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Mettl14-Mediated m6A Modification Is Essential for Germinal Center B Cell Response

Hengjun Huang, Gaopu Zhang, Gui‐Xin Ruan, Yuxing Li, Wenjing Chen, Jia Zou, Rui Zhang, Jing Wang, Sheng‐Jian Ji, Shengli Xu, Xijun Ou

2022The Journal of Immunology44 citationsDOIOpen Access PDF

Abstract

Abstract The germinal center (GC) response is essential for generating memory B and long-lived Ab-secreting plasma cells during the T cell–dependent immune response. In the GC, signals via the BCR and CD40 collaboratively promote the proliferation and positive selection of GC B cells expressing BCRs with high affinities for specific Ags. Although a complex gene transcriptional regulatory network is known to control the GC response, it remains elusive how the positive selection of GC B cells is modulated posttranscriptionally. In this study, we show that methyltransferase like 14 (Mettl14)–mediated methylation of adenosines at the position N6 of mRNA (N6-methyladenosine [m6A]) is essential for the GC B cell response in mice. Ablation of Mettl14 in B cells leads to compromised GC B cell proliferation and a defective Ab response. Interestingly, we unravel that Mettl14-mediated m6A regulates the expression of genes critical for positive selection and cell cycle regulation of GC B cells in a Ythdf2-dependent but Myc-independent manner. Furthermore, our study reveals that Mettl14-mediated m6A modification promotes mRNA decay of negative immune regulators, such as Lax1 and Tipe2, to upregulate genes requisite for GC B cell positive selection and proliferation. Thus, our findings suggest that Mettl14-mediated m6A modification plays an essential role in the GC B cell response.

Topics & Concepts

Germinal centerCenter (category theory)B cellCell biologyBiologyChemistryImmunologyAntibodyCrystallographyRNA modifications and cancerHVDC Systems and Fault ProtectionViral-associated cancers and disorders
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