Their use is essential against pluriserotipic viruses or against latent infections : anyway in acute viroses replication usually preceed symptoms and antimicrobials can't prevent infection. They can interfere with ...
)
:)
binds into a hydrophobic pocket within viral protein 1, stabilizing the
capsid and resulting in the inhibition of cell attachment and RNA uncoatingref.
It is used for treatment of the common coldref,
infantile enterovirus meningitisref1,
ref2
))
antagonistsref
:
downmodulators : 9-benzyl-3-methylene-1,5-di-p-toluenesulfonyl-1,5,9-triazacyclododecane
(CADA) cyclotriazadisulfonamideref
and Influenzavirus Bref1,
ref2)
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[WTO regulations allow for drug patents to be violated in the event of medical emergencies, providing the patent holder is compensated at a later dateref] |
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zanamivir / GG167 / 4-guanidino-Neu5Ac2en
(Relenza®; source : GlaxoSmithKline
(complete
product information, revised on June 2004)), manufactured from a readily
available starting material, N-acetyl-neuraminic-acid (NANA), approved
in 1999. The lactose dose (80 mg per dose) is insufficient to cause symptoms
in lactase-deficient individuals.
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guanidino group => a dry powder that is self-administered via oral
inhalation by using a plastic device (DiskHaler®)
included in the package with the medication. Investigational formulations
include nebulised mist, nasal spray, intravenous.
After inhalation of 10 mg : |
not approved by FDA, but meta-analyses of clinical trials have shown that it is highly effective for postexposure prophylaxis or early treatment in compliant patients with no underlying pulmonary diseaseref1, ref2 | for persons aged > 5-7 years (depending on the country) : 2 inhalations
(one 5-mg blister per inhalation for a total dose of 10 mg) twice daily
(approximately 12 hours apart) for 5 days : take
2 doses on the first day of treatment whenever possible if there are at least 2 hours between doses. No dose adjustment for patients with either mild to moderate or severe impairment in renal function |
while there were reports of bronchospasm post-release,
trials specifically targeting patients with mild-to-moderate asthma or COPD showed that zanamivir was an effbctive treatment and had a similar safety profile to the inhaled lactose placeboref. There were no adverse eff-ect on pulmonary function, however, the pack insert reports that it is not recommended for treatment for patients with underlying airway disease unless used with caution under conditions of appropriate monitoring and supportive care (including the availability of short-acting inhaled bronchodilators) due to reports of >20% decline in FEV1. Oropharyngeal or facial edema have also been reported; no increased incidence of other side effects |
2-3 days of symptom relief in high-risk patients, those presenting
with severe influenza-related
symptoms or those who had symptoms for <30 hours. Older patients, aged >50 years, presenting with severe symptoms derived up to 7 days of benefit, as in this group, untreated patients experienced up to 11.5 days of symptoms; reduced nasal pro-inflammatory cytokine levelsref; no definitive evidence is available regarding the safety or efficacy of zanamivir for persons with underlying respiratory or cardiac disease or for persons with complications of acute influenza. Anyway studies with nebulized and intravenous preparations suggest that zanamivir has good safety and efficacy, even in patients with underlying respiratory diseaseref1, ref2, ref3 |
NA :
E119G (>100 fold reduction in NA sensitivity; isolated in the strain NWS:G70C, a reassortant containing the HA of A:NWS:33 and NA of A:Tern:Australia:G70C:75 (H1N9)ref, A:Turkey:Minnesota: 833:80 (A:Turkey:Minn, H4N2)ref1, ref2 (Gubareva, L.V., Bethell, R.C., Penn, C.R., Webster, R.G., 1996. In vitro characterization of 4-guanidino-Neu5Ac2en -resistant mutants of influenza A virus. In: Brown, L.E., Hampson, A.W., Webster, R.G. (Eds.), Options for the control of Influenza III, Elsevier, Amsterdam, pp. 753–760.), the B:HK:Lee strain, a reassortant with the HA of B:HK:8:73 and NA of B:Lee:40ref, and B:Beijing:1:87 (B:Beijing)ref |
only Germany and India are storing zanamivir up in large quantities, although other European countries and the USA have some stocks. Shorter shelf-life than oseltamivir |
oseltamivir phosphate / GS4104 (Tamiflu®;
developed from a rare natural compound, shikimic acid, and patented by
Gilead
Sciences, South San Francisco, until 2016, described in 1997ref;
in 1996 Roche Holding AG acquired
the worldwide rights to develop and market the drug : Tamiflu was FDA approved
in 1999 and launched in North America (US and Canada) and Switzerland during
1999/2000. In all key European markets, it was launched by 2002/2003. Chugai
Pharmaceutical Co., Ltd. distributes it in Japan; complete
product information, revised on June 2004. Available in blister packages
of 10 capsules (enough for a 5-day bid course per person) (cost US$34-60,
but up to US$190 on some websitesref)
or in glass bottles containing 25 ml of suspension after constitution equivalent
to 300 mg oseltamivir base. Seasonal flu prevention requires at least six
weeks of treatment -- that is 84 pills or about $1,600 of Tamiflu based
on current pricesref
Gilead Sciences, the original
developer, still receives a royalty from Roche equaling about 10% of sales.
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bulky hydrophobic group => orally administered ethyl ester prodrug
(absolute bioavailability = 80%; 30-73% in rodents, ferrets, dogs, and
marmosets) converted by liver and gut esterases to the active metabolite
oseltamivir
carboxylate / GS4071 / Ro 64-0802 / 4-guanidino-2,4- dideoxy-2,3-dehydro-
N-acetylneuraminic
acid (4-guanidino-Neu5Ac2en); detectable in plasma within 30 minutes
and reaches maximal concentrations after 3 to 4 hours (350 ng/ml)
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initially in patients > 13 years of age, but for all ages since 21
Dec 2005ref
: 75 mg capsules once dailyfor at least 7 days. Therapy should
begin within 2 days of exposure. Safety and efficacy have been demonstrated
for up to 6 weeks, but the duration of protection last for as long as dosing
is continued.
In healthy unvaccinated adults (aged 13 to 65 years), oseltamivir 75 mg once daily taken for 42 days during a community outbreak reduced the incidence of laboratory confirmed clinical influenza from 4.8% for the placebo group to 1.2% (>70% protective efficacy) and from 4.4% to 0.4% (92% protective efficacy) in vaccinated (80%) high-risk (14% had COPD, and 43% had cardiac disorders) elderly residents of skilled nursing homes. In a study of post-exposure prophylaxis in household contacts (aged 13 years) of an index case, oseltamivir 75 mg once daily administered within 2 days of onset of symptoms in the index case and continued for 7 days reduced the incidence of laboratory confirmed clinical influenza from 12% in the placebo group to 1% for the oseltamivir group. Index cases did not receive oseltamivir in the studyref |
for people aged >= 1 year recommended treatment dosages for children
vary by the weight of the child:
The treatment dosage for persons aged >13 years is 75 mg capsules bid for 5 days. It needs to be initiated within 2 days of symptom onset achieves and maintains plasma concentrations above the antiviral IC50 for laboratory strains of influenza A and B for 12 hours after a single 75 mg dose, but the relationship between the in vitro antiviral activity in cell culture and the inhibition of influenza virus replication in humans has not been establishedref. A liquid formulation of oseltamivir (2 mg/kg twice daily for 5 days)
is effectiveref.
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from potential traffic injuryref. Separately, the EMEA’s Committee for Medicinal Products for Human Use requested at its Nov. 14-17 meeting that Roche provide a “cumulative safety review of all available data on serious psychiatric disorders, including all case reports with a fatal outcome where Tamiflu was involved,” after 2 cases of alleged suicides in adolescents reported to the EMEA. In Japan, oseltamivir is often dispensed as a powder in Japan, and mixed at the pharmacy, possibly contributing to higher dosing. The length of dosing may also be different, with Japanese patients possibly stopping administration before the recommended period, contributing to recrudescenceref. Roche commissioned Ingenix to investigate the safety of Tamiflu in 63,000 children (1-12 years old) and concluded that there “was no indication of an increased risk of neuropsychiatric events for children aged 1-12 over that already posed by influenza illness alone. A case report was published about the 22-yo Cape Coral resident Lianne Espositoref. In Dec 2005 2 new cases in Japan. A man in his 50s was hospitalized due to a rash he developed 2 days after starting Tamiflu. He died 10 days from toxic epidermal necrosis, which produced fever and MOF. He had also been taking antibiotics, cold medicine and herbal medicine. A man in his 80s was hospitalized for fatigue on the 5th day on Tamiflu and died 3 weeks later from kidney failure. He had been taking 2 types of medicines to treat high blood pressure and stomach problemsref. A single-dose of 1000 mg/kg of oseltamivir phosphate to 7-day-old rats causes 10-fold higher plasma levels and 1500-fold higher brain levels (3-fold for oseltamivir carboxylate) those found in adults because of blood-brain barrier immaturity, and results in deaths, while 2000 mg/kg do not cause effects in 14-day-old rats. No adverse effect occurred at 500 mg/kg/day administered to 7- and 21-day-old rats, at which exposure to prodrug is 800-fold that expected in a 1-year old child. subcutaneous hemorrhagesref : |
reduces the median time to alleviation of all symptoms by 30% (3
vs. 4.3 days) and the median time to become afebrile by 38% (42.3 vs. 69.3
hours) compared with placebo (earlier initiation of therapy associated
with faster resolution), reduces lower respiratory tract complications
resulting in antibiotic therapy, overall antibiotic use, and hospitalization
in both healthy adolescents and adults (4.6% vs 10.3% with placebo, and
14.0% vs 19.1% with placebo, respectively) and "at-risk" adults (12.2%
vs. 18.5% with placebo, and 0.7% vs. 1.7% with placebo, respectively) with
a proven influenza illnessref,
and flu-related death rates (-60-90% in children). >103 infectious
units/mL of virus were detected in some of the patients who did not shed
drug-resistant viruses, even after 5 days of treatmentref.
Anyways zeroing of median virus titers occurs in 60 hrs vs. 108 hrs for
influenzavirus A and in 24 vs. 72 hrs or influenzavirus B (Hayden F, et
al. Efficacy of oral oseltamivir in experimental human influenza B virus
infection. Poster presented at: 37th Annual Meeting of the Infectious Diseases
Society of America; November 18-21, 1999; Philadelphia, Pa.). The durations
of virus shedding from children treated with neuraminidase inhibitors were
not significantly shorter than those of untreated patientsref.
For later-stage intervention in severe influenza illness, please contact WHOinfluenza @who.int for information on clinical trial protocols. In studies of naturally acquired and experimental influenza, oseltamivir did not impair normal humoral antibody response to infection. Initiation of therapy within the first 12 h after fever onset reduced the total median illness duration by 74.6 h (3.1 days; 41%) > intervention at 48 h. Intermediate interventions reduced the illness proportionately compared with 48 h. In addition, the earlier administration of oseltamivir further reduced the duration of fever, severity of symptoms and the times to return to baseline activity and health scoresref; reduced nasal pro-inflammatory cytokine levelsref. Effective and well tolerated in high-risk patients with chronic respiratory or cardiac diseasesref |
develops within day 4 in 8-12% of aged < 12 yrs, 1-4% in aged >
12 yrs, but viruses that develop resistance appear to be less virulent
in laboratory animals and to replicate less efficiently than parent strainsref.
Mutants detected in vitro by passage of virus in the presence of
increasing concentrations (underlined mutants have been found also in clinical
specimens : no drug-induced HA variants have been recognised to date)
HAref1, ref2 :
NA [N2 numbering of aminoacid residues] :
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(developed world: € 7.70 per 1 treatment course; developing world: € 7.00 per 1 treatment course) and Tamiflu caps purchased by governments for pandemic use are at a significant discount (developed world: € 15.00 (US$18) per 1 treatment course; developing world: € 12.00 (US$ 15) per 1 treatment course) compared to the seasonal price (seasonal ex-factory price ranges between € 20 and € 51 in Europe)ref. 7 of the 13 sites involved in making Tamiflu are controlled by subcontractors : on Dec 9 Roche reached agreements with 2 US generic drugmakers (Teva Pharmaceuticals and Mylan Laboratories, Inc.), as well as 13 other drug producers. Roche donated the WHO's stockpile 125,000 packs in 2004 and, 3 million treatment courses in Aug 2005 (enough to delay spread in an affected nation according to models), and 2 million treatment courses in Jan 2006 USA : 5.5 million people (872, 386 pediatrics) treated since 2001, 2.3 million 10-dose courses stockpiled, enough to treat < 1% of Americans, with plans to acquire another 2 million courses by the end of 2005, and projects for 80 million courses to cover about 25% of the population, but Roche could provide only 13 million courses in 2006, followed by 70 million in 2007. On July 19, 2006, < 2 weeks before a federal deadline for states to announce their plans, at least 16 say they're undecided how much Tamiflu and Relenza they'll buy. 13 others — including California, the biggest state — say they plan to buy their full allotments. The federal government plans to buy 44 million antiviral treatment courses for the states this fiscal year and next, enough to cover 17% of their populations. It wants states to buy 31 million more courses, to reach 25%. Even at a discount — about $15 for Tamiflu, about 20% of the Internet retail rate — cost is a concern. Arizona plans to spend $1 million for 70,000 courses. The state's full allotment of 585,780 courses would cost about $8 million, draining funds needed to prepare hospitals. Colorado plans to buy 5,400 courses — not the 477,470 allotted to it. Arizona and Nebraska are trying to get local entities to pay for more anti-virals. So is Oklahoma, which now plans to buy 9% of its allotment but may increase it. Montana and North Dakota also don't plan to buy full allotments. Other states didn't respond. The Aug. 1 deadline will help drugmakers plan, but states can change orders through Dec. 31. Businesses cannot buy the drugs at the federal discountref. Roche has no patents in : |
An influenza B virus from an infant with no history of treatment or contact with neuraminidase inhibitors demonstrated a significant reduction in sensitivity to these drugs. A mixed viral population was isolated that contained a novel D197E amino acid substitution that was responsible for this reductionref
 |
from yew trees, plans to use needles from half a million Christmas trees
discarded in Ontario to mine shikimic acid : it will get 500,000 trees
in January from a Toronto-based firm called Gro-Bark
Ltd, which recycles forest products. Biolyse has a production capacity
of about 2 tons a month and plans to get more tree needles from forestry
companies. 2-3% of the biomass from various pine, spruce and fir trees
is extractible shikimic acid. The company is gearing up to make 50 kilograms
a day of finished product or about 666,000 pills daily. It has been working
on a generic version of Tamiflu for the past 2 years and has developed
a process to shorten the manufacturing process to five weeks. No drug has
yet been manufactured for stockpiling because of Roche's patents. Under
the 2005 Jean Chrétien Pledge to Africa Act, amendments to the Patent
Act give Ottawa authority to grant compulsory licenses of patented drugs
for export to eligible countries in need of lower-cost medicines to address
public health problemsref.
The price of the acid has risen more than 10-fold to $600 a kilogram in
a yearref.
With no other agricultural sources, other than perhaps the leaves of the
gingko
biloba tree, the pharmaceutical industry needs to find an alternative
sustainable supply. Shikimic acid, however, is also a natural intermediate
in the formation of microbial amino acids. Researchers could boost production
of shikimic acid in strains of the bacterium Escherichia coli by
ramping up enzyme activity and feeding the microbe a diet of carbohydrates.
Roche already uses engineered bacteria to boost shikimic acid production.
Today, around 66% of the shikimic acid used for Tamiflu is gained from
star anise and Roche also has access to the remaining shikimic acid through
fermentation. This gives us more flexibility, and in particular allows
us to become more independent from events such as bad harvests. Roche hopes
to scale up its fermentation capacities over the next few years, but there
is no firm timeline as to when this will happen. In theory, there is no
limitation on how much shikimic acid can be produced by fermentation. The
bioproducts industry currently produces 750,000 tons of lysine from glucose
by microbial fermentation for use in products such as animal feed. If needed,
the same tanks could be used to produce shikimic acid from glucose. Microbes
could be engineered to make variations on the Tamiflu starting material
and so allow production of Tamiflu analogues with slightly different pharmacological
properties that could potentially target emerging strains other than H5N1.
Frost, who consulted with Roche on how to grow his E. coli strain
and purify the shikimic acid on a commercial scale, has started up a company
called Draths Industries to help boost supplies of shikimic acid. Draths
already has an agreement with one bioproducts firm to contract-manufacture
200 tons of shikimic acid by fermentation, but it could produce more. Draths
Industries feels that there is enough capacity to access 1,000 tons of
shikimic acid in 14 months. Roche is on record as claiming 0.13 grams
of shikimic acid is needed per Tamiflu capsule. So, 1,000 tons should
provide enough feedstock for > 20 million capsules a month, or enough doses
for 2 million people. This would fulfill Roche's current annual production
but would be inadequate for its planned production of 300 million courses
of Tamiflu in 2007. But the infection rate could be as high as 50% of the
global population — 3.2 billion people. Half of those people would have
inapparent or asymptomatic infections — as is often the case with viral
diseases — but the other 1.6 billion people could become seriously ill.
It is correct that many are now saying that a severe pandemic, along the
lines of 1918, would result in a 2% fatality rate among those who become
ill. Even if only half of those needed treatment with Tamiflu, this would
still require around 30 billion capsules. Tamiflu, however, can be synthesized
from other products in a microbial fermentation tank.
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| Hong Kong 1997 (10 out of 18 patients) : amantadine was used for most of the patients with severe infections. However, the majority of those patients were already at a critical stage of the disease when the drug was administered, and amantadine is known to be most effective when it is given at an early stage of disease (within 2 days of onset)ref | 3 yrs-old male from ? (patient 1) | onset of illness on 10 May 1997; persistent MODS; no major illnesses | acyclovir started at late stage of disease | died 5 days after hospital admission |
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| Hong Kong 1997 (10 out of 18 patients) : amantadine was used for most of the patients with severe infections. However, the majority of those patients were already at a critical stage of the disease (> 4 days after the onset of symptoms ) when the drug was administered, and amantadine is known to be most effective when it is given at an early stage of disease (within 2 days of onset)ref1 (Arabian numerals), ref2 (Roman numerals) | 54 yrs-old male (patient 4) | onset of illness on 24 Nov 1997; fever (39°C) for 6 days, cough, vomiting, shortness of breath, bilateral pneumonia, persistent MODS; WBC 5.8, lymphopenia 0.3, AST 157, ALT 70, acute renal failure, ECG evidence of old myocardial infarct | amantadine started on hospital admission (6 days after the onset of illness) for 6 days | died 7 days after hospital admission with areas of hemorrhage, and fibrinous exudates in air spaces, and extensive acute tubular necrosis | |
| 5-years old female (patient 5 or VI) | onset of illness on 7 Dec 1997; fever (37.8°C) for 3 days, rhinorrhea, vomiting and diarrhea, epistaxis, WBC 8.4, lymphocytosis 6.05, atypical lymphocyte 0.34 x 103/mL, ALT 43, AST 91, fever, URTI symptoms; no major illnesses | amantadine started on hospital admission | recovered | ||
| 24-yrs old female (patient 7) | onset of illness on 4 Dec 1997; fever (39°C) for 3 days, productive cough, rhinorrhea, sore throat, dizziness, headache, decreased appetite, right-upper abdominal pain, congested oropharynx, clinical and radiological signs of severe pneumonia, septic shock, ARDS, bilateral pleural effusion, requiring ventilatory support for 21 days, leukopenia 2.29, lymphopenia 0.28, PLT 161, aPTT 40.7, PT 12.4, AST 60 | amantadine started on the third day after hospital admission | recovered | ||
| 2 yrs-old male (patient 8) | onset of illness on 12 Dec 1997; fever (39°C) for 1 day, sore throat, rhinorrhea and cough; WBC 14.66, neutrophilia 9.31 x 103/ml; glucose-6-phosphate dehydrogenase deficiency | amantadine started on hospital admission | recovered | ||
| 60-years old female (patient 12) | onset of illness on 16 Dec 1997; fever (39.7°C) for 2 days, no pulmonary symptoms or signs, progressive bilateral pneumonia, ARDS, renal failure, progressive MODS; WBC 5.4, lymphopenia 0.3, PLT 147, AST 62, ALT 52, malignant thymoma treated with radiotherapy 10 years ago | amantadine started on the 5th day after hospital admission | died 6 days after hospital admission | ||
| 25-years old Filipino female (patient 13 or V) | onset of illness on 17 Dec 1997; fever (39.6°C) for 4 days, cough, sore throat, rhinorrhea, diarrhoea, headache, dizziness, clinical and radiological signs of left-lower-lobe consolidation, persistent MODS; leukopenia 2.4, lymphopenia 0.4, PLT 106, ALT 74, ARDS, bilateral massive hemorrhagic pleural effusion, no major illnesses | amantadine started on the third day after hospital admission | died 24 days after hospital admission (1 month after the onset of illness) of acute respiratory distress syndrome and multiple organ failure showing features of reactive hemophagocytic syndrome, central lobular necrosis, fatty changes, and extramedullary hematopoiesis in the liver and prominent acute tubular necrosis, congestion, and swelling in the kidneys | ||
| 19-yrs-old female (patient 16 or IX) | onset of illness on 14 Dec 1997, fever (39°C) for 3 days, productive cough, vomiting, clinical and radiological signs or left-lower-lobe pneumonia, progressive bilateral pneumonia/ARDS requiring steroid therapy and ventilatory support for 20 days, pleural effusions requiring tube thoracotomy drainage, WBC 4.0, lymphopenia 0.6, PLT 106; no major illnesses | amantadine started on the third day after hospital admission | recovered |
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| Hong Kong 1997 (1 out of 18 patients)ref | 13-yrs-old female from ? (patient 3 or III) | onset of illness on 20 Nov 1997; fever (39.8°C) for 4 days, rhinorrhea, cough, headache, clnical and radiological signs of patchy right-lower-lobe consolidation. Haemoptysis due to pulmonary hemorrhage; ARDS; gastrointestinal bleeding, renal failure, haemophagocytosis, leukopenia 2.54; lymphopenia 0.18, platelet 31, PT 12.8, aPTT 38.5, urea 30.6, creatinine 222; persistent MODS; no major illnesses in medical history | amantadine and intravenous ribavirin (1 g every 8 h) started on the seventh day after hospital admission | died 25 days after hospital admission | |
| Vietnam 2004 (2 out of 10 patients) : relatively low doses not associated with obvious effectivenessref | 10 yrs-old male from Bac Nihn (patient 3) | student; family members are farmers who kept chickens, which died unexpectedly 5 days before onset of illness; parents and older sibling healthy | cough, dyspnea, fever 39°C, ABP 105/80 mmHg, RR = 64 bpm, crackles, HGB 12.4 g/dl, WBC 2800/ml, lymphocytes 860/ml, neutrophils 1900/ml, platelets 135,000/ml, O2 saturation during receipt of 40% O2 86%, PCR for H5N1 performed on day 9 of illness | 800 mg 3 times a day | died day 14 |
| 8 yrs-old female from Ha Tay (patient 4) | cough, dyspnea, fever 38.5°C, ABP 80/40 mmHg, RR = 60 bpm, bleeding gums, HGB 12.3 g/dl, WBC 1900/ml, lymphocytes 250/ml, neutrophils 780/ml, platelets 91,000/ml, ALT 265 U/l, AST 1,217 U/l, creatinine 27 mmol/l, O2 saturation during receipt of 40% O2 50%, PCR for H5N1 performed on day 6 of illness | 400 mg 3 times a day | died day 7 | ||
| China 2005ref | a 9-yrs-old boy from Hunan | brother of a 12-years old girl who fell ill on Oct 8 died of ARDS, DIC, and MODS on Oct 17 but tested negative for H5-specific antibodies in both microneutralisation and haemagglutination-inhibition assays against the A/Hunan-Xiangtan-he/12/2005 virus, which was isolated from the only live chicken remaining in the household | developed fever and cough on Oct 10 | amantadine, ribavirin, corticosteroids, and broad spectrum antibiotics since Oct 17 | discharged on Nov 12. At his final follow-up on Dec 9, 2005, he remained asymptomatic |
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| Hong Kong, 2003ref | 33-year old man from Hong Kong | father of a family of 5 who visited Fujian province, mainland China, from Jan 26, to Feb 9, 2003. The 7-year-old daughter developed high fever and respiratory symptoms 2 days after arriving there and died of a pneumonia-like illness 7 days after the onset of symptoms. The exact cause of death could not be ascertained since the girl was buried in mainland China. The family returned to Hong Kong on Feb 9, 2003 | admitted on Feb 11, 2003, with a 4-day history of fever, malaise, sore throat, cough with blood-stained sputum, and bone pain. He had a lymphocyte count of 0.6×109/L and radiological evidence of right lower-lobe consolidation. | despite treatment with intravenous cefotaxime and oral clarithromycin, clinical and radiological signs showed that the patient was deteriorating. 2 days after admission (day 6 of illness), oral oseltamivir (75 mg twice daily) was added and continued for 4 days | the patient was electively intubated because of progressive respiratory distress, but his condition worsened and he died 6 days after admission exhibiting virus in the lungs |
| Thailand 2004 (8 patients; 10 out of 17 patients ?) : 7 of 10 patients given oseltamivir died a mean of 11 days after the onset of symptoms (range, 5 to 22 days), as compared with 5 of 7 untreated patients. Oseltamivir was used in conventional doses (75 mg orally, twice daily for 5 to 10 days with a weight-based dose reduction in children) in the majority of recipients. Treatment tended to have been started earlier in those who survived (a median of 4.5 days from onset compared with 9 days for those who died), and both survivors who were treated received the complete 5-day course of drug, whereas 2 of 5 patients who died received the complete 5-day courseref1, ref2 | 2 yrs-old male from Supanburi (patient 1) | raised chickens in backyard. Chickens died unexpectedly 5 days before illness onset. Frequently played with chickens and had direct contact with carcasses. | fever, cough, sore throat, dyspnea, diarrhea, HCT 30%, WBC 4,200/ml, lymphocytes 2,646/ml, platelets 214,000/ml, peak ALT 57 U/l, peak AST 129 U/l | days 5 to 10 + corticosteroids | survived (discharged from hospital on Feb10 2004) |
| 31 yrs-old male from Nakornratchasima (patient 3) | raised chickens in backyard. Three days before onset, chickens started to die. The last patient died on the date he became sick. He buried all carcasses | fever, cough, sore throat, myalgia, dyspnea, diarrhea, HCT 38%, WBC 4,660/ml, lymphocytes 513/ml, platelets 171,000/ml, peak ALT 74 U/l, peak AST 41 U/l, peak BUN 10.7 mg/dl, peak creatinine 1.07 mg/dl | days 4 to 9 + corticosteroids | survived | |
| 5 yrs-old male from Khonkaen (patient 5) | Raised fighting cocks that died 4 days before onset. Reported direct contact with carcasses. Ate chicken with suspected H5N1 influenza | fever, rhinorrhea, cough, sore throat, dyspnea, diarrhea, abdominal pain, HCT 39%, WBC 5,600/ml, lymphocytes 2,296/ml, platelets 94,000/ml, peak ALT 47 U/l, peak AST 70 U/l, peak BUN 12 mg/dl, peak creatinine 0.7 mg/dl | days 9 to 13 | dead on day 13 | |
| 6 years-old male from Kanchanaburi (patient 6) | No poultry in family. Helped slaughter one ill chicken 2 days before onset | fever, rhinorrhea, cough for 5 days, dyspnea on day 6, HCT 32%, WBC 1,200/ml, lymphocytes 624/ml, platelets 89,000/ml, CXR patchy infiltrates in right lower lobe, ARDS, respiratory failure on day 8, hepatitis, peak ALT 150 U/l, peak AST 790 U/l, peak BUN 12 mg/dl, peak creatinine 0.7 mg/dl, proteinuria >= 3 | days 18 to 20 + corticosteroids | dead on day 20 | |
| 6 yrs-old male from Kanchanaburi (patient 8, initials N.C.) | Chickens in backyard died unexpectedly. Grandfather slaughtered ill chickens. No direct contact with chickens but played near slaughtering area | since 24 Jan 2004 fever, cough, sore throat, myalgia, dyspnea, diarrhea, vomiting, HCT 40%, WBC 4,900 (2,900 ?ref)/ml, lymphocytes 1,763 (696 ?ref)/ml, platelets 111,000/ml, ARDS, respiratory failure on day 5, cardiac failure, renal failure, inotropic support, peak ALT 50 U/l, peak AST 280 U/l, peak BUN 22 (50 ?ref) mg/dl, peak creatinine 1.1 (4.6 ?ref) mg/dl | days 5 to 8 + corticosteroids | dead on day 8 (2 Feb 2004) | |
| 7 yrs-old male from Supanburi (patient 9) | No poultry in family. Frequently played on ground near a chicken farm that reported unexpected poultry deaths | since 3 Jan 2004 fever, cough, sore throat, dyspnea on day 6, HCT 41%, WBC 4,100/ml, lymphocytes 1,435/ml, platelets 304,000/ml, ARDS (CXR bilateral interstitial infiltrates), respiratory failure on day 10, cardiac failure, pneumothorax, gastrointestinal bleeding, inotropic support, peak ALT 52 U/l, peak AST 120 U/l, peak BUN 10 mg/dl, peak creatinine 0.7 mg/dl | days 22 to 27ref (18 to 22 ?ref) + corticosteroids | dead on day 29 (2 Feb 2004) | |
| 13 yrs-old male from Chaiyapoum (patient 10) | Helped raise chickens in back yard. Eight days before onset, chickens died unexpectedly and patient assisted with slaughtering | fever, cough, sore throat, dyspnea, vomiting, HCT 37%, WBC 2,000/ml, lymphocytes 580/ml, platelets 150,000/ml, ARDS, inotropic support, peak ALT 47 U/l, peak AST 34 U/l, peak BUN 132 mg/dl, peak creatinine 8.1 mg/dl | days 6 to 11 + corticosteroids | dead on day 16 | |
| 32-year-old female from Kamphaeng Phetref | buried dead chickens on Aug 30, provided bedside care in hospital for her 11-year-old niece for 12 or 13 hours on Sep 7, and attended her funeral on Sep 9 (which died as a suspected case (cremated) part of a cluster involving also her mother - embalmed) | onset of fever, myalgia, and chills on Sep 16. An upper respiratory infection was diagnosed at a clinic on Sep 19, but she had progressive difficulty breathing and was admitted to the district hospital on Sep 23 with a temperature of 39.7°C, WBC 5,400, lymphocyte 1,296, platelet 230,000, and left-lower-lobe consolidation | oseltamivir started on hospital admission | recovered (discharged on Oct 7) | |
| Vietnam 2004 (5 out of 10 patients) : 1 of 5 recipients of oseltamivir recovered, as compared with 1 of 5 untreated patientsref : one of the 2 surviving patients did not start oseltamivir therapy until the 12th day of illness. At that point, she was still antigen-positive and PCR-positive for the virus. | 8 yrs-old female from Ho Chi Minh City (patient 5) | student; patient bought duckling as pet and cared for it in her house for 5 days; duck has diarrhea and died, patient buried it, dug it up a day later and reburied it; both patient and brother handled duck; patient also ate barely cooked eggs (Vietnamese delicacy) 2 days before onset of illness; neighbors kept 40 chickens, but no illness reported in these birds; fevere developed in patient 3 days after she bought duck; no other poultry or animals at home; no other houselhold members or relatives sick | cough, dyspnea, sputum, diarrhea, fever 38.5°C, ABP 104/64 mmHg, RR = 40 bpm, crackles, HGB 11.3 g/dl, WBC 1,200/ml, lymphocytes 300/ml, neutrophils 700/ml, platelets 117,000/ml, CD4:CD8 ratio 0.71, ALT 354 U/l, AST 320 U/l, creatinine 34 mmol/l, O2 saturation during receipt of 40% O2 95%, PCR for H5N1 performed on day 12 of illness | 35 mg twice daily for ? days | recovered |
| 16 yrs-old female from Soc Trang (patient 7) | student, extensive exposure, including handling of 10 dead or dying chickens in patient's homestead; father of patient prepared dead chickens for eating (removed feathers, washed, cut meat) 3 days before onset of illness; no other household members or relatives sick; no other poultry or animals at home | cough, dyspnea, sputum, diarrhea, fever 40°C, ABP 110/60 mmHg, RR = 60 bpm, crackles, HGB 11.9 g/dl, WBC 3,000/ml, lymphocytes 500/ml, neutrophils 2,500/ml, platelets 70,000/ml, CD4:CD8 ratio 0.62, ALT 47 U/l, AST 20 U/l, creatinine 71 mmol/l, glucose 19 mmol/l, O2 saturation during receipt of 40% O2 67%, PCR for H5N1 performed on day 5 of illness, influenza antigens negative | 75 mg twice daily for up to 5 days. | died on day 14 (3 Feb 2004) | |
| 18 yrs-old male from Lam Dong (patient 8) | farmer, direct handling of 50 chickens, including dead chickens, at home (which was also a restaurant); patient and father prepared chickens for eating; no other household members or relatives sick; no other poultry or animals at home | cough, dyspnea, sputum, diarrhea, fever 38.5°C, ABP 100/60 mmHg, RR = 60 bpm, crackles, HGB 14.7 g/dl, WBC 1700/ml, lymphocytes 500/ml, neutrophils 1100/ml, platelets 69,000/ml, CD4:CD8 ratio : 0.75, serum creatine 89 mmol/l, glucose 13.5 mmol/l, O2 saturation during receipt of 40% O2 81%, PCR for H5N1 performed on day 6 of illness, influenza antigens positive | 75 mg twice daily for up to 5 days | died on day 9 | |
| 24 yrs-old male from Lam Dong (patient 9) | farmer, direct handling of chickens in patient's homestead 3 days before onset of ilness; he prepared dead chickens for eating; noone else in family sick | cough, dyspnea, sputum, diarrhea, fever 39.5°C, ABP 110/60 mmHg, RR = 50 bpm, crackles, HGB 15.8 g/dl, WBC 1900/ml, lymphocytes 800/ml, neutrophils 1100/ml, platelets 62,000/ml, CD4:CD8 ratio : 0.59, creatinine 0.43 mmol/l, glucose 11.7 mmol/l, O2 saturation during receipt of 40% O2 80%, PCR for H5N1 performed on day 5 of illness, influenza antigens negative | 75 mg twice daily for up to 5 days | died day 6 | |
| 23 yrs-old male from Lam Dong (patient 10) | direct handling of sick ducks and chickens in patient's home; many sick poultry in the district; no other illness in family | cough, dyspnea, sputum, diarrhea, fever 38.7°C, ABP 120/80 mmHg, RR = 28 bpm, crackles, HGB 17.6 g/dl, WBC 2100/ml, lymphocytes 700/ml, neutrophils 1300/ml, platelets 62,000/ml, ALT 89 U/l, AST 110 U/l, creatinine 121 mmol/l, glucose 11.7 mmol/l, O2 saturation during receipt of 40% O2 90%, PCR for H5N1 performed on day 7 of illness, influenza antigens negative | 75 mg twice daily for up to 5 days | recovered | |
| Ho Chi Minh City 2005 (10 out of 10 patients) | NA | ||||
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| Thailand 2005 | a 6-year-old boyref1, ref2 from Bangrakam district, Phitsanulok province | patient’s family and neighbors raised chickens in the back yard and let them feed freely in the yard and surrounding areas. Chickens in the village started to die in late Dec with diarrhea and hypersecretion, more than in previous years. All of the chickens in the relative’s farm were sick and died or were culled. 4 of the 5 chickens in the patient’s house also died during that time. The patient had helped cull the sick chickens and carried one of them from the farm back home on Dec 28 : the patient’s family did not eat any sick chickens; some neighbors had symptoms of the common cold | intermittent URT symptoms since late Dec 2003, mild until Jan 9, 2004,
when he developed a distinct spike of fever and shortness of breath. On
Jan 12 increased tachypnea, WBC 1200 cells/mm3 (44%
neutrophils, 52% lymphocytes, 2% eosinophils, 2% monocytes), PLT 89,000 cells/mm3. CXR on day 4 of illness revealed right lower lobe opacification => admission to hospital, fever 40°C, ABP 90/60 mmHg, HR = 120 bpm, RR = 48 bpm, SO2 = 85%, AST 790, ALT 150, proteinuria and hematuria |
Daily ceftriaxone intramuscular injections since Jan 10 to 12 . Oseltamivir + methylprednisolone 2 mg/kg/day started on day 15 (imported from abroad) until death and with filgrastim from day 5 to day 10 of illness | died on day 17 as a result of respiratory failure (significant insults from barotraumas, including pneumothorax and pneumomediastinum after treatment with a high frequency ventilator with 100% oxygen on day 10 of illness); particles consistent with influenza virus were detected in the lungs and spleen with electron microscopy and were confirmed with reverse transcription-PCR assays, despite 3 days of oseltamivir therapy. |
| a 7-year-old boy (Ronnarit Benpad) in Panuamthuan (Phanom Thuan) district of Kanchanaburi province (150 km (94 miles) west of Bangkok), which had reported fresh outbreaks of the deadly avian influenza strain in poultry around 100 km (60 miles) west of the capital, Bangkok, son of a 48-year-old male farmer named Bang-orn Benpad who developed symptoms on 13 Oct 2005, was hospitalized on 17 Oct 2005, and died on Wed 19 Oct 2005ref. | had assisted his father with defeathering of the diseased birds | developed respiratory symptoms on 16 Oct 2005 and tested positive on Oct 21 | treated with oseltamivir early in his illness, recovered his appetite and his fever resolved | recovered | |
| Vietnam 2005 | a 5-year-old boy from Nakhon Nayokref | touched some chickens raised by a relative, 4 out of 10 died | fell ill with high fever, stomach pain and vomiting around Nov 25. 2 days after that he was taken to 2 private clinics, and finally moved on day 10 to HRH Princess Maha Chakri Sirindhorn Medical Centre in Nakhon Nayok's Ongkharak district | oseltamivir started on hospital admission (day 10) | died on day 12 (Dec 7, 2005) |
Consideration of use of neuraminidase inhibitors such as oseltamivir and zanamivir in IgA nephropathyref.
Influenza virus with resistance to antiviral drugs emerges with increased frequency in immunocompromised patients and can limit the benefit of M2 and neuraminidase (NA) inhibitors. 3 cases of influenza have been documented in severely immunocompromised patients from whom virus variants with molecular markers of resistance to anti-influenza drugs were recovered. Virus variants recovered from 2 patients had mutations in the M2, NA (with a previously recognized Glu119Val NA substitution), and hemagglutinin genes. The novel Asp198Asn NA mutation was described in an influenza B virus and its decreased susceptibility to both oseltamivir and zanamivirref.
Oseltamivir 5 mg/kg oseltamivir for 5 days (equivalent to the approved human treatment dose of 75 mg twice daily) 4 hours after inoculation prevented viral replication in the upper respiratory tract and effectively treated all infected ferrets, with no deaths. All ferrets in the control group died. Resistance mutations of the H5N1 avian influenza virus were not detectedref.
Zanamivir protects mice against lethal challenge with A/HK/156/97 (H5N1)
influenza virusref
and protects chickens from A/chick/Victoria/1/85 (H7N7),
a highly pathogenic virusref,
but fails to protect chickens from other highly virulent viruses of the
NA subtypes N1, N2, N3, N7,
and N8ref1,
ref2.
There have been recent reports of enhanced potency of multivalent zanamivir
by Sankyo in Japanref1,
ref2
and Biota in Australiaref,
where a single dose of drug may be sufficient for protection. Zanamivir
dimers 8 and 13 are highly potent neuraminidase inhibitors which, along
with dimer 3, are being investigated as potential second generation inhaled
therapies both for the treatment of influenza and for prophylactic use.
Dimer 3 shows NA inhibitory activity against N1 viruses including
the recent highly pathogenic H5N1 A/Chicken/Vietnam/8/2004ref.
Other treatments may have to be considered in patients with rapid disease
progression. Intravenous ribavirin was tried in one case without success.
The use of immune serum from convalescent patients may be another option
worth consideration since neutralising monoclonal antibodies have been
effective in treating established influenza A virus infection in mice with
severe combined immunodeficiencyref.
The efficacy of convalescent immune serum in human beings remains speculative,
but combination therapy with immuneglobulin with high neutralising antibody
titre and aerosolised ribavirin has resulted in improved outcome in adult
bone-marrow-transplant recipients with respiratory syncytial virus diseaseref
Recombinant viruses possessing the 1918 NA or both the 1918 HA and
1918 NA were inhibited effectively in both tissue culture and mice by zanamivir
and oseltamivir. A recombinant virus possessing the 1918 M segment was
inhibited effectively both in tissue culture and in vivo by amantadine
and rimantadineref.
2 mechanisms of resistance have been recognised :
ref1,
ref2,
ref3
:
+ rimantadine or ribavirin
additively or synergistically reduce the yield of clinical H3N2
or H1N1 influenza A isolates in primary rhesus monkey
kidney cellsref |
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:)
: tricyclic antiviral (TAV) drugs / adamantane or aminoadamantane derivatives
(the less expensive class of anti-influenza drugs)
and Parkinson's disease).
Careful observation is advised when amantadine is administered concurrently
with drugs that affect CNS, including CNS stimulants. Concomitant administration
of antihistamines or anticholinergic drugs can increase the incidence of
adverse CNS reactions. No clinically substantial interactions between rimantadine
and other drugs have been identified. Schedule
: 200 mg p.o. q day (peds 2.2-4.4 mg/kg bid, max, 75 mg bid) for at least
10 days (prophylaxis) or for 1-2 days after symptoms resolve (treatment)
activity. Stachyflin is a new class of hemagglutinin fusion inhibitors
of influenza A virus. Several derivatives were synthesized from acetylstachyflin
and subjected to preliminary examination of their structure-activity relationships.
Among them, the 3-oxo and 3,8'-dioxo derivatives showed potent antiviral
activity similar to stachyflin. The 3-epi derivative was 4 times less active
than stachyflin. Modification of the 6'-hydroxy group and the C-5' position
markedly diminished the antiviral activityref.
(effective against HIV-1
T-tropic or X4 strains)
(effective against HIV-1
M-tropic or R5 strains)
and paramyxovirus fusion inhibitor,
HHV-2
/ HSV-2,
HHV-3
/ VZV,
HHV-5
/ CMV,
HHV-6,
HHV-8,
RSV
and HIV-1))
("-navir") (also directly inhibit the growth of Plasmodium
falciparum
in vitro at clinically relevant concentrationsref).
,
fat redistribution (fat decrease in hips and retroorbital regions, fat
increase in breast, back and interscapular region), a condition termed
lipodystrophy
or Launois-Bensaude's syndrome. The severity relates also to administration
of NRTI, which inihibits mitochondrial DNA polymerase
g,
leading to mutations in mtDNA and hyperlactacidemia.
They also cause coronary calcification.
(CA))-tk
or HHV-3 / VZV-tk
or by HHV-5 / CMV-PK.
Then they are transformed into acyclic GTP.
thymidine kinase (EBV-TK) and the BGLF4 gene product, which
phosphorylate the prodrug GCV and convert it into its active cytotoxic
form, are expressed. Phosphorylated GCV inhibits not only the virally encoded
DNA polymerase but also the cellular DNA polymerase, leading to premature
termination of the nascent DNA and cell deathref1,
ref2,
ref3.
In addition, phosphorylated GCV can be transferred to adjacent cells, thus
inducing "bystander" killingref.
Lytic EBV infection also confers sensitivity to the cytotoxic effects of
zidovudine
(AZT), possibly by inducing AZT phosphorylationref1,
ref2,
ref3,
ref4.
-tk-tk
or HHV-3 / VZV-tkor
by HHV-5 / CMV-PK.
Then they are transformed into acyclic TTPs.
IN :
RT
ref1,
ref2,
ref3,
ref4,
ref5
=> toxic myopathy : fatigue, myalgia, mild hyposthenia, mild CK increase,
myelotoxic and neurotoxic (it crosses both the blood-brain and the blood-placenta
barriers)
RT
RT
RT : they also interfere with postintegration transcription of the proviral
DNA to RNA and may have the potential to prevent reactivation of the virus,
which is an interesting added valueref)
ref,
HHV-5
/ CMV
uveitis, Pneumocystis
carinii,
Cryptococcus
neoformans
meningitis or Mycobacterium
avium-intracellulare
lymphadenitis, or the flare-up of viral infections that include hepatitis
and herpes. Low CD4 counts at HAART initiation are the only independent
predictor of IRIS as it is caused by a deferred or partial CD4 response
after HAART is initiated. 22% has IRIS events, which occurr at a median
of 12 weeks (range 3 - 24 weeks) following the initiation of HAART, and
the majority (78%) are due to the occurrence - or the more frequent and/or
more severe recurrence - of dermatological problems: HHV-2
/ HSV-2
(50%); HPVs
(24%); molluscum
contagiosum virus
(9.5%); and HHV-3
/ VZV
(9.5%). Non-dermatological manifestations of IRIS are much less common:
Mycobacterium
avium-intracellulare
(2%), HBV
(2%), and there are rare cases of HHV-8
or Pneumocystis carinii
symptoms. In MTB, the major risk factor for IRD is beginning HAART within
2 months of antituberculosis treatment. This fact has led many experts
to recommend delaying HAART for 2 months, a strategy that may also reduce
the incidence of adverse events. However, a recent retrospective review
suggested that delaying HAART would, particularly in those with CD4 cell
counts <100 cells × 106/L, lead to significant increase
in risk for death and new opportunistic infectionsref.
IRD should always be considered along with treatment failure if a patient's
clinical condition deteriorates after HAART is introduced.
)),
while there seems to be no effect on the host cells. That's why only a
small number of misfolded M proteins disrupt the symmetry characteristic
of the HBV coat and prevent it from escaping the ER
leads to biphasic activation of the Raf/MEK/ERK cascade. Inhibition
of Raf/MEK/ERK signalling cascade
results in nuclear retention of viral ribonucleoprotein (RNP) complexes,
impaired function of the nuclear-export protein (NEP/NS2) and concomitant
inhibition of virus production. Thus, signalling through the mitogenic
cascade seems to be essential for virus production and RNP export from
the nucleus during the viral life cycle. Unfortunately, the kinases also
perform several important jobs in healthy cells, such as controlling how
cells divide or when they die. So before inhibitors of Raf kinase can be
used as anti-flu drugs, researchers will have to devise a way of making
sure that they only get into cells infected with fluref
is a unique phorbol ester that stimulates membrane translocation of classical,
atypical, and expecially novel protein kinase
C (PKC)
isoforms but is nontumor promoting. Remarkably, prostratin is also able
to inhibit de novo HIV-1
infection relating to down-regulation of CD4,
CXCR4
and CCR5expression
yet up-regulate viral expression from latent proviruses in from CD8+
T lymphocyte-depleted peripheral blood mononuclear cells. Prostratin is
a potent mitogen for mononuclear phagocytes possessing many of the activities
of phorbol myristate acetate (PMA) with notable functional differences.
Prostratin, like PMA, accelerates differentiation of the myeloid cell-lines,
HL-60 and THP-1, as well as mononuclear phagocytes from bone marrow and
peripheral blood. Prostratin forces the HIV-1 out of reservoirs in the
body, thus allowing anti-retroviral drugs to attack it : it could upregulate
expression from latent viruses and concluded that it may be an excellent
candidate to augment HAART
by inducing expression of latent HIV-1 with the ultimate goal of eliminating
persistent viral reservoirs in certain individuals infected with HIV-1ref.
It works, at least in part, by stimulating IKK-dependent phosphorylation
and degradation of IkBa,
leading to the rapid nuclear translocation of NF-kB
and activation of the HIV-1 LTR in a kB enhancer-dependent
mannerref.
Under a separate agreement, AIDS
Research Alliance (ARA), will return 20% of any profits from the plant-derived
form of the drug to Samoa
inhibits HCV,
SARS
coronavirus,
and HIV-1
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