed therapies
like PUVA
or potent topical corticosteroids
may be used as adjuvant therapy. Recent studies report beneficial effects
of bexarotene
and alemtuzumab (anti-CD52)
but the long-term effects of these therapies remain to be establishedref1,
ref2,
ref3
-
adult T-cell leukemia/lymphoma
(ATLL) is a T-cell neoplasm etiologically associated with the human
T-cell leukemia virus 1 (HTLV-1).
Skin lesions are generally a manifestation of widely disseminated disease.
However, a slowly progressive form that may have only skin lesions has
been described (smoldering variant)ref
Epidemiology : ATLL is endemic in areas
with a high prevalence of HTLV-1 in the population, such as southwest Japan,
the Caribbean islands, South America, and parts of Central Africa. ATLL
develops in 1% to 5% of seropositive individuals after more than 2 decades
of viral persistence
Symptoms & signs : most patients present
with acute ATLL characterized by the presence of leukemia, lymphadenopathy,
organomegaly, hypercalcemia, and in about 50% skin lesions, most commonly
nodules or tumors (33%), generalized papules (22%), or plaques (19%)ref.
Chronic and smoldering variants frequently present with skin lesions, which
may closely resemble MF, whereas circulating neoplastic T cells are few
or absent.
Laboratory examinations :
-
histopathology : skin lesions show a superficial or more diffuse infiltration
of medium-sized to large T cells with pleomorphic or polylobated nuclei,
which often display marked epidermotropism. The histologic picture may
be indistinguishable from MF. Skin lesions in the smoldering type may show
sparse dermal infiltrates with only slightly atypical cells. The neoplastic
T cells express a CD3+, CD4+, CD8- phenotype.
CD25 is highly expressedref1,
ref2
-
genetic features : TcR genes are clonally rearranged. Clonally integrated
HTLV-1 genes are found in all cases, and are useful in differentiating
between chronic or smoldering variants of ATLL and classical MF or SSref
Prognosis : clinical subtype is the main prognostic
factor. Survival in acute and lymphomatous variants ranges from 2 weeks
to > 1 year. Chronic and smoldering forms have a more protracted clinical
course and a longer survival, but transformation into an acute phase with
an aggressive course may occurref1,
ref2
Therapy : in most cases systemic chemotherapy
is required.98,99 In chronic and smoldering cases mainly affecting the
skin, skin-targeted therapies as in MF may be used.
-
primary
cutaneous CD30+ lymphoproliferative disorders are the second
most common group of CTCLs, accounting for approximately 30% of CTCLs.
This group includes primary cutaneous anaplastic large cell lymphoma (C-ALCL),
lymphomatoid papulosis (LyP), and borderline cases. It is now generally
accepted that C-ALCL and LyP form a spectrum of disease, and that histologic
criteria alone are often insufficient to differentiate between these 2
ends of this spectrumref.
The clinical appearance and course are used as decisive criteria for the
definite diagnosis and choice of treatment. The term "borderline case"
refers to cases in which, despite careful clinicopathologic correlation,
a definite distinction between C-ALCL and LyP cannot be made. Clinical
examination during further follow-up will generally disclose whether the
patient has C-ALCL or LyPref.
-
primary
cutaneous anaplastic large-cell
lymphoma
(C-ALCL) is composed of large cells with an anaplastic, pleomorphic,
or immunoblastic cytomorphology and expression of the CD30 antigen by the
majority (> 75%) of tumor cellsref.
There is no clinical evidence or history of LyP, MF, or another type of
CTCL.
Epidemiology : C-ALCL affects mainly adults
with a male to female ratio of 2-3:1
Symptoms & signs : most patients present
with solitary or localized nodules or tumors, and sometimes papules, and
often show ulcerationref1,
ref2.
Multifocal lesions are seen in about 20% of the patients. Multiple small
lesions (< 1 cm) are more common in LyP, whereas primary cutaneous ALCL
is typified by single or grouped lesions, often > 2 cm in size. These lymphomas
frequently relapse in the skin. Extracutaneous dissemination occurs in
approximately 10% of the patients, and mainly involves the regional lymph
nodes, and most often in patients with multiple lesions.
Laboratory examinations :
-
histopathology. There is a diffuse, nonepidermotropic infiltrate with cohesive
sheets of large CD30+ tumor cells. In most cases the tumor cells
have the characteristic morphology of anaplastic cells, showing round,
oval, or irregularly shaped nuclei, prominent eosinophilic nucleoli, and
abundant cytoplasm. Less commonly (20-25%), they have a nonanaplastic (pleomorphic
or immunoblastic) appearanceref1,
ref2.
Reactive lymphocytes are often present at the periphery of the lesions.
Ulcerating lesions may show a LyP-like histology with an abundant inflammatory
infiltrate of reactive T cells, histiocytes, eosinophils and/or neutrophils,
and relatively few CD30+ cells. In such cases epidermal hyperplasia
may be prominent.Primary cutaneous CD30+lymphoproliferative disease (pcCD30+
LPD). (A) Diffuse dermal infiltrate of large atypical cells admixed with
small lymphocytes. (H&E staining; original magnification, x 300). (B)
The large atypical cells are strongly positive for CD30. (C-D) The histologic
picture in panels A and B can be found both in C-ALC and in LyP. The final
diagnosis depends on the clinical presentation. In combination with the
solitary tumor of the patient shown in panel C the definite diagnosis will
be C-ALC; in combination with recurrent, self-healing papulonecrotic skin
lesions (D), the final diagnosis is LyP. Image acquisition for panels A
and B was performed as described for Figure 1B. An HC Plan APO 20x/0.70
objective was used.
-
immunophenotype : the neoplastic cells generally show an activated CD4+
T-cell phenotype with variable loss of CD2, CD5, and/or CD3, and frequent
expression of cytotoxic proteins (granzyme B, TIA-1, perforin)ref1,
ref2.
Some cases (< 5%) have a CD8+ T-cell phenotype. CD30 must
be expressed by the majority (> 75%) of the neoplastic T cellsref.
Unlike systemic CD30+ lymphomas, most C-ALCLs express the cutaneous
lymphocyte antigen (CLA), but do not express epithelial membrane antigen
(EMA) and anaplastic lymphoma kinase (ALK), indicative of the 2;5 chromosomal
translocation or its variantsref1,
ref2,
ref3.
Unlike Hodgkin and Reed-Sternberg cells in Hodgkin disease, staining for
CD15 is generally negative. Coexpression of CD56 is observed in rare cases,
but does not appear to be associated with an unfavorable prognosisref.
-
cytogenetics : most cases show clonal rearrangement of T-cell receptor
genes. The (2;5)(p23;q35) translocation and its variants, which is a characteristic
feature of systemic ALCL, is not or rarely found in C-ALCLref.
Prognosis : usually favorable with a 10-year
disease-related survival exceeding 90%ref1,
ref2.
Spontaneous regression is the rule for LyP; however, regression also occurs
in approximately 25% of C-ALCL. Patients presenting with multifocal skin
lesions and patients with involvement of only regional lymph nodes have
a similar prognosis to patients with only skin lesionsref.
No difference in clinical presentation, clinical behavior, or prognosis
is found between cases with an anaplastic morphology and cases with a nonanaplastic
(pleomorphic or immunoblastic) morphologyref1,
ref2.
Therapy : radiotherapy
or surgical excision is the first choice of treatment in patients presenting
with a solitary or few localized nodules or tumors. Patients presenting
with multifocal skin lesions can best be treated with radiotherapy in case
of only a few lesions, or with low-dose methotrexate, as in LyPref1,
ref2.
Patients presenting with or developing extracutaneous disease or rare patients
with rapidly progressive skin disease should be treated with doxorubicin-based
multiagent chemotherapy.
Differential diagnosis : C-ALCL should
be distinguished from LyP and
systemic
ALCL
to avoid unnecessarily aggressive therapy.
-
lymphomatoid papulosis (LyP)
is
defined as a chronic, recurrent, self-healing papulonecrotic or papulonodular
skin disease with histologic features suggestive of a (CD30+)
malignant lymphoma.
Epidemiology : LyP generally occurs in
adults (median age, 45 years; male-to-female ratio, 1.5:1), but may occur
in children as wellref1,
ref2,
ref3,
ref4.
LyP is characterized by the presence of papular, papulonecrotic, and/or
nodular skin lesions at different stages of development, predominantly
on the trunk and limbs. Individual skin lesions disappear within 3 to 12
weeks, and may leave behind superficial scars. The duration of the disease
may vary from several months to more than 40 years. In up to 20% of patients
LyP may be preceded by, associated with, or followed by another type of
malignant (cutaneous) lymphoma, generally MF, a (C-)ALCL, or Hodgkin lymphomaref
Laboratory examinations :
-
histopathology. The histologic picture of LyP is extremely variable, and
in part correlates with the age of the biopsied skin lesion. 3 histologic
subtypes of LyP (types A, B, and C) have been described, which represent
a spectrum with overlapping featuresref1,
ref2,
ref3.
In LyP type A lesions, scattered or small clusters of large, sometimes
multinucleated or Reed-Sternberg–like, CD30+ cells are intermingled
with numerous inflammatory cells, such as histiocytes, small lymphocytes,
neutrophils, and/or eosinophils. LyP type C lesions demonstrate a monotonous
population or large clusters of large CD30+ T cells with relatively
few admixed inflammatory cells. LyP type B is uncommon (< 10%) and is
characterized by an epidermotropic infiltrate of small atypical cells with
cerebriform nuclei similar to that observed in MF.
-
immunophenotype. The large atypical cells in the LyP type A and type C
lesions have the same phenotype as the tumor cells in C-ALCLref.
The atypical cells with cerebriform nuclei in the LyP type B lesions have
a CD3+, CD4+, CD8- phenotype and do not
express CD30 antigen.
-
cytogenetics : clonally rearranged T-cell receptor genes have been detected
in approximately 60%-70% of LyP lesionsref.
Identical rearrangements have been demonstrated in LyP lesions and associated
lymphomasref.
The (2;5)(p23;q35) translocation is not detected in LyPref
Prognosis : excellent. In a recent study of
118 LyP patients only 5 (4%) patients developed a systemic lymphoma, and
only 2 (2%) patients died of systemic disease over a median follow-up period
of 77 monthsref.
Risk factors for the development of a systemic lymphoma are unknown.
Therapy : since a curative therapy is
not available and none of the available treatment modalities affects the
natural course of the disease, the short-term benefits of active treatment
should be balanced carefully against the potential side effectsref.
Low-dose oral methotrexate (5-20 mg/wk) is the most effective therapy to
suppress the development of new skin lesionsref.
Beneficial effects have been reported of PUVA and topical chemotherapyref.
However, after discontinuation of treatment the disease generally relapses
within weeks or months. Therefore, in patients with relatively few and
nonscarring lesions, long-term follow-up without active treatment should
be considered.
-
subcutaneous
panniculitis-like T-cell lymphoma (SPTL) is defined as a cytotoxic
T-cell lymphoma characterized by the presence of primarily subcutaneous
infiltrates of small, medium-sized, or large pleomorphic T cells and many
macrophages, predominantly affecting the legs, and often complicated by
a hemophagocytic syndrome.12 Recent studies suggest that at least 2 groups
of SPTL with a different histology, phenotype, and prognosis can be distinguished.
Cases with an a/b+ T-cell phenotype
are usually CD8+, are restricted to the subcutaneous tissue
(no dermal and/or epidermal involvement), and often run an indolent clinical
courseref1,
ref2,
ref3,
ref4.
In contrast, SPTL with a / T-cell phenotype, approximately 25% of all cases,
are typically CD4-, CD8-, and often coexpress CD56,
the neoplastic infiltrates are not confined to the subcutaneous tissue,
but may involve the epidermis and/or dermis as well, and invariably have
a very poor prognosisref1,
ref2,
ref3,
ref4,
ref5.
In the WHO-EORTC classification the term "SPTL" is only used for cases
with an a/b+ T-cell phenotype, whereas
cases with a g/d+ T-cell phenotype
are included in the category of cutaneous
g/d
T-cell lymphomasref.
Epidemiology : SPTL occurs in adults as
well as in young children, and both sexes are equally affected
Symptoms & signs : patients generally
present with solitary or multiple nodules and plaques, which mainly involve
the legs, or may be more generalized. Ulceration is uncommon. Systemic
symptoms such as fever, fatigue, and weight loss may be present. The disease
may be complicated by a hemophagocytic syndrome, which is generally associated
with a rapidly progressive courseref.
However, a hemophagocytic syndrome is probably less common than in cutaneous
g/d
T-cell lymphomas with panniculitis-like lesions. Dissemination to extracutaneous
sites is rare. SPTL may be preceded for years or decades by an seemingly
benign panniculitisref1,
ref2,
ref3
Laboratory examinations :
-
histopathology reveals subcutaneous infiltrates simulating a panniculitis
showing small, medium-sized, or sometimes large pleomorphic T cells with
hyperchromatic nuclei and often many macrophages. The overlying epidermis
and dermis are typically uninvolvedref1,
ref2.
Rimming of individual fat cells by neoplastic T cells is a helpful, though
not completely specific, diagnostic featureref.
Necrosis, karyorrhexis, and cytophagocytosis are common findings. In the
early stages the neoplastic infiltrates may lack significant atypia and
a heavy inflammatory infiltrate may predominateref1,
ref2,
ref3
-
immunophenotype. These lymphomas show a a/b+,
CD3+, CD4-, CD8+ T-cell phenotype, with
expression of cytotoxic proteinsref1,
ref2,
ref3,
ref4.
CD30 and CD56 are rarely, if ever, expressed. Subcutaneous panniculitis-like
T-cell lymphoma. (A) Deeply seated nodular skin lesions and residual lipodystrophy
after disappearance of the skin lesions. (B) Infiltrates are almost exclusively
localized in subcutaneous tissue resembling a lobular panniculitis (H&E
staining; original magnification, x 25). (C) Rimming of individual fat
cells by neoplastic T cells (H&E staining; original magnification,
x 480). (D) Tumor cells show positive staining for CD8. Image acquisition
for panels B-D was performed as described for Figure 1B. An HC FLUOTAR
2.5x/0.07 objective was used for panel B; an HC Plan APO 40x/0.85 objective
was used for panels C and D.
-
cytogenetics : the neoplastic T cells show clonal TCR gene rearrangements.
Specific genetic abnormalities have not been identified. HHV-4
/ EBV
is absent.
Prognosis : in contrast to prior reports indicating
that patients with a SPTL have a rapidly fatal course, recent studies suggest
that many patients with a SPTL (with a CD8+, a/b+
T-cell phenotype) have a protracted clinical course with recurrent subcutaneous
lesions but without extracutaneous dissemination or the development of
a hemophagocytic syndromeref1,
ref2.
Based on the few published reports in which appropriate phenotyping was
performed, the 5-year survival of such patients may be > 80%ref
Therapy : patients have generally been
treated with doxorubicin-based
chemotherapy and radiotherapyref1,
ref2,
ref3,
ref4,
ref5,
ref6.
However, recent studies suggest that many patients can be controlled for
long periods of time with systemic corticosteroidsref1,
ref2
-
extranodal NK/T-cell
lymphoma, nasal type is a nearly always HHV-4
/ EBV+
lymphoma of small, medium, or large cells usually with an NK-cell, or more
rarely a cytotoxic T-cell, phenotype. The skin is the second most common
site of involvement after the nasal cavity/nasopharynx, and skin involvement
may be a primary or secondary manifestation of the disease. Since both
groups show an aggressive clinical behavior and require the same type of
treatment, distinction between "primary" and "secondary" cutaneous involvement
seems not useful for this categoryref1,
ref2,
ref3,
ref4,
ref5.
Therefore, the WHO classification–derived term "extranodal NK/T-cell lymphoma,
nasal type," rather than "(primary) cutaneous NK/T-cell lymphoma, nasal
type," is preferred.
Epidemiology : patients are adults with
a predominance of males. This lymphoma is more common in Asia, Central
America, and South America. Patients generally present with multiple plaques
or tumors preferentially on the trunk and extremities, or in the case of
nasal NK/T-cell lymphoma with a midfacial destructive tumor, previously
also designated "lethal midline granuloma"ref1,
ref2,
ref3,
ref4,
ref5,
ref6,
ref7.
Ulceration is common. Systemic symptoms such as fever, malaise, and weight
loss may be present, and some cases are accompanied by a hemophagocytic
syndrome. The disease is closely related to aggressive NK-cell leukemia,
which also may have cutaneous manifestations, and is also HHV-4
/ EBV
associated.
Laboratory examinations :
-
histopathology : these lymphomas show dense infiltrates involving the dermis
and often the subcutis. Epidermotropism may be present. Prominent angiocentricity
and angiodestruction are often accompanied by extensive necrosisref1,
ref2.
NK/T-cell lymphoma has a broad cytologic spectrum ranging from small to
large cells, with most cases consisting of medium-sized cells. The cells
may have irregular or oval nuclei, moderately dense chromatin, and pale
cytoplasm. In some cases a heavy inflammatory infiltrate of small lymphocytes,
histiocytes, plasma cells, and eosinophils can be seen.
-
immunophenotype : the neoplastic cells express CD2, CD56, cytoplasmic CD3,
and cytotoxic proteins (TIA-1, granzyme B, perforin), but lack surface
CD3.122 In rare CD56- cases detection of EBV by in situ hybridization
and expression of cytotoxic proteins are required for diagnosis (Jaffe
ES, Harris NL, Stein H, Vardiman JW (Eds). World Health Organization Classification
of Tumors: Pathology and Genetics of Tumours of Hematopoietic and Lymphoid
Tissues. Lyon, France: IARC Press;2001). Latent membrane protein-1 (LMP-1)
is inconsistently expressed.
-
cytogenetics : the TcR is usually in germline configuration, but can be
rearranged in rare tumors with a cytotoxic T-cell phenotype. HHV-4
/ EBV
is expressed almost in all cases, suggesting a pathogenetic role of this
virus.18 Primary cutaneous aggressive epidermotropic CD8+ cytotoxic
T-cell lymphoma. (A) Typical presentation with nodules and tumors showing
central ulceration. (B-D) Tumor cells show striking epidermotropism (H&E
staining; original magnification, x 150), and strongly express CD8 (C)
and TIA-1 (D). Image acquisition for panels B-D was performed as described
for Figure 1B. An HC Plan APO 10x/0.40 objective lens was used.
Prognosis : nasal-type NK/T-cell lymphoma
presenting in the skin is a highly aggressive tumor with a median survival
of < 12 monthsref1,
ref2,
ref3,
ref4.
The most important factor predicting poor outcome is the presence of extracutaneous
involvement at presentation. In patients presenting with only skin lesions,
a median survival of 27 months was reported, compared with 5 months for
patients presenting with cutaneous and extracutaneous diseaseref.
CD30+, CD56+ cases reported to have a better prognosis
may have been examples of C-ALCL with coexpression of CD56ref.
Therapy : systemic chemotherapy is the
first choice of treatment, but the results are disappointingref1,
ref2
-
variant. Hydroa vacciniforme-like CTCL is a rare type of HHV-4
/ EBV-associated
lymphoma of CD8+ cytotoxic T cells, which affects children almost
exclusively in Latin America and Asiaref1,
ref2,
ref3.
Patients present with a papulovesicular eruption clinically resembling
hydroa vacciniforme, particularly on the face and upper extremities (sunexposed
areas). The prognosis is poor.
-
primary
cutaneous peripheral T-cell lymphoma,
unspecified
(PTL), in the WHO classification represent a heterogeneous group which
includes all T-cell neoplasms that do not fit into any of the better defined
subtypes of T-cell lymphoma/leukemia. Recent studies have suggested that
primary cutaneous aggressive epidermotropic CD8+ cytotoxic T-cell
lymphoma, cutaneous
g/d T-cell lymphoma, and
primary cutaneous small-medium CD4+ T-cell lymphoma can be separated
out as provisional entities. For the remaining diseases that do not fit
into either of these provisional entities the designation PTL, unspecified,
is maintained. In all cases a diagnosis of MF must be ruled out by complete
clinical examination and an accurate clinical history.
-
primary
cutaneous aggressive epidermotropic CD8+ cytotoxic T-cell lymphoma
(provisional entity) is characterized by a proliferation of epidermotropic
CD8+ cytotoxic T-cells and an aggressive clinical behaviorref1,
ref2.
Differentiation from other types of CTCL expressing a CD8+ cytotoxic
T-cell phenotype, as observed in > 50% of patients with pagetoid reticulosis,
and in rare cases of MF, LyP, and C-ALCL, is based on the clinical presentation
and clinical behaviorref.
In these latter conditions, no difference in clinical presentation or prognosis
between CD4+ and CD8+ cases is found.
Symptoms & signs : localized or disseminated
eruptive papules, nodules, and tumors showing central ulceration and necrosis
or by superficial, hyperkeratotic patches and plaquesref1,
ref2.
The clinical features are very similar to those observed in patients with
a cutaneous / T-cell lymphoma and cases described as generalized pagetoid
reticulosis (Ketron-Goodman type) in the pastref.
These lymphomas may disseminate to other visceral sites (lung, testis,
central nervous system, oral mucosa), but lymph nodes are often sparedref
Laboratory examinations :
-
histopathology : histologically, these lymphomas show an acanthotic or
atrophic epidermis, necrotic keratinocytes, ulceration, and variable spongiosis,
sometimes with blister formationref1,
ref2.
Epidermotropism is often pronounced ranging from a linear distribution
to a pagetoid pattern throughout the epidermis. Invasion and destruction
of adnexal skin structures are commonly seen. Angiocentricity and angioinvasion
may be present. Tumor cells are small-medium or medium-large with pleomorphic
or blastic nuclei.
-
immunophenotype. The tumor cells have a betaF1+, CD3+,
CD8+, granzyme B+, perforin+, TIA-1+,
CD45RA+, CD45RO-, CD2-, CD4-,
CD5-, CD7-/+ phenotyperef1,
ref2,
ref3,
ref4,
ref5.
HHV-4
/ EBV
is generally negative.
-
cytogenetics : the neoplastic T cells show clonal TCR gene rearrangements.
Specific genetic abnormalities have not been described.
Prognosis : these lymphomas often have an
aggressive clinical course with a median survival of 32 monthsref.
There is no difference in survival between cases with a small- or large-cell
morphologyref
Therapy : patients are generally treated
with doxorubicin-based
multiagent chemotherapy.
-
cutaneous
g/d
T-cell lymphoma (CGD-TCL) (provisional entity)
is a lymphoma composed
of a clonal proliferation of mature, activated
g/d
T cells with a cytotoxic phenotype. This group includes cases previously
known as SPTL with a g/d phenotype. A similar
and possibly related condition may present primarily in mucosal sitesref.
Whether cutaneous and mucosal gamma/delta TCL are all part of a single
disease (ie, muco-cutaneous g/d TCL) is not
yet clearref1,
ref2.
Distinction between "primary" and "secondary" cutaneous cases is not useful
in this group, since both groups have a very grim prognosis.
Symptoms & signs : generally present
with disseminated plaques and/or ulceronecrotic nodules or tumors, particularly
on the extremities, but other sites may be affected as wellref1,
ref2,
ref3,
ref4,
ref5.
Involvement of mucosal and other extranodal sites is frequently observedref,
but involvement of lymph nodes, spleen, or bone marrow is uncommon. A hemophagocytic
syndrome may occur in patients with panniculitis-like tumorsref1,
ref2.
Laboratory examinations :
-
histopathology : 3 major histologic patterns of involvement can be present
in the skin: epidermotropic, dermal, and subcutaneous.
Often more than one histologic pattern is present in the same patient in
different biopsy specimens or within a single biopsy specimenref1,
ref2.
The neoplastic cells are generally medium to large in size with coarsely
clumped chromatin. Large blastic cells with vesicular nuclei and prominent
nucleoli are infrequent. Apoptosis and necrosis are common, often with
angioinvasion. The subcutaneous cases may show rimming of fat cells, similar
to SPTL of a/b origin.
-
immunophenotype : the tumor cells characteristically have a bF1-,
CD3+, CD2+, CD5-, CD7+/-, CD56+
phenotype with strong expression of cytotoxic proteins. Most cases lack
both CD4 and CD8, though CD8 may be expressed in some casesref1,
ref2.
In frozen sections the cells are strongly positive for TCR-d.
If only paraffin sections are available, the absence of bF1
may be used to infer a g/d origin under appropriate
circumstancesref1,
ref2.
-
genetic features : the cells show clonal rearrangement of the TCRg
gene. TCRb may be rearranged or deleted, but
is not expressed. HHV-4 / EBV
is generally negativeref1,
ref2.
Prognosis : most patients have aggressive
disease resistant to multiagent chemotherapy and/or radiationref1,
ref2,
ref3,
ref4,
ref5,
ref6.
In a recent series of 33 patients, a median survival of 15 months was notedref.
This study showed a trend for decreased survival for patients who had subcutaneous
fat involvement compared with patients who had epidermal or dermal disease
only.
Therapy : patients should be treated with
systemic chemotherapy, but the results are often disappointing.
-
primary cutaneous CD4+ small/medium-sized pleomorphic T-cell lymphoma
(provisional entity) is a CTCL defined by a predominance of small-to
medium-sized CD4+ pleomorphic T cells without (a history of)
patches and plaques typical of MF, and in most cases, a favorable clinical
courseref.
In contrast to the EORTC classification, in the WHO-EORTC classification
the term "small/medium-sized pleomorphic CTCL" is restricted to cases with
a CD4+ T-cell phenotype. Cases with a CD3+, CD4-,
CD8+ phenotype usually have a more aggressive clinical course
are included in the group of aggressive epidermotropic CD8+
CTCLsref.
Symptoms & signs : characteristically,
these lymphomas present with a solitary plaque or tumor, generally on the
face, the neck, or the upper trunk (Figure 6A). Less commonly, they present
with one or several papules, nodules, or tumorsref1,
ref2,
ref3,
ref4,
ref5
Laboratory examinations :
-
histopathology : these lymphomas show dense, diffuse, or nodular infiltrates
within the dermis with a tendency to infiltrate the subcutis. Epidermotropism
may be present focally. There is a predominance of small/medium-sized pleomorphic
T cells. A small proportion (< 30%) of large pleomorphic cells may be
presentref.
In some cases a considerable admixture with small reactive lymphocytes
and histiocytes may be observed.
-
immunophenotype : by definition these lymphomas have a CD3+,
CD4+, CD8-, CD30- phenotype, sometimes
with loss of pan–T-cell markers. Cytotoxic proteins are generally not expressedref
-
genetic features : the TCR genes are clonally rearrangedref1,
ref2.
No consistent cytogenetic abnormalities have yet been identified. Demonstration
of an aberrant T-cell phenotype and clonality are useful criteria to differentiate
these small/medium-sized pleomorphic CTCLs from pseudo–T-cell lymphomas,
which may also present with a solitary plaque or noduleref.129
Primary cutaneous CD4+ small/medium-sized pleomorphic T-cell
lymphoma. (A) Presentation with a solitary tumor on the scalp. (B) Diffuse
dermal infiltrate mainly composed of small pleomorphic T cells with few
scattered blasts cells (H&E staining; original magnification, x 750).
An HC FLUOTAR 63x/0.90 objective lens was used.
Prognosis : these lymphomas have a rather
favorable prognosis, with an estimated 5-year survival of approximately
60% to 80%ref1,
ref2,
ref3,
ref4,
ref5,
ref6,
ref7,
ref8.
Particularly, cases presenting with a solitary or localized skin lesions
seem to have an excellent prognosisref.
Therapy : in patients with solitary localized
skin lesions, surgical excision or radiotherapy
is the preferred mode of treatment. Cyclophosphamide as single-agent therapy
and interferon alpha have been reported effective in patients with more
generalized skin diseaseref.
However, the optimal treatment for this group has still to be defined.
-
primary
cutaneous peripheral T-cell lymphoma, unspecified : the designation
is maintained for cutaneous T-cell lymphomas that do not fit into any of
the better defined subtypes of CTCL. Hence, other categories of T-cell
lymphoma must be excluded. These include the 3 provisional entities described
earlier.
Symptoms & signs : patients are commonly
adults, who present with solitary, localized, or more frequently generalized
nodules or tumorsref1,
ref2,
ref3,
ref4.
No sites of predilection have been recorded.
Laboratory examinations :
-
histopathology : skin lesions show nodular or diffuse infiltrates with
variable numbers of medium-to large-sized pleomorphic or immunoblast-like
T cells. Epidermotropism is generally mild or absent. Large neoplastic
cells represent at least 30% of the total tumor cell populationref
-
immunophenotype. Most cases show an aberrant CD4+ T-cell phenotype
with variable loss of pan–T-cell antigens. CD30 staining is negative or
restricted to a few scattered tumor cells. Rare cases may show coexpression
of CD56. Expression of cytotoxic proteins is uncommonref
Prognosis : generally poor, with 5-year survival
rates < 20%ref1,
ref2,
ref3,
ref4,
ref5.
No statistical differences in survival were found between cases presenting
with solitary/localized lesions and cases presenting with generalized skin
lesionsref
Therapy : patients should be treated with
multiagent chemotherapy.
Cutaneous B-cell lymphomas
:
primary
cutaneous marginal-zone B-cell
lymphoma
(PCMZL)ref
is an indolent lymphoma composed of small B cells, including marginal zone
(centrocyte-like) cells, lymphoplasmacytoid cells, and plasma cells. It
includes cases previously designated as primary cutaneous immunocytomaref,
and cases of cutaneous follicular lymphoid hyperplasia with monotypic plasma
cellsref.
Exceptional cases of primary cutaneous plasmacytoma without underlying
multiple myeloma (extramedullary plasmacytoma of the skin) show considerable
overlap with PCMZL and are therefore included in this categoryref.
PCMZL is considered part of the broad group of extranodal marginal zone
B-cell lymphomas commonly involving mucosal sites, called MALT (mucosa-associated
lymphoid tissue) lymphomas.
Epidemiology : in Japan ages of the patients
ranged from 26 to 75 years (mean 55.7 years) with a slight female predilectionref
Pathogenesis : the chromosomal aberrations
in MALT lymphoma such as t(11;18)(q21;q21), t(14;18)(q32;q21) and t(3;14)(p14.1;q32)
were not reported in any of the Japanese casesref
Symptoms & signs : in most instances
patients with PCMZL present with red to violaceous papules, plaques, or
nodules localized preferentially on the trunk or extremities, especially
the arms. In contrast to PCFCL, presentation with multifocal skin lesions
is frequent. Ulceration is uncommon. PCMZLs have a tendency to recur in
the skin, but dissemination to extracutaneous sites is exceedingly rareref1,
ref2,
ref3,
ref4.
In some cases spontaneous resolution of the skin lesions may be observed.
The development of anetoderma in spontaneously resolving lesions has been
observedref.
An association with Borrelia
burgdorferi
infection has been reported in a significant minority of European cases
of PCMZL (Italyref
and Scottish Highlandsref),
but not in Asian cases (Japanref1,
ref2)
or cases from the USAref.
Associated autoimmune diseases are uncommon in PCMZL, but rather suggest
secondary cutaneous involvement of a systemic lymphomaref.
2/16 Japanese patients had suffered from Sjogren's
syndromeref.
Laboratory examinations :
-
although all of these neoplasms presumably are monoclonal, monoclonal IgH
rearrangement can only be detected in approximately 75% of cases. Most
molecular studies to assess for clonality have used polymerase chain reaction-based
methods, and thus this false-negative rate may be attributable to somatic
mutation of the IgH variable region genes
-
histopathology : these lymphomas show nodular to diffuse infiltrates with
sparing of the epidermis. The infiltrates are composed of small lymphocytes,
marginal zone B cells (centrocyte-like cells), lymphoplasmacytoid cells,
and plasma cells, admixed with small numbers of centroblast- or immunoblast-like
cells and many reactive T cells. Reactive germinal centers are frequently
observed. They may be surrounded by a population of small-to medium-sized
cells with irregular nuclei, inconspicuous nucleoli, and abundant pale
cytoplasm (marginal zone B cells). Monotypic plasma cells are often located
at the periphery of the infiltrates and in the superficial dermis beneath
the epidermisref1,
ref2,
ref3,
ref4.
periodic acid-schiff (PAS)+ intranuclear or intracytoplasmic
inclusions may be present in cases with a predominance of lymphoplasmacytoid
cells. PCMZLs rarely show transformation into a diffuse large B-cell lymphoma,
but a relative increase in large transformed cells can be seen in some
cases.
-
immunophenotype : the marginal zone B cells express CD20, CD79a, and bcl-2,
but are negative for CD5, CD10, and bcl-6, which may be useful in distinction
from PCFCLref1,
ref2.
Reactive germinal centers are typically bcl-6+, CD10+,
and bcl-2-. Plasma cells express CD138 and CD79a, but generally
not CD20, and show monotypic cytoplasmic immunoglobulin light chain expression
on paraffin sections.
-
cytogenetics : 10-20% of PCMZLs have recurrent chromosomal translocations,
including the t(14;18)(q32;q21)/IgH-malt1, t(11;18)(q21;q21), and t(3;14)(p14;q32)
involving IGH and FOXP1 genesref1,
ref2.
The t(14;18)(q32;q21) and t(11;18)(q21;q21) have been shown to activate
the NF-kB pathway. However, other translocations
observed in gastric MALT lymphomas, such as t(11;18)(q21;q21) and t(1;14)(p22;q32),
have not been found in PCMZLref1,
ref2
Prognosis : excellent with a 5-year survival
close to 100%ref1,
ref2,
ref3,
ref4,
ref5,
ref6
Therapy : patients with a solitary or
a few lesions can be treated with radiotherapy
or surgical excision. In patients with associated B burgdorferi infection,
systemic antibiotics should be tried firstref.
For patients presenting with multifocal skin lesions, chlorambucil
or intralesional or subcutaneous administration of IFN-a
may produce complete responses in approximately 50% of patientsref.
Very good results have also been obtained with the use of systemic or intralesional
rituximabref.
In patients showing frequent skin relapses, topical or intralesional corticosteroids
may be considered; alternatively, an expectant strategy can be followed,
similar to that used in other indolent B-cell lymphomas and leukemias.
Characteristic clinical presentation with multiple nodules and small tumors
on the back and arms :
primary
cutaneous follicle-center lymphoma
(PCFCL) is defined as a tumor of neoplastic follicle center cells,
usually a mixture of centrocytes (small and large cleaved follicle center
cells) and variable numbers of centroblasts (large noncleaved follicle
center cells with prominent nucleoli), with a follicular, a follicular
and diffuse, or a diffuse growth pattern, which generally present on the
head or trunk. Lymphomas with a diffuse growth pattern and a monotonous
proliferation of centroblasts and immunoblasts are, irrespective of site,
excluded and are classified as PCLBCL. Characteristic features of PCFCL
and PCLBCL, leg type :
|
PCFCL |
PCLBCL, leg type |
| morphology |
predominance of centrocytes that are often large,
especially in diffuse lesions. |
predominance or confluent sheets of medium-sized
to large B cells with round nuclei, prominent nucleoli, and coarse chromatin
resembling centroblasts and/or immunoblasts. |
| centroblasts may be present, but not in confluent
sheets. |
diffuse growth pattern. |
| growth pattern may be follicular, follicular
and diffuse, or diffuse (a continuum without distinct categories or grades). |
|
| phenotype |
Bcl-2: -/+ (Faint staining, when present; minority
of cells (see comments in paragraph on PCFCL)) |
Bcl-2: ++ (strong staining; in most neoplastic
cells) |
| Bcl-6: + |
Bcl-6: +/- |
| CD10: -/+ (Diffuse lesions, mostly CD10-) |
CD10: - |
| Mum-1: - |
Mum-1: + |
| clinical features |
middle-aged adults. |
elderly, especially females, |
| localized lesions on head or trunk (90%). |
lesions localized on leg(s), most often below
the knee. |
| multifocal lesions in rare cases. |
rare cases with lesions at other sites than the
leg (10%). |
Symptoms & signs : PCFCL has
a characteristic clinical presentation with solitary or grouped plaques
and tumors, preferentially located on the scalp or forehead or on the trunk,
and rarely on the legsref1,
ref2,
ref3.
Particularly on the trunk, these tumors may be surrounded by erythematous
papules and slightly indurated plaques, which may precede the development
of tumorous lesions for months or even many years. In the past, PCFCLs
with such a typical presentation on the back were referred to as "reticulohistiocytoma
of the dorsum" or "Crosti lymphoma"ref
(Crosti A. Micosi fungoide e reticuloistiocitomi cutanei maligni. Minerva
Dermat. 1951;26: 3-11). Presentation with multifocal skin lesions is observed
in a small minority of patients, but is not associated with a more unfavorable
prognosisref1,
ref2.
If left untreated, the skin lesions gradually increase in size over years,
but dissemination to extracutaneous sites is uncommon. Primary cutaneous
follicle center lymphoma. (A) Typical presentation with tumors on the chest
surrounded by less infiltrated erythematous skin lesions. (B) Presentation
with multiple tumors confined to the scalp. (C) Diffuse dermal infiltrate
mainly consisting of large centrocytes and multilobated cells (H&E
staining; original magnification, x 480). (D-E) Serial sections stained
for CD20 (D) and bcl-2 (E). Bcl-2 is expressed by perivascular T cells,
but not by the neoplastic B cells. Image acquisition for panels A and C-E
was performed as described for Figure 1B. An HC Plan APO objective was
used (40x/0.85 for panel C; 10x/0.40 for panels D and E).
Laboratory examinations :
-
histopathology : PCFCLs show nodular to diffuse infiltrates with almost
constant sparing of the epidermis. The histologic picture is variable,
which relates primarily to the age and the growth rate of the biopsied
skin lesion as well as the locationref1,
ref2.
A clear-cut follicular growth pattern is more commonly observed in lesions
arising on the scalp than those presenting on the trunkref.
Small and early lesions contain a mixture of centrocytes, relatively few
centroblasts, and many reactive T cells. Large centrocytes, often multilobated,
are a common feature of PCFCL (Figure 9C). The large neoplastic B cells
may have a fibroblast-like appearance. In small and/or early lesions a
clear-cut follicular growth pattern or, more often, remnants of a follicular
growth pattern may be observed. If present, the abnormal follicles are
composed of malignant bcl-6+ follicle center cells enmeshed in a network
of CD21+ or CD35+ FDCs. The follicles are ill-defined,
lack tingible body macrophages, and generally have a reduced or absent
mantle zoneref1,
ref2.
With progression to tumorous lesions the neoplastic B cells increase both
in number and size, whereas the number of reactive T cells steadily decreasesref1,
ref2.
Follicular structures, if present before, are no longer visible except
for occasional scattered CD21+ or CD35+ follicular
dendritic cells. Tumorous skin lesions generally show a monotonous population
of large follicle center cells, generally large centrocytes and multilobated
cells, and in rare cases spindle-shaped cells, with a variable admixture
of centroblasts and immunoblastsref1,
ref2,
ref3
,
ref4,
ref5.
Usually, a prominent stromal component is present.
-
immunophenotype : the neoplastic cells express the B-cell–associated antigens
CD20 and CD79a, and may show monotypic staining for surface immunoglobulins
(sIgs). However, absence of detectable sIg is common in tumorous lesions
showing a diffuse population of large follicle center cells. PCFCLs consistently
express bcl-6ref1,
ref2,
ref3.
CD10 expression is particularly observed in cases with a follicular growth
pattern, but is uncommon in PCFCLs with a diffuse growth patternref1,
ref2.
Staining for CD5 and CD43 is negative. Unlike nodal and secondary cutaneous
follicular lymphomas, PCFCLs do not express bcl-2 protein or show faint
bcl-2 staining in a minority of neoplastic B-cellsref1,
ref2,
ref3..
Staining for MUM-1/IRF4 is negativeref
-
cytogenetics : clonally rearranged immunoglobulin genes are present. Somatic
hypermutation of variable heavy and light chain genes has been demonstrated,
which further supports the follicle center cell origin of these lymphomasref1,
ref2.
In most studies PCFCLs, including cases with a follicular growth pattern,
do not show the t(14;18), which is characteristically found in systemic
follicular lymphomas and a proportion of systemic diffuse large B-cell
lymphomaref1,
ref2,
ref3,
ref4.
Inactivation of p15 and p16 tumor suppressor genes by promotor hypermethylation
has been reported in about 10% and 30% of PCFCLs, respectivelyref.
Chromosomal imbalances have been identified by comparative genomic hybridization
(CGH) analysis in a minority of PCFCLs, but a consistent pattern has not
yet emergedref1,
ref2.
In a recent study using interphase fluorescence in situ hybridization,
no evidence for translocations involving IgH, myc, or bcl-6 loci were foundref.
PCFCLs have the gene expression profile of germinal center–like large B-cell
lymphomasref.
Prognosis : regardless of the growth pattern
(follicular or diffuse), the number of blast cells, or the presence of
either localized or multifocal skin disease, these PCFCLs have an excellent
prognosis with a 5-year survival > 95%ref1,
ref2,
ref3,
ref4,
ref5,
ref6,
ref7,
ref8,
ref9,
ref10.
A recent study suggests that strong expression of bcl-2 in PCFCLs with
a diffuse large-cell histology is associated with a more unfavorable prognosisref.
Therapy : in patients with localized or
few scattered skin lesions, radiotherapy
is the preferred mode of treatment, even in cases with a predominance of
large "cleaved" cellsref1,
ref2,
ref3,
ref4,
ref5
(Pimpinelli N, Vallecchi C. Local orthovolt radiotherapy in primary cutaneous
B-cell lymphomas: results in a series of 115 patients. Skin Cancer. 1999;14:
219-224). Cutaneous relapses, observed in approximately 20% of patients,
do not indicate progressive disease and can be treated with radiotherapy
as well. Anthracycline-based chemotherapy is required only in patients
with very extensive cutaneous disease and patients developing extracutaneous
diseaseref1,
ref2.
Recent studies report beneficial effects of systemic or intralesional administration
of rituximab
therapy in small series of PCFCLs, but the long-term effects of this approach
have yet to be determinedref1,
ref2,
ref3
Comment. Characteristically, PCFCLs do not express bcl-2 protein, or
show faint bcl-2 staining in a minority of tumor cells, and do not show
the t(14;18)ref1,
ref2,
ref3.
However, recent studies report the presence of t(14;18) and/or bcl-2 expression
in a significant minority of PCFCLsref1,
ref2,
ref3,
ref4,
ref5.
Whether these discrepant results are the result of differences in patient
selection (eg, incomplete staging) or different definitions for bcl-2 positivity,
or represent regional differences is as yet unknown. Importantly, in PCFCLs
with a follicular growth pattern there are no differences in clinical presentation
and behavior between bcl-2 and/or t(14;18)-positive and -negative casesref1,
ref2,
ref3,
ref4,
ref5.
In contrast, recent studies suggest that expression of bcl-2 protein by
more than 50% of the neoplastic B cells in PCFCLs with a diffuse proliferation
of large centrocytes, observed in approximately 15% of cases, is associated
with a more unfavorable prognosisref.
Further studies are warranted to define the clinical and biological significance
of bcl-2 expression and/or the presence of t(14;18) observed in some cases
of PCFCL. Notwithstanding, demonstration of bcl-2 expression and/or t(14;
18) should always raise suspicion of a systemic lymphoma involving the
skin secondarily.
primary
cutaneous diffuse large B-cell
lymphoma,
leg type is a PCLBCL with a predominance or confluent sheets of centroblasts
and immunoblasts, characteristically presenting with skin lesions on the
(lower) legs. Uncommonly, skin lesions with a similar morphology and phenotype
can arise at sites other than the legs.
Epidemiology : predominantly affects elderly
patients, particularly femalesref1,
ref2,
ref3.
Symptoms & signs : generally rapidly
growing red or bluish-red tumors on one or both (lower) legs. In contrast
to the group of PCFCLs, these lymphomas more often disseminate to extracutaneous
sites and have a more unfavorable prognosisref1,
ref2.
Reports on PCLBCL, leg type, arising at sites other than the leg are few.
In a recent European multicenter study, 16 of 17 patients presented with
solitary or localized skin lesions either on the trunk or head, and 7 of
17 patients developed extracutaneous diseaseref
Laboratory examinations :
-
histopathology : these lymphomas show diffuse infiltrates, which often
extend into the subcutaneous tissue. These infiltrates generally show a
monotonous population or confluent sheets of centroblasts and immunoblastsref1,
ref2.
Mitotic figures are frequently observed. Small B cells are lacking and
reactive T cells are relatively few and often confined to perivascular
areas. A prominent stromal reaction as in PCFCLs is not observed.
-
immunophenotype : the neoplastic B cells express monotypic sIg and/or cIg
and B-cell–associated antigens CD20 and CD79a. In contrast to the group
of PCFCLs, PCLBCL, leg type, shows strong bcl-2 expression, also in cases
not located on the legsref1,
ref2,
ref3,
ref4.
Bcl-6 is expressed by most cases, whereas CD10 staining is generally absent.142
Unlike PCFCL, most PCLBCL, leg types, express MUM-1/IRF4 proteinref1,
ref2
-
genetic features : the t(14;18) is not found in PCLBCLs, although strong
bcl-2 expression is common in this groupref1,
ref2.
In some cases bcl-2 overexpression may result from chromosomal amplification
of the bcl-2 generef.
Inactivation of p15 and p16 tumor suppressor genes by promotor hypermethylation
has been detected in 11% and 44% of PCLBCLs, respectivelyref.
Chromosomal imbalances have been identified in up to 85% of PCLBCLs, with
gains in 18q and 7p and loss of 6q as most common findingsref1,
ref2.
Recent studies demonstrated translocations involving myc, bcl-6, and IgH
genes in 11 of 14 PCLBCL-leg cases, but not in patients with a PCFCL with
a diffuse infiltration of large centrocytesref.
Recent studies suggest that patients with PCLBCL-leg have an activated
B-cell gene expression profileref.
Prognosis : the 5-year survival of 78 cases
included in the Dutch and Austrian registries was 55%. PCLBCLs on the leg
have an inferior prognosis compared to PCLBCLs presenting at other sitesref.
The presence of multiple skin lesions at diagnosis is a significant adverse
risk factor. In a recent study, patients presenting with a single skin
tumor on one leg had a disease-related 5-year survival of 100%, whereas
patients presenting with multiple skin lesions on one or both legs had
a disease-related 5-year survival of 45% and 36%, respectivelyref.
Primary cutaneous diffuse large B-cell lymphoma, leg type. (A) Clinical
presentation with multiple tumors on right lower leg. (B) Monotonous proliferation
of centroblasts and immunoblasts (H&E staining; original magnification,x
480). (C-D) Characteristically, the neoplastic B cells strongly express
bcl-2 (C) and Mum-1/IRF-4 (D). Image acquisition for panels B-D was performed
as described for Figure 1B. An HC Plan APO objective was used (40x/0.85
for panel B; 20x/0.70 for panels C and D).
Therapy : these lymphomas should be treated
as systemic DLBCLs with anthracycline-based chemotherapyref1,
ref2.
In patients presenting with a single small skin tumor, radiotherapy
may sometimes be consideredref.
Systemic administration of rituximab
has proved effective in some patients, but long-term follow-up data are
not available and the place of rituximab in the treatment of PCLBCL, either
as single agent therapy or in combination with systemic chemotherapy remains
to be establishedref1,
ref2.
primary
cutaneous diffuse large B-cell
lymphoma,
other refers to rare cases of large B-cell lymphomas arising in the
skin, which do not belong to the group of PCLBCL, leg type, or the group
of PCFCLs. These cases include morphologic variants of diffuse large B-cell
lymphoma, such as anaplastic or plasmablastic subtypes or T-cell/histiocyte
rich large B-cell lymphomas. Such cases are generally a skin manifestation
of a systemic lymphoma. Plasmablastic lymphomas are seen almost exclusively
in the setting of HIV infection or other immune deficienciesref1,
ref2,
ref3.
Some of these cases had only skin lesions at presentation. Rare cases of
primary cutaneous T-cell/histiocyte-rich B-cell lymphoma, characterized
by the presence of large scattered B cells in a background of numerous
reactive T cells, have been reportedref1,
ref2.
Clinically, they show similarities with the groups of PCFCL and PCMZL.
These lymphomas commonly present with skin lesions on the head, the trunk
or the extremities, and may in fact represent an exaggerated T-cell infiltrate
in association with other forms of CBCL. Unlike their nodal counterparts,
they appear to have an excellent prognosisref1,
ref2.
In addition, rare cases of primary cutaneous intravascular large B-cell
lymphoma may be included in this category.
-
intravascular large
B-cell lymphoma is a well-defined subtype of large B-cell lymphoma,
defined by an accumulation of large neoplastic B cells within blood vessels.
These lymphomas preferentially affect the central nervous system, lungs,
and skin and are generally associated with a poor prognosisref
Symptoms & signs : patients often
have widely disseminated disease, but cases with only skin involvement
may occur. Clinically, intravascular large B-cell lymphoma may present
with violaceous patches and plaques or teleangiectatic skin lesions usually
on the (lower) legs or the trunkref1,
ref2.
Patients presenting with only skin lesions appear to have a significantly
better survival than patients with other clinical presentations (3-year
overall survival: 56% versus 22%)ref.
Interestingly, colonization of cutaneous cherry hemangiomas by neoplastic
cells as the only presenting sign of intravascular large B-cell lymphoma
has been reportedref1,
ref2
Laboratory examinations : histologically,
dilated blood vessels in the dermis and subcutis are filled and often extended
by a proliferation of large neoplastic B cells. These cells may cause vascular
occlusion of venules, capillaries, and arterioles. In some cases small
numbers of tumor cells can also be observed around blood vessels
Therapy : multiagent chemotherapy is the
preferred mode of treatment, also in patients presenting with skin-limited
diseaseref
The WHO-EORTC classification for cutaneous lymphomas presented herein may
be considered as an important step forward. First, the development of this
consensus classification will put an end to the ongoing discussion whether
the EORTC or the WHO scheme can best be used, and is expected to contribute
to a more uniform diagnosis and hence a more uniform treatment of patients
with a cutaneous lymphoma. Second, major progress has been made in a better
definition of some controversial groups of cutaneous lymphoma, in particular
the group of PCFCL/PCLBCL and the group of CTCL other than MF, SS, and
the group of primary cutaneous CD30+ LPD. The new definitions
of the groups of PCFCL, PCLBCL, leg type, and PCLBCL, other, will allow
a more reliable distinction between indolent and more aggressive types
of CBCL, and facilitate the decision whether radiotherapy
or systemic chemotherapy should be selected as first choice of treatment.
Large multicenter studies are now required to validate the current proposals,
and in particular to investigate the diagnostic and prognostic value of
bcl-2 and Mum-1/IRF4 protein expression. The classification of CTCL other
than MF, SS, and the group of primary cutaneous CD30+ LPD is
still difficult, as it requires accurate clinicopathologic correlation
and a number of complementary techniques to arrive at a definite diagnosis.
SPTL (with an a/b phenotype), extranodal NK/T-cell
lymphoma, nasal type, and CD4+/CD56+ hematodermic
neoplasm are now fairly well-defined. However, considerable overlap is
noted between cutaneous (and mucosal) GD-TCL and aggressive epidermotropic
CD8+ CTCL. The similarities in clinical presentation and pattern
of dissemination between these conditions may reflect similarities in homing
profile and biologic function of normal gamma/delta-positive T-cells and
activated CD8+ cytotoxic T cells, respectively. Apart from the
group of SPTLs and the group of CD4+ small/medium-sized pleomorphic
CTCLs, these rare types of CTCL have a very poor prognosis and are generally
resistant to conventional chemotherapy. More aggressive regimens, including
allogeneic bone marrow transplantation, for patients with aggressive types
of CTCL including advanced stages of MF and SS are currently under investigationref1,
ref2.
Recently, studies have started to investigate gene and protein expression
profiles in different types of cutaneous lymphoma. It is expected that
these studies will not only contribute to a better understanding of the
molecular pathways involved in the development and progression of these
lymphomas, but will also provide new molecular targets for diagnosis and
therapeutic intervention, and ultimately to more refined classification
schemesref
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