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乳腺小叶瘤变:病变范围越广泛,后续发生浸润性癌的风险越高。

Lobular neoplasia of the breast: higher risk for subsequent invasive cancer predicted by more extensive disease.

作者信息

Page D L, Kidd T E, Dupont W D, Simpson J F, Rogers L W

机构信息

Department of Pathology, Vanderbilt University School of Medicine, Nashville, TN 37232.

出版信息

Hum Pathol. 1991 Dec;22(12):1232-9. doi: 10.1016/0046-8177(91)90105-x.

Abstract

We have stratified the cancer risk implications of lobular pattern in situ neoplasias of the breast by separating marked examples of this histologic spectrum (lobular carcinoma in situ [LCIS]) from lesser examples (atypical lobular hyperplasia). The lesser-developed examples have been shown previously to have a lower relative risk (RR) of later invasive carcinoma of the breast (IBC). Forty-eight examples of LCIS were found in 10,542 otherwise benign breast biopsies, representing an incidence of 0.5%. Nine patients were excluded from follow-up because of bilateral mastectomy within 6 months of entry biopsy, IBC within 6 months of entry biopsy, or prior IBC. Follow-up of the remaining 39 patients was complete, averaged 18 years, and revealed an RR of subsequent IBC of 6.9 (P less than .00001). Average overall follow-up for LCIS patients was 19 years; it was 25 years for those alive and free of IBC at the time of their follow-up interview. Neither family history of IBC nor postmenopausal estrogen therapy further affected risk. The absolute risk of IBC after LCIS was 17% at 15 years (adjusted for withdrawals), and the RR was 8.0 in the first 15 years of follow-up compared with the general population. An analysis based on a time-dependent hazards model found that during the first 15 years following biopsy women with LCIS had 10.8 times the risk of breast cancer compared with biopsied women of comparable age who lacked proliferative disease. Some previously published articles reporting lobular neoplasia (LN) suggest that those series with the greatest incidences of LN (whether termed LN or LCIS) have the lowest RR of subsequent breast cancer. Those series with higher incidences of LN include less well-developed histologic patterns of LN (atypical lobular hyperplasia). We conclude that our study of LN and studies performed by others support the higher risk of IBC after histologically flagrant examples (LCIS, about nine times higher) and a relatively lower but definable risk after more histologically subtle examples (atypical lobular hyperplasia, four to five times lower). This relative cancer risk is probably not constant over more than 15 years; thus, cancer risk 15 to 25 years after initial diagnosis of LCIS is uncertain.

摘要

我们通过将乳腺小叶原位肿瘤组织学谱系中的典型病例(小叶原位癌[LCIS])与非典型病例(非典型小叶增生)区分开来,对乳腺小叶原位肿瘤的癌症风险影响进行了分层。此前已表明,发育程度较低的病例发生后续乳腺浸润性癌(IBC)的相对风险(RR)较低。在10542例其他方面为良性的乳腺活检中发现了48例LCIS,发病率为0.5%。9例患者因在初次活检后6个月内行双侧乳房切除术、在初次活检后6个月内发生IBC或既往有IBC而被排除在随访之外。其余39例患者的随访完整,平均为18年,结果显示后续发生IBC的RR为6.9(P<0.00001)。LCIS患者的平均总体随访时间为19年;在随访访谈时存活且无IBC的患者为25年。IBC家族史和绝经后雌激素治疗均未进一步影响风险。LCIS后15年发生IBC的绝对风险为17%(根据失访情况进行了调整),与一般人群相比,随访的前15年RR为8.0。基于时间依赖性风险模型的分析发现,活检后的前15年中,患有LCIS的女性患乳腺癌的风险是年龄相仿但无增殖性疾病的活检女性的10.8倍。一些先前发表的报道小叶肿瘤(LN)的文章表明,那些LN发病率最高的系列(无论称为LN还是LCIS)后续患乳腺癌的RR最低。那些LN发病率较高的系列包括组织学发育较差的LN模式(非典型小叶增生)。我们得出结论,我们对LN的研究以及其他人进行的研究支持,在组织学上明显的病例(LCIS,约高9倍)后发生IBC的风险较高,而在组织学上较细微的病例(非典型小叶增生,低4至5倍)后发生IBC的风险相对较低但可确定。这种相对癌症风险在超过15年的时间里可能并非恒定不变;因此,LCIS初次诊断后15至25年的癌症风险尚不确定。

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