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整合基因组和药代动力学数据预测 HIV 相关隐球菌性脑膜炎的临床结局。

Integration of genomic and pharmacokinetic data to predict clinical outcomes in HIV-associated cryptococcal meningitis.

机构信息

Antimicrobial Pharmacodynamics and Therapeutics Group, Department of Pharmacology and Therapeutics, University of Liverpool, Liverpool, United Kingdom.

Malawi Liverpool Wellcome Clinical Research Programme, Blantyre, Malawi.

出版信息

mBio. 2024 Oct 16;15(10):e0159224. doi: 10.1128/mbio.01592-24. Epub 2024 Aug 27.

Abstract

UNLABELLED

Cryptococcal meningitis causes an estimated 112,000 global deaths per annum. Genomic and phenotypic features of the infecting strain of spp. have been associated with outcomes from cryptococcal meningitis. Additionally, population-level pharmacokinetic variability is well documented in these patient cohorts. The relative contribution of these factors to clinical outcomes is unknown. Based in Malawi, we conducted a sub-study of the phase 3 Ambition-CM trial (ISRCTN72509687), collecting plasma and cerebrospinal fluid at serial time points during the first 14 days of antifungal therapy. We explored the relative contribution of pathogen genotype, drug resistance phenotype, and pharmacokinetics on clinical outcomes including lumbar opening pressure, pharmacodynamic effect, and mortality. We report remarkable genomic homogeneity among infecting strains of spp., within and between patients. There was no evidence of acquisition of antifungal resistance in our isolates. Genotypic features of the infecting strain were not consistently associated with adverse or favorable clinical outcomes. However, baseline fungal burden and early fungicidal activity (EFA) were associated with mortality. The strongest predictor of EFA was the level of exposure to amphotericin B. Our analysis suggests the most effective means of improving clinical outcomes from HIV-associated cryptococcal meningitis is to optimize exposure to potent antifungal therapy.

IMPORTANCE

HIV-associated cryptococcal meningitis is associated with a high burden of mortality. Research into the different strain types causing this disease has yielded inconsistent findings in terms of which strains are associated with worse clinical outcomes. Our study suggests that the exposure of patients to potent anti-cryptococcal drugs has a more significant impact on clinical outcomes than the strain type of the infecting organism. Future research should focus on optimizing drug exposure, particularly in the context of novel anticryptococcal drugs coming into clinical use.

摘要

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每年估计有 112000 人死于隐球菌性脑膜炎。 感染株的遗传和表型特征与隐球菌性脑膜炎的结果有关。 此外,这些患者群体中的群体药代动力学变异性得到了很好的记录。 这些因素对临床结果的相对贡献尚不清楚。 我们在马拉维进行了 3 期 Ambition-CM 试验(ISRCTN72509687)的子研究,在抗真菌治疗的前 14 天内的多个时间点收集血浆和脑脊液。 我们探讨了病原体基因型、药物耐药表型和药代动力学对临床结果(包括腰椎开口压、药效学效应和死亡率)的相对贡献。 我们报告了感染的隐球菌属菌株之间以及患者之间存在显著的遗传同质性。 在我们的分离株中没有发现获得抗真菌耐药性的证据。 感染株的遗传特征与不良或有利的临床结果并不一致。 但是,基线真菌负荷和早期杀菌活性(EFA)与死亡率有关。 EFA 的最强预测因子是两性霉素 B 的暴露水平。 我们的分析表明,改善 HIV 相关性隐球菌性脑膜炎临床结果的最有效方法是优化对有效抗真菌治疗的暴露。

重要性

HIV 相关性隐球菌性脑膜炎与高死亡率相关。 对引起这种疾病的不同菌株类型的研究在哪些菌株与更差的临床结果相关方面得出了不一致的发现。 我们的研究表明,患者对抗真菌药物的暴露对临床结果的影响大于感染病原体的菌株类型。 未来的研究应侧重于优化药物暴露,特别是在新型抗隐球菌药物进入临床使用的情况下。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5a23/11481554/1e8e1b1f7200/mbio.01592-24.f001.jpg

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