妊娠会减少老年乳腺中Il33+杂交祖细胞的积累

Andrew Olander, Cynthia M Ramirez, Veronica Haro Acosta, Paloma Medina, Sara Kaushik, Vanessa D Jonsson, Shaheen S Sikandar
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引用次数: 0

摘要

衰老会增加患乳腺癌的风险,而早孕则会降低妇女终身患乳腺癌的风险。有几项研究探讨了衰老或怀孕对乳腺上皮细胞(MECs)的影响,但两者的综合影响仍不清楚。在这里,我们以单细胞分辨率研究了高龄无雌激素小鼠和有雌激素小鼠乳腺的功能和转录组变化,发现妊娠能使与年龄相关的品系组成失衡正常化,同时还能诱导细胞处于分化状态。重要的是,我们发现了少数表达Il33的杂交MECs,它们具有很高的细胞效力,在高龄无阴道小鼠中积累,但在高龄有阴道小鼠中则显著减少。从功能上讲,对来自年轻小鼠的基底上皮细胞(而非管腔上皮细胞)进行IL33处理,可表征老龄无子宫MECs,并促进Trp53基因敲除的器官组织的形成。总之,我们的研究表明,妊娠可通过减少Il33+杂交MECs阻止基底层与年龄相关的品系完整性丧失,这可能有助于妊娠诱导的乳腺癌保护。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Pregnancy Reduces Il33+ Hybrid Progenitor Accumulation in the Aged Mammary Gland
Aging increases breast cancer risk while an early first pregnancy reduces a woman’s life-long risk. Several studies have explored the effect of either aging or pregnancy on mammary epithelial cells (MECs), but the combined effect of both remains unclear. Here, we interrogate the functional and transcriptomic changes at single cell resolution in the mammary gland of aged nulliparous and parous mice to discover that pregnancy normalizes age-related imbalances in lineage composition, while also inducing a differentiated cell state. Importantly, we uncover a minority population of Il33-expressing hybrid MECs with high cellular potency that accumulate in aged nulliparous mice but is significantly reduced in aged parous mice. Functionally, IL33 treatment of basal, but not luminal, epithelial cells from young mice phenocopies aged nulliparous MECs and promotes formation of organoids with Trp53 knockdown. Collectively, our study demonstrates that pregnancy blocks the age-associated loss of lineage integrity in the basal layer through a decrease in Il33+ hybrid MECs, potentially contributing to pregnancy-induced breast cancer protection.
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