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腔面 B 型、HER-2 阳性和三阴性乳腺癌亚型中存在较短的端粒。

Shorter telomeres in luminal B, HER-2 and triple-negative breast cancer subtypes.

机构信息

Department of Pathology, The Johns Hopkins Hospital, Baltimore, MD 21231, USA.

出版信息

Mod Pathol. 2011 Feb;24(2):194-200. doi: 10.1038/modpathol.2010.198. Epub 2010 Nov 5.

DOI:10.1038/modpathol.2010.198
PMID:21057458
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4416483/
Abstract

Telomeres are nucleoprotein structures that protect chromosome ends from degradation and recombination. Cancers often have critically shortened telomeres, contributing to genomic instability. Many of these tumors activate telomerase to stabilize telomeric ends and achieve a capacity for unlimited replication. Telomere shortening has been reported in in situ and invasive carcinomas, including breast, and has been associated with disease recurrence after surgical resection. However, previous studies have not evaluated breast cancer subtypes. The objective of this study was to evaluate telomere lengths in different subtypes of breast cancer. Breast carcinomas (n=103) identified between 2001 and 2010 from patients seen at the Johns Hopkins Hospital were categorized into luminal A (n=18), luminal B (n=28), HER-2-positive (n=20) and triple-negative carcinomas (n=37) based on tumor characteristics. Telomere lengths were assessed directly at the single cell level by fluorescence in situ hybridization, and patient groups were compared using Fisher's exact tests. ER-negative status (P=0.022), PR-negative status (P=0.008), HER-2-positive status (P=0.023) and p53-positive status (P=0.022) were associated with shorter telomere length. A larger proportion of luminal A cancers had normal or long telomere lengths as compared with luminal B cases (P=0.002), HER-2-positive cases (P=0.011) or triple-negative cases (P=0.0003). Luminal B, HER-2-positive and triple-negative cases did not differ significantly. Telomere length was shorter in more aggressive subtypes, such as luminal B, HER-2-positive and triple-negative tumors, suggesting that tumor telomere length may have utility as a prognostic and/or risk marker for breast cancer.

摘要

端粒是一种保护染色体末端免受降解和重组的核蛋白结构。癌症通常具有临界缩短的端粒,导致基因组不稳定。许多这些肿瘤激活端粒酶以稳定端粒末端并实现无限复制的能力。端粒缩短已在原位和浸润性癌中报道,包括乳腺癌,并与手术后疾病复发相关。然而,以前的研究并未评估乳腺癌亚型。本研究的目的是评估不同乳腺癌亚型中端粒的长度。在约翰霍普金斯医院就诊的患者中,于 2001 年至 2010 年间识别的乳腺癌(n=103)根据肿瘤特征分为 luminal A(n=18)、luminal B(n=28)、HER-2 阳性(n=20)和三阴性乳腺癌(n=37)。通过荧光原位杂交直接在单细胞水平评估端粒长度,并使用 Fisher 精确检验比较患者组。ER 阴性状态(P=0.022)、PR 阴性状态(P=0.008)、HER-2 阳性状态(P=0.023)和 p53 阳性状态(P=0.022)与较短的端粒长度相关。与 luminal B 病例(P=0.002)、HER-2 阳性病例(P=0.011)或三阴性病例(P=0.0003)相比,更多 luminal A 癌症具有正常或长端粒长度。luminal B、HER-2 阳性和三阴性病例之间没有显著差异。侵袭性更强的亚型,如 luminal B、HER-2 阳性和三阴性肿瘤,端粒长度较短,提示肿瘤端粒长度可能作为乳腺癌的预后和/或风险标志物具有实用价值。

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