Exciting times for HIV vaccines, less exciting times for the virus

On International HIV Vaccine Awareness Day (the 18th May 2016) at the HIV Vaccine Trial Networks (HVTN) meeting, it was announced that for the first time in 7 years and the first time in Africa, a HIV phase 3 vaccine trial will be taking place. In addition to this the world’s first HIV antibody infusion trial started with its first South African participant in Soweto.

Slowly we seem to be completing a puzzle. Perhaps the most complicated one ever pieced together.

Science is a developing story. Every study, no matter how mundane, adds a puzzle piece to the picture. Sometimes it’s an edge piece, that forms the basis for studies to come and sometimes it’s a middle piece that doesn’t really help anyone at the time but will be imperative to complete the picture. In some cases though, in order to progress, scientists stop fitting in pieces to the main puzzle and start their own. This is a risk because the evidence is leading the field in a particular direction and this direction is fairly certain because multiple people have determined the same thing. Sometimes though, the risk of deviating is worth it. Risk shakes up the field; breaks down dogma and enforces flexibility. And that is what this trial could mean for HIV vaccinology.

I am beyond excited that we are having our first trial in seven years and I’m even more excited that it is happening in South Africa. Capacity building has happened over the last couple of years, allowing for South African clinicians and scientists to run these trials. This means much more opportunity for young scientists, collaborations, funding and all round focus. We are finally in the spotlight. The findings of trials always mean that interest in the field surges again. New ideas will be emerging from unexpected places.

The most recent vaccine trial regimen that showed any protection was the U.S. Military HIV Research Program-led RV144 clinical trial in Thailand completed in 2009. This regimen showed that protection was mediated by something we did not expect. All our data in the field up until that time suggested that antibodies (called broadly cross neutralizing antibodies) that could bind and coat lots of different HIV viruses (preventing entry into cells) would be our best shot at a vaccine. But protection (bear in mind it was only 31%) was achieved by antibodies that weren’t able to block infection of a cell. Instead they are able to bind to an already infected cell and call for backup. Other cells with the ability to secrete substances that pop the infected cell heed the call and come to destroy the infected. Think of the broadly cross-neutralizing antibody as Batman (pretty capable

robin batman 1
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of a fight on his own) and these other antibodies as Robin. The vaccine was tested in Thai people who have a very different epidemic to the part of the world that bears the greatest burden, Southern Africa. So the HVTN has run a series of small trials in South Africans using a vaccine that would be more appropriate for our situation. And now, we are paving the way to HVTN 702 (not to be confused with the talk radio station); the phase 3 trial guaranteed to rock the boat of science.

 

A phase 3 trial is a big deal. A wide range of criteria need to be fulfilled in order to proceed to one and the criteria that were set for HVTN 702 have all been met. However there is much talk in the field that we are progressing for progress’s sake. Many feel like we are creating a vaccine that has both arms tied behind its back and we are expecting it to win an arm wrestling contest. We are expecting robin to win Batman’s fight.  We are pushing a vaccine through that does not create the antibodies we know are going to protect people and are based on historically unimpressive antibodies. Should we be doing trials on things we know are not optimal or should we take the risk and acknowledge that there are clearly things we do not understand? Perhaps what now seems like an arbitrary puzzle piece will start off a new and exciting puzzle.

hero sidekick5400 South Africans will be enrolled from November 2016 and we will know the outcome by 2020. It’s a long time to spend on something that may not work again. What would going back to the drawing board mean for new infections? The bottom line is we have not yet managed to summon Batman to fight for our cause. We have lots of ideas on how to get him there but so far nothing has worked. Should we give up on Robin just because he is not what we expected?

Most vaccines have taken between 25-50 years to develop, so technically 30 years in, we aren’t doing too badly: we have drugs that are very effective at keeping AIDS patients well, which our government has now pledged to provide free of charge to everyone infected; we have drugs that can be used to prevent infection (pre-exposure prophylaxis) and we have lots of ideas bout what will protect people in a vaccine setting.

For me, the proof will be in the pudding. By 2020 we may have even brighter ideas about what we need and how to get there. And potentially the pessimistic view of the current phase 3 if irrelevant if it goes on to form new dogma. If all this phase 3 trial does is encourage bright and motivated young people to tackle arguably one of the most perplexing problems the world has, it will be a win. Either way, now is not a good time to be HIV.

Light @ the end of the tunnel!

In order to really understand the intensity of the light, I would have to paint you a portrait of where I have been, to where I am currently with regards  to my MSc research.  This blog entry reminds me a lot of a song that I like to sing whenever I am in a good mood; “I can see clearly now the rain is gone, I can see all the obstacles in my way. Here is the rainbow I have been waiting for, it’s going to be a bright, bright, sun-shiny day”. Well in my case, it’s going to be a bright, bright tunnel end. For the last two and a half years, I have been on a long, often dark journey.

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http://www.elephantjournal.com/2014/07/the-light-at-the-end-of-the-tunnel/

 

If that journey was to have a sound track, I think it would be “Thunderstruck by AC/DC”.  My journey has had a lot of ups and downs that I would say were filled primarily with downs than ups. Normally, I enjoy going to theme parks for the roller coaster ride but this roller coaster which is my MSc research was different. My past blogs have been mostly about all the things that I have been through and how hard I’ve had to work and struggle just to get my trials going.

This blog is a little bit different, this blog is about nearing the end of my MSc degree, the end of the dark tunnel with a bright light at the end. It’s about seeing the light at the end of the tunnel as my bright future, instead of a train coming to knock all my hard work off the rails, as well as using support structures in your life as a coping mechanism.

Keep your head up. Keep fighting. There is always light at the end of the tunnel, and your struggles only make you better in the end
http://quotesgram.com/keep-up-the-fight-quotes/

The obstacle that has been standing in my way from submitting my dissertation was the fatty acid profile (egg yolk) samples that I had sent to the Agricultural Research Council Lab for profiling. I have to sincerely thank them for their quick turn over time because fatty acid profile analysis normally takes forever and a day. To be honest, my impatient side was starting to get the better of me. At times, the desire to succeed does force us to make irrational decisions that we later regret in life, all in the name of progress. Thank God it never came to that though (Chuckles). So I received the data a few weeks back and since then, I have managed to put the data on Excel, run it using the SAS Procedure, tabulated and finally discussed the obtained results.

The results were not what I originally hypothesised in my proposal. There is no doubt chemically, that Moringa oleifera seeds are exceptional but the results obtained were not at all positive. Moringa oleifera seed meal in my study decreased feed intake and body weights of chickens and did not improve the omega 3, 6 and 9 fatty acids in egg yolks. This was a horribly negative result from my perspective.

But was “negative” really negative?

I was once invited by Caradee Wright to speak at one of her “High School Spaza Science Club” and on our way there, we ended up talking about cancer research. I felt that it was dangerous conducting research as a post graduate on Cancer and other hard to treat diseases because the inability to find a cure would mean your research would’ve failed to produce positive results. She said “Any result in research is a positive result”. At first I was a little puzzled but later it made sense. My “negative” results may not be what i had hypothesised but they were still positive. Having those results meant that no one will ever research this again because now information is available in literature. In the future, the next time a researcher thinks of using these seeds in layers, they will be able to find information (my study!) advising them against that.

Through the dark times in my life, I have always been lucky to have coping mechanisms that assisted me in navigating my way through the dark tunnels of life. Having important individuals travelling with you through the dark times of your life is one of the coping mechanisms. My supervisors, my friends, my family and my girl friend have always been part of that support structure. Any great person will tell you that there are times in life where you doubt yourself, times when you feel like giving up would be easier than to continue.Having such people in your life is awesome, people who will remind you of your talent, your abilities and why you decided to embark on that journey in the first place.

So what’s the bottom line? Well the bottom line is that you will struggle in life, your life

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https://za.pinterest.com/alinekd/amazing-wise-quotes/

will have ups and downs, maybe more downs than ups and you will virtually travel under pitch black tunnels but if you have a rigid support structure and also use all the acquired knowledge and assistance from all the troubles that you faced to navigate those dark tunnels then you will be fine. It will be scary at first but just like me, your tunnel will have a light at the end if you work hard and believe in yourself in whatever you do.