Dual targeting of microtubule and topoisomerase II by α-carboline derivative YCH337 for tumor proliferation and growth inhibition

Both microtubule and topoisomerase II (Top2) are important anticancer targets and their respective inhibitors are widely used in combination for cancer therapy. However, some combinations could be mutually antagonistic and drug resistance further limits their therapeutic efficacy. Here we report YCH...

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Autores principales: Yi, Jun-Mei, Zhang, Xiao-Fei, Huan, Xia-Juan, Song, Shan-Shan, Wang, Wei, Tian, Qian-Ting, Sun, Yi-Ming, Chen, Yi, Ding, Jian, Wang, Ying-Qing, Yang, Chun-Hao, Miao, Ze-Hong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2015
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4496195/
https://www.ncbi.nlm.nih.gov/pubmed/25840421
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author Yi, Jun-Mei
Zhang, Xiao-Fei
Huan, Xia-Juan
Song, Shan-Shan
Wang, Wei
Tian, Qian-Ting
Sun, Yi-Ming
Chen, Yi
Ding, Jian
Wang, Ying-Qing
Yang, Chun-Hao
Miao, Ze-Hong
author_facet Yi, Jun-Mei
Zhang, Xiao-Fei
Huan, Xia-Juan
Song, Shan-Shan
Wang, Wei
Tian, Qian-Ting
Sun, Yi-Ming
Chen, Yi
Ding, Jian
Wang, Ying-Qing
Yang, Chun-Hao
Miao, Ze-Hong
author_sort Yi, Jun-Mei
collection PubMed
description Both microtubule and topoisomerase II (Top2) are important anticancer targets and their respective inhibitors are widely used in combination for cancer therapy. However, some combinations could be mutually antagonistic and drug resistance further limits their therapeutic efficacy. Here we report YCH337, a novel α-carboline derivative that targets both microtubule and Top2, eliciting tumor proliferation and growth inhibition and overcoming drug resistance. YCH337 inhibited microtubule polymerization by binding to the colchicine site and subsequently led to mitotic arrest. It also suppressed Top2 and caused DNA double-strand breaks. It disrupted microtubule more potently than Top2. YCH337 induced reversible mitotic arrest at low concentrations but persistent DNA damage. YCH337 caused intrinsic and extrinsic apoptosis and decreased MCL-1, cIAP1 and XIAP proteins. In this aspect, YCH337 behaved differently from the combination of vincristine and etoposide. YCH337 inhibited proliferation of tumor cells with an averaged IC(50) of 0.3 μM. It significantly suppressed the growth of HT-29 xenografts in nude mice too. Importantly, YCH337 nearly equally killed different-mechanism-mediated resistant tumor cells and corresponding parent cells. Together with the novelty of its chemical structure, YCH337 could serve as a promising lead for drug development and a prototype for a dual microtubule/Top2 targeting strategy for cancer therapy.
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spelling pubmed-44961952015-07-10 Dual targeting of microtubule and topoisomerase II by α-carboline derivative YCH337 for tumor proliferation and growth inhibition Yi, Jun-Mei Zhang, Xiao-Fei Huan, Xia-Juan Song, Shan-Shan Wang, Wei Tian, Qian-Ting Sun, Yi-Ming Chen, Yi Ding, Jian Wang, Ying-Qing Yang, Chun-Hao Miao, Ze-Hong Oncotarget Research Paper Both microtubule and topoisomerase II (Top2) are important anticancer targets and their respective inhibitors are widely used in combination for cancer therapy. However, some combinations could be mutually antagonistic and drug resistance further limits their therapeutic efficacy. Here we report YCH337, a novel α-carboline derivative that targets both microtubule and Top2, eliciting tumor proliferation and growth inhibition and overcoming drug resistance. YCH337 inhibited microtubule polymerization by binding to the colchicine site and subsequently led to mitotic arrest. It also suppressed Top2 and caused DNA double-strand breaks. It disrupted microtubule more potently than Top2. YCH337 induced reversible mitotic arrest at low concentrations but persistent DNA damage. YCH337 caused intrinsic and extrinsic apoptosis and decreased MCL-1, cIAP1 and XIAP proteins. In this aspect, YCH337 behaved differently from the combination of vincristine and etoposide. YCH337 inhibited proliferation of tumor cells with an averaged IC(50) of 0.3 μM. It significantly suppressed the growth of HT-29 xenografts in nude mice too. Importantly, YCH337 nearly equally killed different-mechanism-mediated resistant tumor cells and corresponding parent cells. Together with the novelty of its chemical structure, YCH337 could serve as a promising lead for drug development and a prototype for a dual microtubule/Top2 targeting strategy for cancer therapy. Impact Journals LLC 2015-03-27 /pmc/articles/PMC4496195/ /pubmed/25840421 Text en Copyright: © 2015 Yi et al. http://creativecommons.org/licenses/by/2.5/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Yi, Jun-Mei
Zhang, Xiao-Fei
Huan, Xia-Juan
Song, Shan-Shan
Wang, Wei
Tian, Qian-Ting
Sun, Yi-Ming
Chen, Yi
Ding, Jian
Wang, Ying-Qing
Yang, Chun-Hao
Miao, Ze-Hong
Dual targeting of microtubule and topoisomerase II by α-carboline derivative YCH337 for tumor proliferation and growth inhibition
title Dual targeting of microtubule and topoisomerase II by α-carboline derivative YCH337 for tumor proliferation and growth inhibition
title_full Dual targeting of microtubule and topoisomerase II by α-carboline derivative YCH337 for tumor proliferation and growth inhibition
title_fullStr Dual targeting of microtubule and topoisomerase II by α-carboline derivative YCH337 for tumor proliferation and growth inhibition
title_full_unstemmed Dual targeting of microtubule and topoisomerase II by α-carboline derivative YCH337 for tumor proliferation and growth inhibition
title_short Dual targeting of microtubule and topoisomerase II by α-carboline derivative YCH337 for tumor proliferation and growth inhibition
title_sort dual targeting of microtubule and topoisomerase ii by α-carboline derivative ych337 for tumor proliferation and growth inhibition
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4496195/
https://www.ncbi.nlm.nih.gov/pubmed/25840421
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