Department of Molecular Medicine, The Scripps Research Institute, La Jolla, CA, USA.
Veterans Administration San Diego Healthcare System, San Diego, CA, USA.
J Thromb Haemost. 2018 May;16(5):919-932. doi: 10.1111/jth.13988. Epub 2018 Apr 1.
Essentials Plg-R female mice give birth, but no offspring of Plg-R female mice survive to weaning. Causal mechanisms of potential lactational failure in Plg-R mice are unknown. Plg-R regulates extracellular matrix remodeling, cell proliferation, apoptosis, fibrin surveillance. Plg-R is essential for lactogenesis and mammary lobuloalveolar development.
Background Lactational competence requires plasminogen, the zymogen of the serine protease, plasmin. Plg-R is a unique transmembrane plasminogen receptor that promotes plasminogen activation to plasmin on cell surfaces. Plg-R mice are viable, but no offspring of Plg-R female mice survive to weaning. Objectives We investigated potential lactational failure in Plg-R mice and addressed causal mechanisms. Methods Fibrin accumulation, macrophage infiltration, processing of extracellular matrix components, effects of genetic deletion of fibrinogen, expression of fibrosis genes, and proliferation and apoptosis of epithelial cells were examined in lactating mammary glands of Plg-R and Plg-R mice. Results Milk was not present in the stomachs of offspring of Plg-R female mice and the pups were rescued by foster mothers. Although the mammary ductal tree developed normally in Plg-R glands, lobuloalveolar development was blocked by a hypertrophic fibrotic stroma and infiltrating macrophages were present. A massive accumulation of fibrin was also present in Plg-R alveoli and ducts. Although this accumulation was decreased when Plg-R mice were made genetically heterozygous for fibrinogen, defects in lobuloalveolar development were not rescued by fibrinogen heterozygosity. Transcriptional profiling revealed that EGF was downregulated 12-fold in Plg-R glands. Furthermore, proliferation of epithelial cells was not detectable. In addition, the pro-survival protein, Mcl-1, was markedly downregulated and apoptosis was observed in Plg-R but not Plg-R glands. Conclusions Plg-R is essential for lactogenesis and functions to maintain the appropriate stromal extracellular matrix environment, regulate epithelial cell proliferation and apoptosis, and, by regulating fibrinolysis, preserve alveolar and ductal patency.
Essentials Plg-R 雌性小鼠会生育,但 Plg-R 雌性小鼠的后代无法存活到断奶。Plg-R 小鼠潜在哺乳失败的因果机制尚不清楚。Plg-R 调节细胞外基质重塑、细胞增殖、细胞凋亡、纤维蛋白监测。Plg-R 对泌乳和乳腺小叶肺泡发育至关重要。
背景 泌乳能力需要纤溶酶原,即丝氨酸蛋白酶纤溶酶的酶原。Plg-R 是一种独特的跨膜纤溶酶原受体,可促进纤溶酶原在细胞表面激活为纤溶酶。Plg-R 小鼠具有活力,但 Plg-R 雌性小鼠的后代无法存活到断奶。
目的 我们研究了 Plg-R 小鼠潜在的哺乳失败,并解决了因果机制。
方法 在 Plg-R 和 Plg-R 小鼠的泌乳乳腺中检查纤维蛋白积累、巨噬细胞浸润、细胞外基质成分的处理、纤维蛋白原基因缺失的遗传效应、纤维化基因的表达以及上皮细胞的增殖和凋亡。
结果 Plg-R 雌性小鼠后代的胃中没有乳汁,幼崽由寄养母亲解救。虽然 Plg-R 乳腺的乳腺导管树发育正常,但小叶肺泡发育受阻于肥大的纤维性基质,并且存在浸润的巨噬细胞。Plg-R 肺泡和导管中也存在大量纤维蛋白积累。尽管当 Plg-R 小鼠对纤维蛋白原呈杂合子时,这种积累减少,但小叶肺泡发育缺陷不能通过纤维蛋白原杂合性来挽救。转录谱分析显示,Plg-R 乳腺中 EGF 下调了 12 倍。此外,上皮细胞的增殖无法检测到。此外,Plg-R 但不是 Plg-R 乳腺中观察到促生存蛋白 Mcl-1 明显下调和凋亡。
结论 Plg-R 对泌乳至关重要,其作用是维持适当的间质细胞外基质环境,调节上皮细胞增殖和凋亡,并通过调节纤维蛋白溶解来维持肺泡和导管的通畅性。