Prediction and Treatment for Cancer Immunotherapy Induced Myocarditis

癌症免疫治疗引起的心肌炎的预测和治疗

• 批准号: 10217416
• 负责人: Hua Pan
• 金额: $ 18.69万
• 依托单位: UNIVERSITY OF SOUTH FLORIDA
• 依托单位国家: 美国
• 财政年份: 2021
• 资助国家: 美国
• 起止时间: 2021-05-01 至 2022-01-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/10217416
• 关键词: Address; Affect; Animal Model; Anti-Inflammatory Agents; Autoimmune; Back; Biological Markers; Bladder; Blood Chemical Analysis; Blood Circulation; Blood specimen; Bortezomib; Breast; CTLA4 gene; Cancer Patient; Cardiac; Cardiotoxicity; Cardiovascular system; Cells; Clinical; Clinical Trials; Diagnosis; Disseminated Malignant Neoplasm; Electrocardiogram; Enrollment; Evaluation; Exhibits; FDA approved; Female; Genomic approach; Goals; Heart; Histology; Hodgkin Disease; Immune; Immune checkpoint inhibitor; Immune system; Immunologic Markers; Immunosuppression; Immunotherapy; Impairment; Infiltration; Inflammation; Inflammatory; Intravenous; Investigation; Kidney; Kinetics; Life; Liver; Lung; Lymph Node of Head, Face and Neck; Malignant Neoplasms; Malignant neoplasm of urinary bladder; Medical; Messenger RNA; Metastatic Neoplasm to the Lung; Mus; Myocarditis; NF-kappa B; Nivolumab; Non-Small-Cell Lung Carcinoma; Normal tissue morphology; Organ; Ovary; PD-1 inhibitors; Pathogenesis; Pathway Analysis; Patients; Peptides; Precision therapeutics; Predictive Value; Prevalence; Production; Publishing; RNA; Renal Cell Carcinoma; Renal carcinoma; Reporting; Research; Safety; Sensitivity and Specificity; Signal Pathway; Signal Transduction; Skin; Small Interfering RNA; Small RNA; Steroids; System; T-Lymphocyte; Testing; Therapeutic Effect; Tissues; Toxin; Treatment Efficacy; Troponin; Tumor Immunity; anti-PD-L1; anti-PD1 therapy; anti-cancer; anticancer treatment; autoimmune arthritis; base; body system; cancer cell; cancer immunotherapy; cancer therapy; clinical practice; cohort; cytokine; design; early detection biomarkers; exosome; experience; heart function; immune checkpoint; immune-related adverse events; improved; ipilimumab; knock-down; macrophage; male; melanoma; mouse model; nano; nanoparticle; nanoparticle delivery; nanotherapeutic; new technology; novel; novel strategies; novel therapeutic intervention; p65; pembrolizumab; potential biomarker; predictive marker; programmed cell death ligand 1; programmed cell death protein 1; siRNA delivery; side effect; success; transcriptome sequencing; transcriptomics; tumor microenvironment

Abstract In the past 10 years, the FDA has approved 6 checkpoint inhibitors and quickly expanded indications from melanoma and non-small cell lung cancer to Hodgkin lymphoma, kidney, and bladder cancer. Moreover, there are more than 150 ongoing clinical trials on PD-1 inhibitors treatment alone. Despite the anti-cancer benefits, immunotherapy associated immune related adverse events affect a broad spectrum of organs, including heart. Current diagnosis in clinical practices are troponin test and electrocardiograms, which, however, lack of necessary sensitivity and specificity to myocarditis. Accordingly, in Specific Aim 1, we seek to identify transcriptomic (RNAseq/MirSeq) biomarkers that may have predictive value for checkpoint inhibitor treatment induced myocarditis. In this specific aim, we will be focused on patients who have developed autoimmune myocarditis after receiving checkpoint inhibitor treatments and have blood samples banked. Such patients provided an opportunity to identify new associative and predictive biomarkers that can serve as guideposts for the implementation of new therapeutic approaches to suppress the inflammatory drivers of cardiotoxicity. For medical management of immune Checkpoint Inhibitors associated myocarditis, current practices of subscribing steroids expose patients to immune suppression systemically. In Specific Aim 2, we will evaluate a new anti- inflammatory peptide-based nanoparticle system for delivering siRNA against NF-κB to manage myocarditis induced by immune checkpoint inhibitors. Different from currently existing approaches, the new technology proposed in Specific Aim 2 would enable anti-inflammation treatment delivery only to inflamed region in the heart. Moreover, the testing agent has known anti-cancer effects. Therefore, the success of Specific Aim 2 could provide precision treatment delivery and minimize systemic off-target side effects.

抽象的 过去10年，FDA批准了6种检查点抑制剂，并迅速扩大适应症 黑色素瘤、非小细胞肺癌、霍奇金淋巴瘤、肾癌和膀胱癌。 尽管有抗癌功效，但仍有超过 150 项针对 PD-1 抑制剂治疗的临床试验正在进行中。 免疫治疗相关的免疫相关不良事件影响广泛的器官，包括心脏。 目前临床实践中的诊断方法是肌钙蛋白测试和心电图，但缺乏 因此，在具体目标 1 中，我们力求确定对心肌炎的必要敏感性和特异性。 可能对检查点抑制剂治疗具有预测价值的转录组 (RNAseq/MirSeq) 生物标志物 在这个特定目标中，我们将重点关注患有自身免疫性心肌炎的患者。 接受检查点抑制剂治疗并储存血液样本后出现心肌炎的患者。 提供了一个机会来识别新的关联和预测生物标志物，这些生物标志物可以作为路标 实施新的治疗方法来抑制心脏毒性的炎症驱动因素。 免疫检查点抑制剂相关心肌炎的医疗管理，当前订阅实践 在具体目标 2 中，我们将评估一种新的抗类固醇药物。 基于炎症肽的纳米颗粒系统，用于递送针对 NF-κB 的 siRNA 来治疗心肌炎 与目前现有的方法不同，这项新技术是由免疫检查点抑制剂诱导的。 具体目标 2 中提出的方案将能够仅向心脏发炎区域提供抗炎治疗。 此外，该测试剂具有已知的抗癌作用，因此Specific Aim 2的成功可能。 提供精准的治疗并最大限度地减少系统性脱靶副作用。