Molecular mechanism of chemoresistance by miR-215 in osteosarcoma and colon cancer cells

Molecular mechanism of chemoresistance by miR-215 in osteosarcoma and colon cancer cells

<p>Abstract</p> <p>Background</p> <p>Translational control mediated by non-coding microRNAs (miRNAs) plays a key role in the mechanism of cellular resistance to anti-cancer drug treatment. Dihydrofolate reductase (DHFR) and thymidylate synthase (TYMS, TS) are two of the...

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Main Authors: Formentini Andrea, Botchkina Galina, Titmus Matthew A, Wang Yuan, Song Bo, Kornmann Marko, Ju Jingfang
Format: Article
Language:English
Published: BMC 2010-04-01
Series:Molecular Cancer
Online Access:http://www.molecular-cancer.com/content/9/1/96
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spelling doaj-b71af4364e9440eebb0baa65a0f3ec832020-11-24T21:19:54ZengBMCMolecular Cancer1476-45982010-04-01919610.1186/1476-4598-9-96Molecular mechanism of chemoresistance by miR-215 in osteosarcoma and colon cancer cellsFormentini AndreaBotchkina GalinaTitmus Matthew AWang YuanSong BoKornmann MarkoJu Jingfang<p>Abstract</p> <p>Background</p> <p>Translational control mediated by non-coding microRNAs (miRNAs) plays a key role in the mechanism of cellular resistance to anti-cancer drug treatment. Dihydrofolate reductase (DHFR) and thymidylate synthase (TYMS, TS) are two of the most important targets for antifolate- and fluoropyrimidine-based chemotherapies in the past 50 years. In this study, we investigated the roles of miR-215 in the chemoresistance to DHFR inhibitor methotrexate (MTX) and TS inhibitor Tomudex (TDX).</p> <p>Results</p> <p>The protein levels of both DHFR and TS were suppressed by miR-215 without the alteration of the target mRNA transcript levels. Interestingly, despite the down-regulation of DHFR and TS proteins, ectopic expression of miR-215 resulted in a decreased sensitivity to MTX and TDX. Paradoxically, gene-specific small-interfering RNAs (siRNAs) against DHFR or TS had the opposite effect, increasing sensitivity to MTX and TDX. Further studies revealed that over-expression of miR-215 inhibited cell proliferation and triggered cell cycle arrest at G2 phase, and that this effect was accompanied by a p53-dependent up-regulation of p21. The inhibitory effect on cell proliferation was more pronounced in cell lines containing wild-type p53, but was not seen in cells transfected with siRNAs against DHFR or TS. Moreover, denticleless protein homolog (DTL), a cell cycle-regulated nuclear and centrosome protein, was confirmed to be one of the critical targets of miR-215, and knock-down of DTL by siRNA resulted in enhanced G2-arrest, p53 and p21 induction, and reduced cell proliferation. Additionally, cells subjected to siRNA against DTL exhibited increased chemoresistance to MTX and TDX. Endogenous miR-215 was elevated about 3-fold in CD133+HI/CD44+HI colon cancer stem cells that exhibit slow proliferating rate and chemoresistance compared to control bulk CD133+/CD44+ colon cancer cells.</p> <p>Conclusions</p> <p>Taken together, our results indicate that miR-215, through the suppression of DTL expression, induces a decreased cell proliferation by causing G2-arrest, thereby leading to an increase in chemoresistance to MTX and TDX. The findings of this study suggest that miR-215 may play a significant role in the mechanism of tumor chemoresistance and it may have a unique potential as a novel biomarker candidate.</p> http://www.molecular-cancer.com/content/9/1/96
collection DOAJ
language English
format Article
sources DOAJ
author Formentini Andrea
Botchkina Galina
Titmus Matthew A
Wang Yuan
Song Bo
Kornmann Marko
Ju Jingfang
spellingShingle Formentini Andrea
Botchkina Galina
Titmus Matthew A
Wang Yuan
Song Bo
Kornmann Marko
Ju Jingfang
Molecular mechanism of chemoresistance by miR-215 in osteosarcoma and colon cancer cells
Molecular Cancer
author_facet Formentini Andrea
Botchkina Galina
Titmus Matthew A
Wang Yuan
Song Bo
Kornmann Marko
Ju Jingfang
author_sort Formentini Andrea
title Molecular mechanism of chemoresistance by miR-215 in osteosarcoma and colon cancer cells
title_short Molecular mechanism of chemoresistance by miR-215 in osteosarcoma and colon cancer cells
title_full Molecular mechanism of chemoresistance by miR-215 in osteosarcoma and colon cancer cells
title_fullStr Molecular mechanism of chemoresistance by miR-215 in osteosarcoma and colon cancer cells
title_full_unstemmed Molecular mechanism of chemoresistance by miR-215 in osteosarcoma and colon cancer cells
title_sort molecular mechanism of chemoresistance by mir-215 in osteosarcoma and colon cancer cells
publisher BMC
series Molecular Cancer
issn 1476-4598
publishDate 2010-04-01
description <p>Abstract</p> <p>Background</p> <p>Translational control mediated by non-coding microRNAs (miRNAs) plays a key role in the mechanism of cellular resistance to anti-cancer drug treatment. Dihydrofolate reductase (DHFR) and thymidylate synthase (TYMS, TS) are two of the most important targets for antifolate- and fluoropyrimidine-based chemotherapies in the past 50 years. In this study, we investigated the roles of miR-215 in the chemoresistance to DHFR inhibitor methotrexate (MTX) and TS inhibitor Tomudex (TDX).</p> <p>Results</p> <p>The protein levels of both DHFR and TS were suppressed by miR-215 without the alteration of the target mRNA transcript levels. Interestingly, despite the down-regulation of DHFR and TS proteins, ectopic expression of miR-215 resulted in a decreased sensitivity to MTX and TDX. Paradoxically, gene-specific small-interfering RNAs (siRNAs) against DHFR or TS had the opposite effect, increasing sensitivity to MTX and TDX. Further studies revealed that over-expression of miR-215 inhibited cell proliferation and triggered cell cycle arrest at G2 phase, and that this effect was accompanied by a p53-dependent up-regulation of p21. The inhibitory effect on cell proliferation was more pronounced in cell lines containing wild-type p53, but was not seen in cells transfected with siRNAs against DHFR or TS. Moreover, denticleless protein homolog (DTL), a cell cycle-regulated nuclear and centrosome protein, was confirmed to be one of the critical targets of miR-215, and knock-down of DTL by siRNA resulted in enhanced G2-arrest, p53 and p21 induction, and reduced cell proliferation. Additionally, cells subjected to siRNA against DTL exhibited increased chemoresistance to MTX and TDX. Endogenous miR-215 was elevated about 3-fold in CD133+HI/CD44+HI colon cancer stem cells that exhibit slow proliferating rate and chemoresistance compared to control bulk CD133+/CD44+ colon cancer cells.</p> <p>Conclusions</p> <p>Taken together, our results indicate that miR-215, through the suppression of DTL expression, induces a decreased cell proliferation by causing G2-arrest, thereby leading to an increase in chemoresistance to MTX and TDX. The findings of this study suggest that miR-215 may play a significant role in the mechanism of tumor chemoresistance and it may have a unique potential as a novel biomarker candidate.</p>
url http://www.molecular-cancer.com/content/9/1/96
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