2021
DOI: 10.1021/acs.jmedchem.1c00270
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Development of Alectinib-Based PROTACs as Novel Potent Degraders of Anaplastic Lymphoma Kinase (ALK)

Abstract: A series of novel anaplastic lymphoma kinase (ALK) degraders were designed and synthesized based on proteolysis-targeting chimera (PROTAC) technology by linking two alectinib analogs (36 and 37) with pomalidomide through linkers of different lengths and types. The most promising degrader 17 possessed a high ALK-binding affinity and potent antiproliferative activity in the ALK-dependent cell lines and did not exhibit obvious cytotoxicity in ALK fusion-negative cells. More importantly, the efficacy of compound 1… Show more

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Cited by 42 publications
(35 citation statements)
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“…19 ) also based on Alectinib. 128 The difference from Jiang group was that the E3 ligase ligand they used was pomalidomide, while Jiang group was lenalidomide. They found degrader 71 had the best ALK degradation activity, highest ALK binding affinity and best antiproliferative activity in such ALK-dependent cell lines as H3122 cells and Karpas 299 cells, whose DC 50 were 27.4 nM, 116.5 nM and IC 50 were 62 nM, 42 nM.…”
Section: Protacs Targeting Cancer-related Targetsmentioning
confidence: 99%
“…19 ) also based on Alectinib. 128 The difference from Jiang group was that the E3 ligase ligand they used was pomalidomide, while Jiang group was lenalidomide. They found degrader 71 had the best ALK degradation activity, highest ALK binding affinity and best antiproliferative activity in such ALK-dependent cell lines as H3122 cells and Karpas 299 cells, whose DC 50 were 27.4 nM, 116.5 nM and IC 50 were 62 nM, 42 nM.…”
Section: Protacs Targeting Cancer-related Targetsmentioning
confidence: 99%
“…57 In addition, S N Ar with 6 is a common strategy to synthesise void POI ligand–E3 ligand dimers. 58–60 For instance, chemists from Nathanael Gray's group reacted the piperazine handle of the cyclin-dependent kinases (CDK) 4/6 inhibitor palbociclib with 4-fluorothalidomide (Example 9). However, this reaction sequence is unfavourable if one aims to generate an in-house E3 ligand–linker library for initial PROTAC screening campaigns.…”
Section: Crbn Ligandsmentioning
confidence: 99%
“…PROTAC directly targets and degrades proteins and is unaffected by ALK point mutations; this explains how PROTAC designed with alectinib/brigatinib can degrade the ALK G1202R mutant, which is resistant to the drugs themselves. PROTAC designed with alectinib as the ligand was more effective than alectinib in ALK+ ALCL patients and enhanced ALK degradation ( 115 117 ). ARV-110, the first PROTAC drug targeting the androgen receptor, has been used in patients with metastatic debulking-resistant prostate cancer with promising results ( 118 ).…”
Section: Strategies To Overcome Alk Tki Resistancementioning
confidence: 99%