Cel-mir-237 and its homologue, hsa-miR-125b, modulate the cellular response to ionizing radiation

Cel-mir-237 and its homologue, hsa-miR-125b, modulate the cellular response to ionizing radiation

© 2017 Macmillan Publishers Limited, part of Springer Nature. Elucidating the mechanisms involved in sensitizing radioresistant tumors to ionizing radiation (IR) treatments while minimizing injury to surrounding normal tissue is an important clinical goal. Due to their sequence-derived specificity a...

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Main Authors: C. Metheetrairut, B. D. Adams, S. Nallur, J. B. Weidhaas, F. J. Slack
Other Authors: Yale University
Format: Article
Published: 2018
Subjects:
Biochemistry, Genetics and Molecular Biology
Online Access:https://repository.li.mahidol.ac.th/handle/123456789/42005
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spelling th-mahidol.420052019-03-14T15:03:02Z Cel-mir-237 and its homologue, hsa-miR-125b, modulate the cellular response to ionizing radiation C. Metheetrairut B. D. Adams S. Nallur J. B. Weidhaas F. J. Slack Yale University Harvard Medical School Mahidol University David Geffen School of Medicine at UCLA Biochemistry, Genetics and Molecular Biology © 2017 Macmillan Publishers Limited, part of Springer Nature. Elucidating the mechanisms involved in sensitizing radioresistant tumors to ionizing radiation (IR) treatments while minimizing injury to surrounding normal tissue is an important clinical goal. Due to their sequence-derived specificity and properties as gene regulators in IR-affected pathways, microRNAs (miRNAs) could serve as adjuvant therapeutic agents that alter cellular sensitivity to radiation treatment. To identify radiosensitizing miRNAs, we initially utilized the Caenorhabditis elegans vulval cell model, an in vivo system developed to study IR-dependent radiosensitivity as a measure of clonogenic cell death. We tested several candidate miRNA-deletion mutants post γ-irradiation and identified cel-mir-237 as a miRNA which when deleted caused animals to be more resistant to IR, whereas cel-mir-237 overexpressing strains were IR sensitive. In addition, wild-type animals downregulated cel-mir-237 levels post IR in a time-dependent manner. We identified jun-1 (JUN transcription factor homolog) as a novel target of cel-mir-237. Specifically, jun-1 transcript levels increased in wild-type animals post γ-irradiation, and loss of cel-mir-237 also resulted in higher jun-1 expression. As expected, loss of jun-1 resulted in IR sensitivity, similar to the phenotype of cel-mir-237 overexpressors. As miR-237 is the homolog of human miR-125, we validated our findings in MCF-7 and MDA-MB-231 breast cancer cell lines, which harbor lower hsa-miR-125b levels than normal human mammary epithelial cells (HMECs). Forced expression of hsa-miR-125b in these cells resulted in radiosensitivity, as seen by reduced clonogenic survival, enhanced apoptotic activity and enhanced senescence post IR. Finally, re-expression of c-JUN in MDA-MB-231 cells promoted radioresistance and abrogated miR-125-mediated radiosensitization. Our findings suggest that overexpression of cel-mir-237 and its homolog, hsa-miR-125b, functions as sensitizers to γ-irradiation in both a nematode in vivo model and breast cancer cells, and could potentially be utilized as an adjuvant therapeutic to enhance radiation sensitivity. 2018-12-21T06:56:04Z 2019-03-14T08:03:02Z 2018-12-21T06:56:04Z 2019-03-14T08:03:02Z 2017-01-26 Article Oncogene. Vol.36, No.4 (2017), 512-524 10.1038/onc.2016.222 14765594 09509232 2-s2.0-84975217322 https://repository.li.mahidol.ac.th/handle/123456789/42005 Mahidol University SCOPUS https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=84975217322&origin=inward
institution Mahidol University
building Mahidol University Library
continent Asia
country Thailand
Thailand
content_provider Mahidol University Library
collection Mahidol University Institutional Repository
topic Biochemistry, Genetics and Molecular Biology
spellingShingle Biochemistry, Genetics and Molecular Biology
C. Metheetrairut
B. D. Adams
S. Nallur
J. B. Weidhaas
F. J. Slack
Cel-mir-237 and its homologue, hsa-miR-125b, modulate the cellular response to ionizing radiation
description © 2017 Macmillan Publishers Limited, part of Springer Nature. Elucidating the mechanisms involved in sensitizing radioresistant tumors to ionizing radiation (IR) treatments while minimizing injury to surrounding normal tissue is an important clinical goal. Due to their sequence-derived specificity and properties as gene regulators in IR-affected pathways, microRNAs (miRNAs) could serve as adjuvant therapeutic agents that alter cellular sensitivity to radiation treatment. To identify radiosensitizing miRNAs, we initially utilized the Caenorhabditis elegans vulval cell model, an in vivo system developed to study IR-dependent radiosensitivity as a measure of clonogenic cell death. We tested several candidate miRNA-deletion mutants post γ-irradiation and identified cel-mir-237 as a miRNA which when deleted caused animals to be more resistant to IR, whereas cel-mir-237 overexpressing strains were IR sensitive. In addition, wild-type animals downregulated cel-mir-237 levels post IR in a time-dependent manner. We identified jun-1 (JUN transcription factor homolog) as a novel target of cel-mir-237. Specifically, jun-1 transcript levels increased in wild-type animals post γ-irradiation, and loss of cel-mir-237 also resulted in higher jun-1 expression. As expected, loss of jun-1 resulted in IR sensitivity, similar to the phenotype of cel-mir-237 overexpressors. As miR-237 is the homolog of human miR-125, we validated our findings in MCF-7 and MDA-MB-231 breast cancer cell lines, which harbor lower hsa-miR-125b levels than normal human mammary epithelial cells (HMECs). Forced expression of hsa-miR-125b in these cells resulted in radiosensitivity, as seen by reduced clonogenic survival, enhanced apoptotic activity and enhanced senescence post IR. Finally, re-expression of c-JUN in MDA-MB-231 cells promoted radioresistance and abrogated miR-125-mediated radiosensitization. Our findings suggest that overexpression of cel-mir-237 and its homolog, hsa-miR-125b, functions as sensitizers to γ-irradiation in both a nematode in vivo model and breast cancer cells, and could potentially be utilized as an adjuvant therapeutic to enhance radiation sensitivity.
author2 Yale University
author_facet Yale University
C. Metheetrairut
B. D. Adams
S. Nallur
J. B. Weidhaas
F. J. Slack
format Article
author C. Metheetrairut
B. D. Adams
S. Nallur
J. B. Weidhaas
F. J. Slack
author_sort C. Metheetrairut
title Cel-mir-237 and its homologue, hsa-miR-125b, modulate the cellular response to ionizing radiation
title_short Cel-mir-237 and its homologue, hsa-miR-125b, modulate the cellular response to ionizing radiation
title_full Cel-mir-237 and its homologue, hsa-miR-125b, modulate the cellular response to ionizing radiation
title_fullStr Cel-mir-237 and its homologue, hsa-miR-125b, modulate the cellular response to ionizing radiation
title_full_unstemmed Cel-mir-237 and its homologue, hsa-miR-125b, modulate the cellular response to ionizing radiation
title_sort cel-mir-237 and its homologue, hsa-mir-125b, modulate the cellular response to ionizing radiation
publishDate 2018
url https://repository.li.mahidol.ac.th/handle/123456789/42005
_version_ 1763493718944382976

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