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The involvement of the substance P/neurokinin 1 receptor system in viral infection: focus on the gp120 fusion protein and homologous dipeptide domains

机译:物质p / neurokinin1受体系统在病毒感染中的参与:专注于GP120融合蛋白和同源二肽域

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摘要

The human immunodeficiency virus (HIV) envelope, via a key extracellular amino acid sequence, may simulate the functionality of native undecapeptide substance P (SP) acting through the host's neurokinin 1 (SP preferring) receptor (NK-1R). Human monocytes and macrophages express both NK-1Rs and SP. In HIV/AIDS the NK-1R may function as a chemokine-like G-protein coupled co-receptor that: 1) fuses to the outer envelope of HIV; 2) enables intracellular entry of the envelope-capsid-NK-1R complex; 3) co-opts immune defence via its physiological interaction with the SP-like envelope; 4) may contribute to resistance of CD4/chemokine entry inhibitor type drugs; 5) relaxes the blood-brain barrier to support entry of the HIV into the central nervous system, and 6) mediates most of the common clinical sequelae of HIV/AIDS (encephalopathy and AIDS dementia complex). The data support the idea that NK-1R antagonists could be useful to treat HIV/AIDS.
机译:通过关键细胞外氨基酸序列的人免疫缺陷病毒(HIV)封套可以模拟通过宿主的神经蛋白1(SP优先)受体(NK-1R)的原生未屠肽物质P(SP)的功能。 人单核细胞和巨噬细胞表达NK-1RS和SP。 在艾滋病毒/艾滋病中,NK-1R可以用作趋化因子样G-蛋白偶联的共同受体,即:1)熔合到HIV的外壳; 2)使包膜 - 衣壳-NK-1R复合物的细胞内入口; 3)通过与SP样外壳的生理相互作用共选择免疫防御; 4)可能有助于CD4 /趋化因子进入抑制剂型药物的抗性; 5)放松血脑屏障,以支持艾滋病毒进入中枢神经系统,6)介导艾滋病毒/艾滋病(脑病和艾滋病痴呆复合物)的大部分常见临床后遗症。 数据支持NK-1R拮抗剂可用于治疗艾滋病毒/艾滋病的想法。

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