Novel indazole-based MKK7-TIPRL interaction inhibitors as TRAIL sensitizers = TRAIL sensitizers인 novel indazole 기반 MKK7-TIPRL 결합 저해제

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Title
Novel indazole-based MKK7-TIPRL interaction inhibitors as TRAIL sensitizers = TRAIL sensitizers인 novel indazole 기반 MKK7-TIPRL 결합 저해제
Author(s)
S Gu; M E Jung; Ji Yong Yoon; S E Yoon; Jeong Ju Lee; K Lee; G Choi; Nam-Soon Kim; M K Jeon
Bibliographic Citation
Bulletin of Korean Chemical Society, vol. 39, pp. 1125-1138
Publication Year
2018
Abstract
This work describes the process by which a metabolically unstable TRT-0002 compound exhibiting Tumor necrosis factor-related apoptosis-inducing ligand (TRAIL)-sensitizing activity for Huh7 cells at a high working concentration (40μM) is converted to more potent and metabolically improved analogues by modifying the 5-amino group and the 1-aryl moiety in the 1H-indazole skeleton. The efforts enabled us to identify 5-sulfonamido derivatives, TRT-0029 and TRT-0173 compounds, working at lower concentrations (10 and 20μM, respectively) and with improved metabolic stabilities. As reported previously by us, co-treating cultured Huh7 cells with either TRT-0029 or TRT-0173 and TRAIL resulted in TRAIL-induced apoptosis due to the inhibition of the MKK7-TOR signaling pathway regulator-like (TIPRL) interaction and subsequent phosphorylation of MKK7 and JNK. In addition, the injection of TRT-0029 or TRT-0173 compound suppressed tumor growth in combination with TRAIL in an in vivo hepatocellular carcinoma (HCC) mouse xenograft model. TRT-0029 and TRT-0173 compounds and the relevant structure-activity relationship can provide an insight into further study on optimization of potency and metabolic stability.
Keyword
ApoptosisIndazoleSensitizerTOR signaling pathway regulator-likeTumor necrosis factor-related apoptosis-inducing ligand
ISSN
0253-2964
Publisher
Wiley
DOI
http://dx.doi.org/10.1002/bkcs.11561
Type
Article
Appears in Collections:
Division of Biomedical Research > Rare Disease Research Center > 1. Journal Articles
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