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DOI | 10.1371/journal.pgen.1003549 |
The Gene Desert Mammary Carcinoma Susceptibility Locus Mcs1a Regulates Nr2f1 Modifying Mammary Epithelial Cell Differentiation and Proliferation | |
Smits, Bart M. G.1; Haag, Jill D.1; Rissman, Anna I.1; Sharma, Deepak1; Ann Tran1; Schoenborn, Alexi A.1; Baird, Rachael C.1; Peiffer, Dan S.1; Leinweber, David Q.1; Muelbl, Matthew J.1; Meilahn, Amanda L.1; Eichelberg, Mark R.1; Leng, Ning2; Kendziorski, Christina3; John, Manorama C.4; Powers, Patricia A.4; Alexander, Caroline M.1; Gould, Michael N.1 | |
通讯作者 | Smits, Bart M. G. |
来源期刊 | PLOS GENETICS
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ISSN | 1553-7404 |
出版年 | 2013 |
卷号 | 9期号:6 |
英文摘要 | Genome-wide association studies have revealed that many low-penetrance breast cancer susceptibility loci are located in non-protein coding genomic regions; however, few have been characterized. In a comparative genetics approach to model such loci in a rat breast cancer model, we previously identified the mammary carcinoma susceptibility locus Mcs1a. We now localize Mcs1a to a critical interval (277 Kb) within a gene desert. Mcs1a reduces mammary carcinoma multiplicity by 50% and acts in a mammary cell-autonomous manner. We developed a megadeletion mouse model, which lacks 535 Kb of sequence containing the Mcs1a ortholog. Global gene expression analysis by RNA-seq revealed that in the mouse mammary gland, the orphan nuclear receptor gene Nr2f1/Coup-tf1 is regulated by Mcs1a. In resistant Mcs1a congenic rats, as compared with susceptible congenic control rats, we found Nr2f1 transcript levels to be elevated in mammary gland, epithelial cells, and carcinoma samples. Chromatin looping over similar to 820 Kb of sequence from the Nr2f1 promoter to a strongly conserved element within the Mcs1a critical interval was identified. This element contains a 14 bp indel polymorphism that affects a human-rat-mouse conserved COUP-TF binding motif and is a functional Mcs1a candidate. In both the rat and mouse models, higher Nr2f1 transcript levels are associated with higher abundance of luminal mammary epithelial cells. In both the mouse mammary gland and a human breast cancer global gene expression data set, we found Nr2f1 transcript levels to be strongly anti-correlated to a gene cluster enriched in cell cycle-related genes. We queried 12 large publicly available human breast cancer gene expression studies and found that the median NR2F1 transcript level is consistently lower in ’triple-negative’ (ER-PR-HER2-) breast cancers as compared with ’receptor-positive’ breast cancers. Our data suggest that the non-protein coding locus Mcs1a regulates Nr2f1, which is a candidate modifier of differentiation, proliferation, and mammary cancer risk. |
类型 | Article |
语种 | 英语 |
国家 | USA |
收录类别 | SCI-E |
WOS记录号 | WOS:000321222600028 |
WOS关键词 | BREAST-CANCER SUSCEPTIBILITY ; GENOME-WIDE ASSOCIATION ; QUANTITATIVE TRAIT LOCUS ; COUP-TFI ; TRANSCRIPTION FACTOR ; ESTROGEN-RECEPTOR ; CONFER SUSCEPTIBILITY ; RESPONSE ELEMENTS ; ORPHAN RECEPTORS ; COMMON VARIANTS |
WOS类目 | Genetics & Heredity |
WOS研究方向 | Genetics & Heredity |
资源类型 | 期刊论文 |
条目标识符 | http://119.78.100.177/qdio/handle/2XILL650/179325 |
作者单位 | 1.Univ Wisconsin, McArdle Lab Canc Res, Dept Oncol, Sch Med & Publ Hlth, Madison, WI 53706 USA; 2.Univ Wisconsin, Dept Stat, Madison, WI 53706 USA; 3.Univ Wisconsin, Dept Biostat & Med Informat, Madison, WI USA; 4.Univ Wisconsin, Dept Cell & Regenerat Biol, Madison, WI USA |
推荐引用方式 GB/T 7714 | Smits, Bart M. G.,Haag, Jill D.,Rissman, Anna I.,et al. The Gene Desert Mammary Carcinoma Susceptibility Locus Mcs1a Regulates Nr2f1 Modifying Mammary Epithelial Cell Differentiation and Proliferation[J],2013,9(6). |
APA | Smits, Bart M. G..,Haag, Jill D..,Rissman, Anna I..,Sharma, Deepak.,Ann Tran.,...&Gould, Michael N..(2013).The Gene Desert Mammary Carcinoma Susceptibility Locus Mcs1a Regulates Nr2f1 Modifying Mammary Epithelial Cell Differentiation and Proliferation.PLOS GENETICS,9(6). |
MLA | Smits, Bart M. G.,et al."The Gene Desert Mammary Carcinoma Susceptibility Locus Mcs1a Regulates Nr2f1 Modifying Mammary Epithelial Cell Differentiation and Proliferation".PLOS GENETICS 9.6(2013). |
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