蛇床子素减轻HIV gp120诱发的周围神经病理痛

目的探讨蛇床子素(osthole,Ost)对背根神经节(dorsal root ganglia, DRG)P2X_3受体(P2X_3R)介导人类免疫缺陷病毒(human immunodeficiency virus,HIV)包膜糖蛋白gp120诱发周围神经病理痛的作用及机制。方法建立HIV gp120诱发周围神经病理痛大鼠模型,其中Ost给药组大鼠于建模术前7 d至术后14 d灌胃给药(40 mg·kg^(-1)·d^(-1))。检测各组大鼠机械痛缩足反射阈值(PWT)与热痛缩足反射潜伏期(PWL);实时定量PCR、蛋白印迹、免疫组化等方法检测DRG中神经元P2X_3R、炎性因子及ERK、p-ERK等的表达;全细胞膜片钳检测HEK293细胞三磷酸腺苷(ATP)激活电流及Ost对电流的影响。结果 gp120组大鼠PWT、PWL较假手术组(sham)减小,大鼠DRG中P2X_3R、TNF-αR及p-ERK表达均较sham组明显升高;gp120+Ost组大鼠PWT、PWL较gp120组增大,大鼠DRG中P2X_3R、TNF-αR及p-ERK表达均较gp120组降低;Ost抑制了转染人P2X_3R的HEK293细胞ATP激动电流。结论 Ost下调DRG神经元中P2X_3R,抑制相关信号通路与炎性反应,减轻gp120诱发的周围神经病理痛。

人类免疫缺陷病毒相关神经病理性疼痛的病理生理学机制

人类免疫缺陷病毒(human immunodeficiency virus,HIV)相关的感觉神经病变(HIV-related sensory neuropathy,HIV-SN)主要包含HIV感染引起的远端感觉多神经病变(distal sensory polyneuropathy,DSP)和抗逆转录病毒毒性神经病变(antiretroviral toxic neuropathies,ATN)。文中主要阐述了HIV-DSP可能与gp120诱导产生的促炎细胞因子、趋化因子、活性氧及P物质有关,而HIV-ATN则可能与应用dd C等抗逆转录病毒药物引发的线粒体毒性及小胶质细胞增生有关,并且与HIVDSP的分子机制类似,这意味着目前治疗艾滋病的常规方法可能会进一步加重患者的神经病理性疼痛。因此,开展HIV相关神经病理性疼痛的神经化学和药理机制的研究,将为其新型有效治疗药物提供新的作用靶点。

首个HIV-1附着抑制剂Fostemsavir研究进展

目的为临床应用fostemsavir治疗1型人免疫缺陷病毒(HIV-1)感染提供参考。方法归纳HIV-1附着抑制剂fostemsavir的作用机制、药物代谢动力学、临床试验及不良反应/不良事件的研究进展。结果Fostemsavir可通过与糖蛋白120结合而阻止病毒附着;临床研究结果显示,其对HIV-1具有良好的抗病毒活性,耐受性良好,不良反应多为轻度,且发生率与类似抗逆转录病毒(ARV)药物一致。结论Fostemsavir作用靶点明确,临床研究数据充分,具有独特的抗耐药性,可与其他ARV药物联用,适用于因耐药、药物不耐受或安全性问题而治疗失败的HIV-1成年感染者。

抗人免疫缺陷病毒1型gp120人源单链抗体的表达

目的研究人源抗人免疫缺陷病毒１型（ＨＩＶ－１）ｇｐ１２０单链抗体（ＳｃＦｖ）。方法以人工合成的ＨＩＶ－ｌｇｐ１２０Ｖ３环多肽为抗原，利用噬菌体抗体库技术，筛选含有抗－ｇｐ１２０ＳｃＦｖ基因的噬菌体，提取质粒，转化大肠杆菌ＨＢ２１５１，表达可溶性ＳｃＦｖ。结果经ＳＤＳ－ＰＡＧＥ和Ｗｅｓｔｅｒｎｂｌｏｔ分析，表达产物分子量为２８ｋＤ左右，且具有ｃ－ｍｙｃ活性；ＥＬＩＳＡ和Ｄｏｔｂｌｏｔ结果表明，可溶性ＳｃＦｖ具有较好的抗原结合活性和较强的特异性；竞争性ＥＬＩＳＡ实验结果进一步证明表达产物的特异抗－ｇｐ１２０活性。结论该技术便捷有效，可大量获得人源抗ＨＩＶ抗体片段。

UM15 reinforces a lymphocyte-mimicking nanotrap for precise HIV-1 inhibition

Even the potential of T cell-mimicking nanotrap for long term viral control due to its overcoming of human immunodeficiency virus(HIV)genetic diversity and viral resistance,the robust HIV inhibition was not expected because these nanotraps displayed no obvious advantages compared with the infinite host cells.Herein,a glycoprotein 120(gp120)-targeting polypeptide UM15 reinforced lymphocyte-mimicking nanotrap was constructed,and its improved HIV-1 inhibiting efficacy was validated.According to the results,the constructed nanotraps exhibited evident escaping ability from uptake of the mononuclear phagocyte system and highly improved binding ability with gp120 proteins.The constructed nanotraps neutralized all tested HIV-1 pseudo typed viruses with IC80 of 21.0μg/mL,and inhibited both X4-tropic and R5-tropic HIV-1 with IC80 of 34.4 and 20.6μg/mL,respectively.Approximately 40%of gp120 was observed to be shed from pseudo virus,and above 40%bystander T cells were prevented from gp120-induced death by the constructed nanotraps.The safety of the constructed nanotraps was confirmed both in vitro and in mice.Therefore,the constructed nanotraps could specifically neutralize free HIV-1,selectively bind with gp120 expressing HIV-1 infected cells,cause gp120 shedding,inhibit gp120-induced bystander T cell killing on the premise of safety,and were considered as promising therapeutic agents for precise inhibition of HIV.