Optimization of antiviral dosing in Herpesviridae encephalitis: a promising approach to improve outcome?

IF 10.9 1区医学 Q1 INFECTIOUS DISEASES

Clinical Microbiology and Infection Pub Date : 2024-12-13 DOI:10.1016/j.cmi.2024.12.008

Roland Nau, Jana Seele, Jacob Bodilsen, Uwe Groß

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引用次数: 0

Abstract

Background: Despite established antiviral therapy for herpes simplex virus, varicella zoster and cytomegalovirus encephalitis, the outcome remains poor.

Objectives: To assess pharmacokinetic (PK) and pharmacodynamic (PD) data of antiviral drugs in the central nervous system (CNS) to optimize the treatment of Herpesviridae encephalitis.

Sources: PUBMED search 1950 to September 2024, terms (1) "encephalitis" and ("HSV" or "VZV" or "CMV") or (2) cerebrospinal and ("(val)acyclovir" or "(val)ganciclovir" or "foscarnet" or "cidofovir").

Content: Antivirals against herpes viruses apparently act in a time-dependent manner. To suppress viral replication, drug concentration in the extracellular space at the site of the infection should be kept above the concentrations active in cell cultures for 24 h/d. Most data reflect delayed drug entry into lumbar cerebrospinal fluid (CSF). Ratios of the areas of the concentration/time curves (AUC) in CSF and serum (AUC_CSF/AUC_S) of acyclovir, ganciclovir and foscarnet are 0.15-0.3 in the absence of meningeal inflammation and increase in severe meningoencephalitis. Elimination half-lives (t_1/2β) are longer in CSF than in plasma. CSF concentrations are rough approximations of drug concentrations in the cerebral extracellular fluid. Lumbar CSF concentrations are usually higher than ventricular or cisternal CSF concentrations tending to overestimate cerebral extracellular fluid concentrations. Provided the availability of adequate measurements in individual CNS compartments, antiviral concentrations and efficacy may be predicted by future PK/PD modelling. Probenecid holds the potential to reduce the efflux of antiviral drugs from the CNS.

Implications: The long t_1/2β of antiviral drugs in CSF suggest relatively uniform steady state CSF levels at dosing intervals ≤12h and accumulation after repeated dosing. Probenecid is of unproven utility. To rapidly attain effective concentrations in the infected tissue, physiologically based pharmacokinetic and PK/PD modelling may be helpful. Until reliable PK/PD data are available, doubling the first dose should be considered.

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优化疱疹病毒科脑炎的抗病毒剂量：改善预后的可行方法？

背景：尽管对单纯疱疹病毒（HSV）、水痘带状疱疹病毒（VZV）和巨细胞病毒（CMV）脑炎采用了成熟的抗病毒疗法，但疗效仍然不佳：评估抗病毒药物在中枢神经系统（CNS）中的药动学（PK）和动力学（PD）数据，以优化疱疹病毒科脑炎的治疗：1. "脑炎 "和（"HSV "或 "VZV "或 "CMV"）或 2. 脑脊液和["(val)acyclovir "或"(val)ganciclovir "或 "foscarnet "或 "cidofovir"].内容：抗病毒药物对疱疹病毒的作用显然与时间有关。要抑制病毒复制，感染部位细胞外空间的药物浓度应保持高于细胞培养物中的活性浓度，每天持续 24 小时。大多数数据反映了药物进入腰部脑脊液（CSF）的延迟。阿昔洛韦、更昔洛韦和福斯奈德在 CSF 和血清中的浓度/时间曲线面积（AUC）之比（AUCCSF/AUCS）在无脑膜炎症时为 0.15-0.3，在严重脑膜脑炎时会升高。脑脊液中的消除半衰期（t1/2β）比血浆中长。脑脊液浓度是脑细胞外液（ECF）中药物浓度的粗略近似值。腰部 CSF 的浓度通常高于脑室或椎体内 CSF 的浓度，因此容易高估脑细胞外液（ECF）中的药物浓度。如果中枢神经系统各分区有足够的测量值，未来的 PK/PD 模型就可以预测抗病毒药物的浓度和疗效。丙磺舒具有减少中枢神经系统抗病毒药物外流的潜力：抗病毒药物在脑脊液中的t1/2β较长，这表明在用药间隔≤12小时时，脑脊液的稳态水平相对一致，重复用药后会出现蓄积。丙磺舒的作用尚未得到证实。为了快速达到感染组织中的有效浓度，基于生理的药代动力学（PBPK）和 PK/PD 模型可能会有所帮助。在获得可靠的 PK/PD 数据之前，应考虑将首次剂量加倍。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Clinical Microbiology and Infection 医学-传染病学

CiteScore

25.30

自引率

2.10%

发文量

441

审稿时长

2-4 weeks

期刊介绍： Clinical Microbiology and Infection (CMI) is a monthly journal published by the European Society of Clinical Microbiology and Infectious Diseases. It focuses on peer-reviewed papers covering basic and applied research in microbiology, infectious diseases, virology, parasitology, immunology, and epidemiology as they relate to therapy and diagnostics.