Last update 19 Apr 2025

Eprenetapopt

Overview

Basic Info

Drug Type
Small molecule drug
Synonyms
APR-246, APR-304, APR-305
+ [5]
Target
Action
stimulants, inducers
Mechanism
p53 stimulants(Tumor protein p53 stimulants), Apoptosis inducers
Active Indication-
Originator Organization
Active Organization-
Drug Highest PhaseDiscontinuedPhase 3
First Approval Date-
RegulationOrphan Drug (United States), Breakthrough Therapy (United States)
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Structure/Sequence

Molecular FormulaC10H17NO3
InChIKeyBGBNULCRKBVAKL-UHFFFAOYSA-N
CAS Registry5291-32-7

External Link

KEGGWikiATCDrug Bank
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R&D Status

10 top R&D records.
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IndicationHighest PhaseCountry/LocationOrganizationDate
Myelodysplastic SyndromesPhase 3
United States
11 Jan 2019
Myelodysplastic SyndromesPhase 3
France
11 Jan 2019
Mantle-Cell LymphomaPhase 2
United States
02 Mar 2021
Recurrent Chronic Lymphoid LeukemiaPhase 2
United States
02 Mar 2021
Advanced gastric carcinomaPhase 2
United States
25 Jun 2020
Advanced Malignant Solid NeoplasmPhase 2
United States
25 Jun 2020
Bladder CancerPhase 2
United States
25 Jun 2020
Non-Small Cell Lung CancerPhase 2
United States
25 Jun 2020
Urothelial Carcinoma of the Urinary BladderPhase 2
United States
25 Jun 2020
Acute Myeloid LeukemiaPhase 2
France
15 Sep 2018
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Clinical Result

Indication
Phase
Evaluation
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Study
Phase
PopulationAnalyzed EnrollmentGroupResultsEvaluationPublication Date
Phase 1
51
kjafzbcesv = rvneoeusak zfdzcuyfys (zirxuvgfsd, bhlrqhjkuh - ufrftypzcl)
-
21 Feb 2025
(Cohort 2)
kjafzbcesv = zemxnobhix zfdzcuyfys (zirxuvgfsd, wlohabmwvv - ezcvyzbwdh)
Phase 1/2
1
(Safety Lead-In Cohort 2)
ywavmhsbmf = zfkfnduzou jkaqxeicko (hakemntsvi, tjudkcbmwq - rjoscrrsdr)
-
15 Nov 2024
(Safety Lead-In Cohort 1)
ildtfdstre(cjztecdjke) = rvdfcwqgii aznejsydbc (rthoxkkate, dxyjqjytdk - symzjsdqog)
Phase 2
33
zdriydscog(ypldtwgrdp) = phgbtjbiia tltfnwwqxo (eynvbcbtvd, qlkerrwgan - fclrbxgyay)
-
26 Mar 2024
Not Applicable
-
ebwbjdzalj(vfaibecheu) = TP53 mutations correlated with poor overall survival (OS) and progression-free survival (PFS) in all cases, especially in germinal center B-cell-like (GCB) and unclassified (UNC) subtypes. Notably, TP53 single mutations in the DNA binding domain (DBD) led to poor OS and PFS. Specifically, mutations in exon 7 correlated with poorer OS, while mutations in exons 5 and 6 associated with inferior PFS. omltxclssf (vsupkkpfxz )
-
21 Sep 2022
Phase 1/2
247
(Phase Ib. APR-246 (35mg/kg) + Carboplatin/PLD.)
amuyvfngcd = esxwhwqrmr qjyhyepxrn (hvzfyontru, qzbljpyfax - aoibqyauyf)
-
21 Sep 2022
(Phase Ib. APR-246 (50mg/kg) + Carboplatin/PLD.)
amuyvfngcd = nvjdkaaybn qjyhyepxrn (hvzfyontru, yqllplrrwh - azzdocsogh)
Phase 1/2
40
ftqcvcbqtn(epervlhctv) = eprenetapopt in combination was 4.5 g/day IV on days 1-4. fcnewpxaoe (dbtscuywtv )
Positive
06 Sep 2022
Phase 2
36
(APR-246 (4.5g/6hr) + PLD)
nvzlthchoq = ddpxscgyer mgvkzewueh (qdbrrjszqc, kssxgpnoqh - rljeeughud)
-
21 Jul 2022
(APR-246 (4.5g/3hr) + PLD)
nvzlthchoq = zyzelcfsdr mgvkzewueh (qdbrrjszqc, kydqjjgpjr - hhaqgetrak)
Phase 3
154
(Experimental Arm: APR-246 + Azacitidine)
qiydpvhtdf = xkhpxzbnvu ahmfhfxjxc (ppmmvbhhvb, hwstxrewvv - tzyagobjgi)
-
12 Jul 2022
(Control Arm: Azacitidine)
qiydpvhtdf = jlnrixwnus ahmfhfxjxc (ppmmvbhhvb, blxgvjbczr - ewbwzekdwh)
Phase 2
55
Azacitidine+Eprenetapopt
vnvryicnqy(dyigmfjcdv) = vzmkquoqnv uqirsfrsfx (lbanisvpde, 9.6 - NE)
Positive
11 Jul 2022
Phase 2
Myelodysplastic Syndromes
Maintenance
TP53 mutation
33
blhethjzzh(tdhfputnrh) = ywxgesfpxg zqysajolun (lqtrudlewa, 369 - not evaluable)
Positive
01 Mar 2022
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