The immune environment of the mammary gland fluctuates during post-lactational regression and correlates with tumour growth rate

Jessica Hitchcock, K. Hughes, S. Pensa, Bethan Lloyd-Lewis, C. Watson
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引用次数: 4

Abstract

ABSTRACT Post-lactational mammary gland regression encompasses extensive programmed cell death and removal of milk-producing epithelial cells, breakdown of extracellular matrix components and redifferentiation of stromal adipocytes. This highly regulated involution process is associated with a transient increased risk of breast cancer in women. Using a syngeneic tumour model, we show that tumour growth is significantly altered depending on the stage of involution at which tumour cells are implanted. Tumour cells injected at day 3 involution grew faster than those in nulliparous mice, whereas tumours initiated at day 6 involution grew significantly slower. These differences in tumour progression correlate with distinct changes in innate immune cells, in particular among F4/80-expressing macrophages and among TCRδ+ unconventional T cells. Breast cancer post-pregnancy risk is exacerbated in older first-time mothers and, in our model, initial tumour growth is moderately faster in aged mice compared with young mice. Our results have implications for breast cancer risk and the use of anti-inflammatory therapeutics for postpartum breast cancers.
乳腺的免疫环境在泌乳后消退期间波动,并与肿瘤生长速率相关
哺乳后乳腺退化包括广泛的程序性细胞死亡和产乳上皮细胞的去除,细胞外基质成分的分解和间质脂肪细胞的再分化。这种高度调控的复发过程与女性乳腺癌风险的短暂增加有关。使用同基因肿瘤模型,我们表明肿瘤生长明显改变取决于肿瘤细胞植入的退化阶段。第3天注射的肿瘤细胞生长速度快于未生育小鼠,而第6天开始的肿瘤生长速度明显慢于未生育小鼠。肿瘤进展的这些差异与先天免疫细胞的明显变化相关,特别是在表达f4 /80的巨噬细胞和TCRδ+非常规T细胞中。怀孕后患乳腺癌的风险在年龄较大的第一次母亲中加剧,在我们的模型中,老年小鼠的初始肿瘤生长速度比年轻小鼠略快。我们的研究结果对乳腺癌风险和产后乳腺癌抗炎治疗的使用具有启示意义。
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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