Posted on 08/10/2014 12:46:23 AM PDT by Smokin' Joe
I have spent a little time compiling links to threads about the Ebola outbreak in the interest of having all the links in one thread for future reference.
Please add links to new threads and articles of interest as the situation develops.
Thank You all for you participation.
Author: Nick Owen
Blog:MSF Ebola Blog
Nationality: British
Country: United Kingdom of Great Britain and Northern Ireland
Job Type: Communications Officer
Topic: Ebola
Subject 001016: The Vaccine Trial
06 October 2014 Be the first to comment
Be the first to comment
Its odd to think I currently have a small bit of one of the worlds deadliest viruses coursing through my veins. Its a virus so lethal that up to 90 percent of those who catch it can die. At the moment, its rampaging through West Africa in Liberia, Sierra Leone and Guinea tearing thousands of families apart in its wake. And its in my blood. Thankfully, despite having a part of the virus, I dont stand a chance of catching it. Ive been given an Ebola vaccination, the first of its kind.
Ive just returned from the Jenner Institute at Oxford University where the first ever Ebola vaccination clinical trial is taking place. Sixty of us willing volunteers are taking part. The aim: to test the safety of the vaccine before its taken to the field.
Friends and family have said I must be mad to want to take part, but I struggle to see the issue. As I write, 10 of my MSF colleagues have died treating this virus, along with hundreds of other healthcare workers in West Africa. To me, having a sore arm and potentially feeling a bit fluey is a very small sacrifice to make if it means lives will be saved in the future, and that my colleagues can work without putting themselves at even greater risk.
Now, this blog is usually a place for MSF field staff to write about their daily lives, the patients they meet and the hospitals they help to run. People like Martin and Patricia, who have been or are out in West Africa at the moment. However, the lovely Clare Storry, who runs this marvelous site, has allowed me to try and tell the story of how the Ebola battle is being fought away from the front lines.
The Ebola vaccine
The vaccine Ive been given is called ChAd3, which uses a single benign Ebola virus protein (one seventh of the whole virus) to generate an immune response. Its carried into my body by a vector, in this case a chimpanzee adenovirus or, a common cold. Im deliberately being given a virus as it gets inside cells and produces a particular type of immunity. Its specifically a chimp virus as we are often immune to human common colds, meaning the vaccine wouldnt have a chance to begin to work. Youre essentially tricking your immune system into thinking it has an infection.
The vaccine itself has an unexpected history. Its the product of a decade of research by a collaborative group including the US National Institute of Allergy and Infectious Diseases and an Italian biotechnology company, Okairos, recently bought by GlaxoSmithKline. After the anthrax attack in Florida in 2001, the US government was alerted to the threat of bioterror, with Ebola seen as a potential threat. Research was soon ramped up to find a vaccine for the disease.
Prior to being given the vaccine, I had a few questions that I felt needed answering. I went to speak to Professor Adrian Hill, the Director of the Jenner Institute, who is leading the trial.
The big question is will the immune responses that we generate with the vaccine be strong enough? Thats always a question with new vaccines, says Professor Hill. The volunteers in this trial have been put into three groups, with each group receiving either a low, medium or high dose of the vaccine. Im in the high dose group. One thing that puzzled me was the speed at which this vaccination could potentially be rolled out to the field. Ive heard reports that it could be deployed by late December this year but Im taking part in the trial for six months until March.
The clinical trial team will have early results in immunology by late October, early November, giving them guidance as to whether the vaccine can be used in Liberia, Sierra Leone and Guinea, explains Professor Hill. We keep following people because we want to document safety as much as possible. With any vaccine, objective number one is to determine if its safe. If its not safe, you can forget about it.
With any new vaccine, theres also the question of manufacturing. It can take months to produce a vaccine before the safety trials even begin. The big advantage here was there was some vaccine already made [thanks to the research conducted since 2001]. There was enough to do some trials, but not enough to roll out to healthcare workers, who are our target population. So 15-20,000 doses are being made. The manufacturers are really speeding things up as much as they can."
Blood taken before the vaccinePhoto: Nick Owen
Blood taken before the vaccine was given. I have to go back to the Jenner Institute eight times over the next six months to have my blood tested. These bloods were taken to give a 'baseline' reading.
A 'prevent all' Ebola vaccine?
Being the scientific dolt that I am, I wasnt sure if this vaccine would work for all strains of Ebola. There are five different strains of the virus: Bundibugyo, Ivory Coast, Reston, Sudan and Zaire, named after their places of origin. As it turns out, the reason we might have a working vaccine in the field by December this year is all down to a long series of coincidences.
This particular vaccine is the Zaire strain. It just so happened that the Zaire strain is very similar to the outbreak variant, which is now being called the Guinea variant. At a sequence level its 97 percent identical, and more importantly, immunologically it looks cross reactive so almost certainly this Zaire strain vaccine will work for the Guinea virus. However, it almost certainly wont work for the Sudan strain of Ebola, which is only 60 percent identical.
When the researchers in America and their collaborators in Italy designed an Ebola vaccine some years ago, they were targeting one that would prevent any strain of Ebola. They had to cover as many strains as they thought were reasonably doable and they made two; they made Sudan and Zaire.
Thermostable?
From MSFs perspective, one of the most important characteristics of a vaccine is that its thermostable, meaning that the vaccine doesn't need to be kept in a cold-chain from production to delivery. Unfortunately, with the Ebola vaccine this wont be the case. It needs to be kept below freezing until it's given.
Frankly, there isnt time, implores Professor Hill. To make the existing vaccine thermostable would require a change in the manufacturing process which could mean months, if not years, of delays before the vaccine could be rolled out on a large scale. It can be done, just not right now.
Firstly, you develop a small amount in a process that works in litres, he explains of the manufacturing method. It then works in hundreds of litres, to thousands of litres and that takes time to scale up from small to large and ensure that the manufacturing quality is as good as it was at a small scale.
Although my friends across MSF will be disappointed to hear this, it does make sense. Realistically, we dont have time to change the process, says Hill. We have to use the process that we have and do it more often in more places, and make it more efficient. Its not very cost effective but thats all we can do starting from where we are.
The good news, however, is that this vaccine is not going to cost patients or the people delivering the vaccine. The vaccine in production at the moment is funded by an award from three UK organisations: the Medical Research Council, the Wellcome Trust and the Department for International Development. The research that has gone into the disease and the results from the trial will all be open source, too.
EBL-001016 trial participant
No name! This is how I'll be known to those conducting the trial from now on. For the first 28-days after the vaccine is given I have to keep an electronic diary recording any symptoms that I may experience.
Other outbreak pathogens
The final question I had for Professor Hill was a personal one: how has it made him feel to be a part of such a groundbreaking trial?
Im excited, he says emphatically. Were developing a vaccine that might be used by the end of the year which is fantastically invigorating for the whole team.
Hopefully this will bring more money into the field and more attention to outbreak pathogens. Remember, theres not just Ebola out there. Theres Marburg, Lassa fever, Rift Valley fever, MERS. There are a lot of outbreak pathogens we dont have vaccines for, so if that could change that would be fantastic.
So what needs to change?
We need stockpiles of these vaccines. If, instead of having a vaccine made but not tested for Ebola six months ago, we had a stockpile of vaccines that are shown to be safe and tested in small clinical trials sitting in the relevant regions, maybe Central or West Africa, available to be used as soon as an outbreak happened, you might well have been in a position to stop the outbreak.
You cant guarantee that but it would have been worth trying. So I think thats where we should be next time. Even if this vaccine cannot be used quickly enough to stop the current outbreak, then for next time, we should be better prepared.
Im hoping that my taking part in this trial does just that.
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end article
I want to see Freiden and his posse outfitted exactly as recommended and attending to Ebola patients— real footage, not photo ops.
AS IF they would follow their own suggested protocol.
Or there might just be some sort of screwup.
I had searched for Liberia, and got a red tag with an X—nothing more. Then I went to the blogs and got the entry by the communications guy on the vaccine trials dated Oct. 6. There was another entry (different person) on October 7, but I didn’t copy that and post it.
Only a Dim-Dem would not have seen this coming. A totally indoctrinated fool.
I found the vaccine post on the blogs section, thanks! I’ve made a habit of looking at the news section of the MSF site and it’s always had posts, but now nothing at all.
That doesn’t make sense unless there is a server problem, a website screwup, or someone scrubbed it.
It’s not a server issue because I can access data on MSF using Bing and the site specific tag. The links on their homepage/subpages have been deactivated completely.
I wonder if this has something to do with the Liberian government forbidding any more reporting. If so, what does that say about MSF?
Ah, I’ve never used that URL. I’ve always used msf.org. Thanks!
One of the reasons I really don't trust the MSM is because in my life I have had personal, direct knowledge of about 5 events that made national or international news, and what I witnessed, or otherwise had personal knowledge of, bore no resemblance to what was reported.
While I do not have direct knowledge of what happened at Texas Health Presbyterian, I do have direct knowledge of the Epic EMR software. I am not an Epic employee, but I do use Epic and configure it on a daily basis. It is my day job. I have it running right now on the same computer I'm writing this post on. My son (also not an Epic employee) has implemented their ASAP Emergency Department application in both adult and pediatric emergency departments in three hospitals. What I can say is this:
Epic is an extremely complicated, comprehensive, highly configurable, integrated system of computer applications. NO hospital installs Epic without doing massive configuration to customize it to run the way they want. Many of those customizations have to do with who sees what data entered by whom. It is far more likely that the problem at Texas Health Presbyterian Hospital was due to the way they configured the system than to any inherent bug in Epic.
The fact that this has disappeared from the news is probably because Judy Faulkner, the owner/CEO/founder of Epic, probably called Texas Health Presbyterian and threatened to sue them for blaming their software. As soon as I saw that news article blaming Epic, I thought to myself "I'll bet Judy's gonna jump on that and squash it fast." And if it was due to Texas Health Presbyterian's configuration of Epic, and not to Epic itself, I don't blame her at all.
On my mobile I get the same red x both times using Liberia and the Liberia ebola.
Thanks! I was starting to wonder if I’d entered a parallel universe or something.
Makes sense. Thanks for the tip! I have to wonder if the whole EMR push is going to make things like this much more common.
Sierra Leone burial crews reportedly on strike, leaving Ebola victims in the street
http://www.freerepublic.com/focus/f-news/3212666/posts
“over lack of hazard pay” — how on earth can this bottleneck rise up with Daddy Warbucks Obama on the case?
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2863629/
That’s a paper that discusses the Russian drug.
Similar to the others, but not exactly so.
If it treats the stuff it seems to:
http://www.ncbi.nlm.nih.gov/pubmed/?term=Triazavirin
It would be a great thing to have in case of resistant strains.
Click through to the article on the Russian site for a pic of how the RUSSIANS will be garbing their medicos in the event of an outbreak.
Compare and contrast with how we will be garbing ours at the al.com article.
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