Infection and depletion of CD4+ group-1 innate lymphoid cells by HIV-1 via type-I interferon pathway.
Juanjuan ZhaoLiang ChengHongbo WangHaisheng YuBo TuQiang FuGuangming LiQi WangYanling SunXin ZhangZhenwen LiuWeiwei ChenLiguo ZhangLishan SuZheng ZhangPublished in: PLoS pathogens (2018)
Innate lymphoid cells (ILCs) are severely depleted during chronic HIV-1 infection by unclear mechanisms. We report here that human ILC1s comprising of CD4+ and CD4- subpopulations were present in various human lymphoid organs but with different transcription programs and functions. Importantly, CD4+ ILC1s expressed HIV-1 co-receptors and were productively infected by HIV-1 in vitro and in vivo. Furthermore, chronic HIV-1 infection activated and depleted both CD4+ and CD4- ILC1s, and impaired their cytokine production activity. Highly active antiretroviral (HAART) therapy in HIV-1 patients efficiently rescued the ILC1 numbers and reduced their activation, but failed to restore their functionality. We also found that blocking type-I interferon (IFN-I) signaling during HIV-1 infection in vivo in humanized mice prevented HIV-1 induced depletion or apoptosis of ILC1 cells. Therefore, we have identified the CD4+ ILC1 cells as a new target population for HIV-1 infection, and revealed that IFN-I contributes to the depletion of ILC1s during HIV-1 infection.
Keyphrases
- antiretroviral therapy
- nk cells
- hiv infected
- hiv positive
- human immunodeficiency virus
- cell cycle arrest
- hiv infected patients
- hiv aids
- induced apoptosis
- hiv testing
- hepatitis c virus
- cell death
- men who have sex with men
- endoplasmic reticulum stress
- oxidative stress
- endothelial cells
- type diabetes
- public health
- dendritic cells
- stem cells
- signaling pathway
- end stage renal disease
- adipose tissue
- south africa
- drug induced
- mesenchymal stem cells
- peritoneal dialysis
- transcription factor
- bone marrow
- smoking cessation