Simufilam
Clinical data | |
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Other names | PTI-125, PTI-910 |
ATC code |
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Pharmacokinetic data | |
Elimination half-life | 4.5 hrs[1] |
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Simufilam (PTI-125) is an experimental medication for the treatment of Alzheimer's disease.[2][3] It is being developed by the American pharmaceutical firm Cassava Sciences. The drug is in phase III clinical trials as of October 2023. There are two phase III clinical studies: RETHINK-ALZ, a 52-week trial, is set to complete in 2024,[4] and REFOCUS-ALZ, spanning 76 weeks, is projected to finish in 2025.[5]
The US
After the FDA said that the citizen petition was the improper procedure to request an investigation, Reuters reported in July 2022 that a criminal investigation of Cassava Sciences was started by the United States Department of Justice (DOJ) over research results related to the experimental drug.[9] The U.S. Securities and Exchange Commission (SEC), the U.S. National Institutes of Health (NIH), and City University of New York (CUNY) are also investigating whether Cassava or individuals manipulated data.[10]
History
From research funded by Cassava Sciences (then Pain Therapeutics),
Wang separately identified a large protein associating with the alpha 7 nicotinic receptor when Abeta42 bound and signaled through this receptor in Alzheimer's disease models. He identified it as FLNA, and Wang and Burns tested the hypothesis that it was critical to the toxic signaling of soluble amyloid. In 2012, they stated in The Journal of Neuroscience that the compound PTI-125 disrupted FLNA linkage with the alpha 7 nicotinic receptor as well as the toxic signaling of Abeta42, presenting PTI-125 as a novel therapeutic strategy for Alzheimer's disease.[12][14] The Journal of Neuroscience issued an expression of concern in 2022.[6]
Wang, Burns and co-authors reported in Neurobiology of Aging in 2017 showed that PTI-125 induced improvements in Alzheimer's disease pathology as it binds, and restores to normal, an altered conformation of FLNA in experimental Alzheimer's disease transgenic mice.[15][16] Neurobiology of Aging issued an expression of concern for this paper in 2022.[6]
In 2018, the
Open-label studies started in March 2020,[6] and Cassava Sciences reported in May 2020 that initial biomarker analysis of cerebrospinal fluid (CSF) samples from its phase IIb clinical trials of PTI-125 had failed, but reported in September 2020 that a new analysis by an "outside lab" showed improvements in biomarkers, adding that individuals with Alzheimer's also showed improvements in cognition with simufilam.[6][20][21] It was later revealed that the outside lab was Wang's CUNY lab.[20][6]
In October 2021, larger trials were initiated;[6] Cassava Sciences announced in December 2021 that the first phase III trial of simufilam would enroll about 750 participants, and the second 1,000.[6][22] In the first quarter of 2022, 60 participants were enrolled;[6] Stat stated that enrollment had slowed as of April 2022, as people were deterred from enlisting due to the prevailing controversies.[23] In August 2022, Cassava stated that over 400 patients had enrolled in the trials.[24]
Pharmacology
Burns and Wang reported in 2008 that FLNA contains the high-affinity binding site of naloxone and naltrexone in preventing opioid tolerance and dependence,[11] and in 2020 that by disrupting that simufilam reduces the ultra-tight binding of amyloid beta 42 to the alpha-7 nicotinic receptor.[1][14] Burns and Wang say that the FLNA linkage to the alpha 7 nicotinic receptor is critical to amyloid's toxic signaling through this receptor and that simufilam disrupts FLNA's linkage to this receptor to stop this toxic signaling.[14] They later demonstrated, by isoelectric focusing, that simufilam restores to normal an altered conformation of FLNA in Alzheimer's disease models or postmortem human brain tissue.[15][16]
A 2020 study found simufilam improved epilepsy in a mouse model where FLNA was overexpressed.[25]
Allegations of research irregularities
As of July 2022, Cassava Sciences and papers published by Burns and Wang are under investigation by the
Research papers demonstrating the mechanism of action of simufilam contained an error of units in methods (one instance of milligrams noted as micrograms) and erroneous duplication of images, but neither journal found evidence of data manipulation that was previously alleged.[28][29] Two papers unrelated to Alzheimer's disease that reported FLNA binding by certain opioid antagonists and FLNA's role in opioid tolerance and dependence were retracted for "similarities in background pixels" in western blot images without evidence of data manipulation.[30][31]
Lawrence Sterling Honig, professor of neurology at Columbia University Irving Medical Center, had remarked on Burns and Wang's claims: "But in fact, all the evidence seems to be from this [Wang's] lab."[6] Robert Howard, professor of psychiatry at the University College London, is concerned on the lack of placebo and small sample size and said that the research "at the very least is implausible". Thomas C. Südhof, Nobel laureate neuroscientist at Stanford University, also commented: "The overall conclusions with regard to Alzheimer's disease make no sense to me whatsoever... [The findings of Burns and Wang] are not in the mainstream of the field, and to me they seem implausible and contrived."[6]
In October 2023, a leaked CUNY report indicated that they could obtain none of Wang's original data, which meant that they were unable to either prove or disprove allegations that the images were improperly manipulated;[7][32] they paused the investigation a few weeks later over concerns about confidentiality and integrity of the process.[33]
References
- ^ S2CID 211039039.
- ^ "A Phase 3, Randomized, Double-blind, Placebo-controlled, Parallel-group, 52-week Study Evaluating the Safety and Efficacy of Simufilam 100 mg Tablets in Subjects with Mild-to-Moderate Alzheimer's Disease". May 25, 2022. Archived from the original on June 6, 2022. Retrieved June 6, 2022.
- ^ "A Phase 3, Randomized, Double-blind, Placebo-controlled, Parallel-group, 76-week Study Evaluating the Safety and Efficacy of Two Doses of Simufilam in Subjects with Mild-to-Moderate Alzheimer's Disease". June 2, 2022.
- ^ "A Phase 3, Randomized, Double-blind, Placebo-controlled, Parallel-group, 52-week Study Evaluating the Safety and Efficacy of Simufilam 100 mg Tablets in Subjects With Mild-to-Moderate Alzheimer's Disease | Alzheimers.gov". www.nia.nih.gov.
- ^ "A Phase 3, Randomized, Double-blind, Placebo-controlled, Parallel-group, 76-week Study Evaluating the Safety and Efficacy of Two Doses of Simufilam in Subjects With Mild-to-Moderate Alzheimer's Disease | Alzheimers.gov". www.nia.nih.gov.
- ^ a b c d e f g h i j k l Mandavilli A (April 18, 2022). "Scientists Question Data Behind an Experimental Alzheimer's Drug". The New York Times. Archived from the original on April 27, 2022. Retrieved April 28, 2022.
- ^ .
- ^ Mandavilli A (October 14, 2023). "Scientists Investigating Alzheimer's Drug Faulted in Leaked Report". The New York Times. Archived from the original on October 15, 2023. Retrieved October 15, 2023.
- ^ Taylor M, Spector M (July 27, 2022). "Exclusive: Cassava Sciences faces U.S. criminal probe tied to Alzheimer's drug, sources say". Reuters. Archived from the original on July 30, 2022. Retrieved July 31, 2022.
- ^ from the original on May 3, 2022. Retrieved April 29, 2022.
- ^ PMID 18253501.
- ^ PMID 34295950.
- PMID 19172190.
- ^ PMID 22815492.
- ^ S2CID 207163555.
- ^ PMID 33297460.
- ^ "Multiple Ascending Dose clinical trial of PTI-125, a novel AD therapeutic candidate". nih.gov. 2018. Archived from the original on June 2, 2022. Retrieved April 29, 2022.
- ^ Cassava Sciences, Inc. (September 7, 2021). "A Phase 2b, Randomized, Double-blind, Placebo-controlled, Multiple Dose, Biomarker and Safety Study of PTI-125 in Mild-to-moderate Alzheimer's Disease Patients". National Institute on Aging (NIA).
- ^ "Cassava Sciences Announces Lead Drug Candidate PTI-125 Is Assigned the Chemical Drug Name 'sumifilam' by USAN" (Press release). Cassava Sciences. August 24, 2020. Archived from the original on May 3, 2022. Retrieved May 3, 2022 – via GlobeNewswire.
- ^ a b Keefe PR (January 15, 2022). "Jordan Thomas's Army of Whistle-Blowers". The New Yorker. Archived from the original on July 22, 2022. Retrieved April 29, 2022.
- ^ "Cassava Sciences Announces Final Results of a Phase 2b Clinical Study of Sumifilam in Patients with Alzheimer's Disease" (Press release). Cassava Sciences. September 14, 2020. Archived from the original on August 31, 2022. Retrieved August 31, 2022.
- ^ "Cassava Sciences Launches Clinical Website to Support Phase 3 Studies of Oral Simufilam in Alzheimer's Disease". GlobeNewswire News Room (Press release). Cassava Sciences, Inc. December 23, 2021. Archived from the original on December 23, 2021. Retrieved April 30, 2022.
- ^ Feuerstein A (April 5, 2022). "Troubles mount for Cassava Sciences, as patient enrollment lags for Alzheimer's drug studies". Stat. Retrieved April 30, 2022.
- ^ Cassava Sciences, Inc. (August 3, 2022). "Cassava Sciences Reports Second Quarter Financial Results for 2022, Mid-year Corporate Update and Interim Analysis of Open-label Study". Archived from the original on August 9, 2022. Retrieved August 5, 2022.
- PMID 32075941.
- ^ Taylor M, Spector M (July 27, 2022). "Exclusive: Cassava Sciences faces U.S. criminal probe tied to Alzheimer's drug, sources say". Reuters. Archived from the original on July 30, 2022. Retrieved July 31, 2022.
- S2CID 250953611. Archived from the originalon August 28, 2022.
- PMID 34921050.
- S2CID 247586479.
- PMID 35353861.
- PMID 35353864.
- ProQuest 2876611078.
- ^ Mandavilli A (October 28, 2023). "CUNY Halts Investigation of Alzheimer's Researcher". The New York Times. Retrieved October 29, 2023.
External links
- CUNY investigation report
- Crespi S (July 2022). "Possible fabrications in Alzheimer's research, and bad news for life on Enceladus" (Podcast). .