成人创伤性脑损伤与神经变性相关的血清素2A受体自身抗体增加

Journal of endocrinology and diabetes Pub Date : 2020-04-07

Mark B Zimering, Amy T Pulikeyil, Catherine E Myers, Kevin C Pang

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摘要

目的:创伤性脑损伤(TBI)通过未知的机制与晚期神经退行性并发症的风险增加相关。据报道，循环神经毒性5-羟色胺2A受体(5-HT2AR)自身抗体在有微血管并发症的肥胖2型糖尿病亚群中增加。我们测试了5-HT2AR自身抗体在创伤性脑损伤后是否与神经退行性并发症相关。方法:对35例创伤性脑损伤的中老年退伍军人(平均65岁)的血浆进行蛋白-a亲和层析。所得免疫球蛋白(Ig) G部分在小鼠N2A神经母细胞瘤细胞中进行了神经毒性(急性神经突退缩和加速细胞死亡)测试，或与与人类5-HT2A受体第二细胞外环区域对应的线性合成肽结合。结果:近三分之二的外伤性脑损伤患者循环中存在5-HT2AR自身抗体。活性TBI自身抗体引起小鼠N2A神经母细胞瘤细胞的神经突缩回，并加速N2A细胞的损失，通过与250纳摩尔浓度的M100907(一种高选择性5-HT2AR拮抗剂)共孵育，可以有效地预防这种情况。RhoA/Rho激酶和Gq11/磷脂酶C/肌醇三磷酸受体信号通路拮抗剂阻断TBI自身抗体诱导的神经突收缩。创伤性脑损伤后，合并帕金森病(n=3)、痴呆(n=5)和疼痛性神经病变(n=8)的患者自身抗体结合5- ht2a受体肽的水平明显高于无神经或微血管并发症的TBI亚群(n=20)。自身抗体滴度在经历多次神经创伤的TBI亚群中显著升高，而不是单一的TBI。血浆白细胞是全身性炎症的标志物，两者相关性显著(相关系数r =0.52;P < 0.01)与tbi自身抗体的5-HT2A受体肽结合。结论:这些数据表明，成人外伤性脑损伤后循环神经毒性5-羟色胺2A受体激动剂自身抗体增加与晚期神经退行性并发症有关。

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Serotonin 2A Receptor Autoantibodies Increase in Adult Traumatic Brain Injury In Association with Neurodegeneration.

Objective: Traumatic brain injury (TBI) is associated with an increased risk of late neurodegenerative complications via unknown mechanisms. Circulating neurotoxic 5-hydroxytryptamine 2A receptor (5-HT2AR) autoantibodies were reported to increase in subsets of obese type 2 diabetes having microvascular complications. We tested whether 5-HT2AR autoantibodies increase in adults following traumatic brain injury in association with neurodegenerative complications.

Methods: Plasma from thirty-five middle-aged and older adult veterans (mean 65 years old) who had suffered traumatic brain injury was subjected to protein-A affinity chromatography. The resulting immunoglobulin (Ig) G fraction was tested for neurotoxicity (acute neurite retraction, and accelerated cell death) in mouse N2A neuroblastoma cells or for binding to a linear synthetic peptide corresponding to the second extracellular loop region of the human 5-HT2A receptor.

Results: Nearly two-thirds of traumatic brain injured-patients harbored 5-HT2AR autoantibodies in their circulation. Active TBI autoantibodies caused neurite retraction in mouse N2A neuroblastoma cells and accelerated N2A cell loss which was substantially prevented by co-incubation with a two hundred and fifty nanomolar concentration of M100907, a highly selective 5-HT2AR antagonist. Antagonists of RhoA/Rho kinase and Gq11/phospholipase C/inositol triphosphate receptor signaling pathways blocked TBI autoantibody-induced neurite retraction. Following traumatic brain injury, autoantibody binding to a 5-HT2A receptor peptide was significantly increased in patients having co-morbid Parkinson's disease (n=3), dementia (n=5), and painful neuropathy (n=8) compared to TBI subsets without neurologic or microvascular complication (n=20). Autoantibody titer was significantly elevated in TBI subsets experiencing multiple neurotraumatic exposures vs. single TBI. Plasma white blood cell, a marker of systemic inflammation, correlated significantly (correlation coefficient r =0.52; P < 0.01) with, 5-HT2A receptor peptide binding of the TBI-autoantibody.

Conclusion: These data suggest that circulating neurotoxic 5-hydroxytryptamine 2A receptor agonist autoantibodies increase in adults following traumatic brain injury in association with late neurodegenerative complications.

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Journal of endocrinology and diabetes

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