Health Committee on May 25th, 2020

Well, I can tell you that getting data is like pulling teeth out of a mouth, so we're delayed, because the data-sharing hasn't been easy. However, the goal of that study is to look at the differential response to a vaccine in males and females. Our basic hypothesis is that females will answer better and will have better immune response but may also have more adverse events in terms of local adverse events. It just goes hand in hand. The goal was to look at clinical trials that have been done in the past and reanalyze the data on males versus females. As I said, we're having a hard time getting to those data, but it will come.

When we look at the first data out, males seem to have more mortality than females, which could also mean that their immune response might not be as strong, but it's very early on. Because we don't have a good denominator, those proportions are always hard to interpret.

It's something interesting to see. The male versus female response to infectious diseases is not the same. A man's cold is actually something that seems to exist.

My understanding of the data that's emerging, for example from the study in the States on remdesivir, is that it's okay. It has some efficacy, but certainly, what we know from other viral infections is that, with a single agent as an antiviral, often even with some efficacy, the virus will quickly mutate around that.

I think as we understand what cocktails we can use, similar to how we've used cocktails for HIV, even if each individual antiviral drug is okay and not spectacular, a cocktail approach is often very useful.

As for convalescent serum, I understand there are a number of studies or instances where they've used convalescent serum and seen some efficacy. Certainly, at McMaster and across Canada there's a new study starting called the CONCOR-1 study, which is in more than 60 hospitals. They're specifically going to have sufficient power to be able to really understand the convalescent serum, and along with that, they will also be looking at the levels of the antibodies and trying to understand, not just if there are antibodies, but at what levels and how efficacious they are so that we can better understand if it does work, why it's working and how it works.

There have been some studies that have looked at that, and there are certainly some studies now looking at patients who were infected with the original SARS, so SARS-CoV-1. Again, in those studies the immunity lasts really only for two to three years, so even though there are potentially some low levels of protection, coronaviruses don't generate historically long-lasting protection.

Children have a very high natural immunity. Their immune system is often quite active, whereas that wanes as they get older, so part of the reason children and young adults aren't getting as severely ill could be that they have the most robust and natural or innate immune response.

That's a broad question that I don't have the answer to. If I did, I would have said it by now. That said, my sense is that the Public Health Agency of Canada definitely has a role to play, and I think it's trying to do that. The fact remains, however, that, at the provincial level, data also belong to the provinces.

I know all the parties have tried to reach agreements in the past, including the multi-lateral information sharing agreement, or MLISA for short. It doesn't seem to allow for data transfer, at least not in real time. Eventually they are transferred, but not until they've been validated, often nearly a year later. I'm not well versed enough in Canada's Constitution to say how a direct transfer should work. All I can tell you is that it doesn't work for those of us on the receiving end.

What we all fear is that the second peak will hit quickly. If the lockdown isn't lifted in the right way, meaning, we follow the example of some of the southern states—Texas, Georgia and Alabama, where the number of cases has started to climb back up—and if people don't continue to wear masks and respect physical distancing guidelines, the number of cases could start rising again.

Testing is very important, but the public absolutely must abide by the recommendations. We shall see what happens.

In opposition to a regular randomized controlled trial, in which you would vaccinate a patient and wait for that person to be exposed to the disease to see whether the vaccine would be then protective, in a challenge trial you actually squirt the virus directly into the nose of a person who's been either vaccinated or not, to see if those who are vaccinated are more protected than those who are not.

We haven't done any challenge trials in Canada thus far with any virus, but two challenge units have been built as part of a CFI, one in Dalhousie, where they are doing that first phase one study, and one at the MUHC in Montreal. Those challenge units were built to do studies on influenza vaccines after vaccination, but there haven't been any. I think that to do a challenge trial, you would need to be in at least phase two or three of a vaccine, because before that you would still be studying the safety of the vaccine and its immunogenicity, but instead of vaccinating and then just letting people be and hoping that they would be exposed soon enough to see whether that vaccine works, you would have a challenge trial.

They've also done that for norovirus vaccines.