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In vivo imaging biomarkers of neuroinflammation in the development and assessment of stroke therapies - towards clinical translation

机译:中风疗法的开发和评估中神经炎症的体内成像生物标志物-走向临床翻译

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摘要

Modulation of the inflammatory microenvironment after stroke opens a new avenue for the development of novel neurorestorative therapies in stroke. Understanding the spatio-temporal profile of (neuro-)inflammatory imaging biomarkers in detail thereby represents a crucial factor in the development and application of immunomodulatory therapies. The early integration of quantitative molecular imaging biomarkers in stroke drug development may provide key information about (i) early diagnosis and follow-up, (ii) spatio-temporal drug-target engagement (pharmacodynamic biomarker), (iii) differentiation of responders and non-responders in the patient cohort (inclusion/exclusion criteria; predictive biomarkers), and (iv) the mechanism of action. The use of targeted imaging biomarkers for may thus allow clinicians to decipher the profile of patient-specific inflammatory activity and the development of patient-tailored strategies for immunomodulatory and neuro-restorative therapies in stroke. Here, we highlight the recent developments in preclinical and clinical molecular imaging biomarkers of neuroinflammation (endothelial markers, microglia, MMPs, cell labeling, future developments) in stroke and outline how imaging biomarkers can be used in overcoming current translational roadblocks and attrition in order to advance new immunomodulatory compounds within the clinical pipeline.
机译:中风后炎性微环境的调节为中风中新型神经修复疗法的发展开辟了一条新途径。因此,详细了解(神经)炎症成像生物标志物的时空分布是免疫调节疗法发展和应用中的关键因素。定量分子成像生物标记物在中风药物开发中的早期整合可能提供有关以下方面的关键信息:(i)早期诊断和随访,(ii)时空药物靶标参与(药效生物标记物),(iii)应答者与非应答者的区分-患者队列中的反应者(纳入/排除标准;预测性生物标志物),以及(iv)作用机理。因此,使用靶向成像生物标记物可以使临床医生了解患者特异性炎症活动的概况,并开发针对卒中的免疫调节和神经修复疗法的针对患者的策略。在这里,我们重点介绍中风神经炎症的临床前和临床分子成像生物标记物(内皮标记物,小胶质细胞,MMP,细胞标记,未来发展)的最新发展,并概述如何将成像生物标记物用于克服当前的翻译障碍和耗损,从而在临床流程中推进新的免疫调节化合物。

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