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Merck
  • Gli1+ mesenchymal stromal cells form a pathological niche to promote airway progenitor metaplasia in the fibrotic lung.

Gli1+ mesenchymal stromal cells form a pathological niche to promote airway progenitor metaplasia in the fibrotic lung.

Nature cell biology (2020-10-14)
Monica Cassandras, Chaoqun Wang, Jaymin Kathiriya, Tatsuya Tsukui, Peri Matatia, Michael Matthay, Paul Wolters, Ari Molofsky, Dean Sheppard, Hal Chapman, Tien Peng
摘要

Aberrant epithelial reprogramming can induce metaplastic differentiation at sites of tissue injury that culminates in transformed barriers composed of scar and metaplastic epithelium. While the plasticity of epithelial stem cells is well characterized, the identity and role of the niche has not been delineated in metaplasia. Here, we show that Gli1+ mesenchymal stromal cells (MSCs), previously shown to contribute to myofibroblasts during scarring, promote metaplastic differentiation of airway progenitors into KRT5+ basal cells. During fibrotic repair, Gli1+ MSCs integrate hedgehog activation signalling to upregulate BMP antagonism in the progenitor niche that promotes metaplasia. Restoring the balance towards BMP activation attenuated metaplastic KRT5+ differentiation while promoting adaptive alveolar differentiation into SFTPC+ epithelium. Finally, fibrotic human lungs demonstrate altered BMP activation in the metaplastic epithelium. These findings show that Gli1+ MSCs integrate hedgehog signalling as a rheostat to control BMP activation in the progenitor niche to determine regenerative outcome in fibrosis.

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Sigma-Aldrich
泰莫西芬, ≥99%
Sigma-Aldrich
脱氧核糖核酸酶 I 来源于牛胰腺, lyophilized powder, Protein ≥85 %, ≥400 Kunitz units/mg protein
Sigma-Aldrich
霍乱毒素 来源于霍乱弧菌, ≥90% (SDS-PAGE), lyophilized powder
Sigma-Aldrich
抗-Prosurfactant蛋白C(proSP-C)抗体, serum, Chemicon®
Sigma-Aldrich
抗磷酸Smad1/Smad5/Smad8(Ser463/465), from rabbit, purified by affinity chromatography
Sigma-Aldrich
抗细胞角蛋白14抗体,克隆LL002, clone LL002, Chemicon®, from mouse