Targeting resitin and RELM-beta to treat pulmonary hypertension

靶向抵抗素和 RELM-β 治疗肺动脉高压

• 批准号: 8757198
• 负责人: Roger A Johns
• 金额: $ 156.28万
• 依托单位: JOHNS HOPKINS UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2014
• 资助国家: 美国
• 起止时间: 2014-09-22 至 2016-06-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8757198
• 关键词: Animal Model; Animals; Antibodies; Antibody Affinity; Antigens; Biological Assay; Biological Availability; Biological Markers; Cardiac; Cell Line; Cells; Chronic; Clinical; Common Epitope; Data; Dependovirus; Development; Diagnosis; Disease; Drug Formulations; Drug Kinetics; Etiology; Fibroblasts; Fibrosis; Functional disorder; Gene Expression; Genetic; Genetic Polymorphism; Genomics; Heart; Heart Hypertrophy; Heart failure; Human; Human Development; Hypertension; Hypoxia; Image; Inflammatory; Interleukin-2; Investigational Drugs; Investigational New Drug Application; Knock-out; Lead; Lesion; Lung; Modeling; Muscle Cells; Myofibroblast; Pathway interactions; Patients; Pharmacodynamics; Production; Protein Family; Proteins; Pulmonary Hypertension; Research; Research Project Grants; Right Ventricular Dysfunction; Right ventricular structure; Risk; Rodent; Rodent Model; Role; Sampling; Sarcomeres; Scleroderma; Series; Serum; Severities; Specialized Center; Testing; Therapeutic; Therapeutic antibodies; Toxicology; Validation; Vascular remodeling; Work; abstracting; base; chemokine; clinical efficacy; cysteine-rich secreted protein FIZZ3; cytokine; gain of function; hemodynamics; human data; immunogenicity; in vivo; loss of function; manufacturing scale-up; monocyte; mouse model; novel; overexpression; patient population; peripheral blood; preclinical evaluation; preclinical study; prevent; pulmonary arterial hypertension; resistin; response; small hairpin RNA; therapeutic target

DESCRIPTION (provided by applicant): The resistin-like molecule (RELM) family of proteins comprises pleiotropic cytokines critically involved in the vascular remodeling and cardiac dysfunction seen in animal and human pulmonary arterial hypertension (PH). Our rodent and human work and the work of others strongly suggests that human resistin (hResistin) and human RELM¿ (hRELM¿) are mechanistically important to the etiology of human PH and associated right ventricular dysfunction (RVD) and serve as potential biomarkers and therapeutic targets for this disease. IN the CADET I we accomplished target validation and developed a series of human antibodies against hResistin and against hRELM¿ including some that recognized both targets. The first aim (UH2) will identify an optimal lead antibody through biophysical and antigen-antibody interaction studies, antibody inhibition of target effects in cell based assays, and clinical efficacy studies of antibodies in our humanized overexpressing resistin and RELM¿ mouse models of PH. It will also include antibody affinity maturation and optimization as needed and initial GLP cell line selection and optimization. This aim will further assess the selectivity, functionality and "drugability" of our lead candidates. The second aim (UH3) will evaluate the in vivo pharmacokinetics and pharmacodynamics of our lead candidate(s), perform toxicology, immunogenicity and bioavailability studies in animal models, further optimize cell production efficiency of the lead antibody, and manufacture and scale-up GMP production of the lead antibody(ies). It will include pre-formulation development and clinical formulation development. It will end with creation and filing of our IND application with the FDA. The third aim (UH2, UH3) will explore and develop the biomarker potential of human resistin and RELM¿ to assess severity and progression of PH and to predict response to therapy, by studying the functional role of genetic polymorphisms, PBMC gene expression, and serum levels for these proteins, and integrating and correlating these findings with the demographic, hemodynamic, clinical, genetic and genomic data already obtained in our recent SCCOR grant on pulmonary arterial hypertension, with a primary focus on PH and cardiac function. (End of Abstract)

描述（由申请人提供）：抵抗素样分子（RELM）蛋白家族包含与动物和人类肺动脉高压（PH）中观察到的血管重塑和心脏功能障碍密切相关的多效性细胞因子。其他人强烈建议人类抵抗素（hResistin）和人类 RELM¿ (hRELM¿) 对于人类 PH 和相关右心室功能障碍 (RVD) 的病因学具有重要的机制，并可作为该疾病的潜在生物标志物和治疗靶点。在 CADET I 中，我们完成了靶点验证并开发了一系列针对 hResistin 的人类抗体。并反对 hRELM¿第一个目标（UH2）将通过生物物理和抗原抗体相互作用研究、抗体抑制细胞中的靶点效应来确定最佳的先导抗体。 基于我们的人源化过表达抵抗素和 RELM 中抗体的测定和临床功效研究它还将包括根据需要进行抗体亲和力成熟和优化以及初始 GLP 细胞系选择和优化。第二个目标 (UH3) 将进一步评估我们的主要候选药物的选择性、功能和“成药性”。评估我们的主要候选药物的体内药代动力学和药效学，在动物模型中进行毒理学、免疫原性和生物利用度研究，进一步优化先导抗体的细胞生产效率，并制造和扩大先导抗体的 GMP 生产它将包括预制剂开发和临床制剂开发，最终将向 FDA 提交 IND 申请。第三个目标（UH2、UH3）将探索和开发人类抵抗素的生物标志物潜力。和 RELM¿通过研究遗传多态性、PBMC 基因表达和这些蛋白质的血清水平的功能作用，并将这些发现与人口统计学、血流动力学、临床、遗传和我们最近获得的关于肺动脉高压的 SCCOR 资助中已经获得了基因组数据，主要关注肺动脉高压和心脏功能。 （摘要完）