MICAL2 Mediates p53 Ubiquitin Degradation through Oxidating p53 Methionine 40 and 160 and Promotes Colorectal Cancer Malignance

Molecule interacting with CasL2 (MICAL2), a microtubule-associated monooxygenase, is highly expressed in various cancers and is involved in cancer pathogenesis, but the mechanisms underlying its regulation in carcinogenesis are unclear. In this study, we aim to clarify the mechanism by which MICAL2...

Descripción completa

Detalles Bibliográficos
Autores principales: Lu, Jinping, Li, Yuejin, Wu, Yuanzhong, Zhou, Shan, Duan, Chaojun, Dong, Zigang, Kang, Tiebang, Tang, Faqing
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2018
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6276083/
https://www.ncbi.nlm.nih.gov/pubmed/30555547
http://dx.doi.org/10.7150/thno.28228
_version_ 1783377943985127424
author Lu, Jinping
Li, Yuejin
Wu, Yuanzhong
Zhou, Shan
Duan, Chaojun
Dong, Zigang
Kang, Tiebang
Tang, Faqing
author_facet Lu, Jinping
Li, Yuejin
Wu, Yuanzhong
Zhou, Shan
Duan, Chaojun
Dong, Zigang
Kang, Tiebang
Tang, Faqing
author_sort Lu, Jinping
collection PubMed
description Molecule interacting with CasL2 (MICAL2), a microtubule-associated monooxygenase, is highly expressed in various cancers and is involved in cancer pathogenesis, but the mechanisms underlying its regulation in carcinogenesis are unclear. In this study, we aim to clarify the mechanism by which MICAL2 participates in colorectal cancer (CRC) and identify novel markers for predicting prognosis of CRC patients. Methods: The value of MICAL2 in CRC prognosis was determined by immunohistochemical analysis of a CRC biopsy array. A short hairpin RNA target MICAL2 (shMICAL2) was designed to knock down MICAL2 expression and observe MICAL2's function on CRC cell growth. mRNA expression array was used to screen target molecules of MICAL2. HCT116 p53(+/+) and HCT116 p53(-/-) cells were used to confirm whether MICAL2 exerts its oncogenic effect through p53. The in vivo effect of MICAL2 on CRC growth was assessed by subcutaneously injecting MICAL2-knockout CRC cells into the dorsal flank of each mouse. Immunofluorescence was used to observe the effect of MICAL2 on p53 cellular location. Reverse-phase nano ESI-LCMS analysis was used to investigate if MICAL2 mediates p53 oxidation. Results: MICAL2 was found to be highly expressed in CRC tissues, and its expression was associated with CRC carcinogenesis and poor patient outcome. MICAL2-knockdown decreased growth and colony formation of CRC cells, which was linked with cell cycle arrest and apoptosis. MICAL2 physically interacted with p53 and retained p53 in the cytoplasm. MICAL2 shortened the half-life of p53, and ectopic MICAL2 expression decreased p53 protein stability through ubiquitin degradation. MICAL2 was also found to oxidize p53 at methionine 40 and 160, which mediated p53 ubiquitin degradation. MICAL2-promoted CRC growth in vivo was confirmed in nude mice. Conclusion: MICAL2 binds to p53, retains p53 in the cytoplasm and oxidizes it at Met 40 and 160, promotes p53 ubiquitination, and decreases p53 function. MICAL2-reduced p53 promotes CRC development.
format Online
Article
Text
id pubmed-6276083
institution National Center for Biotechnology Information
language English
publishDate 2018
publisher Ivyspring International Publisher
record_format MEDLINE/PubMed
spelling pubmed-62760832018-12-14 MICAL2 Mediates p53 Ubiquitin Degradation through Oxidating p53 Methionine 40 and 160 and Promotes Colorectal Cancer Malignance Lu, Jinping Li, Yuejin Wu, Yuanzhong Zhou, Shan Duan, Chaojun Dong, Zigang Kang, Tiebang Tang, Faqing Theranostics Research Paper Molecule interacting with CasL2 (MICAL2), a microtubule-associated monooxygenase, is highly expressed in various cancers and is involved in cancer pathogenesis, but the mechanisms underlying its regulation in carcinogenesis are unclear. In this study, we aim to clarify the mechanism by which MICAL2 participates in colorectal cancer (CRC) and identify novel markers for predicting prognosis of CRC patients. Methods: The value of MICAL2 in CRC prognosis was determined by immunohistochemical analysis of a CRC biopsy array. A short hairpin RNA target MICAL2 (shMICAL2) was designed to knock down MICAL2 expression and observe MICAL2's function on CRC cell growth. mRNA expression array was used to screen target molecules of MICAL2. HCT116 p53(+/+) and HCT116 p53(-/-) cells were used to confirm whether MICAL2 exerts its oncogenic effect through p53. The in vivo effect of MICAL2 on CRC growth was assessed by subcutaneously injecting MICAL2-knockout CRC cells into the dorsal flank of each mouse. Immunofluorescence was used to observe the effect of MICAL2 on p53 cellular location. Reverse-phase nano ESI-LCMS analysis was used to investigate if MICAL2 mediates p53 oxidation. Results: MICAL2 was found to be highly expressed in CRC tissues, and its expression was associated with CRC carcinogenesis and poor patient outcome. MICAL2-knockdown decreased growth and colony formation of CRC cells, which was linked with cell cycle arrest and apoptosis. MICAL2 physically interacted with p53 and retained p53 in the cytoplasm. MICAL2 shortened the half-life of p53, and ectopic MICAL2 expression decreased p53 protein stability through ubiquitin degradation. MICAL2 was also found to oxidize p53 at methionine 40 and 160, which mediated p53 ubiquitin degradation. MICAL2-promoted CRC growth in vivo was confirmed in nude mice. Conclusion: MICAL2 binds to p53, retains p53 in the cytoplasm and oxidizes it at Met 40 and 160, promotes p53 ubiquitination, and decreases p53 function. MICAL2-reduced p53 promotes CRC development. Ivyspring International Publisher 2018-10-22 /pmc/articles/PMC6276083/ /pubmed/30555547 http://dx.doi.org/10.7150/thno.28228 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
Lu, Jinping
Li, Yuejin
Wu, Yuanzhong
Zhou, Shan
Duan, Chaojun
Dong, Zigang
Kang, Tiebang
Tang, Faqing
MICAL2 Mediates p53 Ubiquitin Degradation through Oxidating p53 Methionine 40 and 160 and Promotes Colorectal Cancer Malignance
title MICAL2 Mediates p53 Ubiquitin Degradation through Oxidating p53 Methionine 40 and 160 and Promotes Colorectal Cancer Malignance
title_full MICAL2 Mediates p53 Ubiquitin Degradation through Oxidating p53 Methionine 40 and 160 and Promotes Colorectal Cancer Malignance
title_fullStr MICAL2 Mediates p53 Ubiquitin Degradation through Oxidating p53 Methionine 40 and 160 and Promotes Colorectal Cancer Malignance
title_full_unstemmed MICAL2 Mediates p53 Ubiquitin Degradation through Oxidating p53 Methionine 40 and 160 and Promotes Colorectal Cancer Malignance
title_short MICAL2 Mediates p53 Ubiquitin Degradation through Oxidating p53 Methionine 40 and 160 and Promotes Colorectal Cancer Malignance
title_sort mical2 mediates p53 ubiquitin degradation through oxidating p53 methionine 40 and 160 and promotes colorectal cancer malignance
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6276083/
https://www.ncbi.nlm.nih.gov/pubmed/30555547
http://dx.doi.org/10.7150/thno.28228
work_keys_str_mv AT lujinping mical2mediatesp53ubiquitindegradationthroughoxidatingp53methionine40and160andpromotescolorectalcancermalignance
AT liyuejin mical2mediatesp53ubiquitindegradationthroughoxidatingp53methionine40and160andpromotescolorectalcancermalignance
AT wuyuanzhong mical2mediatesp53ubiquitindegradationthroughoxidatingp53methionine40and160andpromotescolorectalcancermalignance
AT zhoushan mical2mediatesp53ubiquitindegradationthroughoxidatingp53methionine40and160andpromotescolorectalcancermalignance
AT duanchaojun mical2mediatesp53ubiquitindegradationthroughoxidatingp53methionine40and160andpromotescolorectalcancermalignance
AT dongzigang mical2mediatesp53ubiquitindegradationthroughoxidatingp53methionine40and160andpromotescolorectalcancermalignance
AT kangtiebang mical2mediatesp53ubiquitindegradationthroughoxidatingp53methionine40and160andpromotescolorectalcancermalignance
AT tangfaqing mical2mediatesp53ubiquitindegradationthroughoxidatingp53methionine40and160andpromotescolorectalcancermalignance

Ejemplares similares