研究方案药物在 TB-PRACTECAL 临床试验中的群体药代动力学和药效学：一项随机对照试验中的前瞻性嵌套研究方案。

Population pharmacokinetics and pharmacodynamics of investigational regimens' drugs in the TB-PRACTECAL clinical trial (the PRACTECAL-PKPD study): a prospective nested study protocol in a randomised controlled trial.

机构信息

Manson Unit, Médecins Sans Frontières, London, UK

Clinical research Department, London School of Hygiene & Tropical Medicine, London, UK.

出版信息

BMJ Open. 2021 Sep 6;11(9):e047185. doi: 10.1136/bmjopen-2020-047185.

DOI:10.1136/bmjopen-2020-047185

PMID:34489274

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8422304/

Abstract

INTRODUCTION

Drug-resistant tuberculosis (TB) remains a global health threat, with little over 50% of patients successfully treated. Novel regimens like the ones being studied in the TB-PRACTECAL trial are urgently needed. Understanding anti-TB drug exposures could explain the success or failure of these trial regimens. We aim to study the relationship between the patients' exposure to anti-TB drugs in TB-PRACTECAL investigational regimens and their treatment outcomes.

METHODS AND ANALYSIS

Adults with multidrug-resistant TB randomised to investigational regimens in TB-PRACTECAL will be recruited to a nested pharmacokinetic-pharmacodynamic (PKPD) study. Venous blood samples will be collected at 0, 2 and 23 hours postdose on day 1 and 0, 6.5 and 23 hours postdose during week 8 to quantify drug concentrations in plasma. Trough samples will be collected during week 12, 16, 20 and 24 visits. Opportunistic samples will be collected during weeks 32 and 72. Drug concentrations will be quantified using liquid chromatography-tandem mass spectrometry. Sputum samples will be collected at baseline, monthly to week 24 and then every 2 months to week 108 for MICs and bacillary load quantification. Full blood count, urea and electrolytes, liver function tests, lipase, ECGs and ophthalmology examinations will be conducted at least monthly during treatment.PK and PKPD models will be developed for each drug with nonlinear mixed effects methods. Optimal dosing will be investigated using Monte-Carlo simulations.

ETHICS AND DISSEMINATION

The study has been approved by the Médecins sans Frontières (MSF) Ethics Review Board, the LSHTM Ethics Committee, the Belarus RSPCPT ethics committee and PharmaEthics and the University of Witwatersrand Human Research ethics committee in South Africa. Written informed consent will be obtained from all participants. The study results will be shared with public health authorities, presented at scientific conferences and published in a peer-reviewed journal.

TRIAL REGISTRATION NUMBER

NCT04081077; Pre-results.

摘要

简介

耐多药结核病（TB）仍然是全球健康威胁，仅有略多于 50%的患者成功治愈。因此，迫切需要新的治疗方案，例如正在 TB-PRACTECAL 试验中研究的方案。了解抗结核药物的暴露情况可以解释这些试验方案的成败。我们旨在研究 TB-PRACTECAL 试验中患者接受的抗结核药物暴露与治疗结果之间的关系。

方法和分析

将招募参加 TB-PRACTECAL 试验的多药耐药性结核病成人患者参加嵌套药代动力学-药效学（PKPD）研究。在第 1 天的第 1 天和第 8 周的第 23 小时以及第 8 周的第 6.5 小时和第 23 小时，将采集静脉血样以测量血浆中的药物浓度。在第 12、16、20 和 24 次就诊时采集谷样。在第 32 和 72 周收集机会样本。使用液相色谱-串联质谱法定量药物浓度。在基线、每月至第 24 周，然后每 2 个月至第 108 周收集痰样进行 MIC 和细菌载量定量。在治疗期间，每月至少进行一次全血细胞计数、尿素和电解质、肝功能检查、脂肪酶、心电图和眼科检查。使用非线性混合效应方法为每种药物建立 PK 和 PKPD 模型。使用蒙特卡罗模拟法研究最佳剂量。

伦理和传播

该研究已获得无国界医生组织（MSF）伦理审查委员会、伦敦卫生与热带医学学院伦理委员会、白俄罗斯 RSPCPT 伦理委员会、PharmaEthics 和南非威特沃特斯兰德大学人类研究伦理委员会的批准。将从所有参与者处获得书面知情同意。研究结果将与公共卫生当局共享，在科学会议上展示，并在同行评议的期刊上发表。

试验注册号

NCT04081077；预结果。

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研究方案药物在 TB-PRACTECAL 临床试验中的群体药代动力学和药效学：一项随机对照试验中的前瞻性嵌套研究方案。

Population pharmacokinetics and pharmacodynamics of investigational regimens' drugs in the TB-PRACTECAL clinical trial (the PRACTECAL-PKPD study): a prospective nested study protocol in a randomised controlled trial.

机构信息

出版信息

INTRODUCTION

METHODS AND ANALYSIS

ETHICS AND DISSEMINATION

TRIAL REGISTRATION NUMBER

简介

方法和分析

伦理和传播

试验注册号

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