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具有妊娠特异性活性的多能乳腺祖细胞的证据。

Evidence for a multipotent mammary progenitor with pregnancy-specific activity.

作者信息

Kaanta Alice S, Virtanen Carl, Selfors Laura M, Brugge Joan S, Neel Benjamin G

出版信息

Breast Cancer Res. 2013;15(4):R65. doi: 10.1186/bcr3459.

Abstract

INTRODUCTION

The mouse mammary gland provides a powerful model system for studying processes involved in epithelial tissue development. Although markers that enrich for mammary stem cells and progenitors have been identified, our understanding of the mammary developmental hierarchy remains incomplete.

METHODS

We used the MMTV promoter linked to the reverse tetracycline transactivator to induce H2BGFP expression in the mouse mammary gland. Mammary epithelial cells (MECs) from virgin mice were sorted by flow cytometry for expression of the mammary stem cell/progenitor markers CD24 and CD29, and H2BGFP. Sorted populations were analyzed for in vivo repopulation ability, expression of mammary lineage markers, and differential gene expression.

RESULTS

The reconstituting activity of CD24⁺/CD29⁺ cells in cleared fat pad transplantation assays was not distinguished in GFP⁺ compared to GFP⁻ subpopulations. However, within the CD24⁺/CD29(lo) luminal progenitor-enriched population, H2BGFP⁺, but not H2BGFP⁻, MECs formed mammary structures in transplantation assays; moreover, this activity was dramatically enhanced in pregnant recipients. These outgrowths contained luminal and myoepithelial mammary lineages and produced milk, but lacked the capacity for serial transplantation. Transcriptional microarray analysis revealed that H2BGFP⁺/CD24⁺/CD29(lo) MECs are distinct from H2BGFP⁻/CD24⁺/CD29(lo) MECs and enriched for gene expression signatures with both the stem cell (CD24⁺/CD29⁺) and luminal progenitor (CD24⁺/CD29(lo)/CD61⁺) compartments.

CONCLUSIONS

We have identified a population of MECs containing pregnancy-activated multipotent progenitors that are present in the virgin mammary gland and contribute to the expansion of the mammary gland during pregnancy.

摘要

引言

小鼠乳腺为研究上皮组织发育过程提供了一个强大的模型系统。尽管已经鉴定出了富集乳腺干细胞和祖细胞的标志物,但我们对乳腺发育层次的理解仍不完整。

方法

我们使用与反向四环素反式激活因子相连的MMTV启动子在小鼠乳腺中诱导H2BGFP表达。通过流式细胞术对处女鼠的乳腺上皮细胞(MECs)进行分选,以检测乳腺干细胞/祖细胞标志物CD24和CD29以及H2BGFP的表达。对分选后的细胞群体进行体内再增殖能力、乳腺谱系标志物表达和差异基因表达分析。

结果

在清除脂肪垫移植试验中,与GFP⁻亚群相比,GFP⁺的CD24⁺/CD29⁺细胞的重建活性没有差异。然而,在富含腔面祖细胞的CD24⁺/CD29(lo)群体中,H2BGFP⁺而非H2BGFP⁻的MECs在移植试验中形成了乳腺结构;此外,在怀孕受体中这种活性显著增强。这些生长物包含腔面和肌上皮乳腺谱系并产生乳汁,但缺乏连续移植的能力。转录微阵列分析显示,H2BGFP⁺/CD24⁺/CD29(lo) MECs与H2BGFP⁻/CD24⁺/CD29(lo) MECs不同,并且富含干细胞(CD24⁺/CD29⁺)和腔面祖细胞(CD24⁺/CD29(lo)/CD61⁺)区室的基因表达特征。

结论

我们鉴定出了一群含有妊娠激活的多能祖细胞的MECs,它们存在于处女乳腺中,并在妊娠期间促进乳腺的扩张。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0229/3979108/23bdbe6e9063/bcr3459-1.jpg

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