Rho GTPase 激活蛋白 10（ARHGAP10/GRAF2）是自身免疫性脑炎患者的一种新的自身抗体靶标。

Rho GTPase-activating protein 10 (ARHGAP10/GRAF2) is a novel autoantibody target in patients with autoimmune encephalitis.

机构信息

Molecular Neuroimmunology Group, Department of Neurology, University of Heidelberg, Heidelberg, Germany.

Institute for Experimental Immunology, EUROIMMUN Medizinische Labordiagnostika AG, Lübeck, Germany.

出版信息

J Neurol. 2022 Oct;269(10):5420-5430. doi: 10.1007/s00415-022-11178-9. Epub 2022 May 27.

DOI:10.1007/s00415-022-11178-9

PMID:35624318

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9468106/

Abstract

BACKGROUND

In 2010, we described a novel immunoglobulin G (IgG) autoantibody (termed anti-Ca after the index case) targeting Rho GTPase-activating protein 26 (ARHGAP26, also termed GTPase regulator associated with focal adhesion kinase [GRAF], or oligophrenin-like protein 1 [OPHN1L]) in autoimmune cerebellar ataxia (ACA). Later, ARHGAP26-IgG/anti-Ca was reported in patients with limbic encephalitis/cognitive decline or peripheral neuropathy. In several of the reported cases, the syndrome was associated with cancer. ARHGAP10/GRAF2, which is expressed throughout the central nervous system, shares significant sequence homology with ARHGAP26/GRAF. Mutations in the ARHGAP10 gene have been linked to cognitive and psychiatric symptoms and schizophrenia.

OBJECTIVE

To assess whether ARHGAP26-IgG/anti-Ca co-reacts with ARHGAP10.

METHODS

Serological testing for ARHGAP10/GRAF2 autoantibodies by recombinant cell-based assays and isotype and IgG subclass analyses.

RESULTS

26/31 serum samples (84%) from 9/12 (75%) ARHGAP26-IgG/anti-Ca-positive patients and 4/6 ARHGAP26-IgG/anti-Ca-positive CSF samples from four patients were positive also for ARHGAP10-IgG. ARHGAP10-IgG (termed anti-Ca2) remained detectable in the long-term (up to 109 months) and belonged mainly to the complement-activating IgG1 subclass. Median ARHGAP26-IgG/anti-Ca and median ARHGAP10-IgG/anti-Ca2 serum titres were 1:3200 and 1:1000, respectively, with extraordinarily high titres in some samples (ARHGAP26-IgG/anti-Ca: up to 1:1000,000; ARHGAP10-IgG: up to 1:32,000). ARHGAP26/anti-Ca serum titres exceeded those of ARHGAP10-IgG in all samples but one. A subset of patients was positive also for ARHGAP10-IgM and ARHGAP10-IgA. CSF/serum ratios and antibody index calculation suggested intrathecal production of ARHGAP26-IgG/anti-Ca and anti-ARHGAP10. Of 101 control samples, 100 were completely negative for ARHGAP10-IgG; a single control sample bound weakly (1:10) to the ARHGAP10-transfected cells.

CONCLUSIONS

We demonstrate that a substantial proportion of patients with ARHGAP26-IgG/anti-Ca-positive autoimmune encephalitis co-react with ARHGAP10. Further studies on the clinical and diagnostic implications of ARHGAP10-IgG/anti-Ca2 seropositivity in patients with autoimmune encephalitis are warranted.

摘要

背景

2010 年，我们在自身免疫性小脑性共济失调（ACA）患者中描述了一种新型免疫球蛋白 G（IgG）自身抗体（以索引病例命名为抗-Ca），该抗体靶向 Rho GTPase 激活蛋白 26（ARHGAP26，也称为与焦点黏附激酶相关的 GTPase 调节因子 [GRAF]或寡脑蛋白样蛋白 1 [OPHN1L]）。后来，在边缘性脑炎/认知能力下降或周围神经病患者中也报告了 ARHGAP26-IgG/抗-Ca。在一些报告的病例中，该综合征与癌症有关。ARHGAP10/GRAF2 在中枢神经系统中广泛表达，与 ARHGAP26/GRAF 具有显著的序列同源性。ARHGAP10 基因的突变与认知和精神症状以及精神分裂症有关。

目的

评估 ARHGAP26-IgG/抗-Ca 是否与 ARHGAP10 共同反应。

方法

通过重组细胞基础检测和同种型和 IgG 亚类分析对 ARHGAP10/GRAF2 自身抗体进行血清学检测。

结果

9/12（75%）ARHGAP26-IgG/抗-Ca 阳性患者的 31 份血清样本（84%）和 4 名患者的 4/6 份 ARHGAP26-IgG/抗-Ca 阳性脑脊液样本中，有 26 份（84%）也呈 ARHGAP10-IgG 阳性。ARHGAP10-IgG（称为抗-Ca2）在很长一段时间内（长达 109 个月）仍然可检测到，主要属于补体激活的 IgG1 亚类。中位 ARHGAP26-IgG/抗-Ca 和 ARHGAP10-IgG/抗-Ca2 血清滴度分别为 1:3200 和 1:1000，一些样本的滴度非常高（ARHGAP26-IgG/抗-Ca：高达 1:1000000；ARHGAP10-IgG：高达 1:32000）。所有样本中 ARHGAP26/抗-Ca 血清滴度均高于 ARHGAP10-IgG，但有一个样本除外。一部分患者还呈 ARHGAP10-IgM 和 ARHGAP10-IgA 阳性。CSF/血清比值和抗体指数计算提示 ARHGAP26-IgG/抗-Ca 和抗-ARHGAP10 的鞘内产生。在 101 份对照样本中，100 份完全为 ARHGAP10-IgG 阴性；一份对照样本与转染的 ARHGAP10 细胞弱结合（1:10）。