Constitutive expression of HIV-1 viral proteins induces progressive synaptodendritic alterations in medium spiny neurons: implications for substance use disorders

K. McLaurin, Hailong Li, C. Mactutus, R. Booze
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引用次数: 1

Abstract

Abstract Objectives Perinatally-infected adolescents living with HIV-1 (pALHIV) appear uniquely vulnerable to developing substance use disorders (SUD). Medium spiny neurons (MSNs) in the nucleus accumbens core (NAcc), an integrator of cortical and thalamic input, have been implicated as a key structural locus for the pathogenesis of SUD. To date, however, how constitutive expression of HIV-1 viral proteins alters the development of MSNs in the NAcc has not been systematically evaluated. Methods An innovative ballistic labeling technique was utilized to examine MSNs in the NAcc, and associated dendritic spines, in HIV-1 transgenic (Tg) and control animals. First, a time-sequential longitudinal experimental design was implemented, whereby animals were sacrificed at 30-day intervals from postnatal day (PD) 30 to PD 180. Second, the therapeutic efficacy of S-Equol for HIV-1-associated synaptic dysfunction in MSNs was evaluated using a cross-sectional experimental design. Results Constitutive expression of HIV-1 viral proteins disrupted the development of MSNs, evidenced by alterations in neuritogenesis and synaptogenesis. Furthermore, age-related, progressive synaptodendritic alterations were observed in the patterning of dendritic branches and dendritic spines, as well as dendritic spine head diameter, in HIV-1 Tg, relative to control, animals. Treatment with S-Equol during the formative period, however, led to long-term enhancements in synaptic function (i.e., PD 180). Conclusions Developmental and progressive synaptodendritic alterations in MSNs induced by chronic HIV-1 viral protein exposure may underlie the increased propensity for pALHIV to develop SUD. Elucidating a potential neural mechanism underlying the unique vulnerability of pALHIV to SUD affords a fundamental opportunity for the evaluation of therapeutics.
HIV-1病毒蛋白的组成型表达诱导中棘神经元进行性突触树突改变:与物质使用障碍的关系
摘要目的围产期感染的HIV-1(pALHIV)青少年似乎特别容易患上物质使用障碍(SUD)。伏隔核核心(NAcc)中的中棘神经元(MSNs)是皮层和丘脑输入的整合器,被认为是SUD发病机制的关键结构位点。然而,到目前为止,HIV-1病毒蛋白的组成型表达如何改变NAcc中MSNs的发育尚未得到系统评估。方法采用创新的弹道标记技术检测HIV-1转基因(Tg)和对照动物的NAcc和相关树突棘中的MSNs。首先,实施时间序列纵向实验设计,从出生后第30天(PD)到第180天,每隔30天处死动物。其次,使用横断面实验设计评估了S-Equol对MSNs中HIV-1相关突触功能障碍的治疗效果。结果HIV-1病毒蛋白的组成型表达破坏了MSNs的发育,神经炎发生和突触发生的改变证明了这一点。此外,与对照组相比,在HIV-1Tg动物的树突分支和树突棘的模式以及树突棘头部直径中观察到与年龄相关的进行性突触树突改变。然而,在形成期用S-Equol治疗会导致突触功能的长期增强(即PD 180)。结论慢性HIV-1病毒蛋白暴露诱导的MSNs的发育和进行性突触树突改变可能是pALHIV发展为SUD倾向增加的原因。阐明pALHIV对SUD独特脆弱性的潜在神经机制为评估治疗方法提供了基本机会。
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