A small molecular compound CC1007 induces cross-lineage differentiation by inhibiting HDAC7 expression and HDAC7/MEF2C interaction in BCR-ABL1(−) pre-B-ALL

Histone deacetylase 7 (HDAC7), a member of class IIa HDACs, has been described to be an important regulator for B cell development and has a potential role in B cell acute lymphoblastic leukemia (B-ALL). CC1007, a BML-210 analog, is designed to indirectly inhibit class IIa HDACs by binding to myocyt...

Descripción completa

Detalles Bibliográficos
Autores principales: Wang, Zhihua, Zhang, Yang, Zhu, Shicong, Peng, Hongling, Chen, Yongheng, Cheng, Zhao, Liu, Sufang, Luo, Yunya, Li, Ruijuan, Deng, Mingyang, Xu, Yunxiao, Hu, Guoyu, Chen, Lin, Zhang, Guangsen
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2020
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7483467/
https://www.ncbi.nlm.nih.gov/pubmed/32913188
http://dx.doi.org/10.1038/s41419-020-02949-1
_version_ 1783580922360102912
author Wang, Zhihua
Zhang, Yang
Zhu, Shicong
Peng, Hongling
Chen, Yongheng
Cheng, Zhao
Liu, Sufang
Luo, Yunya
Li, Ruijuan
Deng, Mingyang
Xu, Yunxiao
Hu, Guoyu
Chen, Lin
Zhang, Guangsen
author_facet Wang, Zhihua
Zhang, Yang
Zhu, Shicong
Peng, Hongling
Chen, Yongheng
Cheng, Zhao
Liu, Sufang
Luo, Yunya
Li, Ruijuan
Deng, Mingyang
Xu, Yunxiao
Hu, Guoyu
Chen, Lin
Zhang, Guangsen
author_sort Wang, Zhihua
collection PubMed
description Histone deacetylase 7 (HDAC7), a member of class IIa HDACs, has been described to be an important regulator for B cell development and has a potential role in B cell acute lymphoblastic leukemia (B-ALL). CC1007, a BML-210 analog, is designed to indirectly inhibit class IIa HDACs by binding to myocyte enhancer factor-2 (MEF2) and blocking the recruitment of class IIa HDACs to MEF2-targeted genes to enhance the expression of these targets. In this study, we investigated the anticancer effects of CC1007 in breakpoint cluster region-Abelson 1 fusion gene-negative (BCR-ABL1(−)) pre-B-ALL cell lines and primary patient-derived BCR-ABL1(−) pre-B-ALL cells. CC1007 had obvious antileukemic activity toward pre-B-ALL cells in vitro and in vivo; it also significantly prolonged median survival time of pre-B-ALL-bearing mice. Interestingly, low dose of CC1007 could inhibit proliferation of BCR-ABL1(−) pre-B-ALL cells in a time-dependent manner not accompanied by significant cell apoptosis, but along with cross-lineage differentiation toward monocytic lineage. From a mechanistic angle, we showed that HDAC7 was overexpressed in BCR-ABL1(−) pre-B-ALL cells compared to normal bone marrow samples, and CC1007 could reduce the binding of HDAC7 at the promoters of monocyte–macrophage-specific genes via inhibition of HDAC7 expression and HDAC7:MEF2C interaction. These data indicated that CC1007 may be a promising agent for the treatment of BCR-ABL1(−) pre-B-ALL.
format Online
Article
Text
id pubmed-7483467
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher Nature Publishing Group UK
record_format MEDLINE/PubMed
spelling pubmed-74834672020-09-21 A small molecular compound CC1007 induces cross-lineage differentiation by inhibiting HDAC7 expression and HDAC7/MEF2C interaction in BCR-ABL1(−) pre-B-ALL Wang, Zhihua Zhang, Yang Zhu, Shicong Peng, Hongling Chen, Yongheng Cheng, Zhao Liu, Sufang Luo, Yunya Li, Ruijuan Deng, Mingyang Xu, Yunxiao Hu, Guoyu Chen, Lin Zhang, Guangsen Cell Death Dis Article Histone deacetylase 7 (HDAC7), a member of class IIa HDACs, has been described to be an important regulator for B cell development and has a potential role in B cell acute lymphoblastic leukemia (B-ALL). CC1007, a BML-210 analog, is designed to indirectly inhibit class IIa HDACs by binding to myocyte enhancer factor-2 (MEF2) and blocking the recruitment of class IIa HDACs to MEF2-targeted genes to enhance the expression of these targets. In this study, we investigated the anticancer effects of CC1007 in breakpoint cluster region-Abelson 1 fusion gene-negative (BCR-ABL1(−)) pre-B-ALL cell lines and primary patient-derived BCR-ABL1(−) pre-B-ALL cells. CC1007 had obvious antileukemic activity toward pre-B-ALL cells in vitro and in vivo; it also significantly prolonged median survival time of pre-B-ALL-bearing mice. Interestingly, low dose of CC1007 could inhibit proliferation of BCR-ABL1(−) pre-B-ALL cells in a time-dependent manner not accompanied by significant cell apoptosis, but along with cross-lineage differentiation toward monocytic lineage. From a mechanistic angle, we showed that HDAC7 was overexpressed in BCR-ABL1(−) pre-B-ALL cells compared to normal bone marrow samples, and CC1007 could reduce the binding of HDAC7 at the promoters of monocyte–macrophage-specific genes via inhibition of HDAC7 expression and HDAC7:MEF2C interaction. These data indicated that CC1007 may be a promising agent for the treatment of BCR-ABL1(−) pre-B-ALL. Nature Publishing Group UK 2020-09-10 /pmc/articles/PMC7483467/ /pubmed/32913188 http://dx.doi.org/10.1038/s41419-020-02949-1 Text en © The Author(s) 2020 Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/.
spellingShingle Article
Wang, Zhihua
Zhang, Yang
Zhu, Shicong
Peng, Hongling
Chen, Yongheng
Cheng, Zhao
Liu, Sufang
Luo, Yunya
Li, Ruijuan
Deng, Mingyang
Xu, Yunxiao
Hu, Guoyu
Chen, Lin
Zhang, Guangsen
A small molecular compound CC1007 induces cross-lineage differentiation by inhibiting HDAC7 expression and HDAC7/MEF2C interaction in BCR-ABL1(−) pre-B-ALL
title A small molecular compound CC1007 induces cross-lineage differentiation by inhibiting HDAC7 expression and HDAC7/MEF2C interaction in BCR-ABL1(−) pre-B-ALL
title_full A small molecular compound CC1007 induces cross-lineage differentiation by inhibiting HDAC7 expression and HDAC7/MEF2C interaction in BCR-ABL1(−) pre-B-ALL
title_fullStr A small molecular compound CC1007 induces cross-lineage differentiation by inhibiting HDAC7 expression and HDAC7/MEF2C interaction in BCR-ABL1(−) pre-B-ALL
title_full_unstemmed A small molecular compound CC1007 induces cross-lineage differentiation by inhibiting HDAC7 expression and HDAC7/MEF2C interaction in BCR-ABL1(−) pre-B-ALL
title_short A small molecular compound CC1007 induces cross-lineage differentiation by inhibiting HDAC7 expression and HDAC7/MEF2C interaction in BCR-ABL1(−) pre-B-ALL
title_sort small molecular compound cc1007 induces cross-lineage differentiation by inhibiting hdac7 expression and hdac7/mef2c interaction in bcr-abl1(−) pre-b-all
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7483467/
https://www.ncbi.nlm.nih.gov/pubmed/32913188
http://dx.doi.org/10.1038/s41419-020-02949-1
work_keys_str_mv AT wangzhihua asmallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT zhangyang asmallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT zhushicong asmallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT penghongling asmallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT chenyongheng asmallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT chengzhao asmallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT liusufang asmallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT luoyunya asmallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT liruijuan asmallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT dengmingyang asmallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT xuyunxiao asmallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT huguoyu asmallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT chenlin asmallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT zhangguangsen asmallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT wangzhihua smallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT zhangyang smallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT zhushicong smallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT penghongling smallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT chenyongheng smallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT chengzhao smallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT liusufang smallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT luoyunya smallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT liruijuan smallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT dengmingyang smallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT xuyunxiao smallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT huguoyu smallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT chenlin smallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball
AT zhangguangsen smallmolecularcompoundcc1007inducescrosslineagedifferentiationbyinhibitinghdac7expressionandhdac7mef2cinteractioninbcrabl1preball

Ejemplares similares