Korobova Zoia R, Arsentieva Natalia A, Butenko Anastasia A, Batsunov Oleg K, Lyubimova Natalia E, Ostankova Yulia V, Anufrieva Ekaterina V, Maslov Sergey A, Kozlov Konstantin V, Sulima Dmitrii L, Rishnyak Oksana Yu, Totolian Areg A
Saint Petersburg Pasteur Institute, Mira St. 14, 197101 St. Petersburg, Russia.
Department of Immunology, Pavlov First State Medical University of St. Petersburg, L'va Tolstogo St. 6-8, 197022 St. Petersburg, Russia.
Int J Mol Sci. 2025 Aug 11;26(16):7761. doi: 10.3390/ijms26167761.
Hepatic viruses, such as hepatitis B and C (HBV and HCV), evade immune defenses and drive liver cirrhosis and cancer. They remain a major global health burden, requiring deeper research into immune responses; specifically, adaptive immunity. This study aims to analyze T cellular subsets in chronic HBV and HCV infection and investigate their potential role in the immunopathogenesis of these conditions.
For our study, we collected 123 blood samples taken from patients infected with HCV ( = 36) and HBV ( = 34) and healthy volunteers ( = 53). With the use of flow cytometry, we assessed levels of CD4+ and CD8+ minor T cell subpopulations (naïve, central, and effector memory cells (CM and EM), terminally differentiated EM (TEMRA), Th1, Th2, Th17, Tfh, Tc1, Tc2, Tc17, Tc17.1).
Despite similar total CD4+ T cell frequencies across chronic HCV, HBV, and healthy groups, patients with hepatitis showed elevated TEMRA, EM, and CM subsets alongside depleted naïve Th cells and specific CM subpopulations compared to controls. Patients with chronic HCV and HBV showed elevated CD8+ T cell frequencies versus controls, with disease-specific shifts: reduced EM CTLs but increased TEMRA CTLs, Tc1/Tc17.1 depletion (notably Tc17.1 in HCV), and higher Tc2 levels.
Viral clearance in HBV and HCV requires a delicate balance between immunity and viral activity. Despite similar T cell frequencies (CD3+/CD4+/CD8+), minor subsets revealed distinct patterns differentiating HCV, HBV, and healthy controls.
乙型和丙型肝炎病毒(HBV和HCV)等肝脏病毒可逃避免疫防御,导致肝硬化和癌症。它们仍然是全球主要的健康负担,需要对免疫反应,特别是适应性免疫进行更深入的研究。本研究旨在分析慢性HBV和HCV感染中的T细胞亚群,并研究它们在这些疾病免疫发病机制中的潜在作用。
在我们的研究中,我们收集了123份血液样本,这些样本来自感染HCV(n = 36)和HBV(n = 34)的患者以及健康志愿者(n = 53)。使用流式细胞术,我们评估了CD4+和CD8+次要T细胞亚群(初始、中央和效应记忆细胞(CM和EM)、终末分化EM(TEMRA)、Th1、Th2、Th17、Tfh、Tc1、Tc2、Tc17、Tc17.1)的水平。
尽管慢性HCV、HBV和健康组的总CD4+ T细胞频率相似,但与对照组相比,肝炎患者的TEMRA、EM和CM亚群升高,同时初始Th细胞和特定CM亚群减少。慢性HCV和HBV患者的CD8+ T细胞频率高于对照组,且存在疾病特异性变化:EM CTL减少,但TEMRA CTL增加,Tc1/Tc17.1减少(尤其是HCV中的Tc17.1),Tc2水平升高。
HBV和HCV的病毒清除需要免疫和病毒活性之间的微妙平衡。尽管T细胞频率(CD3+/CD4+/CD8+)相似,但次要亚群显示出区分HCV、HBV和健康对照的不同模式。
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