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Mfge8 Is Critical for Mammary Gland Remodeling during Involution

机译:Mfge8对于内卷化过程中的乳腺重塑至关重要

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摘要

Apoptosis is a critical process in normal mammary gland development and the rapid clearance of apoptotic cells prevents tissue injury associated with the release of intracellular antigens from dying cells. Milk fat globule-EGF-factor 8 (Mfge8) is a milk glycoprotein that is abundantly expressed in the mammary gland epithelium and has been shown to facilitate the clearance of apoptotic lymphocytes by splenic macrophages. We report that mice with disruption of Mfge8 had normal mammary gland development until involution. However, abnormal mammary gland remodeling was observed postlactation in Mfge8 mutant mice. During early involution, Mfge8 mutant mice had increased numbers of apoptotic cells within the mammary gland associated with a delay in alveolar collapse and fat cell repopulation. As involution progressed, Mfge8 mutants developed inflammation as assessed by CD45 and CD11b staining of mammary gland tissue sections. With additional pregnancies, Mfge8 mutant mice developed progressive dilatation of the mammary gland ductal network. These data demonstrate that Mfge8 regulates the clearance of apoptotic epithelial cells during mammary gland involution and that the absence of Mfge8 leads to inflammation and abnormal mammary gland remodeling.
机译:凋亡是正常乳腺发育中的关键过程,凋亡细胞的快速清除可防止与组织中与死亡细胞释放细胞内抗原有关的组织损伤。乳脂小球EGF因子8(Mfge8)是一种乳糖蛋白,在乳腺上皮细胞中大量表达,并已被证明可以促进脾巨噬细胞清除凋亡的淋巴细胞。我们报告与破坏Mfge8的小鼠具有正常的乳腺发育直至复旧。但是,在Mfge8突变小鼠中观察到乳腺重塑异常。在早期的复性过程中,Mfge8突变型小鼠的乳腺内凋亡细胞数量增加,与肺泡塌陷和脂肪细胞重新聚集有关。随着对合的进行,通过乳腺组织切片的CD45和CD11b染色评估,Mfge8突变体发生了炎症。随着额外的怀孕,Mfge8突变小鼠发展了乳腺导管网络的进行性扩张。这些数据表明,Mfge8在乳腺退化过程中调节凋亡上皮细胞的清除,并且缺少Mfge8会导致炎症和异常的乳腺重塑。

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