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Profile of neuronal exosomes in HIV cognitive impairment exposes sex differences

机译:艾滋病毒认知障碍中神经元外泌体的概况暴露了性差异

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Objective: To use plasma neuron-derived exosomes (NDEs) to detect proteins that diagnose HIV-associated neurocognitive disorders (HAND). To compare NDE cargo from HAND with Alzheimer's disease. Design: Eighty plasma samples were assayed including men (n = 29) and women (n = 51) with and without HAND. Methods: Plasma NDEs were isolated by immunoadsorption with neuron specific L1 cell adhesion molecule antibody. NDE proteins were quantified by ELISA and proximity extension assays for 184 targets. Results: Neuronal enrichment of NDE was confirmed with elevated synaptophysin and normalized to the exosomal marker, apoptosis-linked gene-2-interacting protein X (ALIX). NDE from men and women had significant divergent results. High mobility group box 1 and neurofilament light were significantly increased in NDE from cognitively impaired men and were unchanged in women. NDE from HIV+ men had decreased p-T181-tau, a marker increased in Alzheimer's disease, compared with no difference in women. NDE amyloid beta was not increased in cognitive impairment. Proximity extension assays analysis showed 25 proteins were differentially expressed in HIV infection alone. Seven proteins identified asymptomatic and mild cognitive impairment in HIV+ women. NDE from women had significantly decreased cathepsin S, total tau, neuronal cell adhesion molecule and contactin 5 in mild impairment. Twelve proteins were increased in NDE from cognitively impaired men, including carboxypeptidase M, cadherin 3, colony stimulating factor 2 receptor alpha subunit and mesencephalic astrocyte-derived neurotropic factor. Conclusion: NDE proteins differ in HIV infection alone and cognitive impairment between men and women suggesting mechanistic sex differences associated with HAND. Several NDE targets are different from that reported for Alzheimer's disease.
机译:目的:使用血浆神经元衍生的外泌体(NDES)检测诊断艾滋病毒相关神经认知障碍(手)的蛋白质。将NDE货物与阿尔茨海默病的疾病进行比较。设计:测定八十血浆样品,包括男性(n = 29)和女性(n = 51),无人驾齐。方法:通过用神经元特异性L1细胞粘附分子抗体免疫吸收血浆NDES。 NDE蛋白通过ELISA和184个靶标的邻近延伸测定量定量。结果:NDE的神经元富集用升高的突触蛋白证实并标准化为外泌体标志物,凋亡 - 连接基因-2-相互作用蛋白X(ALIX)。来自男性和女性的NDE具有显着的不同结果。高迁移率组箱1和神经丝光从认知性受损的男性中显着增加,并且在女性中没有变化。来自艾滋病毒+男性的NDE已经减少了P-T181-Tau,在阿尔茨海默病的疾病中增加了标志物,而女性没有差异。 NDE淀粉样蛋白β未在认知障碍中增加。接近延伸测定分析显示25种蛋白质单独用HIV感染差异表达。七种蛋白质鉴定了艾滋病毒+女性中的无症状和轻度认知障碍。来自妇女的NDE在轻度损伤中显着降低了组织蛋白酶,TAU,TAU,神经元细胞粘附分子和接触5。 NDE从认知受损的男性中增加12个蛋白质,包括羧肽酶M,Cadherin 3,菌落刺激因子2受体α亚基和脑脑偶数星形细胞衍生的神经疗法因子。结论:NDE蛋白在单独艾滋病毒感染和男女之间的认知障碍,暗示与手相关的机械性别差异。几个NDE靶标不同于阿尔茨海默病的报告。

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