| Literature DB >> 36037365 |
Ying Wang1, Jun Liu1, Chizuru Akatsu2, Runyun Zhang1, Hai Zhang3, Han Zhu4, Kangwei Liu4, Han-Ying Zhu1, Qing Min3, Xin Meng1, Chaoqun Cui1, Yue Tang1, Meiping Yu3, Yaxuan Li1, Xiaoqian Feng1, Hao Wei1, Zichao Wen1, Sihan Ji1, Martin G Weigert5, Takeshi Tsubata2, Ji-Yang Wang1,3,6,7,8.
Abstract
Elimination of autoreactive developing B cells is an important mechanism to prevent autoantibody production. However, how B cell receptor (BCR) signaling triggers apoptosis of immature B cells remains poorly understood. We show that BCR stimulation up-regulates the expression of the lysosomal-associated transmembrane protein 5 (LAPTM5), which in turn triggers apoptosis of immature B cells through two pathways. LAPTM5 causes BCR internalization, resulting in decreased phosphorylation of SYK and ERK. In addition, LAPTM5 targets the E3 ubiquitin ligase WWP2 for lysosomal degradation, resulting in the accumulation of its substrate PTEN. Elevated PTEN levels suppress AKT phosphorylation, leading to increased FOXO1 expression and up-regulation of the cell cycle inhibitor p27Kip1 and the proapoptotic molecule BIM. In vivo, LAPTM5 is involved in the elimination of autoreactive B cells and its deficiency exacerbates autoantibody production. Our results reveal a previously unidentified mechanism that contributes to immature B cell apoptosis and B cell tolerance.Entities:
Keywords: B cell tolerance; E3 ubiquitin ligase; apoptosis; immature B cell; lysosomal-associated transmembrane protein 5
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Year: 2022 PMID: 36037365 PMCID: PMC9457450 DOI: 10.1073/pnas.2205629119
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 12.779