Mote Patricia A, Leary Jennifer A, Avery Kelly A, Sandelin Kerstin, Chenevix-Trench Georgia, Kirk Judy A, Clarke Christine L
Westmead Institute for Cancer Research, University of Sydney at Westmead Millennium Institute, Westmead Hospital, Westmead, Australia.
Genes Chromosomes Cancer. 2004 Mar;39(3):236-48. doi: 10.1002/gcc.10321.
The breast cancer susceptibility genes BRCA1 and BRCA2 are responsible for a large proportion of familial breast and ovarian cancer, yet little is known of how disruptions in the functions of the proteins these genes encode increased cancer risk preferentially in hormone-dependent tissue. There is no information on whether a germ-line mutation in BRCA1 or BRCA2 causes disruptions in hormone-signaling pathways in the normal breast. In this study markers of hormone responsiveness were measured in prophylactically removed normal breast tissue (n = 31) in women bearing a germ-line pathogenic mutation in one of the BRCA genes. The estrogen receptor (ER) and proteins associated with ER action in hormone-sensitive tissues, namely, PS2 and the progesterone receptor (PR), were detected immunohistochemically. ER expression was not different in BRCA mutation carriers than in noncarriers, but there was a reduction in PS2 expression. PR expression was also reduced, and there was a striking lack of expression of the PRB isoform, which resulted in cases with PRA-only expression in BRCA1 and BRCA2 mutation carriers. The alterations in PS2 and PR expression were similar in the BRCA1 and BRCA2 carriers, demonstrating that although these proteins are structurally and functionally distinct, there is overlap in their interaction with hormone-signaling pathways. This study provides evidence for altered cell function arising from loss of function of one BRCA allele in the normal breast, leading to PS2 loss, preferential PRB loss, and expression of PRA alone. In breast cancer development, PRA overexpression becomes evident in premalignant lesions and is associated with features of poor prognosis in invasive disease and altered cell function in vitro. The results of this study suggest that heterozygosity for a germ-line mutation in BRCA1 or BRCA2 results in development of PRA predominance. This is likely to lead to changes in progesterone signaling in hormone-dependent tissues, which may be a factor in the increased risk of cancer in these tissues in women with germ-line BRCA1 or BRCA2 mutations.
乳腺癌易感基因BRCA1和BRCA2与大部分家族性乳腺癌和卵巢癌有关,但对于这些基因所编码蛋白质功能的破坏如何优先增加激素依赖组织中的癌症风险,人们知之甚少。目前尚无关于BRCA1或BRCA2种系突变是否会导致正常乳腺中激素信号通路紊乱的信息。在本研究中,对携带BRCA基因之一种系致病突变的女性预防性切除的正常乳腺组织(n = 31)中的激素反应性标志物进行了检测。通过免疫组织化学检测雌激素受体(ER)以及与ER在激素敏感组织中的作用相关的蛋白质,即PS2和孕激素受体(PR)。BRCA突变携带者的ER表达与非携带者并无差异,但PS2表达有所降低。PR表达也降低,且PRB亚型明显缺乏表达,这导致BRCA1和BRCA2突变携带者中仅出现PRA表达的情况。BRCA1和BRCA2携带者中PS2和PR表达的改变相似,这表明尽管这些蛋白质在结构和功能上有所不同,但它们与激素信号通路的相互作用存在重叠。本研究提供了证据,表明正常乳腺中一个BRCA等位基因功能丧失会导致细胞功能改变,进而导致PS2缺失、PRB优先缺失以及仅PRA表达。在乳腺癌发展过程中,PRA过表达在癌前病变中变得明显,并且与侵袭性疾病的不良预后特征以及体外细胞功能改变有关。本研究结果表明,BRCA1或BRCA2种系突变的杂合性会导致PRA优势的形成。这可能会导致激素依赖组织中孕激素信号的变化,这可能是携带BRCA1或BRCA2种系突变的女性这些组织中癌症风险增加的一个因素。
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