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Article: OPCML is a broad tumor suppressor for multiple carcinomas and lymphomas with frequently epigenetic inactivation
Title | OPCML is a broad tumor suppressor for multiple carcinomas and lymphomas with frequently epigenetic inactivation | ||||||
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Authors | |||||||
Issue Date | 2008 | ||||||
Publisher | Public Library of Science. The Journal's web site is located at http://www.plosone.org/home.action | ||||||
Citation | Plos One, 2008, v. 3 n. 8 How to Cite? | ||||||
Abstract | Background: Identification of tumor suppressor genes (TSGs) silenced by CpG methylation uncovers the molecular mechanism of tumorigenesis and potential tumor biomarkers. Loss of heterozygosity at 11q25 is common multiple tumors including nasopharyngeal carcinoma (NPC). OPCML, located at 11q25, is one of the downregulated genes we identified through digital expression subtraction. Methodology/Principal Findings: Semi-quantitative RT-PCR showed frequent OPCML silencing in NPC and other common tumors, with no homozygous deletion detected by multiplex differential DNA-PCR. Instead, promoter methylation of OPCML was frequently detected in multiple carcinoma cell lines (nasopharyngeal, esophageal, lung, gastric, colon, liver, breast, cervix, prostate), lymphoma cell lines (non-Hodgkin and Hodgkin lymphoma, nasal NK/T-cell lymphoma) and primary tumors, but not in any non-tumor cell line and seldom weakly methylated in normal epithelial tissues. Pharmacological and genetic demethylation restored OPCML expression, indicating a direct epigenetic silencing. We further found that OPCML is stress-responsive, but this response is epigenetically impaired when its promoter becomes methylated. Ecotopic expression of OPCML led to significant inhibition of both anchorage-dependent and -indendent growth of carcinoma cells with endogenous silencing. Conlusions/Significance: Thus, through functional epigenetics, we identified OPCML as a broad tumor suppressor, which is frequently inactivated by methylation in multiple malignancies. © 2008 Cui et al. | ||||||
Persistent Identifier | http://hdl.handle.net/10722/58183 | ||||||
ISSN | 2023 Impact Factor: 2.9 2023 SCImago Journal Rankings: 0.839 | ||||||
ISI Accession Number ID |
Funding Information: This project was supported by a Hong Kong RGC Central Allocation Grant (CA06/07.SC03 to QT) and a Chinese University of Hong Kong direct grant. | ||||||
References |
DC Field | Value | Language |
---|---|---|
dc.contributor.author | Cui, Y | en_HK |
dc.contributor.author | Ying, Y | en_HK |
dc.contributor.author | Van Hasselt, A | en_HK |
dc.contributor.author | Ng, KM | en_HK |
dc.contributor.author | Yu, J | en_HK |
dc.contributor.author | Zhang, Q | en_HK |
dc.contributor.author | Jin, J | en_HK |
dc.contributor.author | Liu, D | en_HK |
dc.contributor.author | Rhim, JS | en_HK |
dc.contributor.author | Rha, SY | en_HK |
dc.contributor.author | Loyo, M | en_HK |
dc.contributor.author | Chan, ATC | en_HK |
dc.contributor.author | Srivastava, G | en_HK |
dc.contributor.author | Tsao, GSW | en_HK |
dc.contributor.author | Sellar, GC | en_HK |
dc.contributor.author | Sung, JJY | en_HK |
dc.contributor.author | Sidransky, D | en_HK |
dc.contributor.author | Tao, Q | en_HK |
dc.date.accessioned | 2010-05-31T03:25:22Z | - |
dc.date.available | 2010-05-31T03:25:22Z | - |
dc.date.issued | 2008 | en_HK |
dc.identifier.citation | Plos One, 2008, v. 3 n. 8 | en_HK |
dc.identifier.issn | 1932-6203 | en_HK |
dc.identifier.uri | http://hdl.handle.net/10722/58183 | - |
dc.description.abstract | Background: Identification of tumor suppressor genes (TSGs) silenced by CpG methylation uncovers the molecular mechanism of tumorigenesis and potential tumor biomarkers. Loss of heterozygosity at 11q25 is common multiple tumors including nasopharyngeal carcinoma (NPC). OPCML, located at 11q25, is one of the downregulated genes we identified through digital expression subtraction. Methodology/Principal Findings: Semi-quantitative RT-PCR showed frequent OPCML silencing in NPC and other common tumors, with no homozygous deletion detected by multiplex differential DNA-PCR. Instead, promoter methylation of OPCML was frequently detected in multiple carcinoma cell lines (nasopharyngeal, esophageal, lung, gastric, colon, liver, breast, cervix, prostate), lymphoma cell lines (non-Hodgkin and Hodgkin lymphoma, nasal NK/T-cell lymphoma) and primary tumors, but not in any non-tumor cell line and seldom weakly methylated in normal epithelial tissues. Pharmacological and genetic demethylation restored OPCML expression, indicating a direct epigenetic silencing. We further found that OPCML is stress-responsive, but this response is epigenetically impaired when its promoter becomes methylated. Ecotopic expression of OPCML led to significant inhibition of both anchorage-dependent and -indendent growth of carcinoma cells with endogenous silencing. Conlusions/Significance: Thus, through functional epigenetics, we identified OPCML as a broad tumor suppressor, which is frequently inactivated by methylation in multiple malignancies. © 2008 Cui et al. | en_HK |
dc.language | eng | en_HK |
dc.publisher | Public Library of Science. The Journal's web site is located at http://www.plosone.org/home.action | en_HK |
dc.relation.ispartof | PLoS ONE | en_HK |
dc.rights | This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License. | - |
dc.title | OPCML is a broad tumor suppressor for multiple carcinomas and lymphomas with frequently epigenetic inactivation | en_HK |
dc.type | Article | en_HK |
dc.identifier.email | Srivastava, G:gopesh@pathology.hku.hk | en_HK |
dc.identifier.email | Tsao, GSW:gswtsao@hkucc.hku.hk | en_HK |
dc.identifier.authority | Srivastava, G=rp00365 | en_HK |
dc.identifier.authority | Tsao, GSW=rp00399 | en_HK |
dc.description.nature | published_or_final_version | - |
dc.identifier.doi | 10.1371/journal.pone.0002990 | en_HK |
dc.identifier.pmid | 18714356 | - |
dc.identifier.scopus | eid_2-s2.0-52049115449 | en_HK |
dc.identifier.hkuros | 150709 | en_HK |
dc.relation.references | http://www.scopus.com/mlt/select.url?eid=2-s2.0-52049115449&selection=ref&src=s&origin=recordpage | en_HK |
dc.identifier.volume | 3 | en_HK |
dc.identifier.issue | 8 | en_HK |
dc.identifier.isi | WOS:000264420900016 | - |
dc.publisher.place | United States | en_HK |
dc.identifier.scopusauthorid | Cui, Y=55196756600 | en_HK |
dc.identifier.scopusauthorid | Ying, Y=36889049800 | en_HK |
dc.identifier.scopusauthorid | Van Hasselt, A=6603932076 | en_HK |
dc.identifier.scopusauthorid | Ng, KM=16053249400 | en_HK |
dc.identifier.scopusauthorid | Yu, J=35351306800 | en_HK |
dc.identifier.scopusauthorid | Zhang, Q=20735917800 | en_HK |
dc.identifier.scopusauthorid | Jin, J=55166586700 | en_HK |
dc.identifier.scopusauthorid | Liu, D=8707626800 | en_HK |
dc.identifier.scopusauthorid | Rhim, JS=35389591400 | en_HK |
dc.identifier.scopusauthorid | Rha, SY=7006023235 | en_HK |
dc.identifier.scopusauthorid | Loyo, M=24068858900 | en_HK |
dc.identifier.scopusauthorid | Chan, ATC=13404833700 | en_HK |
dc.identifier.scopusauthorid | Srivastava, G=7202242238 | en_HK |
dc.identifier.scopusauthorid | Tsao, GSW=7102813116 | en_HK |
dc.identifier.scopusauthorid | Sellar, GC=6603033630 | en_HK |
dc.identifier.scopusauthorid | Sung, JJY=35405352400 | en_HK |
dc.identifier.scopusauthorid | Sidransky, D=7102109701 | en_HK |
dc.identifier.scopusauthorid | Tao, Q=7102578359 | en_HK |
dc.identifier.citeulike | 10379631 | - |
dc.identifier.issnl | 1932-6203 | - |