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蛋白酪氨酸磷酸酶受体C(CD45)中的C77G不是卵巢癌的风险等位基因,但与侵袭性较低的疾病相关。

C77G in PTPRC (CD45) is no risk allele for ovarian cancer, but associated with less aggressive disease.

作者信息

Landskron Johannes, Kraggerud Sigrid M, Wik Elisabeth, Dørum Anne, Bjørnslett Merete, Melum Espen, Helland Øystein, Bjørge Line, Lothe Ragnhild A, Salvesen Helga B, Taskén Kjetil

机构信息

Centre for Molecular Medicine Norway, Nordic EMBL Partnership, University of Oslo and Oslo University Hospital, Oslo, Norway.

K.G. Jebsen Centre for Cancer Immunotherapy, University of Oslo, Oslo, Norway.

出版信息

PLoS One. 2017 Jul 31;12(7):e0182030. doi: 10.1371/journal.pone.0182030. eCollection 2017.

Abstract

The pan lymphocyte marker CD45 exists in various isoforms arising from alternative splicing of the exons 4, 5 and 6. While naïve T cells express CD45RA translated from an mRNA containing exon 4, exons 4-6 are spliced out to encode the shorter CD45R0 in antigen-experienced effector/memory T cells. The SNP C77G (rs17612648) is located in exon 4 and blocks the exon's differential splicing from the pre-mRNA, enforcing expression of CD45RA. Several studies have linked C77G to autoimmune diseases but lack of validation in other cohorts has left its role elusive. An incidental finding in an ovarian cancer patient cohort from West Norway (Bergen region, n = 312), suggested that the frequency of C77G was higher among ovarian cancer patients than in healthy Norwegians (n = 1,357) (3.0% vs. 1.8% allele frequency). However, this finding could not be validated in a larger patient cohort from South-East Norway (Oslo region, n = 1,198) with 1.2% allele frequency. Hence, C77G is not associated with ovarian cancer in the Norwegian population. However, its frequency was increased in patients with FIGO stage II, endometrioid histology or an age at diagnosis of 60 years or older indicating a possible association with a less aggressive cancer type.

摘要

全淋巴细胞标志物CD45存在多种由外显子4、5和6可变剪接产生的异构体。幼稚T细胞表达由包含外显子4的mRNA翻译而来的CD45RA,而在经历过抗原刺激的效应/记忆T细胞中,外显子4至6被剪接掉,以编码较短的CD45R0。单核苷酸多态性C77G(rs17612648)位于外显子4中,可阻止该外显子从前体mRNA中进行差异剪接,从而强制CD45RA的表达。多项研究已将C77G与自身免疫性疾病联系起来,但在其他队列中缺乏验证,其作用仍不明确。在挪威西部(卑尔根地区,n = 312)的一组卵巢癌患者中偶然发现,卵巢癌患者中C77G的频率高于健康挪威人(n = 1357)(等位基因频率分别为3.0%和1.8%)。然而,这一发现无法在挪威东南部(奥斯陆地区,n = 1198)的一个更大的患者队列中得到验证,该队列的等位基因频率为1.2%。因此,在挪威人群中,C77G与卵巢癌无关。然而,在国际妇产科联盟(FIGO)II期、子宫内膜样组织学或诊断年龄为60岁及以上的患者中,其频率有所增加,这表明它可能与侵袭性较小的癌症类型有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/57e6/5536273/3acdecd6a497/pone.0182030.g001.jpg

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