Structure and Self-assembly of NLRP10

作者： Leng Fang-Wei ¹ Wang Da-Cheng ¹ Leng Fang-Wei ² Wang Da-Cheng ² Leng Fang-Wei ³ Xie Can ³
作者单位：

1. Chinese Acad Sci, Inst Biophys, Beijing 100101, Peoples R China.

2. Univ Chinese Acad Sci, Beijing 100049, Peoples R China.

3. Peking Univ, Coll Life Sci, Beijing 100871, Peoples R China.
提交时间：2016-05-12 08:40:38

摘要: NLRP10 is a special member of NOD-like receptors (NLRs) family that lacks the leucine-rich repeats, suggesting that NLRP10 may act as an immunity regulator rather than directly receptor recognizing intracellular pathogen products. Previous studies on NLRP10 show that NLRP10 can interact with several components of NOD1 pathway thereby enhancing NOD1-mediated innate immune responses. In particular models, NLRP10 also negatively affects the activation of NLRP3 inflammasome. It has been proposed that NLRP10 oligomers interact with ASC to form a multi-protein platform for the recruitment of caspase-1 or other signaling components. Here, we show that pyrin-like domain (PYD) degradation induce the formation of NLRP10 oligomers, which present stick-shaped and circular structure. With the NLRP10 mutant G173A made by means of site-directed mutagenesis, we successfully obtain homogeneous full-length NLRP10 preparations. Corresponding gel filtration analysis and electron microscope (EM) data further proved that the PYD domain is important in protecting NLRP10 against aggregation.

INFLAMMASOME INNATE DEATH

期刊： PROGRESS IN BIOCHEMISTRY AND BIOPHYSICS
分类： 生物学 >> 生物物理学 >> 生物物理、生物化学与分子生物学
引用： ChinaXiv:201605.01377 (或此版本 ChinaXiv:201605.01377V1)
DOI:10.12074/201605.01377V1
CSTR:32003.36.ChinaXiv.201605.01377.V1
推荐引用方式： Leng Fang-Wei,Wang Da-Cheng,Leng Fang-Wei,Wang Da-Cheng,Leng Fang-Wei,Xie Can.(2016).Structure and Self-assembly of NLRP10.PROGRESS IN BIOCHEMISTRY AND BIOPHYSICS.[ChinaXiv:201605.01377] (点此复制)

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[V1]

2016-05-12 08:40:38

ChinaXiv:201605.01377V1

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