Luminal epithelial cells integrate variable responses to aging into stereotypical changes that underlie breast cancer susceptibility.

IF 6.4 1区生物学 Q1 BIOLOGY

eLife Pub Date : 2024-11-15 DOI:10.7554/eLife.95720

Rosalyn W Sayaman, Masaru Miyano, Eric G Carlson, Parijat Senapati, Arrianna Zirbes, Sundus F Shalabi, Michael E Todhunter, Victoria E Seewaldt, Susan L Neuhausen, Martha R Stampfer, Dustin E Schones, Mark LaBarge

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Abstract

Effects from aging in single cells are heterogenous, whereas at the organ- and tissue-levels aging phenotypes tend to appear as stereotypical changes. The mammary epithelium is a bilayer of two major phenotypically and functionally distinct cell lineages: luminal epithelial and myoepithelial cells. Mammary luminal epithelia exhibit substantial stereotypical changes with age that merit attention because these cells are the putative cells-of-origin for breast cancers. We hypothesize that effects from aging that impinge upon maintenance of lineage fidelity increase susceptibility to cancer initiation. We generated and analyzed transcriptomes from primary luminal epithelial and myoepithelial cells from younger <30 (y)ears old and older >55y women. In addition to age-dependent directional changes in gene expression, we observed increased transcriptional variance with age that contributed to genome-wide loss of lineage fidelity. Age-dependent variant responses were common to both lineages, whereas directional changes were almost exclusively detected in luminal epithelia and involved altered regulation of chromatin and genome organizers such as SATB1. Epithelial expression of gap junction protein GJB6 increased with age, and modulation of GJB6 expression in heterochronous co-cultures revealed that it provided a communication conduit from myoepithelial cells that drove directional change in luminal cells. Age-dependent luminal transcriptomes comprised a prominent signal that could be detected in bulk tissue during aging and transition into cancers. A machine learning classifier based on luminal-specific aging distinguished normal from cancer tissue and was highly predictive of breast cancer subtype. We speculate that luminal epithelia are the ultimate site of integration of the variant responses to aging in their surrounding tissue, and that their emergent phenotype both endows cells with the ability to become cancer-cells-of-origin and represents a biosensor that presages cancer susceptibility.

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腔隙上皮细胞将对衰老的不同反应整合成刻板的变化，这些变化是乳腺癌易感性的基础。

衰老对单细胞的影响是多方面的，而在器官和组织层面，衰老表型往往表现为刻板的变化。乳腺上皮是由表型和功能上截然不同的两大细胞系组成的双层结构：管腔上皮细胞和肌上皮细胞。乳腺管腔上皮细胞会随着年龄的增长而发生巨大的刻板变化，值得关注，因为这些细胞是乳腺癌的原发细胞。我们假设，衰老会影响血统保真度的维持，从而增加癌症发生的几率。我们生成并分析了来自 55 岁年轻女性的原发性管腔上皮细胞和肌上皮细胞的转录组。除了基因表达随年龄而发生的方向性变化外，我们还观察到转录变异随年龄的增长而增加，这导致了全基因组范围内血统保真度的丧失。年龄依赖性变异反应在两个谱系中都很常见，而方向性变化几乎只在管腔上皮中检测到，并且涉及染色质和基因组组织者（如 SATB1）调控的改变。上皮细胞间隙连接蛋白 GJB6 的表达随着年龄的增长而增加，在异时性共培养物中调节 GJB6 的表达显示，它提供了一个来自肌上皮细胞的通信管道，推动了管腔细胞的方向性变化。与年龄相关的管腔转录组构成了一个突出的信号，可在衰老和向癌症过渡的过程中在大块组织中检测到。基于管腔特异性老化的机器学习分类器能区分正常组织和癌症组织，并能高度预测乳腺癌亚型。我们推测，管腔上皮是其周围组织对衰老的变异反应的最终整合点，其出现的表型既赋予了细胞成为癌症原发细胞的能力，又代表了一种预示癌症易感性的生物传感器。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

eLife BIOLOGY-

CiteScore

12.90

自引率

3.90%

发文量

3122

审稿时长

17 weeks

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