SCA Therapeutics Development

Last updated on November 3, 2024

This page lists some therapeutics (mostly drugs; sorted by company name) being developed for spinocerebellar ataxia (SCA)—leaning towards SCA3, which I have—and Huntington’s disease (HD). There are reasonably no claims to stop, prevent, or cure the diseases.

The National Ataxia Foundation’s take on this.

Why include Huntington’s disease?

The SCA that I have (SCA3) and HD both are polyglutamine diseases, and gene-based therapeutics for one can likely be stepping stones for the other. Though HD and SCA3 are genetically similar, the mutant toxic huntingtin protein affects the whole brain and especially the basal ganglia, whereas mutant toxic ataxin 3 primarily affects the cerebellum. In other words, the neurons that deteriorate and die are in the brain but different parts of the brain, so there could be different drug delivery mechanics. HD prevalence is higher than SCA prevalence and a worse disease, so it’s usually given higher priority. Polyglutamine-SCA therapeutics are quite literally waiting for success of some kind first with HD before attempts are made to ride on its coattails.

How different is Friedreich’s ataxia?

Friedreich’s ataxia (FA) and SCA(3) are different diseases. Will there be leverage between therapeutics, like I assume there will be for polyglutamine diseases such as HD and SCA(3)?

• Since FA is autosomal recessive, the inheritance pattern is completely different from SCA. Also, FA comes on earlier and stronger and is fatal to children.
• The prevalence of FA is about the same as all the SCAs combined. There are at least a dozen pharmaceutical companies working on therapies for FA but only a small handful working on SCA.
• The genetic defect that causes SCA(3) is in an exon and causes a ubiquitous protein to become toxic primarily to the cerebellum. The genetic defect that causes FA is in an intron and causes a protein to not be created that is needed in various areas of the body, such as the brain and muscles (including the heart).
• Because of the exon/intron situation, SCA(3) can be modified at the DNA or RNA level, but FA can be modified at the DNA level but not the RNA level.
• Therapeutic approaches to each disease that don’t involve gene therapy tend to be entirely unrelated.
• CRISPR with viral delivery might be able to repair billions of mature neurons with either kind of defect eventually. If this happens, then FA will probably be addressed before SCA(3) by a few years because of its higher prevalence and overall “worseness.”

Continuing…

See here for a general description of trial phases.

From this PDF, the overall probability of success was 63% in phase 1 trials, 31% in phase 2 trials, 58% in phase 3 trials and 85% during the regulatory review process, for an overall success rate (phase 1 to approval) of 9.6% (63% × 31% × 58% × 85% = 9.6%). The success rate of going from phase 2 to approval was 15% (three make it for seventeen that don’t).

The following lists are alphabetical.

Specific to SCA or SCA3

Biogen

• www.biogen.com
• Pipeline [find with Google]
• Drug for SCA3
  • Code name: BIIB132 (those are ‘i’s; BIIB is the Nasdaq stock symbol for Biogen).
  • Added to pipeline in 2022 [find with Google].
  • Technology: ASO.
  • Administration: intrathecal.
  • NCT05160558 (phase 1)
    • 2022-02-02 through 2025-12-12 (about four years).
    • At UCSF.

Blade Therapeutics (maybe)

• www.blademed.com; founded in 2015; in San Francisco, CA, U.S.A.
• Pipeline [find with Google]
• Drug for SCA3? This might be untrue, as they seem to still be finding their way (2021-10-24).
  • Code name: BLD-2736 [find with Google]
  • As of 2021-10-07, this is the only mention of SCA3 on the website.
  • 2021-10-24: this is where I first heard about this.

Lacerta Therapeutics (maybe)

• lacertatx.com (on Twitter); founded in 2017; in Florida, U.S.A.
• Approx. pipeline (interactive page only as of late-2020) [find with Google]
• Founded in 2017 in Florida, U.S., there isn’t much to go on now in late-2020.
• Viral (AAV-based) gene silencing for SCA3. No real details as of late-2020.
  • Term to know: capsid (protein shell of a virus).
• Find with Google: Lacerta and ataxia

Vico Therapeutics

• vicotx.com
• Pipeline [find with Google]
• Founded in Q4 2019 in The Netherlands, they have essentially no info on their website in early-2021.
• Drug for SCA, possibly for polyglutamine SCA
  • Code name: VO659
  • Technology: ASO, slated to address HD, multiple SCAs, and Rett syndrome.
  • 2020-07-29. First news release, which reveals a tiny bit.
  • 2020-08-05. Technology licensed from OHSU (Oregon Health & Science University).
  • 2021-02-10. European Commission (EC) grants orphan-drug designation for VO659.
  • 2021-06-29. Orphan-drug designation (for SCA) in the U.S.
• Find with Google: Vico and ataxia

Specific to SCA but a don’t-care

Biohaven, Ltd.

• www.biohaven.com
• Pipeline [find with Google]
• Drug for SCA
  • Code name: BHV-4157 (link goes to my own assessment).
  • Generic name: troriluzole (renamed from trigriluzole; link goes to my own assessment).
  • Administration: by mouth.
  • Mechanism of action: reduces glutamate in the brain.
    • [find with Google]
  • General goal: slow cerebellar degeneration by reducing needless excitement of neurons. No claims are made about stopping or preventing the disease.
  • Stage in 2017-November: phase 2 failed in the U.S. Yet it persists.
  • Skepticism alert.
    • The same drug is being tested with Alzheimer’s disease and OCD, indicating a hit-or-miss riluzole repurposing extravaganza.
    • A supposed-to-be-simple sublingual reformulation of riluzole failed to get FDA approval for ALS, and they dropped it like a hot potato.
  • 2022-05-23. SCA testing fails again.
  • 2022-05-26. And, again, “they” just can’t let it go.
  • 2023-07-27.  The end of troriluzole and SCA3.
• 2022-05-10. Biohaven bought by Pfizer. My guess: this is only for their migraine medicine (Nurtec). I expect other drugs, such as troriluzole, to be eliminated completely. They deny this, of course, but mark my words: this spells the end for troriluzole.
• Find with Google: Biohaven and ataxia

Cadent Therapeutics

• www.cadenttx.com (acquired by Novartis on 2020-12-17)
• Pipeline [find with Google]
• Drug for essential tremor (ET) with possibly unspecified (or unknown) additional benefits for SCA.
  • Code name: CAD-1883. Note: with the Novartis acquisition in 2020, this seems to have fallen off the radar.
    • Phase 2a trial for those with ET (having SCA is a disqualifier), with 2019-09 completion date. Completed 2019-09-10, but they have one year from then to publish results.
    • Phase 2 trial for those with SCA. From 2020-08 to 2021-12.
  • In early 2018, the website said that CAD-1883 was for those with SCA and ET, making it sound like you needed to have both SCA and ET to benefit. As of late 2018, they’ve decoupled the benefits to those with ET and those with SCA, but that only reveals the nebulous expectations on SCA: clearly, the drug is expected to help with ET (however acquired), but the expectations on SCA beyond ET (if any) have not been yet revealed. The prevalence of ET is so much higher than SCA, it really makes one wonder why they chose to highlight SCA at all. This is some odd chain-yanking.
    • I thought SCA was known more for intention tremor than essential tremor.
  • Good term to know: SK channel (small conductance calcium-activated potassium channel).
  • Allosteric activator: improves regulation of brain activity to help restore motor and cognitive function.
  • No claims are made about this being an SCA disease modifier; rather, this is symptom relief.
  • 2018-03-12: transition to phase 1. Also announced a partnership with Saniona.
  • Possibly related to (in competition with) Cavion and their CX-8998 product.
    • CX-8998 in phase 2 trial from 2017-06 to 2018-09.
    • Let’s step back and let the pros spin failure.
  • 2018-11-15 (URL deleted 2021-01-23): ET testing is moving forward and SCA is falling behind (see the pipeline) for the same drug; in other words, the drug is for ET, and the mystery of why SCA is highlighted at all deepens.
  • 2019-05-29: FDA orphan drug designation, but the mystery deepens even further as to what the SCA benefits are supposed to be.
  • 2020-12-17. Cadent acquired by Novartis.
  • 2021-04-08 (?). “Withdrawn.”
• Find with Google: Novartis and ataxia

Intrabio

• intrabio.com
• Pipeline [find with Google]
• Kitchen sink drug for currently 19 maladies. A repurposing extravaganza?
  • Code name: the IB1000 series.
  • Generic name: acetyl-DL-leucine, sometimes given as acetylleucine or acetyl-leucine. It’s been sold since 1957 (60+ years now) under the brand name Tanganil (vertigo treatment).
    • Not to be confused with the amino acid supplement l-leucine, which is chemically different, though possibly similar.
    • The meaning of acetyl-.
  • Tanganil has been studied and taken for years, for SCA; I have no positive expectations.
    • 2013-07-09: example SCA study.
    • 2017-07-07: a trial completed.
  • 2018-12-05: “IntraBio Receives SCA European Orphan Drug Designation”
  • 2018-12-10: “IntraBio Receives SCA Orphan Drug Designation from the FDA”

Seelos Therapeutics

• https://seelostherapeutics.com/
• Pipeline
• Therapeutic—in the form of trehalose—for SCA3 and other diseases, such as Sanfilippo syndrome a.k.a. MPS III. The fact that it “treats” FA and SCA3 proves it’s part of a hit-or-miss testing extravaganza and is symptom treatment rather than disease modification, and thus a don’t-care.
  • It’s trehalose but called SLS-005.
  • An SCA3 study in Malaysia completed on 2018-09-07 (no results published?).
  • 2019-08-14. A case for oral trehalose.
  • It’s back in a phase 1 trial with people with SCA3 in Malaysia, finishing 2021-09-30.
  • 2020-07-17. Trehalose details on SCAsource.
  • 2021-11-08. FDA Fast Track designation.
  • 2022-04-18. Clinical trial from 2022-08 to 2024-12. Phase 2.

Steminent Biotherapeutics, Inc.

• https://steminent.com
• Pipeline [find with Google].
• Stem cell therapy for SCA3 and other polyQ SCAs.
  • Drug name: Stemchymal® SB-IB02. It’s not clear to me whether this company has multiple products or if the same product is used to treat multiple issues.
  • Administration: intravenous infusion.
  • Derived from adipose (fat) tissue. See my earlier article for more on mesenchymal terminology.
  • 2015-12: U.S. FDA orphan drug designation.
  • 2018-02: Phase 2 completed in Taiwan. See NCT02540655.
    • A similar phase 2 stem cell trial, also in China.
  • 2018-07-18: Transition to phase 3 announced.
  • In partnership with ReproCELL in Japan since 2016.
    • 2020-02-28 progress.
  • 2020-10-13 licensing news.
  • 2021-02-25. A case against treating SCA with stem cells (not directly related).

Vybion, Inc

• www.vybion.com
• Pipeline [find with Google]
• Drug first for HD and then for SCA.
  • Code name: INT41
  • The same drug, INT41, is being pushed along for HD and trailed by SCA (a total of six diseases). By definition, then, I have no positive expectations.
  • Highly informative interview from 2017-02-20.
  • INT41: Gene therapy delivery of an intrabody that stabilizes the polyglutamine protein and inhibits its binding to DNA, which works to detoxify it. Delivered via an AAV.
    • Intrabody: an intracellular (inside the cell) antibody (protein that neutralizes pathogens such as bacteria and viruses).
    • AAV = adeno-associated virus
  • Stage in 2020-June: preclinical for HD; R&D for SCA3.
    • No change in three years or so.
  • 2018-12-03. Orphan drug designation by the FDA.
• Find with Google:
  • Vybion and ataxia
  • Vybion and Huntington’s disease

Defunct (or presumed defunct)

Bioblast Pharma Ltd.

• bioblastpharma.com (website gone on 2019-03-28)
• Therapeutic for SCA3
  • Code name: Cabaletta.
  • Generic name: trehalose, a disaccharide in the same family as table sugar (sucrose).
  • Administration: intravenous.
  • Described by Bioblast as a mutant protein stabilizer.
  • Described here as an autophagy enhancer.
  • General goal: slow cerebellar degeneration. No claims are made about stopping or preventing the disease.
  • 2016-November: phase 2a successful and complete in Israel (see next section). NCT02147886.
• Find with Google: Bioblast and ataxia

News:

• 2017-01-18. Bioblast published positive phase 2a trial results. SCA3 progression did not worsen in 14 people after 6 months nor in 5 people after 12 months.
• Bioblast has spent most of 2017 in financial trouble, seeking partnership or merger opportunities. The company is using JSB Partners to assist in business development.
• 2018-01-04: Trehalose has been dominating the news with how it might be proliferating some fatal superbugs.
• 2018-11-19. Merger with Enlivex. Bioblast will go away. Bioblast will try to sell off Cabaletta.
• 2019-02-19. Cabaletta sold to Seelos Therapeutics. It’s called SLS-005. See above.
• 2019-03-22. Therapeutic trehalose lives! Including for SCA3.

Dystrogen

• dystrogen.com
• Pipeline [find with Google]
• Drugs tailored for polyQ diseases like HD and SCA3
  • Code name (for SCA3 therapeutic): DYST202
    • Pre-pre-clinical in 2019.
  • Technology: based on RNAi, and it’s viral!
    • Patent applied for in 2014; received in 2018.
  • Administration: intrathecal.
  • 2019-01-xx: a highly-informative PDF, likely to be removed soon.
  • 2019-04-05: honesty abounds as they have not reached the nonsensical marketing stage yet. The hope is to significantly delay symptoms.
  • 2019-November: discontinued.
• Find with Google:
  • Dystrogen and ataxia

Ionis Pharmaceuticals, Inc.

• www.ionispharma.com
  • Changed name from Isis to Ionis in 2012.
• Pipeline [find with Google]
• This company seems to be a hotbed of ASO activity—activity related to antisense oligonucleotides.
  • My own take on the ASO situation.
• They have three preclinical therapeutics for undisclosed neurodegenerative diseases: IONIS-BIIB5_Rx, IONIS-BIIB6_Rx, and IONIS-BIIB7_Rx. Maybe SCA is in there somewhere?
• Drug for HD
  • Code name: tominersen; was IONIS-HTT_Rx or sometimes ISIS 443139
  • Rumblings of existence on Google in 2007, but more results in 2011.
  • Administration: intrathecal, monthly.
  • 2017-12-11. Positive initial phase 1,2 results; some hype. From Ionis.
    • Trial started 2015-08-31: NCT02519036.
  • 2017-12-19. A slight dose of realism: “The drug has not yet shown (nor has it had a fair chance to show) that it is an effective clinical treatment for HD.”
  • Collaborating with Roche (RG6042). Roche will manage future trials, starting with phase 3.
  • Phase 2 (open-label): NCT03342053
    • From 2017-11 through 2019-09.
  • 2018-04-24. Press release status update from Ionis. Doesn’t really say anything new.
  • 2021-03-22. Trial canceled. We don’t know why.
  • 2022-01-18. Resurrection?
    • Details  More
• SCA3
  • 2018-04-20. No real details given, but Biogen is buying its way into Ionis’s ASO drug discovery stage.
    • 2018-07-13. Many more details.
  • 2018-06-20. Signs of life between SCA3 and Ionis. (The article uses strangely inaccurate prevalence information.)
• Find with Google:
  • Ionis and ataxia
  • Ionis and Huntington’s disease

Triplet Therapeutics, Inc.

• www.triplettx.com; founded in 2019-12; in Massachusetts, U.S.A.
  • 2022-11-07: domain registration waned; company defunct.
• Drug for SCA3
  • Code name: TTX-3360
  • Approach: DDR (DNA-damage response)

uniQure nv

• www.uniqure.com; founded in 1998; in The Netherlands and Massachusetts, U.S.A.
• Pipeline [find with Google]
• Drug for SCA3
  • Code name: AMT-150 (following in the footsteps of AMT-130 for HD).
  • Technology: AAV5-based gene silencing
    • AAV5 = adeno-associated virus, serotype 5
      • AAV is the delivery mechanism, not the gene-silencing mechanism.
    • Gene-silencing technology (miQURE™) is a form of RNAi similar to miRNA (in the same family as ASOs).
    • miQURE™ lodges inside neurons and though it does not modify the genome (DNA) like CRISPR would, it permanently modifies the neurons so that any future protein they create is repaired / silenced (via RNA) by the viral payload that stays there.
  • “AMT-150 is a one-time, intrathecally administered, AAV gene therapy incorporating the company’s proprietary miQURE™ silencing technology that is designed to halt SCA3 in early manifest SCA3 patients.”
    • Note: AMT-150 (for SCA3) is administered intrathecally, whereas AMT-130 (for HD) is administered intracranially (i.e., into brain tissue via holes drilled into the skull).
  • 2019-05-07. Progress with AMT-150.
    • AMT-150 in mice.
  • 2020-10-27. Progress with AMT-150.
    • Recently initiated a safety and toxicology study to support a 2021 IND (investigational new drug) application.
  • 2022-02-25. “Deprioritized” and removed from pipeline.
• Find with Google:
  • uniQure and ataxia
  • uniQure and Huntington’s disease
• In 2018, uniQure’s claim to fame was having the most expensive pharmaceutical ever produced (also viral and long-acting). Only 31 people in the world took it, and it was discontinued.
• News for AMT-130 for HD
  • 2019-01-22. FDA clearance.
    • FDA clearance enables initiating its planned dose-escalating, randomized, and controlled phase 1/2 clinical trial to assess safety, tolerability, and efficacy.
  • 2019-01-29. A detailed article.
  • 2019-02-18.  Some success with ALS and miQURE™ (in mice).
  • 2019-04-08. FDA fast track status granted.
  • 2019-07-17. News + details.
  • 2020-06-19. Clinical progress.
  • NCT04120493: 2019-09-06 through 2026-05.
    • Phases 1 and 2.
    • 2021-04-05. Enrollment completed.
    • 2021-12-16. Clinical update: positive news.
  • 2021-04-15. Progress.
  • 2022-02-07. Open-label Phase 1b/2 clinical trial begins.
    • 2022-03-21. Completion of enrollment in the first two cohorts.
• 2021-03-29. Did gene therapy for hemophilia cause liver cancer? Independent investigation concludes No, but people are spooked.
• 2022-08-29. Side effects.

Roche

• www.roche.com
• Pipeline [find with Google]
• ASO drug for HD (with Ionis).
  • Code name: tominersen, AKA RG6042 (was IONIS-HTT_Rx)
  • 2018-08-03: granted European Medicines Agency PRIME (PRIority MEdicines) status.
  • 2019-01-28. First patients enrolled in three+-year phase 3 study.
    • NCT03761849: from 2019-01-17 to 2022-03, maybe to 2022-08.
  • 2019-05-07. Incremental progress.
  • 2021-03-22. Canceled.
• Find with Google:
  • Roche and ataxia
  • Roche and Huntington’s disease

Shionogi & Co., Inc.

• www.shionogi.com/global/en/
• Pipeline [find with Google]
• Drug for SCA
  • Code name: S-0373, or KPS-0373 at partner Kissei Pharmaceuticals (pipeline)
  • Generic name: rovatirelin.
  • Non-peptide mimetic of thyrotropin-releasing hormone (TRH)
    • Mimetic: essentially an imitation. In other words, it’s synthetic TRH.
    • TRH is now available as a pharmaceutical called protirelin.
  • TRH is thought to improve neurologic dysfunction by improving cerebral blood flow. The effect is temporary and does not stop or prevent the disease.
  • Possibly a follow-on of some sort to taltirelin, approved in Japan in 2000 as an SCA therapeutic—the first-ever SCA therapeutic. See here for drug regulation in Japan.
    • Taltirelin retrialed in Korea for 2020 June. Results unknown.
  • 2018-05-30. Phase 3 negative trial results.
    • It appears to have been in phase 3 since 2014; it was in phase 1 in 2006.
    • 2021-12-22. Resurrection?
  • 2020-01-14: a rehash of news that’s five years old? “…no significant difference between rovatirelin and placebo…”
• Find with Google:
  • Shionogi and ataxia
  • TRH and ataxia

Wave Life Sciences

• wavelifesciences.com
• Pipeline [find with Google]
• Drug for HD
  • Code names: WVE-120101 and WVE-120102.
    • Also known as SNP1 (rs362307) and SNP2 (rs362331).
    • SNP = single-nucleotide polymorphism.
  • Technology: ASO.
  • Administration: intrathecal.
  • 2016-06-21: orphan status granted.
  • Phase 1b/2a (NCT03225833 and NCT03225846)
    • Started 2017-07-17. Planned completion 2019-09.
    • “Stereopure” = this term is over my head. ASOs come in two types: stereopure and mixture-based. Stereopure has something to do with the precise 3D arrangement of atoms.
    • 2019-04-11. Small delays.
    • 2020-01-03. Less than stellar results. Trials extended to 2020-03 or later.
  • 2018-02-20: collaboration with Takeda announced, including an SCA3 therapeutic, to be named Q4 2018.
  • 2020-02-10. The future is uncertain.
  • 2021-03-30. Failed and canceled because of 0% efficacy.
• Find with Google:
  • Wave Life Sciences and ataxia
  • Wave Life Sciences and Huntington’s disease

Huntington’s disease, preclinical

Sangamo Therapeutics, Inc.

• www.sangamo.com
• Pipeline [find with Google]
• Focused on a genome editing tool called zinc finger nucleases (ZFNs), a technique in the same family as CRISPR/Cas9.
  • Zinc fingers explained.
• 2017-11-15: Sangamo in the news for MPS II, a disease with prevalence around 0.15 per 100,000 or 1/30 as prevalent as SCA.
• Find with Google:
  • Sangamo and ataxia
    • Warning: sickle-cell anemia and spinocerebellar ataxia are both abbreviated SCA.
  • Sangamo and Huntington’s disease
• 2018-09-06. Underwhelming results.

Spark Therapeutics

• sparktx.com
• Pipeline [find with Google]
• Preclinical for HD (misspelled) in documents dated 2016 (image here).
• Technology: AAV-based gene therapy (?)
  • AAV = adeno-associated virus
• Find with Google:
  • Spark and ataxia
  • Spark and Huntington’s disease
• 2019-02-25. Acquired by Roche.

Others

• AFFiRiS: pipeline
  • 2019-08-11: No longer?
• LOCANAbio: pipeline
  • SCA1 is the only SCA variation addressed
• Neurimmune: pipeline (NI-302)
• nLife Therapeutics: (NLF-HD)
  • 2018-07-09: No longer?
• Prana Biotechnology: (PBT2)
  • 2018: No longer?
  • Acquired by Alterity. I think PBT2 is gone.
• PTC Therapeutics: pipeline
• reMYND: pipeline
• Voyager Therapeutics: pipeline (VY-HTT01)