HIV-1 Drug Resistance in Different Subtypes

不同亚型的 HIV-1 耐药性

• 批准号: 7906662
• 负责人: Rami Kantor
• 金额: $ 63.93万
• 依托单位: STANFORD UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2008
• 资助国家: 美国
• 起止时间: 2008-09-01 至 2013-08-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7906662
• 关键词: AIDS/HIV problem; Acquired Immunodeficiency Syndrome; Affect; Africa; Anti-HIV Agents; Anti-Retroviral Agents; Antiretroviral resistance; Arts; Asia; Biological Assay; Caring; Cercopithecine Herpesvirus 1; China; Clinical Data; Codon Nucleotides; Collaborations; Country; Data; Databases; Diagnostic tests; Drug Exposure; Drug resistance; Effectiveness; Emergency Situation; Epidemic; Europe; Evolution; Failure; Frequencies; Genbank; Genetic; Genetic Polymorphism; Genotype; Goals; HIV; HIV drug resistance; HIV-1; HIV-1 drug resistance; Incidence; India; Individual; Infection; International; Knowledge; Life; Link; Literature; Methods; Monitor; Mutation; Patients; Pattern; Peptide Hydrolases; Persons; Pharmaceutical Preparations; Phylogenetic Analysis; Plasma; Population; Positioning Attribute; Predisposition; Prevalence; Principal Investigator; Protocols documentation; Public Health; Publishing; RNA-Directed DNA Polymerase; Recombinants; Regimen; Research; Research Infrastructure; Resistance; Resources; Sampling; Science; Sensitivity and Specificity; Shipping; Ships; Specimen; Surveillance Program; Testing; Thailand; Treatment Failure; Treatment Protocols; Validation; Variant; Vertebral column; Viral Genes; Viremia; Virus; Work; antiretroviral therapy; base; cohort; cost; design; experience; novel; pandemic disease; population based; programs; public health relevance; recombinant virus; resistance mutation; response; scale up; stem; transmission process; treatment center; treatment program; treatment strategy; working group

DESCRIPTION (provided by applicant): The human immunodeficiency virus (HIV-1) pandemic is due to multiple subtypes and emerging recombinant viruses that are widely distributed around the world. An important response to the epidemic is the global scale-up of access to antiretroviral treatment (ART) programs, potentially delivering ART to millions of infected individuals. A barrier to successful long term treatment is the emergence of drug resistance, caused by mutations selected in viral genes, which are both a cause and a consequence of ART failure. Knowledge about drug resistance comes largely from the US and Europe, focused on one HIV-1 variant, subtype B. However, 90% of infections globally, are in resource limited settings in Africa and Asia, where other distinct, non-B HIV-1 subtypes predominate. There is strong preliminary evidence that pre-therapy genotypes differ among subtypes and that distinct mutations at positions related to resistance may occur, even before treatment, among non-B subtypes. Furthermore, distinct, new mutations are detected in non-B subtypes after drug-exposure. Information on susceptibility and resistance of non-B viruses is critical for strategies to sustain the benefit of ART. Prevalence and incidence of transmitted and acquired drug resistance will drive decisions about diagnostic testing, initial and second-line therapies in public health HIV treatment programs in resource limited settings. The focus of this proposal is to build the scientific infrastructure for surveillance and monitoring of drug resistance in three Resource-limited settings, where specific non- B subtypes predominate. Through these studies we will develop a robust sequence database of HIV-1 non-B variants for genotypic analyses and phenotypic validation of resistance mutations and patterns. We have designed a program to first develop quality assured, low cost drug resistance monitoring strategies using dried filter specimens for resistance testing. These strategies will be implemented in Thailand, India and china, to study differences between HIV-1 subtypes in drug resistance to current first-line, WHO- recommended treatment regimens. In collaboration with Monogram Biosciences we will assess the importance of mutations and patterns in these samples using an advanced method for phenotypic resistance testing. The goals of this proposal are to (i) validate low-cost resistance testing; (ii) determine frequency and patterns of virological failure and drug resistance after 1 and 2 years of ART; and (iii) conduct genotypic analyses and phenotypic validation of subtype-specific mutations and patterns. PUBLIC HEALTH RELEVANCE: The HIV-1 pandemic is a global emergency caused by multiple subtypes. Evolution of anti-HIV drug resistance is the main cause and consequence of drug treatment failure. Most knowledge about drug resistance stems from work in the US and Europe on the relatively uncommon subtype B HIV-1. In resource limited settings, where the majority of the pandemic prevails, non-B subtypes and circulating recombinant forms (CRF) predominate. Treatment access programs are rapidly increasing the numbers of AIDS patients, throughout the world, who are receiving combinations of antiretroviral therapies (ART). Our long-term goal is to determine the how different subtypes of HIV-1 respond to treatment with antiretroviral drugs and the significance of subtype in the selection and the evolution of drug resistance.

描述(申请人提供)：人类免疫缺陷病毒(HIV-1)大流行是由于世界各地广泛分布的多种亚型和新出现的重组病毒。对这种流行病的一个重要应对措施是在全球范围内扩大获得抗逆转录病毒治疗(ART)计划的机会，可能会向数百万受感染的人提供抗逆转录病毒治疗。成功长期治疗的一个障碍是出现耐药性，这种耐药性是由病毒基因中选择的突变引起的，这既是ART失败的原因，也是ART失败的后果。有关抗药性的知识主要来自美国和欧洲，主要集中在一种艾滋病毒-1变种-B亚型上。然而，全球90%的感染发生在非洲和亚洲的资源有限的环境中，在那里，其他不同的非B型艾滋病毒-1亚型占主导地位。有强有力的初步证据表明，治疗前的基因型在不同的亚型中不同，甚至在治疗前，在非B亚型中，与耐药性相关的位置可能会发生明显的突变。此外，在接触药物后，在非B亚型中检测到明显的新突变。有关非B类病毒的易感性和耐药性的信息对于维持抗逆转录病毒疗法的益处的战略至关重要。在资源有限的情况下，传播和获得性耐药的流行率和发病率将推动公共卫生艾滋病毒治疗计划中关于诊断测试、初始和二线治疗的决定。这项提议的重点是在三个资源有限的环境中建立监测和监测耐药性的科学基础设施，在这些环境中，特定的非B亚型占主导地位。通过这些研究，我们将开发一个强大的HIV-1非B变种序列数据库，用于耐药突变和模式的基因分析和表型验证。我们设计了一个计划，首先开发质量保证、低成本的耐药性监测策略，使用干燥的过滤器样本进行耐药性测试。这些战略将在泰国、印度和中国实施，以研究艾滋病毒-1亚型对当前世卫组织推荐的一线治疗方案的耐药性差异。我们将与Mongraph生物科学公司合作，使用一种先进的表型耐药性测试方法来评估这些样本中突变和模式的重要性。这项建议的目标是(I)验证低成本的耐药性测试；(Ii)在接受抗逆转录病毒治疗1年和2年后确定病毒学失败和耐药性的频率和模式；以及(Iii)对特定亚型的突变和模式进行基因分析和表型验证。 公共卫生相关性：艾滋病毒-1大流行是由多种亚型引起的全球紧急情况。抗HIV耐药性的演变是药物治疗失败的主要原因和后果。有关耐药性的大部分知识来自美国和欧洲在相对不常见的B型HIV-1亚型方面的工作。在资源有限的情况下，大多数大流行流行，非B亚型和循环重组形式(CRF)占主导地位。获得治疗方案正在迅速增加全世界接受抗逆转录病毒疗法(ART)组合的艾滋病患者的数量。我们的长期目标是确定不同的HIV-1亚型对抗逆转录病毒药物治疗的反应，以及亚型在选择和耐药进化中的意义。