INSERM, U1043, Toulouse, France.
CNRS, U5282, Toulouse, France.
Sci Rep. 2018 Nov 21;8(1):17215. doi: 10.1038/s41598-018-35478-1.
Human HIV-1 infection leads inevitably to a chronic hyper-immune-activation. However, the nature of the targeted receptors and the pathways involved remain to be fully elucidated. We demonstrate that X4-tropic gp120 induced the production of TNF-α and IL-10 by monocytes through activation of a cell membrane receptor, distinct from the CD4, CXCR4, and MR receptors. Gp120 failed to stimulate IL-10 and TNF-α production by monocytes in Ca free medium. This failure was total for IL-10 and partial for TNF-α. However, IL-10 and TNF-α production was fully restored following the addition of exogenous calcium. Accordingly, addition of BAPTA-AM and cyclosporine-A, fully and partially inhibited IL-10 and TNF-α respectively. The PKA pathway was crucial for IL-10 production but only partially involved in gp120-induced TNF-α. The PLC pathway was partially and equivalently involved in gp120-induced TNF-α and IL-10. Moreover, the inhibition of PI3K, ERK1/2, p38 MAP-kinases and NF-κB pathways totally abolished the production of both cytokines. In conclusion, this study revealed the crucial calcium signaling pathway triggered by HIV-1 gp120 to control the production of these two cytokines: TNF-α and IL-10. The finding could help in the development of a new therapeutic strategy to alleviate the chronic hyper-immune-activation observed in HIV-1 infected patients.
人类 HIV-1 感染不可避免地导致慢性超免疫激活。然而,目标受体的性质和涉及的途径仍有待充分阐明。我们证明,X4 嗜性 gp120 通过激活不同于 CD4、CXCR4 和 MR 受体的细胞膜受体诱导单核细胞产生 TNF-α 和 IL-10。gp120 不能在无 Ca2+ 培养基中刺激单核细胞产生 IL-10 和 TNF-α。这种失败对于 IL-10 是完全的,对于 TNF-α 是部分的。然而,添加外源性钙完全恢复了 IL-10 和 TNF-α 的产生。因此,添加 BAPTA-AM 和环孢菌素 A 分别完全和部分抑制了 IL-10 和 TNF-α 的产生。PKA 途径对于 IL-10 的产生至关重要,但仅部分参与 gp120 诱导的 TNF-α。PLC 途径部分且等效地参与 gp120 诱导的 TNF-α和 IL-10。此外,PI3K、ERK1/2、p38 MAP 激酶和 NF-κB 途径的抑制完全消除了这两种细胞因子的产生。总之,这项研究揭示了 HIV-1 gp120 触发的关键钙信号通路,以控制这两种细胞因子:TNF-α 和 IL-10 的产生。这一发现可能有助于开发新的治疗策略,以减轻 HIV-1 感染患者中观察到的慢性超免疫激活。
