4.6 Article

New human in vitro co-culture model of keratinocytes and sensory neurons like cells releasing substance P with an evaluation of the expression of ZIKV entry receptors: A potent opportunity to test Zika virus entry and to study Zika virus' infection in neurons?

期刊

EXPERIMENTAL DERMATOLOGY
卷 32, 期 9, 页码 1563-1568

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WILEY
DOI: 10.1111/exd.14870

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itch; neuropeptides; receptors; sensory neurons; virus; Zika

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Pruritus is a common symptom during acute ZIKV infection and is often associated with dysautonomic manifestations, suggesting involvement of the peripheral nervous system. This study aimed to develop a functional human model for ZIKV infection by co-culturing keratinocytes and sensory neurons derived from induced pluripotent stem cells. The expression of ZIKV entry receptors in these cells indicates the potential for ZIKV infection.
During the course of acute ZIKV infection, pruritus is a cardinal symptom widely documented in the literature. Its frequent association with dysesthesia and several dysautonomic manifestations, suggests a pathophysiological mechanism involving the peripheral nervous system. The aim of this study was to develop a functional human model to potentially able to be infected by ZIKV: by demonstrating the functionality on a new human model of co-culture of keratinocyte and sensory neuron derived from induced pluripotent stem cells using a classical method of capsaicin induction and SP release, and verify the presence of ZIKV entry receptor in these cells. Depending of cellular type, receptors of the TAMs family, TIMs (TIM1, TIM3 and TIM4) and DC-SIGN and RIG1 were present/detected. The cells incubations with capsaicin resulted in an increase of the substance P. Hence, this study demonstrated the possibility to obtain co-cultures of human keratinocytes and human sensory neurons that release substance P in the same way than previously published in animal models which can be used as a model of neurogenic skin inflammation. The demonstration of the expression of ZIKV entry receptors in these cells allows to considerate the potent possibility that ZIKV is able to infect cells.

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