生物
细胞毒性T细胞
胆道闭锁
库普弗电池
免疫系统
T细胞
发病机制
免疫学
炎症
肝移植
内科学
医学
移植
生物化学
体外
作者
Jun Wang,Yanhui Xu,Zhanghua Chen,Jiankun Liang,Zefeng Lin,Huiying Liang,Yiping Xu,Qi Wu,Xuanjie Guo,Junli Nie,Bingtai Lu,Bing Huang,Huifang Xian,Xiaohui Wang,Qiang Wu,Jixiao Zeng,Chengwei Chai,Mei-Xue Zhang,Yuzhen Lin,Li Zhang
出处
期刊:Cell
[Cell Press]
日期:2020-11-27
卷期号:183 (7): 1867-1883.e26
被引量:123
标识
DOI:10.1016/j.cell.2020.10.048
摘要
Biliary atresia (BA) is a severe cholangiopathy that leads to liver failure in infants, but its pathogenesis remains to be fully characterized. By single-cell RNA profiling, we observed macrophage hypo-inflammation, Kupffer cell scavenger function defects, cytotoxic T cell expansion, and deficiency of CX3CR1+effector T and natural killer (NK) cells in infants with BA. More importantly, we discovered that hepatic B cell lymphopoiesis did not cease after birth and that tolerance defects contributed to immunoglobulin G (IgG)-autoantibody accumulation in BA. In a rhesus-rotavirus induced BA model, depleting B cells or blocking antigen presentation ameliorated liver damage. In a pilot clinical study, we demonstrated that rituximab was effective in depleting hepatic B cells and restoring the functions of macrophages, Kupffer cells, and T cells to levels comparable to those of control subjects. In summary, our comprehensive immune profiling in infants with BA had educed that B-cell-modifying therapies may alleviate liver pathology.
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