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褐家鼠乳腺癌易感性1b(Mcs1b)指定变体的鉴定与功能分析。

Identification and functional analysis of Rattus norvegicus Mammary carcinoma susceptibility 1b (Mcs1b) nominated variants.

作者信息

Sanders Jennifer, Kalbfleisch Theodore S, Le Sasha, Xu Xin, Cummins Timothy D, Powell David W, Samuelson David J

机构信息

Department of Biochemistry and Molecular Genetics, University of Louisville, Louisville, KY, USA.

Gluck Equine Research Center, University of Kentucky, Lexington, KY, USA.

出版信息

Mamm Genome. 2025 Sep 19. doi: 10.1007/s00335-025-10157-5.

Abstract

Rattus norvegicus (a.k.a. laboratory rat or Brown Rat) Mammary carcinoma susceptibility 1b (Mcs1b) is a concordant ortholog of a female breast cancer risk allele at human 5q11.2. Previously, Mcs1b was delimited to a 1.8 Mb interval of RNO2 and Map3k1 along with Mier3 were determined to be Mcs1b-nonminated genes. This conclusion was based on shared synteny with human 5q11.2 and differential gene expression between cancer susceptible and Mcs1b resistant mammary glands. In this study, targeted genome sequencing of cancer susceptible and Mcs1b resistance associated alleles was used to identify three Mcs1b-nominated quantitative trait nucleotides (QTNs) in noncoding DNA. In vitro approaches, luciferase activity and electromobility shift assays, were used to suggest these variants reside in potential gene regulatory elements. One of these variants, UL-A74-SNV-17, resulted in luciferase activities that were 2.6× higher for the susceptibility associated variant compared to the resistance associated variant. These results recapitulated Mcs1b nominated gene transcript level differences between Mcs1b genotypes in mammary epithelial cells (MECs), where Map3k1 and Mier3 were 1.5- to 2.0-fold higher for the susceptible genotype compared to the Mcs1b resistance-associated genotype. Evidence of a chromatin loop in Mcs1b that may position Mcs1b QTNs near distal genes was uncovered using chromosome confirmation capture (3C). Rat Mcs1b was also functionally characterized by determining that Mcs1b genotype had effects on the amount of luminal MECs in adult mammary glands. In conclusion, UL-A74-SNV-17 is a priority candidate Mcs1b QTN with a hypothesized mechanistic role in the differential regulation of Mcs1b nominated genes, Mier3 and Map3k1.

摘要

褐家鼠(又称实验大鼠或褐鼠)乳腺癌易感性1b(Mcs1b)是人类5q11.2处女性乳腺癌风险等位基因的同源直系基因。此前,Mcs1b被限定在RNO2的1.8 Mb区间内,并且Map3k1以及Mier3被确定为未被Mcs1b提名的基因。这一结论基于与人类5q11.2的共线性以及癌症易感和Mcs1b抗性乳腺之间的差异基因表达。在本研究中,对癌症易感和Mcs1b抗性相关等位基因进行靶向基因组测序,以在非编码DNA中鉴定出三个被Mcs1b提名的数量性状核苷酸(QTN)。采用体外方法、荧光素酶活性和电泳迁移率变动分析,提示这些变异位于潜在的基因调控元件中。其中一个变异体UL-A74-SNV-17,与抗性相关变异体相比,易感性相关变异体的荧光素酶活性高出2.6倍。这些结果重现了乳腺上皮细胞(MECs)中Mcs1b基因型之间Mcs1b提名基因转录水平的差异,其中与Mcs1b抗性相关基因型相比,易感基因型的Map3k1和Mier3高1.5至2.0倍。使用染色体构象捕获(3C)发现了Mcs1b中一个染色质环,它可能将Mcs1b QTN定位在远端基因附近。通过确定Mcs1b基因型对成年乳腺中管腔MECs数量有影响,对大鼠Mcs1b进行了功能表征。总之,UL-A74-SNV-17是一个优先候选的Mcs1b QTN,在Mcs1b提名基因Mier3和Map3k1的差异调控中具有假设的机制作用。

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