利基炎症信号控制乳腺振荡再生,保护干细胞免受细胞毒性压力的影响

IF 19.8 1区 医学 Q1 CELL & TISSUE ENGINEERING
Chunye Liu, Yishu Xu, Guowei Yang, Yu Tao, Jiali Chang, Shihui Wang, Tom H. Cheung, Jianfeng Chen, Yi Arial Zeng
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引用次数: 0

摘要

众所周知,干细胞在应激后具有恢复力和更强的活性。在发情周期中,乳腺会经历频繁的重塑和反复的应激,但乳腺干细胞(MaSCs)如何应对应激并促进再生仍不清楚。我们发现,细胞毒性应激诱导的CD11c+导管巨噬细胞活化有助于干细胞存活并防止分化。在发情周期中,这些巨噬细胞通过IL1β-IL1R1-NF-κB信号以振荡的方式促进Procr+ MaSC的活性。在MaSCs中删除IL1R1会导致干细胞损失和管腔分化偏斜。此外,在化疗药物紫杉醇的细胞毒性压力下,导管巨噬细胞会分泌更高水平的IL1β,促进造血干细胞存活并阻止分化。抑制IL1R1可使MaSCs对紫杉醇敏感。我们的研究结果揭示了一个调节再生的反复炎症过程,为压力诱导的炎症及其对干细胞存活的影响提供了见解,这可能会影响癌症疗法的疗效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Niche inflammatory signals control oscillating mammary regeneration and protect stem cells from cytotoxic stress

Niche inflammatory signals control oscillating mammary regeneration and protect stem cells from cytotoxic stress

Stem cells are known for their resilience and enhanced activity post-stress. The mammary gland undergoes frequent remodeling and is subjected to recurring stress during the estrus cycle, but it remains unclear how mammary stem cells (MaSCs) respond to the stress and contribute to regeneration. We discovered that cytotoxic stress-induced activation of CD11c+ ductal macrophages aids stem cell survival and prevents differentiation. These macrophages boost Procr+ MaSC activity through IL1β-IL1R1-NF-κB signaling during the estrus cycle in an oscillating manner. Deleting IL1R1 in MaSCs results in stem cell loss and skewed luminal differentiation. Moreover, under cytotoxic stress from the chemotherapy agent paclitaxel, ductal macrophages secrete higher IL1β levels, promoting MaSC survival and preventing differentiation. Inhibiting IL1R1 sensitizes MaSCs to paclitaxel. Our findings reveal a recurring inflammatory process that regulates regeneration, providing insights into stress-induced inflammation and its impact on stem cell survival, potentially affecting cancer therapy efficacy.

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来源期刊
Cell stem cell
Cell stem cell 生物-细胞生物学
CiteScore
37.10
自引率
2.50%
发文量
151
审稿时长
42 days
期刊介绍: Cell Stem Cell is a comprehensive journal covering the entire spectrum of stem cell biology. It encompasses various topics, including embryonic stem cells, pluripotency, germline stem cells, tissue-specific stem cells, differentiation, epigenetics, genomics, cancer stem cells, stem cell niches, disease models, nuclear transfer technology, bioengineering, drug discovery, in vivo imaging, therapeutic applications, regenerative medicine, clinical insights, research policies, ethical considerations, and technical innovations. The journal welcomes studies from any model system providing insights into stem cell biology, with a focus on human stem cells. It publishes research reports of significant importance, along with review and analysis articles covering diverse aspects of stem cell research.
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