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Merck

Inhibiting p53 Acetylation Reduces Cancer Chemotoxicity.

Cancer research (2017-06-29)
Shunsheng Zheng, Xin Yu Koh, Hui Chin Goh, Siti Aishah B Rahmat, Le-Ann Hwang, David P Lane
摘要

Chemotoxicity due to unwanted p53 activation in the bone marrow remains an unmet clinical challenge. Doxorubicin, a first-line chemotherapy drug, often causes myelosuppression in patients, thus limiting its effectiveness. In this study, we discovered that C646, a reversible p300 inhibitor, downregulates p53 transcription and selectively protects noncancerous cells from p53-dependent apoptosis. C646 treatment blocked acetylation of specific lysine residues that regulate p53 activity. Exploitation of differential p53 genetic backgrounds between human hematopoietic and colorectal cancer cells improved the therapeutic index of doxorubicin with C646 cotreatment. C646 administration in mice afflicted with p53-mutant tumors protected them from doxorubicin-induced neutropenia and anemia while retaining antitumor efficacy. We deduce that temporary and reversible inhibition of p53 acetylation in cancer subjects, especially those with p53-mutant tumors, may protect them from severe chemotoxicity while allowing treatment regimens to effectively proceed. Cancer Res; 77(16); 4342-54. ©2017 AACR.

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Sigma-Aldrich
抗-β-肌动蛋白−过氧化物酶抗体,小鼠单克隆 小鼠抗, clone AC-15, purified from hybridoma cell culture
Sigma-Aldrich
(S)-(+)-喜树碱, ≥90% (HPLC), powder
Sigma-Aldrich
2-苯基吲哚, technical grade, 95%
Sigma-Aldrich
乙酰化p53(Lys320)抗体, from rabbit, purified by affinity chromatography