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维生素 C 通过表观遗传重塑增强浆细胞分化。

Epigenetic remodeling by vitamin C potentiates plasma cell differentiation.

机构信息

Department of Microbial Infection and Immunity, The Ohio State University, Columbus, OH, United States.

Division of Gene Expression and Signaling, La Jolla Institute for Immunology, San Diego, CA, United States.

出版信息

Elife. 2022 Sep 7;11:e73754. doi: 10.7554/eLife.73754.

Abstract

Ascorbate (vitamin C) is an essential micronutrient in humans. The severe chronic deficiency of ascorbate, termed scurvy, has long been associated with increased susceptibility to infections. How ascorbate affects the immune system at the cellular and molecular levels remained unclear. From a micronutrient analysis, we identified ascorbate as a potent enhancer for antibody response by facilitating the IL-21/STAT3-dependent plasma cell differentiation in mouse and human B cells. The effect of ascorbate is unique as other antioxidants failed to promote plasma cell differentiation. Ascorbate is especially critical during early B cell activation by poising the cells to plasma cell lineage without affecting the proximal IL-21/STAT3 signaling and the overall transcriptome. As a cofactor for epigenetic enzymes, ascorbate facilitates TET2/3-mediated DNA modification and demethylation of multiple elements at the locus. DNA demethylation augments STAT3 association at the promoter and a downstream enhancer, thus ensuring efficient gene expression and plasma cell differentiation. The results suggest that an adequate level of ascorbate is required for antibody response and highlight how micronutrients may regulate the activity of epigenetic enzymes to regulate gene expression. Our findings imply that epigenetic enzymes can function as sensors to gauge the availability of metabolites and influence cell fate decisions.

摘要

抗坏血酸(维生素 C)是人类必需的微量营养素。严重的慢性抗坏血酸缺乏,即坏血病,长期以来一直与增加感染易感性有关。抗坏血酸如何在细胞和分子水平上影响免疫系统仍不清楚。从微量营养素分析中,我们发现抗坏血酸通过促进小鼠和人 B 细胞中 IL-21/STAT3 依赖性浆细胞分化,是增强抗体反应的有效增强剂。抗坏血酸的作用是独特的,因为其他抗氧化剂未能促进浆细胞分化。抗坏血酸在早期 B 细胞激活期间尤为关键,它使细胞向浆细胞谱系倾斜,而不影响近端的 IL-21/STAT3 信号和整个转录组。作为表观遗传酶的辅助因子,抗坏血酸促进 TET2/3 介导的 基因座多个元件的 DNA 修饰和去甲基化。DNA 去甲基化增强了 启动子和下游增强子处 STAT3 的结合,从而确保有效的基因表达和浆细胞分化。这些结果表明,抗体反应需要足够水平的抗坏血酸,并强调了微量营养素如何调节表观遗传酶的活性来调节基因表达。我们的研究结果表明,表观遗传酶可以作为传感器来衡量代谢物的可用性,并影响细胞命运决定。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/583a/9451539/33a424d59716/elife-73754-fig1.jpg

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