Feedback from a PD research scientist in ... - Cure Parkinson's

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Feedback from a PD research scientist in the department of Clinical Neuroscience at the University of Cambridge (UK), on PASADENA Trial...

p-oui profile image
28 Replies

I am interested in participating in the best clinical trial I can get in to and specifically those targeting Alpha synuclein. So I want to understand ASN and related trials and here is how I interpret the info I've read:

Alpha synuclein (ASN) is one of the most common proteins in your brain – it makes up about 1% of the protein in each neuron. It is very plentiful. What does alpha synuclein do? One thing we know is alpha synuclein is involved with normal synaptic functioning. More recently, we have learned that alpha synuclein is playing an important role in the handling of vesicles at the synapse. It acts as a protein buffer, helping to cluster vesicles at the synapse without affecting the release of the chemical messengers.

That is my basic understanding and I find it super helpful to follow this blog:

scienceofparkinsons.com/about/

I reached out to Simon, the research scientist who runs the blog, and asked about the PASADENA study and expressed my concerns about indiscriminate removal of ASN. Here is what he shared:

"It is important to understand that the approach the researchers are using in the PASADENA study is not ‘indiscriminate’ in its removal of alpha synuclein. PRX002 (the drug being tested in the PASADENA study) is an antibody-based treatment that targets a specific aggregated (or clustered) form of the alpha synuclein protein which is believed to be toxic. It does not affect normal (un-aggregated) alpha synuclein. Exactly what PRX002 is targeting (the precise epitope) is a trade secret for company running the trial: Prothena.

As to the long term consequences of this approach, it all depends on where you stand in the great ‘alpha synuclein’ debate. If you think that aggregated alpha synuclein is the bad guy in PD, then removing it is probably a good idea. If, however, you think that aggregated alpha synuclein is simply an innocent man getting caught in the wrong place at the wrong time, then maybe it’s not such a great idea to remove it. There is some evidence to suggest that the aggregated form of alpha synuclein may be a defensive mechanism inside the cell – playing a role in protecting cells from viruses

(scienceofparkinsons.com/201.... Only time will tell if the PASADENA approach will work. One concern I do have with the study is that the clearance of alpha synuclein alone may not be enough. Perhaps they also need a anti-inflammatory or neuroprotective approach to real slow/stop PD. Follow up studies will be required to address this. Interesting times for Parkinson’s research."

IF ANYONE IS IN THE PASADENA OR ANY ASN RELATED TRIAL PLEASE SHARE YOUR FIRST HAND EXPERIENCE:-) OF COURSE I WELCOME ANY RELATED INSIGHTS.

Check out this blog on his site:

(scienceofparkinsons.com/201....

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28 Replies
MBAnderson profile image
MBAnderson

Simon said, "... it may not be such a good idea." (if a/syn is a consequence and not a cause.) I wish he would've elaborated on what the downside might be. Can it be both protective and toxic at the same time? Also, isn't that in conflict with the goal of Nilotinib being to up regulate autophagy? Seems like everything we've read, for years, says that when a/syn aggregates into the Lewy bodies, it becomes toxic. As you know, I'm a DIY Nilotinib user for the purpose of clearing the gunk out. It's a tough decision, p-oui. I also wish the authors of the theory that it's protective would've explained what it's protecting against, or did they?

park_bear profile image
park_bear in reply to MBAnderson

Indeed confirmation of the nilotinib results will help prove ASN aggregates are the cause. Have you received any benefit?

MBAnderson profile image
MBAnderson in reply to park_bear

I can't tell because I take a lot of other stuff, do fasting, exercise, etc. I take about a dozen supplements and didn't want to waste the time taking 2 or 3 months for each one individually. I believe I'm progressing slowly, though. Could be genetic, a robust regimen, plain, dumb luck or a combination thereof. I suspect if I was eligible for this trial, I'd get in. Seems like there would be more upside then downside from clearing out Lewy bodies. But, who knows?

JANVAN profile image
JANVAN in reply to MBAnderson

Hi MBAnderson : what is the meaning of "I'm a DIY Nilotinib user for the purpose of clearing the gunk out..."

And, considering you have posted a lot of good researched posts, I'm asking you >>> what do you think of Marty Hinz and his protokoll.....??

MBAnderson profile image
MBAnderson in reply to JANVAN

JANVAN,

"DIY" = do-it-yourself, i.e., I don't have the benefit of medical supervision. "Clearing out the gunk" refers to stimulating autophagy which is the process by which cells excrete or expel dead material, in our case a/syn.

Just in case you're considering this - don't. Nilotinib is a dangerous drug and if I haven't dissuaded you, I'll explain why.

I haven't read Marty Hinz's book or much of what he has published, so cannot comment.

p-oui profile image
p-oui in reply to MBAnderson

This exchange took place over a very well written blog called The Science of Parkinson's. I posted my question at the end of this blog as Pamela and you can find it here: scienceofparkinsons.com/201...

I am also very interested in a calcium trial and hope to get into one. My question to Simon focused on trials generally and specifically those aimed at removing ASN clumps.

Simon, the researcher / blogger seems very receptive to questions and responded quickly.

As for the PASADENA trial, I struggled with the decision on this direct approach to removing ASN clumps via Prothena's experimental new drug for these reasons but also because Phase I of the drug showed no improvements though, to be fair, these were safety studies. Still...

Another blog more focused on ASN on the same site: scienceofparkinsons.com/201...

You may pose questions directly to Simon at the end of each blog.

MBAnderson profile image
MBAnderson in reply to p-oui

Whew. Brain chemistry is more complex than astrophysics or even my relationship with my EX. I lucked out on this one though - I've been taking 5 mg, 2/day of Isradapine for couple years, now. I didn't see any reference to it being dose-dependent though. I guess this goes to show, if we take enough stuff, a few of them are bound to do some good.

p-oui profile image
p-oui in reply to MBAnderson

Tell me about it! I am hoping that some combination of blind luck and a good guess will get me somewhere. I am starting with two 2.5 MG 2x Daily and will titrate up to 10MG daily on the Israpidine to mirror the trial out of Rochester but I am on the look out for other trials testing more highly targeted channel blockers.

MBAnderson profile image
MBAnderson in reply to p-oui

Because I get my health care at the VA, they don't prescribe off label, so from shopping around I found that Isradapine is cheapest if you get a 90 day prescription and use a GoodRx coupon at Walmart - though I hate giving Walmart my business.

MBAnderson profile image
MBAnderson in reply to p-oui

I don't know if you have to start at 2.5 mg, because Isradapine is such a weak drug, it takes 6 weeks for the blood serum to reach a therapeutic level

p-oui profile image
p-oui in reply to MBAnderson

My GP has prescribed as he understands the potential value but wants to start cautiously.

jeffreyn profile image
jeffreyn

About a year ago there was a paper out of Georgetown that suggested a role for alpha synuclein in the immune response to (some) infections.

The corresponding links are contained in this thread:

healthunlocked.com/parkinso...

jeffreyn profile image
jeffreyn in reply to jeffreyn

Actually, the following AlzForum article is a much better reference than the Georgetown press release (imho).

Article: Put ’Em Up: Does α-Synuclein Help Fight Microbes in the Gut?

alzforum.org/news/research-...

MBAnderson profile image
MBAnderson in reply to jeffreyn

Well written article.

p-oui profile image
p-oui in reply to MBAnderson

very

Dee1980 profile image
Dee1980

I haven't looked into ASN all that much, could it be similar to plaque in arteries? Ie the body lays down plaque where there's micro-tears, cholesterol doing a patch job?

The body does amazing things in the face of disease, but it's can be difficult to tell between what the body's response is and what the actual underlying problem is. Hope this trial reveals more.

M1tz1 profile image
M1tz1

All this makes me think of the contradictory attitudes towards amyloid plaques in Alzheimer's. It used to be seen as the villain in this condition (and still is in some circles) but a number of scientists are beginning to regard it as protective.

jeffreyn profile image
jeffreyn in reply to M1tz1

A couple of years ago there was something along these lines in "Science":

Article: Alzheimer’s protein may help brain fight infection.

sciencemag.org/news/2016/05...

p-oui profile image
p-oui in reply to jeffreyn

another thought provoking article, as offered in another article "it might make sense to treat it more like cholesterol—which is needed by all cells but dangerous in high levels—than something that needs to be completely eliminated"

jeffreyn profile image
jeffreyn in reply to p-oui

I don't know a lot about Alzheimer's, but I think that the cholesterol analogy applies quite well to alpha-syn and PD.

It fits in with a key finding from familial PD, that too much alpha-syn (resulting from duplication, or triplication, of the SNCA gene), in and of itself, can cause PD.

M1tz1 profile image
M1tz1

Thank you, Jeffeyn. Maybe it was that study which triggered the comments I encountered.

Hikoi profile image
Hikoi

More from Simon re alpha/syn

scienceofparkinsons.com/201...

Short version below

scienceofparkinsons.com/alp...

Lewy bodies

scienceofparkinsons.com/201...

p-oui profile image
p-oui in reply to Hikoi

Riveting. Thank you for posting. After reading through the articles I keep wondering how the challenge to our thinking around lewy bodies might be related to newly discovered Pa-Syn? I asked Simon and will share what I hear back if he hasn't kicked me off the blog LOL

scienceofparkinsons.com/201...

jeffreyn profile image
jeffreyn

Some information on Biogen's Phase 1 clinical trial, from the recent AAN conference in Los Angeles.

New Alzheimer’s and Parkinson’s Immunotherapy Data at AAN:

alzforum.org/news/conferenc...

(information on Biogen's BIIB054 is at the bottom of the page, after the heading "On to Parkinson's")

p-oui profile image
p-oui in reply to jeffreyn

Thanks for sharing this! It is so difficult to find any info on data from the trials and it takes too long for these reports to get generated. RE this:

"Brys said that as in healthy volunteers, BIIB054 formed complexes with α-synuclein in plasma. That both doses formed similar amounts of complex suggested near-complete saturation of blood synuclein with antibody. Attendees wondered why the antibody bound so much plasma synuclein if its affinity for monomers is so low. Brys explained that, although BIIB054 is more selective for aggregated than soluble α-synuclein, at high doses, it is expected to bind the soluble form. Brys said there were no serious adverse events, and no obvious worsening of PD symptoms in either placebo or treatment arms during this short trial. The SPARK Phase 2 study of BIIB054 is enrolling now.—Marina Chicurel."

What do you make of that?

jeffreyn profile image
jeffreyn in reply to p-oui

It looks okay to me. They seem to be collecting the right kind of data. This should enable them to continue to move forward.

I would guess that the final dose selected will be closer to the low dose (15 mg/kg) rather than the high dose (45 mg/kg), since "both doses formed similar amounts of complex".

But it is still early days (i.e. Phase 1).

p-oui profile image
p-oui in reply to jeffreyn

Thank you - If I were eligible (I am not due to Azilect) I would be very interested in this trial. Those who are not yet on PD RX might seriously consider it.

ddmagee1 profile image
ddmagee1

Very interesting.

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