Subcommittee on Neurological Disease Committee on June 8th, 2010

I previously worked in the United States on Huntington's, for which a system exists. Let us say that we are successful in finding new drugs that are effective in the model system, be it with a fly, a worm or a mouse. We then move on to clinical trials. There is a system in place for Huntington's disease, but there is still nothing for ALS.

In fact, the present problem is that, even if I discover something that works very well with another model, what am I going to do if I do not have the money to carry out a test on a mouse? Clinical trials are assuredly too costly. I cannot pay for everything.

Agreed.

Yes, I think so. From my lab, I know the recent genes we've identified in ALS affect toxicity in our models for Huntington's disease and also our model for Alzheimer's disease. There's a definite crossover. I don't know about Parkinson's because we don't have that in our lab.

It's somewhat surprising, but maybe not. The point is well taken that anything we find in one of these diseases, for the most part, will have a good chance in functioning across other late onset neurogenetic diseases as well.

It's Sunnybrook Hospital. They've had one clinical trial, and that entailed the use of lithium. I think it was going to be—and please correct me if I'm wrong—an 18-month study. It was stopped midway through because it was found to be totally inefficacious.

I think there is a trial under way shortly...

Ceftriaxone.

Ceftriaxone, yes.

To follow up on this point, I was on the lithium trial. This was based on a study in Italy. Unfortunately, I think it had a lot of holes in it.

I think everybody is desperate to grab on to something hopeful. I began the study around February 2008. They stopped it in September after six months, and then it took me six months to find out whether I was on the lithium or the placebo. In the end they found that people who had been on the lithium had trended a little more downward. That put so much fear into me. You put your life in the way of...you don't know.

I'm sorry, I need a drink.

I get bits and pieces from the hospital, from the integrated clinic; otherwise I would say I make myself knowledgeable.

I would think there is not a collective reality around services. I don't want to say there are no services--there are--but I don't feel they are coordinated and presented in a thorough and needed way.

I don't know if that was your experience.

Definitely.

You have to be smart and you have to ask questions. That's true in life anywhere. You have to be your own advocate, even with ALS, and there is only so much energy and so much room you have, but the reality is, I would say, you have to go after your own treatment and your own sense of taking care of yourself. You really have to manage and find your way through that system.

There is a lot of stuff online, and there are doctors in the States, but I just feel that we haven't coordinated everything. The communication, I feel, is not strong. Most of the communication is so depressing--seriously, not that I'm a bundle of joy here. It is so depressing that you don't get a sense that there is a forward movement of advocacy for real change. You feel lost in the system and you don't feel there is a real forward-thinking movement and approach to shift this to a new place.

Not for awareness, obviously, but for the actual research itself...? How much? Any increase is great; I'm not going to say anything bad about that. We are asking for an across-the-board increase of 1%, and that would benefit all research itself. How much would it be just for the neurological diseases? I suppose an extra....

With an average CIHR grant, for example, if you're lucky, you can get about $300,000 over five years. That's a lot; that would set up a new lab like the one I have for a long time. But those are so hard to come by.

On the amount of funding you get, it's kind of the same. It's just that the number awarded is very low. So if it could be bumped up even a percentage point, that would make a big difference. What happens now is you have an idea and you have to go around to smaller, different agencies and hopefully package enough research to go for the big one, and then if you get it you can finish a project and hopefully find something interesting. That is hard to do.

Right now I have a small amount of funding from the CIHR. I'm very grateful for the support from ALS Canada, and I have funding from Switzerland. As a new person, it has been hard to get into the big grants from the CIHR.

I don't know. Just an increase...I can't give you a dollar amount because I don't have a budget.

Our clinical trials network is running a trial on ceftriaxone, and a few of the centres are running a second trial. Some of our clinicians work as part of American groups also, so there's an advantage there. We could carry out more trials, because there are things on the launch pad waiting to be tried. For example, I was at the American Academy of Neurology conference in April, and in the session they were talking about the progression of clinical trials from phase one, which is just safety, through phase three, which is the full-blown proper clinical trial. And there are a number of candidates sort of waiting their turn.

There are drugs that act on different mechanisms. One of them is supposedly going to act on intercellular protein aggregates, which has something in common with a number of neurodegenerative disorders. So it's a compound that works on that. That's from a small biotech company. There is something from another small biotech company that is working on the main system of cell death in motor neurons, which has been identified in the lab.

There are a few problems. Small biotech companies can only go so far because of their commercial reality. If something isn't snapped up by a large biotech company and individual clinical trial centres don't have funding--which they don't--this is the stuff that sort of sits by the wayside.