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Thank you Dr. James. It has been a long time
I rather suspected you might be out at the tip of the spear with regard to research.
Had not heard anything about Indomethacin as a treatment for Covid 19, so this is very exciting.
Was down with Covid 19 symptoms about 5 weeks ago after a pre-Mardi Gras trip to New Orleans.
Here they were only testing if symptoms were severe enough to warrant hospitalization. My symptoms weren’t pleasant, but fortunately resolved on their own. I wouldn’t necessarily recommend this for anyone else, but I dealt with the symptoms with 800 mg of Ibuprofen every 4 -6 hours to deal the severe body aches, general inflammation, and fever. I also used an Ventolin HFA inhaler (left over from a bout with pneumonia a couple of years ago) when it felt like I wasn’t getting quite enough air.About 10 days in, I sought out and found Cinchona tablets, and some rather powerful low sugar high quinine tonic water, and perhaps it was placebo effect, but I began to feel better within a very short time after starting the Cinchona and tonic combination.
Thanks once again for the fantastic information, and for taking the time to respond at length. I’ll print out the papers and make sure my GP gets them!
Thanks also for saving my life. You’re one of a kind, and the world is lucky to have you!
Warm regards,
Fitz
Not that that’s a bad thing at all if it works.
Sadly it does not.
https://www.thelancet.com/journals/lancet/article/PIIS0140-6736(20)31022-9/fulltext
Interpretation
In this study of adult patients admitted to hospital for severe COVID-19, remdesivir was not associated with statistically significant clinical benefits.Worse, the NIH did an emergency review and emergency press release because they knew this study was coming out.
Ignoring the Anthony Fauci backed, non-peer reviewed, non-published, interim analysis from NIH from 2 days ago https://www.niaid.nih.gov/news-events/nih-clinical-trial-shows-remdesivir-accelerates-recovery-advanced-covid-19 or not ignoring that and noting that report states:
Results also suggested a survival benefit, with a mortality rate of 8.0% for the group receiving remdesivir versus 11.6% for the placebo group (p=0.059) is far more accurately worded:
Results FAILED TO DEMONSTRATE ANY STATISTICALLY SIGNIFICANT survival benefit, with a mortality rate of 8.0% for the group receiving remdesivir versus 11.6% for the placebo group (p=0.059)
(despite being n=>1000…
IF remdesivir delivers any benefit whatsoever it is, at best, in the ballpark of the benefit of ribavirin which, when added to Sofosbuvir and an NS5A is ~ 1% extra SVR12 ie so small you can barely measure it.
In short, remdesivir
- is not a potent NUC,
- it is not even close to a potent NUC and
- even at n > 1000 it has failed to demonstrate any significant benefit.
Compared to a real NUC like sofosbuvir it is complete and utter rubbish, leaving aside the issues that it is IV only and exists only at experimental scale.
Here is a reasonably thorough analysis of the remdesivir trials (credit Dr Andrew Hill)
There are 5 main randomised trials of remdesvir. We need all the results from these 5 clinical trials to be combined. Then we could interpret the overall outcomes in a meaningful way.
When the World Health Organisation review a drug, they always run a systematic review and meta-analysis of all available data.
A: Chinese trial of remdesivir versus placebo showed no benefits (Lancet publication), n=237
1. There is no effect of remdesivir on coronavirus viral load levels – they are the same as the control arm. With 237 patients, this trial show easily have enough statistical power to detect an effect on viral load.
2. Remdesivir was stopped early for adverse events in 12% of patients, versus four (5%) who stopped placebo early.
3. Mortality was 14% for remdesivir versus 13% for placebo.
https://www.thelancet.com/journals/lancet/article/PIIS0140-6736(20)31022-9/fulltext
B: Gilead’s trial in severe infection seem to suggest that 5 days of treatment is better than 10 days. What does this tell us about how well the drug works? Why should less treatment show trends for better outcomes?
1. Clinical recovery: 65% for 5 days, 54% for 10 days of treatment
2. Mortality: 8% for 5 days, 11% for 10 days
3. Adverse events leading to discontinuation: 5% for 5 days, 10% for 10 days
C: NIH trial. Why was the clinical endpoint and sample size changed in the middle of the trial? n=1063, unpublished interim analysis.
This study, announced by Anthony Fauci, shows a slightly lower mortality for remdesivir (8.0%) versus placebo (11.6%), but this is not statistically significant. Remember that in the comparison of 5 versus 10 days of remdesivir, we also had 8% mortality for 5 days of remdesivir, versus 11% for 10 days of treatment. How do we interpret these two non-significant trends in the two trials?
Combined with the Chinese survival data, any difference in survival between remdesivir and placebo will be small and not statistically significant.
D: Missing data from the second Chinese trial.
This study of 308 patients was suspended for poor recruitment, but no results are available for the people who were actually recruited before April 15th. The website mentions 308 patients. What results are available? When will they be published?
https://clinicaltrials.gov/ct2/show/NCT04252664?cond=remdesivir&draw=2&rank=4
E: Main Gilead trial of remdesivir for people with moderate coronavirus infection (n=1600).
This trial is still ongoing, with results not yet available. We should see these results by the end of May.
https://clinicaltrials.gov/ct2/show/NCT04292730?cond=remdesivir&draw=2&rank=7
Even if remdesivir does show overall efficacy, there is the question of drug supplies. Will there be enough drug to treat everyone in need? Also the daily IV infusions of remdesivir will be a large burden on healthcare services.
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