Neuroinflammation and EIF2 Signaling Persist despite Antiretroviral Treatment in an hiPSC Tri-culture Model of HIV Infection

在HIP感染的hiPSC三培养模型中,尽管接受了抗逆转录病毒治疗,神经炎症和EIF2信号通路仍然持续存在。

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作者:Sean K Ryan ,Michael V Gonzalez ,James P Garifallou ,Frederick C Bennett ,Kimberly S Williams ,Nathaniel P Sotuyo ,Eugene Mironets ,Kieona Cook ,Hakon Hakonarson ,Stewart A Anderson ,Kelly L Jordan-Sciutto

Abstract

HIV-associated neurocognitive disorders (HAND) affect over half of HIV-infected individuals, despite antiretroviral therapy (ART). Therapeutically targetable mechanisms underlying HAND remain elusive, partly due to a lack of a representative model. We developed a human-induced pluripotent stem cell (hiPSC)-based model, independently differentiating hiPSCs into neurons, astrocytes, and microglia, and systematically combining to generate a tri-culture with or without HIV infection and ART. Single-cell RNA sequencing analysis on tri-cultures with HIV-infected microglia revealed inflammatory signatures in the microglia and EIF2 signaling in all three cell types. Treatment with the antiretroviral compound efavirenz (EFZ) mostly resolved these signatures. However, EFZ increased RhoGDI and CD40 signaling in the HIV-infected microglia. This activation was associated with a persistent increase in transforming growth factor α production by microglia. This work establishes a tri-culture that recapitulates key features of HIV infection in the CNS and provides a new model to examine the effects of infection, its treatment, and other co-morbid conditions. Keywords: EIF2; HIV; astrocyte; efavirenz; hiPSC; microglia; model; neuroinflammation; neuron; tri-culture.

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