PHARMACOKINETICS AND TOXICITY OF SECONDLINE ANTITUBERCULOSIS DRUGS IN HIV-INFECTE

二线抗结核药物在 HIV 感染者中的药代动力学和毒性

• 批准号: 8134115
• 负责人: Anneke Catharina Hesseling
• 金额: $ 42.17万
• 依托单位: STELLENBOSCH UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2011
• 资助国家: 美国
• 起止时间: 2011-06-10 至 2016-03-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8134115
• 关键词: 15 year old; 2 year old; Acids; Adult; Adverse drug effect; Adverse effects; Age; Amikacin; Anti-Retroviral Agents; Antitubercular Agents; CD4 Lymphocyte Count; Capromycin; Cartilage; Chemoprophylaxis; Chest; Child; Child health care; Childhood; Clinical; Data; Diagnostic; Disease; Dose; Drug Interactions; Drug Kinetics; Drug Resistant Tuberculosis; Drug resistance in tuberculosis; Drug usage; Enrollment; Ensure; Epidemic; Equilibrium; Ethionamide; Ethnic Origin; Exanthema; Extreme drug resistant tuberculosis; Fluoroquinolones; Genotype; Goals; HIV; HIV Infections; Hepatotoxicity; Hospital Referrals; Hospitals; Hour; Hypothyroidism; Immunity; Incidence; Infection; Intestines; Knowledge; Lamivudine; Linezolid; Lopinavir; Measures; Medicine; Multi-Drug Resistance; Multidrug-Resistant Tuberculosis; Nutritional status; Ofloxacin; Outcome; Outcome Measure; Patients; Pediatric Hospitals; Pharmaceutical Preparations; Plasma; Population; Population Study; Prevalence; Prevention; Prophylactic treatment; Prospective Studies; Province; Reference Values; Regimen; Renal function; Resistance; Rifampin; Ritonavir; Safety; Sampling; Schedule; Severities; Simulate; South Africa; Staging; Time; Toxic effect; Tuberculosis; Viral Load result; Weight; abacavir; age effect; aged; antiretroviral therapy; base; burden of illness; chemotherapy; design; dosage; drug metabolism; efavirenz; experience; improved; interest; isoniazid; ototoxicity; pharmacokinetic model; prevent; prospective; transmission process; treatment response; tuberculosis drugs; tuberculosis treatment

DESCRIPTION (provided by applicant): The long-term goal of the project is to improve the health of children with drug-resistant tuberculosis (DR-TB) in need of second-line anti-tuberculosis (anti-TB) drugs, through studying the pharmacokinetics (PK), safety profile and toxicity of commonly used second-line anti-TB drugs in children with and without HIV co-infection. The specific aims are: 1) to compare the PK of second-line anti-tuberculosis drugs in children (< 15 years) by age; 2) to compare the plasma concentrations of antiretroviral (ARV) drugs in HIV-infected children (< 15 years) on second-line anti-TB drugs to those not on anti-TB therapy; and 3) to characterize the tolerability and toxicity of second-line anti-TB drugs in HIV-infected and uninfected children. Childhood TB represents 15-20% of the disease burden in settings where TB and HIV infection is prevalent. Multidrug-resistant TB (MDR-TB; i.e. resistance to both rifampin and isoniazid) is an emerging epidemic, with an estimated 489 000 global cases annually. MDR-TB patients often experience prolonged diagnostic delay, resulting in transmission of these strains especially to young children with a sharp increase in the numbers of children on treatment and prophylaxis for MDR-TB. This hospital-based study will be implemented in Cape Town, Western Cape Province, South Africa at 2 referral hospitals - Brooklyn Hospital for Chest Diseases and Tygerberg Children's Hospital. The prevalence of MDR-TB amongst children with culture-confirmed TB was 8.6% and the prevalence of HIV infection in children with TB was 25-30% during 2009. The most frequently used second-line anti-TB drugs in children in the PIs' setting are ethionamide, fluoroquinolones, amikacin and terizidone. Capreomycin, linezolid and PAS are typically used for treatment of extensively drug-resistant TB. Although second-line anti-TB drugs are routinely given and recommended in children, there is limited information available to inform the accurate dosing in young and in HIV-infected children, who may have altered drug metabolism and drug-drug interactions. There are limited data on toxicity of these anti-TB drugs in children, who are typically treated for 18-24 months for DR-TB. The PIs will complete a prospective, longitudinal, hospital-based, observational PK study in HIV-infected and uninfected children aged 0-15 years who are receiving routine chemotherapy or chemoprophylaxis for the treatment or prevention of DR-TB. They will enroll 310 total children consecutively over 3.5 years for intensive PK sampling of second-line anti-TB drugs at baseline. HIV-infected children will have ARV PK sampling done at baseline. Approximately 30% of the PIs' sample will be HIV-infected. An equal number of HIV-infected children with and without anti-TB therapy (concurrent controls; 42 on efavirenz and 22 on lopinavir) will be enrolled based on the required age strata to allow for comparison of the effect of second-line TB drugs on ARV levels in HIV-infected children with and without TB treatment. The PIs will follow children on treatment for DR disease until treatment completion for clinical outcomes including TB treatment response and drug adverse effects. Enrolment will be balanced by HIV status and age to ensure adequate number of the children 0-2 years of age and HIV-infected children. PUBLIC HEALTH RELEVANCE: Although childhood TB can be treated by taking medicines, some strains of TB are resistant to commonly used TB medications (drug-resistant TB). These children need medications that are less effective, have more side effects, of which little is known which dosage (amount) children should receive and how to check whether these medications are safe in young and HIV-infected children. Knowledge gained through this study will help find out how to best give the correct amount of medication to safely treat and prevent drug-resistant TB in young and HIV-infected children.

项目描述（由申请人提供）：该项目的长期目标是通过研究常用二线抗结核药物在合并和未合并HIV感染的儿童中的药代动力学（PK）、安全性特征和毒性，改善需要二线抗结核药物的耐药结核病（DR-TB）儿童的健康。具体目标是：1）按年龄比较二线抗结核药物在儿童（< 15岁）中的PK; 2）比较接受二线抗结核药物治疗的HIV感染儿童（< 15岁）与未接受抗结核药物治疗的HIV感染儿童（< 15岁）中抗逆转录病毒（ARV）药物的血浆浓度; 3）描述HIV感染和未感染儿童中二线抗结核药物的耐受性和毒性。在结核病和艾滋病毒感染流行的环境中，儿童结核病占疾病负担的15-20%。耐多药结核病（MDR-TB;即对利福平和异烟肼的耐药性）是一种新兴的流行病，估计全球每年有489 000例病例。耐多药结核病患者往往经历长时间的诊断延误，导致这些菌株传播，特别是传播给幼儿，接受耐多药结核病治疗和预防的儿童人数急剧增加。这项基于医院的研究将在南非西开普省开普敦的2家转诊医院-布鲁克林胸部疾病医院和Tygerberg儿童医院实施。2009年期间，经培养确认的结核病儿童中耐多药结核病的流行率为8.6%，结核病儿童中艾滋病毒感染的流行率为25-30%。在PI环境中，儿童最常用的二线抗结核药物是乙硫异烟胺、氟喹诺酮类、阿米卡星和特立齐酮。卷曲霉素、利奈唑胺和PAS通常用于治疗广泛耐药结核病。虽然二线抗结核药物是常规给予和建议的儿童，有有限的信息，以告知年轻人和艾滋病毒感染的儿童，谁可能改变了药物代谢和药物相互作用的准确剂量。关于这些抗结核药物在儿童中的毒性数据有限，儿童通常接受18-24个月的耐药结核治疗。PI将在接受常规化疗或化学预防治疗或预防耐药结核的0-15岁HIV感染和未感染儿童中完成一项前瞻性、纵向、基于医院的观察性PK研究。他们将在3.5年内连续入组共计310名儿童，在基线时进行二线抗结核药物的密集PK采样。HIV感染儿童将在基线时进行ARV PK采样。大约30%的PI样本将感染艾滋病毒。将根据所需的年龄分层招募相同数量的接受和未接受抗结核治疗的HIV感染儿童（同期对照; 42例接受依法韦仑治疗，22例接受洛匹那韦治疗），以比较二线结核药物对接受和未接受结核治疗的HIV感染儿童中ARV水平的影响。PI将随访接受DR疾病治疗的儿童，直至治疗完成，以获得临床结局，包括TB治疗反应和药物不良反应。将根据艾滋病毒状况和年龄平衡纳入，以确保有足够数量的0-2岁儿童和艾滋病毒感染儿童。 公共卫生相关性：虽然儿童结核病可以通过服药治疗，但某些结核病菌株对常用的结核病药物具有耐药性（耐药结核病）。这些儿童需要的药物效果较差，副作用较多，其中很少有人知道儿童应该接受的剂量（数量）以及如何检查这些药物对年幼和感染艾滋病毒的儿童是否安全。通过这项研究获得的知识将有助于找出如何最好地给予正确的药物剂量，以安全地治疗和预防年轻人和艾滋病毒感染儿童的耐药结核病。