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癌前病变中的乳腺癌风险:骨桥蛋白剪接变体预示预后。

Breast cancer risk in premalignant lesions: osteopontin splice variants indicate prognosis.

机构信息

Department of Pathology, Wroclaw Medical University, Wroclaw, Poland.

College of Medicine, University of Cincinnati Academic Health Center, Cincinnati, OH, USA.

出版信息

Br J Cancer. 2018 Nov;119(10):1259-1266. doi: 10.1038/s41416-018-0228-1. Epub 2018 Oct 24.

Abstract

BACKGROUND

Premalignant breast lesions pose variable risks for transformation, raising the question who should receive treatment to counteract the potential progression to breast cancer. Because the secreted metastasis mediator Osteopontin (OPN) is a marker for breast cancer aggressiveness, its presence in these lesions may reflect progression risk.

METHODS

By immunohistochemistry, we analyse the association of Osteopontin variant expression in healthy breasts, hyperplasias, papillomas, and carcinomas in situ from 434 women to assess a) staining for OPN exon 4 (present in OPN-a and OPN-b) or OPN-c in low-risk to high-risk lesions b) correlations between staining and progression (DCIS with invasion, invasive cancer) or survival.

RESULTS

The markers correlate with risk, and they are prognostic for ensuing invasive disease and survival. About 10% of OPN-c pathology score 0-1 (intensity), vs. 40% of score 3 experience cancer over 5 years. More than 90% of women, who progress, had pathology scores of 2-3 for OPN-c intensity at the time of initial diagnosis. When combining OPN-c and OPN exon 4 staining, all of the low intensity patients are alive after 5 years, whereas women in the high category have a close to 30% chance to die within 5 years. Of patients who succumb, close to 80% had a high combined score at the time of initial diagnosis.

CONCLUSION

The combined information of OPN splice variant immunohistochemistry can provide a foundation for very reliable prognostication and has the potential to aid decision making in the treatment of early breast lesions.

摘要

背景

癌前乳腺病变具有不同的恶变风险,这就提出了一个问题,即应该对哪些患者进行治疗以对抗乳腺癌的潜在进展。因为分泌性转移介质骨桥蛋白(OPN)是乳腺癌侵袭性的标志物,所以它在这些病变中的存在可能反映了进展风险。

方法

通过免疫组织化学分析,我们分析了 434 名女性的健康乳房、增生、乳突瘤和原位癌中 Osteopontin 变异表达的相关性,以评估 a)OPN 外显子 4(存在于 OPN-a 和 OPN-b 中)或 OPN-c 在低风险到高风险病变中的染色情况;b)染色与进展(DCIS 伴浸润、浸润性癌)或生存之间的相关性。

结果

这些标志物与风险相关,并且对随后发生的浸润性疾病和生存具有预后价值。OPN-c 病理评分 0-1(强度)的患者约为 10%,而评分 3 的患者中有 40%在 5 年内发生癌症。在初始诊断时,超过 90%进展的女性 OPN-c 强度病理评分在 2-3 之间。当结合 OPN-c 和 OPN 外显子 4 染色时,所有低强度患者在 5 年内都存活,而高分类的女性在 5 年内死亡的可能性接近 30%。在死亡的患者中,接近 80%的患者在初始诊断时的综合评分较高。

结论

OPN 剪接变体免疫组化的综合信息可以为非常可靠的预后提供基础,并有可能为早期乳腺病变的治疗决策提供帮助。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/64b5/6251032/a59a861c2a91/41416_2018_228_Fig1_HTML.jpg

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