LXJ (2023-01-30 21:35):
#paper doi: 10.1016/j.immuni.2022.11.002 ,B cell expansion hinders the stroma-epithelium regenerative cross talk during mucosal healing,Immunity,2022 促进肠道再生的治疗前景广阔,但确定影响组织再生的细胞机制仍然是一个尚未解决的挑战。为了深入了解粘膜愈合的过程,作者纵向检查了肠道损伤和再生过程中的免疫细胞组成。B细胞是愈合结肠中的主要细胞类型,单细胞RNA测序(scRNA-seq)显示在实验性粘膜愈合过程中IFN诱导的B细胞亚群的扩增,主要位于受损区域并与结肠炎严重程度相关。B细胞耗竭加速了损伤后的恢复,减少了上皮溃疡,并增强了与组织重建相关的基因表达程序。来自上皮和基质室的scRNA-seq结合空间转录组学和多重免疫染色显示,B细胞在粘膜愈合期间减少了基质和上皮细胞之间的相互作用。活化的B细胞破坏了维持类器官生存所需的上皮间质串扰。因此,损伤过程中B细胞的扩张会损害粘膜愈合所需的上皮-基质细胞相互作用,这对IBD的治疗有意义。
IF:25.500Q1 Immunity, 2022-12-13. DOI: 10.1016/j.immuni.2022.11.002 PMID: 36462502
B cell expansion hinders the stroma-epithelium regenerative cross talk during mucosal healing
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Abstract:
Therapeutic promotion of intestinal regeneration holds great promise, but defining the cellular mechanisms that influence tissue regeneration remains an unmet challenge. To gain insight into the process of mucosal healing, we longitudinally examined the immune cell composition during intestinal damage and regeneration. B cells were the dominant cell type in the healing colon, and single-cell RNA sequencing (scRNA-seq) revealed expansion of an IFN-induced B cell subset during experimental mucosal healing that predominantly located in damaged areas and associated with colitis severity. B cell depletion accelerated recovery upon injury, decreased epithelial ulceration, and enhanced gene expression programs associated with tissue remodeling. scRNA-seq from the epithelial and stromal compartments combined with spatial transcriptomics and multiplex immunostaining showed that B cells decreased interactions between stromal and epithelial cells during mucosal healing. Activated B cells disrupted the epithelial-stromal cross talk required for organoid survival. Thus, B cell expansion during injury impairs epithelial-stromal cell interactions required for mucosal healing, with implications for the treatment of IBD.
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