481 采用 CTS 团队方法,研究患者生物工程肌肉平台中的骨骼肌疾病和对策

Karly Caples, Zehra Fasih, Elisabeth Barton, S. Malany
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引用次数: 0

摘要

目标/目的:我们的团队开发了一个高通量三维患者肌肉平台,用于研究与骨骼肌疾病相关的信号通路。该平台将用于研究基因突变和衰老过程导致的人类肌肉病变,以及改善肌肉质量、功能和性能的药物干预。方法/研究对象:在目前的研究中,三维骨骼肌由年轻健康的男性样本形成。用尿皮质素 II(UCNII)或载体对样本进行为期十天的处理,并对组织性能进行评估。功能评估包括使用数字图像相关性(DIC)分析电脉冲刺激过程中收集的视频的实时收缩幅度,以及初始和重复张力产生的终点测量。功能测量可提供与药物疗效和毒性相关的患者肌肉同步性、力量和耐力指数,我们将通过 Luminex 将这些指数与促生长蛋白信号相关联。我们还将通过组织学和显微镜分析这些样本的一部分,以评估肌肉纤维密度、类型和大小,以及肌管融合指数和肌节均匀性。结果/预期结果:我们预计,在为期七天的电脉冲刺激方案中,接受 UCNII 治疗的健康肌肉在 DIC 分析中的同步性和收缩幅度都会增加。我们还希望在电脉冲刺激结束时看到 DIC 分析中的持续收缩幅度,这表明与未用药对照组相比,用药治疗组具有抗疲劳性。与我们的实时 DIC 数据一样,我们预计药物治疗组的初始和持续最大产力都会增加。我们预计,药物治疗组肌肉的纤维密度、纤维直径、融合指数和均匀的肌节都将增加。最后,我们预计药物治疗组与对照组相比,促进生长的信号通路会增加。讨论/意义:目前的研究将作为对内源性配体 UCNII 的初步调查,以提高人体肌肉中骨骼肌的质量和性能,为未来的药效和毒性研究奠定框架。这一平台最终将促进肌肉疾病的研究,并将治疗方法应用于临床。
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481 A CTS Team Approach to Investigate Skeletal Muscle Diseases and Countermeasures in a Patient-Derived Bioengineered Muscle Platform
OBJECTIVES/GOALS: Our team has developed a high-throughput 3D patient-derived muscle platform to study signaling pathways associated with skeletal muscle disease. This platform will be used to study pathologies of human muscle that arise from genetic mutations and processes of aging along with pharmacologic interventions to improve mass, function, and performance. METHODS/STUDY POPULATION: In the current study, 3D skeletal muscle is formed from young healthy male samples. Samples are treated with urocortin II (UCNII) or vehicle for ten days and evaluated for tissue performance. Functional assessments include real-time contraction magnitudes using digital image correlation (DIC) analysis of video collected during electrical pulse stimulation and end-point measures of initial and repeated tetanic force production. Functional measures provide indices of patient muscle synchronicity, strength, and endurance related to drug efficacy and toxicity which we will correlate to pro-growth protein signaling via Luminex. A subset of these samples will also be analyzed by histology and microscopy to assess muscle fiber density, type, and size, as well as myotube fusion index and sarcomere uniformity. RESULTS/ANTICIPATED RESULTS: We anticipate that healthy muscle treated with UCNII will have increased synchronicity and contraction magnitudes in DIC analysis throughout their seven-day electrical pulse stimulation protocol. We also expect to see sustained contraction magnitudes in DIC analysis at the end of electrical pulse stimulation indicating fatigue resistance in the drug treated group compared to no-drug control. Like our real-time DIC data, we anticipate increases to initial and sustained maximal force production in the drug treated group. We expect that drug treated muscle will present with an increased fiber density, fiber diameter, and fusion index with uniform sarcomeres. Finally, we expect heightened pro-growth signaling pathways in treated vs. controls. DISCUSSION/SIGNIFICANCE: The current study will serve as an initial investigation of the endogenous ligand UCNII for enhancing skeletal muscle mass and performance in human muscle laying the framework for future drug efficacy and toxicity studies. This platform will ultimately enhance the study of muscle diseases and translation of therapeutics to clinical settings.
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