Health Committee on Oct. 26th, 2009

What was the advice you were given that was different?

Well, they will. It will be in the materials they receive that have been rolling out through the provinces in terms of the product monograph, etc. They would be expected to read those materials before they actually immunize anybody. I'm surprised. Perhaps they don't watch the news.

There are materials that will be going with the product that nurses and others will read. I don't know if these are officials who actually give immunizations or just people who are working in public health. The materials are there. The materials will be there.

Public health units, every year, do immunization against influenza. This is another influenza vaccine. The only difference is the addition of the adjuvant that improves immunity. There are not issues with allergies with this adjuvant.

The issue with authorizing on data generated in Europe is not quite true. It's a whole package of data, which I tried to express. The data from Europe was really on the efficacy of the H1N1; that was the early data coming in. The safety package was primarily from the H5N1, which has been tested in Europe and the United States and in Canada as well.

So the data are coming in, to start with from Europe, but there are data from Canada. There are safety data coming in from Canada as well. It's the same vaccine. So you cannot wait to get the data from Canada as well; you already have the data from European studies.

I think that's what you're asking.

With respect to the vaccine in Canada, the vaccine is basically the same as the one GSK makes in Europe. The only small difference is a slight difference in the manufacturing process, but for all intents and purposes it's the same vaccine.

Could I answer that one?

I think she was referring to a group trial of 130 in Europe. It's bigger than that; there are two trials there. It's actually double that. I think the figures may have been mixed up somewhere. It's not just 130. There are two studies done in Europe with slightly different concentrations of the adjuvant and the antigen, essentially, so the numbers are not quite correct.

On the safety side, as I did explain originally, there is a whole safety database. For adjuvanted vaccines, it's H5N1, and then you switch over to the H1N1 virus for the actual efficacy part.

I think Paul wants to add to that.

As for the safety of the H1N1 adjuvanted vaccines, you would anticipate it to be the same as the H5N1 adjuvanted vaccine that has been approved in Europe. When you look at all of the adjuvanted vaccines, H5N1, H1N1, and adjuvanted seasonal vaccines, there are over 40,000 people who have been vaccinated with that adjuvant.

With the annual seasonal flu vaccine, which is licensed, all that happens every year is that there's a strain change. There is a small clinical study of the same size that takes place. Some of them are in Europe, some of them are in Canada. Every year, it's the same. It's following the same pattern. There's nothing special about this.

It is the same message. The vaccine without the adjuvant is preferable because we have less data about the vaccine with the adjuvant during pregnancy. This is an option for women. This week and last week, the recommendation was the same, i.e. less than 20 weeks. The risk for pregnant women is the same as for other women of the same age group. However, after 20 weeks of pregnancy, the risks go up almost four-fold. If the illness is present in the community, the risk is greater than the theoretical risk of the vaccine.

Could I first clarify the point about the timing?

I think the idea was—and Dr. Butler-Jones can help me with this one—that we didn't want to say we were going to be able to have a vaccine available in mid-October when we weren't really sure we would be. The conservative approach was to say November. However, the data that we were waiting for—some quality data and some early data in terms of the actual efficacy—came in early from GSK, so we could actually look at those data early on, much earlier than we had expected. There was no point, then, in waiting another month or so to move forward. Basically, the data were in early, we could evaluate those data, and everything looked fine.

As to the data you're asking for on the safety, as with all vaccines and all drugs, usually the manufacturer conducts all these activities. There are other activities now going to take place with already licensed vaccines, and the Public Health Agency will be doing some of these studies. Usually these are not done prior. It's usually the manufacturer that does these particular studies, because it's not a publicly available product, essentially.

Do you want to comment on that, Paul?

I can comment, first of all, on the clinical trials that we're doing on H1N1. We're doing 16 clinical trials around the world.

Just to the point about studies being done in Canada, those 16 trials will include over 10,000 subjects, and 2,000 of those will be Canadian—

Not really. When products are licensed in Canada, the data from the manufacturer is usually assessed. It's not an independent assessment. It may involve independent investigators, which is a different issue, but it's all manufacturers' data.

There are independent researchers who are contracted to do the research, but it is from the company. But it is transparent; the regulator sees all the data, good or bad, with it. So that's not an issue.

We are doing additional trials, and again, to be clear in terms of when we were talking before about what was planned, that has not changed. Nothing has been short-cut. But what we found is that after one dose there was good immunity. The six weeks would be required for two doses and the results of two doses before you'd know.

In Canada we have said, and I've been saying from the beginning, that we were working to have it available as soon as possible in terms of safe and effective vaccine, confident about the beginning of November. Nothing was shorted. The only additional thing the regulator might look for is immunity data following the second dose, etc., which would not change the decision about when to immunize.