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人源 Toll 样受体 3 胞外结构域的分泌受单核苷酸多态性影响,并受 Unc93b1 调控。

Secretion of the human Toll-like receptor 3 ectodomain is affected by single nucleotide polymorphisms and regulated by Unc93b1.

机构信息

Department of Molecular and Cellular Biochemistry, Indiana University, Bloomington, Indiana 47401-3700, USA.

出版信息

J Biol Chem. 2010 Nov 19;285(47):36635-44. doi: 10.1074/jbc.M110.144402. Epub 2010 Sep 20.

Abstract

The innate immune receptor Toll-like receptor 3 (TLR3) can be present on the surface of the plasma membranes of cells and in endolysosomes. The Unc93b1 protein has been reported to facilitate localization of TLR7 and 9 and is required for TLR3, -7, and -9 signaling. We demonstrate that siRNA knockdown of Unc93b1 reduced the abundance of TLR3 on the cell surface without altering total TLR3 accumulation. In addition, siRNA to Unc93b1 reduced the secretion of the TLR3 ectodomain (T3ECD) into the cell medium. Furthermore, two human single nucleotide polymorphisms that affected herpesvirus and influenza virus encephalopathy as well as a natural isoform generated by alternative splicing were found to be impaired for T3ECD secretion and decreased the abundance of TLR3 on the cell surface. The locations of the SNP P554S and the deletion in the isoform led to the identification of a loop in the TLR3 ectodomain that is required for secretion and a second whose presence decreased secretion. Finally, a truncated protein containing the N-terminal 10 leucine-rich repeats of T3ECD was sufficient for secretion in an Unc93b1-dependent manner.

摘要

天然免疫受体 Toll 样受体 3(TLR3)可以存在于细胞膜表面和内体溶酶体中。已有报道称 Unc93b1 蛋白有助于 TLR7 和 9 的定位,并且是 TLR3、-7 和 -9 信号所必需的。我们证明,Unc93b1 的 siRNA 敲低减少了细胞表面 TLR3 的丰度,而不改变 TLR3 的总积累。此外,针对 Unc93b1 的 siRNA 减少了 TLR3 胞外结构域(T3ECD)分泌到细胞培养基中。此外,发现两种影响疱疹病毒和流感病毒脑炎的人类单核苷酸多态性以及通过选择性剪接产生的天然同工型,其 T3ECD 分泌减少,并降低了细胞表面 TLR3 的丰度。SNP P554S 和同工型缺失的位置导致鉴定出 TLR3 胞外结构域中需要分泌的环,以及存在会降低分泌的第二个环。最后,包含 T3ECD 的 N 端 10 个亮氨酸丰富重复序列的截断蛋白足以依赖于 Unc93b1 进行分泌。

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