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Modification of risk for subsequent cancer after female breast cancer by a family history of breast cancer

机译:通过乳腺癌家族史改变女性乳腺癌后发生后续癌症的风险

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An increased risk of second primary cancers may depend on many reasons, including therapy for the first cancer and heritable causation. Population level data are not available exploring the risks of subsequent cancers after breast cancer considering a familial history of breast cancers. We used the nation-wide Swedish Family-Cancer Database to investigate such risks, based on 43,398 first invasive female breast cancers. Standardized incidence ratios (SIRs) were calculated for the second cancer after breast cancer using rates for first cancer as a reference. Many cancers at discordant sites were increased after breast cancer. SIRs for subsequent neoplasms in women who had a family history of breast cancer were increased for ovarian (2.0) and endometrial (1.8) cancers and for acute lymphoid leukemia (12.7) and myelofibrosis (9.4). The data suggest that the familial aggregation of breast and endometrial cancers may be explained by yet unidentified heritable causes. The remarkably high risks for second acute lymphoid leukemia and myelofibrosis, both characterized by chromosomal aberrations, in women with a family history of breast cancer may signal heritable defects in the ability to process DNA damage caused by ionizing radiation and chemotherapy.
机译:第二原发癌的风险增加可能取决于许多原因,包括对第一原癌的治疗和遗传原因。考虑到乳腺癌的家族史,无法获得人口水平的数据来探讨乳腺癌后发生后续癌症的风险。我们使用了全国范围内的瑞典家庭癌症数据库,根据43398例首次侵入性女性乳腺癌调查了此类风险。使用第一个癌症的发生率作为参考,计算乳腺癌后第二个癌症的标准化发生率(SIR)。乳腺癌后,不协调部位的许多癌症增加。对于患有乳腺癌家族史的女性,其后续肿瘤的SIR对于卵巢癌(2.0)和子宫内膜癌(1.8)以及急性淋巴白血病(12.7)和骨髓纤维化(9.4)均增加。数据表明,乳腺癌和子宫内膜癌的家族聚集可能由尚未确定的遗传原因解释。在患有乳腺癌家族史的女性中,以染色体畸变为特征的第二次急性淋巴白血病和骨髓纤维化的风险非常高,这可能预示着由电离辐射和化学疗法引起的DNA损伤能力的遗传缺陷。

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