The cell-penetrating FOXM1 N-terminus (M1-138) demonstrates potent inhibitory effects on cancer cells by targeting FOXM1 and FOXM1-interacting factor SMAD3

Transcription factor FOXM1 is involved in stimulating cell proliferation, enhancing DNA damage repair, promoting metastasis of cancer cells, and the inhibition of FOXM1 has been shown to prevent the initiation and progression of multiple cancers and FOXM1 is considered to be an effective target for...

Descripción completa

Detalles Bibliográficos
Autores principales: Zhang, Zhenwang, Bu, Huitong, Yu, Jingwei, Chen, Yan, Pei, Chaozhu, Yu, Li, Huang, Xiaoqin, Tan, Guixiang, Tan, Yongjun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2019
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6568178/
https://www.ncbi.nlm.nih.gov/pubmed/31244930
http://dx.doi.org/10.7150/thno.32693
_version_ 1783427211485773824
author Zhang, Zhenwang
Bu, Huitong
Yu, Jingwei
Chen, Yan
Pei, Chaozhu
Yu, Li
Huang, Xiaoqin
Tan, Guixiang
Tan, Yongjun
author_facet Zhang, Zhenwang
Bu, Huitong
Yu, Jingwei
Chen, Yan
Pei, Chaozhu
Yu, Li
Huang, Xiaoqin
Tan, Guixiang
Tan, Yongjun
author_sort Zhang, Zhenwang
collection PubMed
description Transcription factor FOXM1 is involved in stimulating cell proliferation, enhancing DNA damage repair, promoting metastasis of cancer cells, and the inhibition of FOXM1 has been shown to prevent the initiation and progression of multiple cancers and FOXM1 is considered to be an effective target for tumor therapeutic drug development. The N-terminus of FOXM1 has been found to prevent transcriptional activities of FOXM1 and to mediate the interaction between FOXM1 and SMAD3. Methods: A recombinant FOXM1 N-terminal domain (1-138aa) fused with a nine arginine cell-penetrating peptide is produced with an E. coli expression system and named as M1-138. The effects of M1-138 on the proliferation, migration, and tumorigenic ability of cancer cells are analyzed in vitro with cell counting, transwell assays, and colony formation assays. Electrophoretic mobility shift assays (EMSAs) and Luciferase activity assays are used to test the DNA binding ability and transcriptional activity of transcription factors. The levels of mRNAs and proteins are measured by quantitative-PCR, Western blotting or Immunohistochemistry. The interactions among proteins are analyzed with Pull-down and Co-immunoprecipitation (Co-IP) assays. The nude mouse engrafted tumor models are used to test the inhibitory effects of M1-138 in vivo. Results: M1-138 diminishes the proliferation and migration abilities of cancer cells through binding to FOXM1 and FOXM1-interacting factor SMAD3, and consequently attenuating FOXM1 transcriptional activities from both direct and indirect FOXM1-promoter binding mechanisms and interfering with the interaction between FOXM1 and SMAD3. Treatment of M1-138 prevents tumorigenicity of cancer cells and inhibits tumor growth in nude mouse xenograft models with no obvious signs of toxicity. Conclusion: M1-138 is a promising drug candidate for the development of anti-cancer therapeutics targeting FOXM1 and SMAD3.
format Online
Article
Text
id pubmed-6568178
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher Ivyspring International Publisher
record_format MEDLINE/PubMed
spelling pubmed-65681782019-06-26 The cell-penetrating FOXM1 N-terminus (M1-138) demonstrates potent inhibitory effects on cancer cells by targeting FOXM1 and FOXM1-interacting factor SMAD3 Zhang, Zhenwang Bu, Huitong Yu, Jingwei Chen, Yan Pei, Chaozhu Yu, Li Huang, Xiaoqin Tan, Guixiang Tan, Yongjun Theranostics Research Paper Transcription factor FOXM1 is involved in stimulating cell proliferation, enhancing DNA damage repair, promoting metastasis of cancer cells, and the inhibition of FOXM1 has been shown to prevent the initiation and progression of multiple cancers and FOXM1 is considered to be an effective target for tumor therapeutic drug development. The N-terminus of FOXM1 has been found to prevent transcriptional activities of FOXM1 and to mediate the interaction between FOXM1 and SMAD3. Methods: A recombinant FOXM1 N-terminal domain (1-138aa) fused with a nine arginine cell-penetrating peptide is produced with an E. coli expression system and named as M1-138. The effects of M1-138 on the proliferation, migration, and tumorigenic ability of cancer cells are analyzed in vitro with cell counting, transwell assays, and colony formation assays. Electrophoretic mobility shift assays (EMSAs) and Luciferase activity assays are used to test the DNA binding ability and transcriptional activity of transcription factors. The levels of mRNAs and proteins are measured by quantitative-PCR, Western blotting or Immunohistochemistry. The interactions among proteins are analyzed with Pull-down and Co-immunoprecipitation (Co-IP) assays. The nude mouse engrafted tumor models are used to test the inhibitory effects of M1-138 in vivo. Results: M1-138 diminishes the proliferation and migration abilities of cancer cells through binding to FOXM1 and FOXM1-interacting factor SMAD3, and consequently attenuating FOXM1 transcriptional activities from both direct and indirect FOXM1-promoter binding mechanisms and interfering with the interaction between FOXM1 and SMAD3. Treatment of M1-138 prevents tumorigenicity of cancer cells and inhibits tumor growth in nude mouse xenograft models with no obvious signs of toxicity. Conclusion: M1-138 is a promising drug candidate for the development of anti-cancer therapeutics targeting FOXM1 and SMAD3. Ivyspring International Publisher 2019-04-25 /pmc/articles/PMC6568178/ /pubmed/31244930 http://dx.doi.org/10.7150/thno.32693 Text en © Ivyspring International Publisher This is an open access article distributed under the terms of the Creative Commons Attribution (CC BY-NC) license (https://creativecommons.org/licenses/by-nc/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Zhang, Zhenwang
Bu, Huitong
Yu, Jingwei
Chen, Yan
Pei, Chaozhu
Yu, Li
Huang, Xiaoqin
Tan, Guixiang
Tan, Yongjun
The cell-penetrating FOXM1 N-terminus (M1-138) demonstrates potent inhibitory effects on cancer cells by targeting FOXM1 and FOXM1-interacting factor SMAD3
title The cell-penetrating FOXM1 N-terminus (M1-138) demonstrates potent inhibitory effects on cancer cells by targeting FOXM1 and FOXM1-interacting factor SMAD3
title_full The cell-penetrating FOXM1 N-terminus (M1-138) demonstrates potent inhibitory effects on cancer cells by targeting FOXM1 and FOXM1-interacting factor SMAD3
title_fullStr The cell-penetrating FOXM1 N-terminus (M1-138) demonstrates potent inhibitory effects on cancer cells by targeting FOXM1 and FOXM1-interacting factor SMAD3
title_full_unstemmed The cell-penetrating FOXM1 N-terminus (M1-138) demonstrates potent inhibitory effects on cancer cells by targeting FOXM1 and FOXM1-interacting factor SMAD3
title_short The cell-penetrating FOXM1 N-terminus (M1-138) demonstrates potent inhibitory effects on cancer cells by targeting FOXM1 and FOXM1-interacting factor SMAD3
title_sort cell-penetrating foxm1 n-terminus (m1-138) demonstrates potent inhibitory effects on cancer cells by targeting foxm1 and foxm1-interacting factor smad3
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6568178/
https://www.ncbi.nlm.nih.gov/pubmed/31244930
http://dx.doi.org/10.7150/thno.32693
work_keys_str_mv AT zhangzhenwang thecellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT buhuitong thecellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT yujingwei thecellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT chenyan thecellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT peichaozhu thecellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT yuli thecellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT huangxiaoqin thecellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT tanguixiang thecellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT tanyongjun thecellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT zhangzhenwang cellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT buhuitong cellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT yujingwei cellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT chenyan cellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT peichaozhu cellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT yuli cellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT huangxiaoqin cellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT tanguixiang cellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3
AT tanyongjun cellpenetratingfoxm1nterminusm1138demonstratespotentinhibitoryeffectsoncancercellsbytargetingfoxm1andfoxm1interactingfactorsmad3

Ejemplares similares