Plasma Serotonin 2A Receptor Autoantibodies Predict Rapid, Substantial Decline in Neurocognitive Performance in Older Adult Veterans with TBI.

Mark B Zimering, Mihal Grinberg, Catherine E Myers, Gideon Bahn
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Abstract

Aim: Traumatic brain injury (TBI) was associated with increased plasma serotonin 2A receptor (5-HT2AR) autoantibodies in adults who experienced neurodegenerative complications. We tested whether the baseline presence of plasma serotonin 2A receptor (5-HT2AR) autoantibodies was a significant predictor of the two-year rate of cognitive decline in middle-aged and older adult TBI.

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. One-fortieth dilution of the resulting immunoglobulin (Ig) G fraction was tested for binding (in ELISA) to a linear synthetic peptide corresponding to the second extracellular loop region of the human 5-HT2A receptor. All available patients completed baseline and two-year follow-up neurocognitive tests of memory (St Louis University Mental Status), processing speed (Digit Symbol Substitution Test) and executive function (Trails-making Test, Part B). Change in cognitive performance was computed as (two-year - baseline) raw test score.

Results: Eighteen patients completed both baseline and two-year follow up neurocognitive tests. TBI patients harboring plasma 5-HT2AR autoantibodies at the baseline examination (n=13) did not differ significantly in their baseline clinical characteristics (age, education level) compared to TBI patients lacking baseline plasma autoantibodies (n=5). Plasma serotonin 2AR antibody-positive patients experienced a significantly greater post-baseline decline in performance on the St Louis University Mental Status test (P=0.0118) and in the Digit Symbol Substitution Test (P=0.011), but not in Trails-making Part B (P=0.129) compared to serotonin 2AR antibody-negative patients. In multivariable linear regression analyses that adjusted for age, baseline presence of plasma 5-HT2AR autoantibody was a significant predictor of the two-year rate of decline in memory, and processing speed. Binding of plasma autoantibody to the serotonin 2A receptor peptide in the enzyme linked immunosorbent assay was also significantly higher (at 1/160th titer of the protein-A eluate= 1 μg/mL IgG) in TBI patients harboring vs. those not harboring baseline plasma 5-HT2AR autoantibodies.

Conclusion: These data suggest that plasma 5-hydroxytryptamine 2A receptor autoantibodies which were increased in approximately two-thirds of middle-aged and older adults following traumatic brain injury predicts rapid and substantial declines in cognitive function (memory and processing speed), independent of age.

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血浆5 -羟色胺2A受体自身抗体预测老年创伤性脑损伤退伍军人神经认知能力的快速、实质性下降。
目的:创伤性脑损伤(TBI)与经历神经退行性并发症的成人血浆5-羟色胺2A受体(5-HT2AR)自身抗体升高相关。我们测试了血浆5-羟色胺2A受体(5-HT2AR)自身抗体的基线存在是否是中老年TBI患者两年认知能力下降率的重要预测因子。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。将所得免疫球蛋白(Ig) G部分稀释四十分之一,检测其与与人5-HT2A受体第二细胞外环区对应的线性合成肽的结合(ELISA)。所有患者均完成了基线和两年随访的神经认知测试,包括记忆(圣路易斯大学精神状态)、处理速度(数字符号替代测试)和执行功能(轨迹制作测试,B部分)。认知表现的变化以(两年基线)原始测试分数计算。结果:18例患者完成了基线和两年随访的神经认知测试。在基线检查中携带血浆5- ht2ar自身抗体的TBI患者(n=13)与缺乏基线血浆自身抗体的TBI患者(n=5)相比,其基线临床特征(年龄,教育水平)没有显着差异。血浆5 -羟色胺2AR抗体阳性的患者在圣路易斯大学精神状态测试(P=0.0118)和数字符号替代测试(P=0.011)中的表现在基线后明显下降,但与5 -羟色胺2AR抗体阴性的患者相比,在trail -making Part B中没有(P=0.129)。在调整年龄的多变量线性回归分析中,血浆5-HT2AR自身抗体的基线存在是两年记忆和处理速度下降率的重要预测因子。在酶联免疫吸附试验中,携带血浆5-HT2AR自身抗体的TBI患者血浆自身抗体与血清素2A受体肽的结合也显著高于未携带基线血浆5-HT2AR自身抗体的TBI患者(蛋白a洗脱液的1/160滴度= 1 μg/mL IgG)。结论:这些数据表明,大约三分之二的中老年人在创伤性脑损伤后血浆5-羟色胺2A受体自身抗体增加,这预示着认知功能(记忆和处理速度)的快速和实质性下降,与年龄无关。
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