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帕金森病相关的 LRRK2 在循环和组织免疫细胞中表达,并在识别微生物结构后上调。

Parkinson's disease-linked LRRK2 is expressed in circulating and tissue immune cells and upregulated following recognition of microbial structures.

机构信息

Division of Neuroscience, Ottawa Hospital Research Institute, Ottawa, ON, Canada.

出版信息

J Neural Transm (Vienna). 2011 May;118(5):795-808. doi: 10.1007/s00702-011-0653-2. Epub 2011 May 7.

Abstract

Sequence variants at or near the leucine-rich repeat kinase 2 (LRRK2) locus have been associated with susceptibility to three human conditions: Parkinson's disease (PD), Crohn's disease and leprosy. As all three disorders represent complex diseases with evidence of inflammation, we hypothesized a role for LRRK2 in immune cell functions. Here, we report that full-length Lrrk2 is a relatively common constituent of human peripheral blood mononuclear cells (PBMC) including affinity isolated, CD14(+) monocytes, CD19(+) B cells, and CD4(+) as well as CD8(+) T cells. Up to 26% of PBMC from healthy donors and up to 43% of CD14(+) monocytes were stained by anti-Lrrk2 antibodies using cell sorting. PBMC lysates contained full-length (>260 kDa) and higher molecular weight Lrrk2 species. The expression of LRRK2 in circulating leukocytes was confirmed by microscopy of human blood smears and in sections from normal midbrain and distal ileum. Lrrk2 reactivity was also detected in mesenteric lymph nodes and spleen (including in dendritic cells), but was absent in splenic mononuclear cells from lrrk2-null mice, as expected. In cultured bone marrow-derived macrophages from mice we made three observations: (i) a predominance of higher molecular weight lrrk2; (ii) the reduction of autophagy marker LC3-II in (R1441C)lrrk2-mutant cells (<31%); and (iii) a significant up-regulation of lrrk2 mRNA (>fourfold) and protein after exposure to several microbial structures including bacterial lipopolysaccharide and lentiviral particles. We conclude that Lrrk2 is a constituent of many cell types in the immune system. Following the recognition of microbial structures, stimulated macrophages respond with altered lrrk2 gene expression. In the same cells, lrrk2 appears to co-regulate autophagy. A pattern recognition receptor-type function for LRRK2 could explain its locus' association with Crohn's disease and leprosy risk. We speculate that the role of Lrrk2 in immune cells may also be relevant to the susceptibility of developing PD or its progression.

摘要

LRRK2 基因座的序列变异与三种人类疾病的易感性有关:帕金森病(PD)、克罗恩病和麻风病。由于所有三种疾病均为具有炎症证据的复杂疾病,我们假设 LRRK2 在免疫细胞功能中起作用。在这里,我们报告全长 Lrrk2 是人类外周血单核细胞(PBMC)的常见成分,包括亲和分离的 CD14(+)单核细胞、CD19(+)B 细胞以及 CD4(+)和 CD8(+)T 细胞。来自健康供体的多达 26%的 PBMC 和多达 43%的 CD14(+)单核细胞可通过细胞分选被抗 Lrrk2 抗体染色。PBMC 裂解物含有全长(>260 kDa)和高分子量 Lrrk2 种类。通过人血涂片显微镜检查和正常中脑和远端回肠切片证实循环白细胞中的 LRRK2 表达。LRRK2 反应性也在肠系膜淋巴结和脾脏(包括树突状细胞)中检测到,但在 lrrk2 缺失小鼠的脾单核细胞中缺失,这是预期的。在我们从小鼠骨髓来源的巨噬细胞中进行了三项观察:(i)存在高分子量 lrrk2 的优势;(ii)(R1441C)lrrk2 突变细胞中自噬标记物 LC3-II 的减少(<31%);和(iii)暴露于几种微生物结构后,包括细菌脂多糖和慢病毒颗粒,lrrk2 mRNA(>四倍)和蛋白的显著上调。我们得出结论,LRRK2 是免疫系统中许多细胞类型的组成部分。在识别微生物结构后,受刺激的巨噬细胞会以改变的 lrrk2 基因表达做出反应。在相同的细胞中,lrrk2 似乎共同调节自噬。LRRK2 的模式识别受体样功能可以解释其基因座与克罗恩病和麻风病风险的关联。我们推测,LRRK2 在免疫细胞中的作用也可能与帕金森病的易感性或其进展有关。

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