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核 HIF1A 表达在散发性而非家族性男性乳腺癌中具有很强的预后价值。

Nuclear HIF1A expression is strongly prognostic in sporadic but not familial male breast cancer.

机构信息

1] Department of Pathology, Peter MacCallum Cancer Center, Melbourne, Australia [2] Department of Pathology and the Sir Peter MacCallum Department of Oncology, University of Melbourne, Melbourne, Australia.

Department of Oncology, Clinical Sciences and CREATE Health Strategic Center for Translational Cancer Research, Lund University, Lund, Sweden.

出版信息

Mod Pathol. 2014 Sep;27(9):1223-30. doi: 10.1038/modpathol.2013.231. Epub 2014 Jan 24.

Abstract

Male breast cancer is poorly understood with a large proportion arising in the familial context particularly with the BRCA2 germline mutation. As phenotypic and genotypic differences between sporadic and familial male breast cancers have been noted, we investigated the importance of a hypoxic drive in these cancers as this pathway has been shown to be of importance in familial female breast cancer. Expression of two major hypoxia-induced proteins, the hypoxia-inducible factor-1α (HIF1A) and the carbonic anhydrase IX (CA9), examined within a large cohort including 61 familial (3 BRCA1, 28 BRCA2, 30 BRCAX) and 225 sporadic male breast cancers showed that 31% of all male breast cancers expressed either HIF1A (25%) and/or CA9 (8%) in the combined cohort. Expression of HIF1A correlated with an increased incidence of a second-major malignancy (P=0.04), histological tumor type (P=0.005) and basal phenotype (P=0.02). Expression of CA9 correlated with age (P=0.004) in sporadic cases and an increased tumor size (P=0.003). Expression of HIF1A was prognostic for disease-specific survival in sporadic male breast cancers (HR: 3.8, 95% CI: 1.5-9.8, P=0.006) but not within familial male breast cancer, whereas CA9 was only prognostic in familial male breast cancers (HR: 358.0, 95% CI: 9.3-13781.7, P=0.002) and not in sporadic male breast cancer. This study found that hypoxic drive is less prevalent in male breast cancer compared with female breast cancer, possibly due to a different breast microenvironment. The prognostic impact of HIF1A is greatest in sporadic male breast cancers with an alternate dominant mechanism for the oncogenic drivers suggested in high risk familial male breast cancers.

摘要

男性乳腺癌的研究还不够深入,很大一部分发生在家族环境中,特别是与 BRCA2 种系突变有关。由于已经注意到散发性和家族性男性乳腺癌之间存在表型和基因型差异,我们研究了缺氧驱动在这些癌症中的重要性,因为该途径在家族性女性乳腺癌中具有重要意义。在包括 61 例家族性(3 例 BRCA1、28 例 BRCA2、30 例 BRCAX)和 225 例散发性男性乳腺癌在内的大队列中,检测了两种主要缺氧诱导蛋白(缺氧诱导因子-1α(HIF1A)和碳酸酐酶 IX(CA9)的表达情况,结果显示,在联合队列中,所有男性乳腺癌中有 31%(25%为 HIF1A 和/或 8%为 CA9)表达这两种蛋白。HIF1A 的表达与第二大恶性肿瘤的发生率增加相关(P=0.04),与组织学肿瘤类型(P=0.005)和基底表型(P=0.02)相关。CA9 的表达与散发性病例的年龄相关(P=0.004),与肿瘤大小增加相关(P=0.003)。HIF1A 的表达对散发性男性乳腺癌的疾病特异性生存具有预后意义(HR:3.8,95%CI:1.5-9.8,P=0.006),但在家族性男性乳腺癌中无此意义,而 CA9 仅在家族性男性乳腺癌中具有预后意义(HR:358.0,95%CI:9.3-13781.7,P=0.002),而在散发性男性乳腺癌中无此意义。本研究发现,与女性乳腺癌相比,男性乳腺癌中的缺氧驱动作用较少,这可能是由于不同的乳腺微环境所致。HIF1A 的预后影响在散发性男性乳腺癌中最大,提示高危家族性男性乳腺癌中有替代的致癌驱动因素。

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