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患有持续性长新冠症状患者体内针对G蛋白偶联受体的功能性自身抗体。

Functional autoantibodies against G-protein coupled receptors in patients with persistent Long-COVID-19 symptoms.

作者信息

Wallukat Gerd, Hohberger Bettina, Wenzel Katrin, Fürst Julia, Schulze-Rothe Sarah, Wallukat Anne, Hönicke Anne-Sophie, Müller Johannes

机构信息

Experimental and Clinical Research Center, Charité Campus Buch, Max-Delbrück Center for Molecular Medicine, Berlin, Germany.

Berlin Cures GmbH, Berlin; Germany.

出版信息

J Transl Autoimmun. 2021;4:100100. doi: 10.1016/j.jtauto.2021.100100. Epub 2021 Apr 16.

Abstract

Impairment of health after overcoming the acute phase of COVID-19 is being observed more and more frequently. Here different symptoms of neurological and/or cardiological origin have been reported. With symptoms, which are very similar to the ones reported but are not caused by SARS-CoV-2, the occurrence of functionally active autoantibodies (AABs) targeting G-protein coupled receptors (GPCR-AABs) has been discussed to be involved. We, therefore investigated, whether GPCR-AABs are detectable in 31 patients suffering from different Long-COVID-19 symptoms after recovery from the acute phase of the disease. The spectrum of symptoms was mostly of neurological origin (29/31 patients), including post-COVID-19 fatigue, alopecia, attention deficit, tremor and others. Combined neurological and cardiovascular disorders were reported in 17 of the 31 patients. Two recovered COVID-19 patients were free of follow-up symptoms. All 31 former COVID-19 patients had between 2 and 7 different GPCR-AABs that acted as receptor agonists. Some of those GPCR-AABs activate their target receptors which cause a positive chronotropic effect in neonatal rat cardiomyocytes, the read-out in the test system for their detection (bioassay for GPCR-AAB detection). Other GPCR-AABs, in opposite, cause a negative chronotropic effect on those cells. The positive chronotropic GPCR-AABs identified in the blood of Long-COVID patients targeted the β-adrenoceptor (β-AAB), the α-adrenoceptor (α-AAB), the angiotensin II AT1-receptor (AT1-AAB), and the nociceptin-like opioid receptor (NOC-AAB). The negative chronotropic GPCR-AABs identified targeted the muscarinic M-receptor (M-AAB), the MAS-receptor (MAS-AAB), and the ETA-receptor (ETA-AAB). It was analysed which of the extracellular receptor loops was targeted by the autoantibodies.

摘要

在克服新冠病毒病急性期后出现健康损害的情况越来越常见。在此,已报告了不同的神经和/或心脏来源的症状。对于那些与所报告症状非常相似但并非由严重急性呼吸综合征冠状病毒2(SARS-CoV-2)引起的症状,有人讨论认为靶向G蛋白偶联受体的功能性自身抗体(AABs,即GPCR-AABs)的出现与之有关。因此,我们调查了31例在从疾病急性期康复后患有不同新冠后综合征症状的患者中是否能检测到GPCR-AABs。症状谱大多源于神经方面(29/31例患者),包括新冠后疲劳、脱发、注意力缺陷、震颤等。31例患者中有17例报告有神经和心血管联合障碍。两名康复的新冠患者没有后续症状。所有31例曾患新冠的患者有2至7种不同的作为受体激动剂的GPCR-AABs。其中一些GPCR-AABs激活其靶受体,在新生大鼠心肌细胞中产生正性变时效应,这是检测它们的测试系统中的读出指标(用于GPCR-AAB检测的生物测定)。相反,其他GPCR-AABs对这些细胞产生负性变时效应。在新冠后患者血液中鉴定出的产生正性变时效应的GPCR-AABs靶向β肾上腺素能受体(β-AAB)、α肾上腺素能受体(α-AAB)、血管紧张素II AT1受体(AT1-AAB)和孤啡肽样阿片受体(NOC-AAB)。鉴定出的产生负性变时效应的GPCR-AABs靶向毒蕈碱M受体(M-AAB)、MAS受体(MAS-AAB)和ETA受体(ETA-AAB)。分析了自身抗体靶向细胞外受体环中的哪一个。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2bd7/8094909/b8174e105f29/gr1.jpg

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