Health Committee on March 18th, 2010

Maybe I can just start, Madam Chair.

I would be happy to bring Dr. Gully back. Dr. Gully is with us not just for H1N1 but is providing public health advice generally to first nations and Inuit health branch. Obviously we'd be happy to find an appropriate time to explore that issue.

If you would like, we can address the issue a little bit further this morning. I'd ask my associate deputy minister, Glenda Yeates, to perhaps speak to this.

Okay.

Canada was very much interested in being part of global efforts to develop a vaccine. At the time that started, one of the deficiencies, or one of the challenges, was having trial-lot production facilities for clinical trials. That's why, as part of Canada's CHVI strategy, that was one of the areas of focus. In the subsequent time, that has now been addressed, so those resources are better used elsewhere.

No. As you can appreciate, there are tremendous challenges in the development of a vaccine against a retrovirus. One of the key concerns is that you don't want to actually stimulate... Since the action of the retrovirus is to create a challenge for the immune system, you don't want to actually recreate a challenge to the immune system in otherwise healthy people.

With the complexity of the vaccine, as we've seen in multiple clinical trials, they've been very challenged, and even the one that has some promise still had very marginal benefit. The issue now is finding good models for vaccines that might have the prospect of working. There have been multiple trials that have not worked well, and it has not been about manufacturing; it has been about the basic vaccine itself.

We were proceeding on with the process. As it turned out, none of the applicants crossed the bar. At the same time, given the time elapsed and given the recognition that things had changed in the world, Gates commissioned the study to look at capacity to make sure that we were on the right track. That turned out to illustrate that in fact capacity had increased and that the needs and circumstances had changed, so since we did not have a successful applicant and the capacity issue was now addressed, it seemed much better to use that money elsewhere.

Whenever that takes place, it's a bit like arguing that we could have done something different about H1N1 because H1N1 arrived in April and surely we should have known that it was going to be H1N1 a year before that. You only know what you know as you know it, and there were in fact reviews that identified, when we started the process, that there was this need. By the time we got to that point last year, there was no longer that need. The world changes no matter what we do.

In the report itself they identify the limitations, but there is clearly sufficient evidence there about the change in circumstances that convinced people that we now need to redirect those resources to other areas of HIV vaccine work.

For this purpose, yes. You can't do everything and you can't follow everything, but certainly for this purpose, yes.

These production facilities are all subject, where they are, to the usual kinds of regulatory controls, as would be a facility were we to build it here. If we built it here, there's no guarantee that it would be any better than one built anywhere else. That's just a practical reality.

The point is that for the clinical trials, for ethics reviews, for all of these purposes, they have to meet those standards. It's in the scientific world; you're not going to be able to cover 99.9999% of every issue or every question. The point is that the capacity is there and it's with reputable organizations, and the feeling is that there is sufficient capacity now to address what we need going forward.

Thank you for the question.

I am going to ask Ms. Boudreau. I am going to ask her whether she can explain the difference between the figures from the Library of Parliament researchers and hers.

Thank you.

I am certainly going to try to explain the figures and I admit they can sometimes cause confusion.

In part, it is because we are using two terms. I am going to use the English term because I think it expresses it better. In French, we would say it is the same term. In English, we say “addressed”, while in French, we say “traité”. When we talk about the term “addressed” in English, we mean that either the licence has been issued for the product or we are in the process of processing the application, that is, we have reviewed the application, we are in the process of evaluating it and we have at least sent a request for further information in order to complete the application. We are talking about these three things when we use the term “addressed”, which is not easy to express in French. In that language, we say “traité”. So it is that number, 193 applications, that are left to be addressed, as I said the other day.

No, because for the term “complete”, I'm going to come back to that.

Right, I apologize if I said that, but the distinction is that 193 applications are left to be addressed, and in the total exact figure, which is 3,098, the rest, that is, the 3,098 less the 193, all the applications can be completed with a final decision by the end of December. However, between now and then, I can't tell you that we will have completed the 9,764 remaining applications. So it isn't just the backlog, it is the normal workload. That is the distinction to be made, because I know the two different terms can cause confusion.