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05-04-2017, 09:52 AM | #1 | ||
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05-06-2017, 12:42 AM | #2 | ||
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From the research paper:
"The results presented herein reveal potential protective side effects for doxycycline in the pathogenesis cycle of synucleinopathies that could be exploited repurposing an old safe drug." "This data strongly suggests that doxycycline in subantibiotic doses (20–40 mg/day) would be enough to exert neuroprotection." From the ScienceDaily article: "This treatment could stop Parkinson's from progressing, and we therefore plan to start a clinical trial shortly." Could this be another clinical trial worthy of a fast-track process? Repurposing doxycycline for synucleinopathies: remodelling of α-synuclein oligomers towards non-toxic parallel beta-sheet structured species : Scientific Reports (this is an open-access research paper) |
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"Thanks for this!" says: | kiwi33 (05-06-2017) |
05-06-2017, 03:32 AM | #3 | |||
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Grand Magnate
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An impressive piece of biophysics and cell biology.
I think that the comments in the link are worth considering.
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05-06-2017, 07:22 AM | #4 | ||
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Well spotted, kiwi33. I missed those comments, and they are significant.
It would seem that a fast-tracked clinical trial would not be appropriate. |
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"Thanks for this!" says: | Tupelo3 (05-06-2017) |
05-06-2017, 09:09 AM | #5 | ||
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Quote:
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05-06-2017, 09:11 AM | #6 | ||
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05-06-2017, 10:15 PM | #7 | ||
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No worries, Tupelo3.
When I wrote those words, I had in the back of my mind the recent discussions about the desirability of speeding up the clinical-trials phase for PD drugs in general. So it wasn't that this one stood out particularly (although it did seem like a good candidate), it was more that I'd lowered the bar! The question mark at the end was (secret?) code for "I'm interested in a discussion". :-) But after that, kiwi33 alerted me to some expert comments, which shed new light on things. |
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05-09-2017, 08:49 AM | #8 | ||
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From the same paper, curcumin is mentioned. While everyone waits for re-purposed drugs to make it out of these trials, maybe curcumin could help now.
Curcumin (diferuloylmethane) also reduces significantly cell toxicity of α-Syn aggregates by binding to preformed oligomers and fibrils46 with effectiveness comparable with doxycycline (1:1 molar ratio)47. However, the instability, low solubility, little oral bioavailability of curcumin limit its clinical applications and to overcome this drawback, some structural curcumin analogues with antiaggregation properties are been developed. In this context, no human long-term toxicity studies have been reported until now with curcumin structural analogues48. On the contrary, oral administration of doxycycline proved to be a safe and effective drug for dermatologically long-term treatments49,50. Moreover, it was also reported that sub-antibiotic doses of doxycycline have no effect on the composition or antibiotic resistance of different microflora51. |
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05-09-2017, 05:31 PM | #9 | |||
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Quote:
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"Thanks for this!" says: | jeffreyn (05-09-2017) |
06-04-2017, 04:34 PM | #10 | ||
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Junior Member
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I started taking 20 mg a day of Doxy about a week ago. So far, no observable effects.
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"Thanks for this!" says: | GerryW (06-07-2017) |
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