Department of Molecular Biology, Princeton University , Princeton, New Jersey, USA.
Department of Medicine, The Program for Experimental & Theoretical Modeling, Division of Hepatology, Stritch School of Medicine, Loyola University Chicago , Maywood, Illinois, USA.
mBio. 2023 Aug 31;14(4):e0100823. doi: 10.1128/mbio.01008-23. Epub 2023 Jul 12.
Chronic infection with hepatitis B and delta viruses (HDV) is the most serious form of viral hepatitis due to more severe manifestations of an accelerated progression to liver fibrosis, cirrhosis, and hepatocellular carcinoma. We characterized early HDV kinetics post-inoculation and incorporated mathematical modeling to provide insights into host-HDV dynamics. We analyzed HDV RNA serum viremia in 192 immunocompetent (C57BL/6) and immunodeficient (NRG) mice that did or did not transgenically express the HDV receptor-human sodium taurocholate co-transporting polypeptide (hNTCP). Kinetic analysis indicates an unanticipated biphasic decline consisting of a sharp first-phase and slower second-phase decline regardless of immunocompetence. HDV decline after re-inoculation again followed a biphasic decline; however, a steeper second-phase HDV decline was observed in NRG-hNTCP mice compared to NRG mice. HDV-entry inhibitor bulevirtide administration and HDV re-inoculation indicated that viral entry and receptor saturation are not major contributors to clearance, respectively. The biphasic kinetics can be mathematically modeled by assuming the existence of a non-specific-binding compartment with a constant on/off-rate and the steeper second-phase decline by a loss of bound virus that cannot be returned as free virus to circulation. The model predicts that free HDV is cleared with a half-life of 35 minutes (standard error, SE: 6.3), binds to non-specific cells with a rate of 0.05 per hour (SE: 0.01), and returns as free virus with a rate of 0.11 per hour (SE: 0.02). Characterizing early HDV-host kinetics elucidates how quickly HDV is either cleared or bound depending on the immunological background and hNTCP presence. IMPORTANCE The persistence phase of HDV infection has been studied in some animal models; however, the early kinetics of HDV is incompletely understood. In this study, we characterize an unexpectedly HDV biphasic decline post-inoculation in immunocompetent and immunodeficient mouse models and use mathematical modeling to provide insights into HDV-host dynamics.
慢性乙型肝炎和丁型肝炎病毒(HDV)感染是最严重的病毒性肝炎形式,因为其纤维化、肝硬化和肝细胞癌的进展速度更快。我们描述了接种后 HDV 的早期动力学,并结合数学模型来深入了解宿主-HDV 动力学。我们分析了在 192 只免疫功能正常(C57BL/6)和免疫缺陷(NRG)小鼠的血清 HDV RNA 病毒血症,这些小鼠或不转染 HDV 受体-人牛磺胆酸钠共转运蛋白(hNTCP)。动力学分析表明,无论免疫功能如何,都会出现意想不到的两相下降,包括急剧的第一相和较慢的第二相下降。再次接种后 HDV 的下降再次遵循两相下降;然而,与 NRG 小鼠相比,NRG-hNTCP 小鼠的第二相 HDV 下降更为陡峭。HDV 进入抑制剂 bulevirtide 给药和 HDV 再接种表明,病毒进入和受体饱和分别不是清除的主要因素。两相动力学可以通过假设存在一个具有恒定的结合/解离速率的非特异性结合隔室来进行数学建模,而陡峭的第二相下降则是由于结合的病毒无法作为游离病毒返回循环而丢失。该模型预测,游离 HDV 的半衰期为 35 分钟(标准误差,SE:6.3),以每小时 0.05 的速率与非特异性细胞结合,并以每小时 0.11 的速率返回游离病毒(SE:0.02)。早期 HDV-宿主动力学的特征阐明了 HDV 是根据免疫背景和 hNTCP 存在而迅速清除还是结合。重要性 HDV 感染的持续期已在一些动物模型中进行了研究;然而,HDV 的早期动力学尚未完全了解。在这项研究中,我们描述了免疫功能正常和免疫缺陷小鼠模型中接种后 HDV 的意外两相下降,并使用数学模型来深入了解 HDV-宿主动力学。
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