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首页> 外文期刊>Medicine. >A Pilot Study of MicroRNAs Expression Profile in Serum and HBsAg Particles Predictors of Therapeutic Vaccine Efficacy in Chronic Hepatitis B Patients
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A Pilot Study of MicroRNAs Expression Profile in Serum and HBsAg Particles Predictors of Therapeutic Vaccine Efficacy in Chronic Hepatitis B Patients

机译:慢性乙型肝炎患者治疗性疫苗疗效的血清和HBsAg颗粒预测因子中microRNA表达谱的初步研究

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摘要

Chronic hepatitis B (CHB) remains a global health problem. Therapeutic vaccination has been successfully employed to treat a subpopulation of CHB patients. Personalized treatment can not only improve therapeutic efficacy, but also decrease the cost of medical care. Since microRNAs (miRNAs) are highly conserved and are involved in many cellular processes, exploring their expression profiles in CHB patients in association with responsiveness to therapeutic vaccination may be an approach for personalized treatment. In this study, we examined the kinetic expression profiles of 13 miRNAs in sera and serum-derived hepatitis surface antigen (HBsAg) particles in 10 CHB patients including 5 responders and 5 nonresponders selected from a large cohort of 136 patients enroled in a phase III clinical trial using antigen-antibody immunogenic complex based therapeutic vaccine (YIC). Eight miRNAs were detected in both sera and HBsAg particles. Among them, the levels of serum miRNAs and serum-derived HBsAg-carried miRNAs (let-7f, miR-22, miR-30a, and miR-122) were significantly lower in the responders group compared to those in the nonresponders group at baseline and throughout the course of treatment. The lower baseline levels of serum miRNAs and HBsAg-carried miRNAs were also associated with hepatitis e antigen clearance at week 76 and hepatitis e antigen seroconversion during the study period. In summary, our study suggests that lower baseline levels of serum miRNAs and HBsAg-carried miRNAs (let-7f, miR-22, miR-30a, and miR-122) associated with YIC treatment response and the variation trend of these 4 miRNAs could have a prognostic value for responsiveness to YIC treatment.
机译:慢性乙型肝炎(CHB)仍然是全球性的健康问题。治疗性疫苗接种已成功用于治疗CHB患者的亚人群。个性化治疗不仅可以提高治疗效果,而且可以降低医疗费用。由于microRNA(miRNA)高度保守并且涉及许多细胞过程,因此在CHB患者中探索其表达谱以及对治疗疫苗的反应性可能是个性化治疗的一种方法。在这项研究中,我们检查了10名CHB患者的血清和血清源性肝炎表面抗原(HBsAg)颗粒中13种miRNA的动力学表达谱,其中包括5名响应者和5名无响应者,这些患者选自136名III期临床研究的大批患者使用基于抗原抗体免疫原性复合物的治疗性疫苗(YIC)进行的试验。在血清和HBsAg颗粒中均检测到八个miRNA。其中,与基线时无反应者相比,反应者组中的血清miRNA和源自血清的HBsAg携带的miRNA(let-7f,miR-22,miR-30a和miR-122)的水平明显低于无反应者组。在整个治疗过程中。血清miRNA和HBsAg携带的miRNA的基线水平较低还与研究第76周时的戊型肝炎抗原清除率和戊型肝炎抗原血清转化有关。总之,我们的研究表明,与YIC治疗反应相关的血清miRNA和HBsAg携带的miRNA(let-7f,miR-22,miR-30a和miR-122)的基线水平较低,这4种miRNA的变化趋势可能对YIC治疗的反应性具有预后价值。

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