Nettere Danielle, White Scott, Williams Grant, Jha Shalini, Moody M Anthony, Chan Cliburn, Ferrari Guido, Naggie Susanna
Department of Surgery, Duke University School of Medicine, Durham, NC, United States.
Molecular Genetics and Microbiology, Duke University School of Medicine, Durham, NC, United States.
Front Immunol. 2025 Apr 22;16:1469473. doi: 10.3389/fimmu.2025.1469473. eCollection 2025.
Hepatitis C virus (HCV) infection remains a leading cause of morbidity and mortality in people with human immunodeficiency virus (HIV). Liver fibrosis progression is more rapid in people with HIV/HCV coinfection compared to HCV monoinfection and the rate of resolution of liver fibrosis after HCV cure is unknown in people with HIV. Invariant natural killer T (iNKT) cells are enriched in the liver and play important roles in initiating immune responses to hepatotropic pathogens and promoting healing following injury. It was recently reported that the pro-healing CD4+ iNKT cells are preferentially infected and depleted in early HIV infection, but this effect on HCV-related liver disease outcomes is unclear.
Here we examined and compared peripheral blood iNKT cells from people with HIV/HCV coinfection and people with HIV and HCV monoinfection or no infection (controls). We evaluated the iNKT cells' expansion potential and phenotype using an unbiased Uniform Manifold Approximation and Projection (UMAP) and clustering based approach.
We observed that circulating iNKT cells from people with HIV and HIV/HCV coinfection have impaired expansion to T-cell receptor (TCR) stimulation. We also observed an enrichment of the CD8+ and CD57+ iNKT subsets, which are thought to represent terminally differentiated iNKT cells. HCV monoinfection on the other hand minimally impacted iNKT phenotypes compared to controls.
The changes observed in iNKT phenotype and proliferative ability in people with HIV/HCV coinfection suggest an impairment that may be contributing to the enhanced pathogenesis during coinfection and could inform novel therapeutic approaches.
丙型肝炎病毒(HCV)感染仍然是人类免疫缺陷病毒(HIV)感染者发病和死亡的主要原因。与单纯HCV感染相比,HIV/HCV合并感染患者的肝纤维化进展更快,且HIV感染者在HCV治愈后肝纤维化的消退率尚不清楚。不变自然杀伤T(iNKT)细胞在肝脏中富集,在启动对嗜肝病原体的免疫反应和促进损伤后愈合中发挥重要作用。最近有报道称,在早期HIV感染中,具有促进愈合作用的CD4+ iNKT细胞优先被感染并耗竭,但这种情况对HCV相关肝病结局的影响尚不清楚。
在此,我们检测并比较了HIV/HCV合并感染患者、HIV和HCV单感染患者或未感染者(对照组)的外周血iNKT细胞。我们使用无偏均匀流形逼近和投影(UMAP)以及基于聚类的方法评估了iNKT细胞的扩增潜力和表型。
我们观察到,HIV感染者和HIV/HCV合并感染患者的循环iNKT细胞对T细胞受体(TCR)刺激的扩增能力受损。我们还观察到CD8+和CD57+ iNKT亚群增多,这些亚群被认为代表终末分化的iNKT细胞。另一方面,与对照组相比,单纯HCV感染对iNKT表型的影响最小。
在HIV/HCV合并感染患者中观察到的iNKT表型和增殖能力的变化表明存在一种损伤,这可能导致合并感染期间发病机制增强,并为新的治疗方法提供依据。
