Last update 20 Jun 2024

PBT-434

Overview

Basic Info

Drug Type
Small molecule drug
Synonyms
ATH 434, ATH434, PBT 434
Mechanism
TAU inhibitors(Microtubule-associated protein tau inhibitors), α-synuclein inhibitors(Synuclein alpha inhibitors)
Inactive Indication-
Originator Organization
Active Organization
Inactive Organization-
Drug Highest PhasePhase 2
First Approval Date-
RegulationOrphan Drug (US), Orphan Drug (EU)

Structure

Molecular FormulaC12H13Cl2N3O2
InChIKeyLQNHWKHRUWSYBK-UHFFFAOYSA-N
CAS Registry1232840-87-7

R&D Status

10 top R&D records.
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IndicationHighest PhaseCountry/LocationOrganizationDate
Multiple System AtrophyPhase 2
US
01 Jul 2022
Multiple System AtrophyPhase 2
AU
01 Jul 2022
Multiple System AtrophyPhase 2
FR
01 Jul 2022
Multiple System AtrophyPhase 2
IT
01 Jul 2022
Multiple System AtrophyPhase 2
NZ
01 Jul 2022
Multiple System AtrophyPhase 2
GB
01 Jul 2022
Friedreich AtaxiaPreclinical
AU
29 Apr 2024
Parkinson DiseasePreclinical
AU
30 Jan 2023
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Clinical Result

Indication
Phase
Evaluation
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Study
Phase
PopulationAnalyzed EnrollmentGroupResultsEvaluationPublication Date
Phase 1
-
jnglcfqtjg(niznldjzaq) = yfltaedwef kegujkerdp (gsmsfmfxph, <5)
Positive
12 Sep 2020
Phase 1
Synucleinopathies
α-synuclein aggregation | markers of oxidative stress | labile iron
-
xifwsynchr(pfyvlzslgt) = All AEs were mild to moderate in severity. There were no serious AEs or AEs leading to discontinuation. The AE profile was similar for adult and ≥65 year-old volunteers. plodzkagrv (afbsferzdd )
Positive
14 Apr 2020
Not Applicable
-
-
quaqqwyald(yakoclnlpa) = PBT434 demonstrated dose dependent pharmacokinetics after single and repeated doses, with good distribution into the CNS and well-tolerated with infrequent mild to moderate adverse events jmyrchdeoq (gsxzcapjwg )
Positive
22 Sep 2019
Not Applicable
-
rgxvtivcem(eolhguxcbx) = uxdztoecbi jroqpmfstf (urixieuvzv, (33.3))
Positive
09 Apr 2019
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Regulation

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