内源性 TLR7 和 TLR3 RNA 配体激活自身反应性 B 细胞。
Activation of autoreactive B cells by endogenous TLR7 and TLR3 RNA ligands.
机构信息
Department of Microbiology, Boston University School of Medicine, Boston, Massachusetts 02118, USA.
出版信息
J Biol Chem. 2012 Nov 16;287(47):39789-99. doi: 10.1074/jbc.M112.383000. Epub 2012 Sep 27.
Abstract
The key step in the activation of autoreactive B cells is the internalization of nucleic acid containing ligands and delivery of these ligands to the Toll-like Receptor (TLR) containing endolysosomal compartment. Ribonucleoproteins represent a large fraction of autoantigens in systemic autoimmune diseases. Here we demonstrate that many uridine-rich mammalian RNA sequences associated with common autoantigens effectively activate autoreactive B cells. Priming with type I IFN increased the magnitude of activation, and the range of which RNAs were stimulatory. A subset of RNAs that contain a high degree of self-complementarity also activated B cells through TLR3. For the RNA sequences that activated predominantly through TLR7, the activation is proportional to uridine-content, and more precisely defined by the frequency of specific uridine-containing motifs. These results identify parameters that define specific mammalian RNAs as ligands for TLRs.
摘要
自身反应性 B 细胞激活的关键步骤是含有核酸的配体的内化,并将这些配体递送到含有 Toll 样受体 (TLR) 的内体溶酶体隔室。核糖核蛋白是系统性自身免疫性疾病中自身抗原的很大一部分。在这里,我们证明许多与常见自身抗原相关的富含尿嘧啶的哺乳动物 RNA 序列有效地激活了自身反应性 B 细胞。I 型 IFN 的引发增加了激活的幅度,以及刺激 RNA 的范围。含有高度自身互补性的 RNA 亚类也通过 TLR3 激活 B 细胞。对于主要通过 TLR7 激活的 RNA 序列,激活与尿嘧啶含量成正比,并且更精确地由特定含尿嘧啶基序的频率定义。这些结果确定了定义特定哺乳动物 RNA 作为 TLR 配体的参数。
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