HIV糖蛋白Gp120通过激活Tak1信号通路损害快速轴突运输

IF 3.9 4区 医学 Q2 NEUROSCIENCES ASN NEURO Pub Date : 2016-11-01 DOI:10.1177/1759091416679073
S. Berth, Nichole A. Mesnard-Hoaglin, Bin Wang, Hajwa Kim, Yuyu Song, Maria L. Sapar, G. Morfini, S. Brady
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引用次数: 7

摘要

感觉神经病变是HIV最常见的神经系统并发症。其中,远端感觉多神经病变(DSP)是由HIV感染直接引起的,其特征是背根神经节(DRG)神经元的长度依赖性轴突变性。DSP轴突变性的机制尚不清楚,但最近的实验表明,HIV糖蛋白gp120内化并定位于DRG神经元的轴突内。基于这些发现,我们研究了轴突内gp120是否可能损害快速轴突运输(FAT),这是一个对轴突室适当维持至关重要的细胞过程。值得注意的是,我们发现gp120严重损害了顺行和逆行的FAT。药理学实验为这些作用提供了机制基础,揭示了多种磷酸转移酶参与了这种毒性作用,包括丝裂原活化蛋白激酶途径的成员(Tak-1、p38和c-Jun n-末端激酶(JNK))、kappa- b -激酶2 (IKK2)抑制剂和PP1。细胞系和原代培养物的生化实验和轴突生长测定进一步证实了这些发现。gp120对DRG神经元神经突生长的损伤可通过Tak-1抑制剂修复,这表明Tak-1有丝分裂原激活的蛋白激酶途径与gp120神经毒性有关。综上所述,这些观察结果表明,FAT中基于激酶的损伤代表了gp120神经毒性的新机制,与DSP中所见的枯死变性一致。用特异性激酶抑制剂靶向脂肪中基于gp120的损伤可能为预防DSP轴突变性提供一种新的治疗策略。
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HIV Glycoprotein Gp120 Impairs Fast Axonal Transport by Activating Tak1 Signaling Pathways
Sensory neuropathies are the most common neurological complication of HIV. Of these, distal sensory polyneuropathy (DSP) is directly caused by HIV infection and characterized by length-dependent axonal degeneration of dorsal root ganglion (DRG) neurons. Mechanisms for axonal degeneration in DSP remain unclear, but recent experiments revealed that the HIV glycoprotein gp120 is internalized and localized within axons of DRG neurons. Based on these findings, we investigated whether intra-axonal gp120 might impair fast axonal transport (FAT), a cellular process critical for appropriate maintenance of the axonal compartment. Significantly, we found that gp120 severely impaired both anterograde and retrograde FAT. Providing a mechanistic basis for these effects, pharmacological experiments revealed an involvement of various phosphotransferases in this toxic effect, including members of mitogen-activated protein kinase pathways (Tak-1, p38, and c-Jun N-terminal Kinase (JNK)), inhibitor of kappa-B-kinase 2 (IKK2), and PP1. Biochemical experiments and axonal outgrowth assays in cell lines and primary cultures extended these findings. Impairments in neurite outgrowth in DRG neurons by gp120 were rescued using a Tak-1 inhibitor, implicating a Tak-1 mitogen-activated protein kinase pathway in gp120 neurotoxicity. Taken together, these observations indicate that kinase-based impairments in FAT represent a novel mechanism underlying gp120 neurotoxicity consistent with the dying-back degeneration seen in DSP. Targeting gp120-based impairments in FAT with specific kinase inhibitors might provide a novel therapeutic strategy to prevent axonal degeneration in DSP.
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来源期刊
ASN NEURO
ASN NEURO NEUROSCIENCES-
CiteScore
7.70
自引率
4.30%
发文量
35
审稿时长
>12 weeks
期刊介绍: ASN NEURO is an open access, peer-reviewed journal uniquely positioned to provide investigators with the most recent advances across the breadth of the cellular and molecular neurosciences. The official journal of the American Society for Neurochemistry, ASN NEURO is dedicated to the promotion, support, and facilitation of communication among cellular and molecular neuroscientists of all specializations.
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