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首页> 外文期刊>Cell cycle >Serum and urinary biomarker signatures for rapid preclinical in vivo assessment of CDK inhibition as a therapeutic approach for PKD.
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Serum and urinary biomarker signatures for rapid preclinical in vivo assessment of CDK inhibition as a therapeutic approach for PKD.

机译:血清和尿液生物标志物签名,用于临床前体内CDK抑制的快速评估,作为PKD的治疗方法。

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摘要

Recent advances in understanding the molecular pathogenesis of polycystic kidney diseases (PKD) are being translated into promising treatments. Currently, a response to therapy in preclinical animal models of PKD can only be evaluated after several weeks of treatment. The availability of biomarkers for rapid efficacy assessment would greatly facilitate the drug development process. Here we applied SELDI-TOF technology to establish serum and urinary biomarker signatures associated with a rapid therapeutic response to cyclin dependent kinase (CDK) inhibitor roscovitine in the jck mouse model of PKD. A set of 74 serum and 56 urinary markers was identified in the group receiving chronic treatment over 5 weeks. This set was further screened for early efficacy biomarkers in acutely (3-5 days) treated animals with mild (26 days of age) and advanced disease (50 days of age). A third group with intermediate disease (33 days of age) received a single injection to monitor rapid changes in protein profiles within 4, 24 or 48 hours after drug administration. Multifactorial comparative analysis of the acutely treated groups identified a set of 20 urinary and 21 serum efficacy biomarkers. This biomarker signature provides a necessary tool for further assessment of CDK inhibitors as therapeutic agents for PKD.
机译:在了解多囊性肾脏疾病(PKD)的分子发病机理方面的最新进展已转化为有前途的治疗方法。目前,只有在治疗几周后才能评估PKD临床前动物模型对治疗的反应。用于快速功效评估的生物标志物的可用性将极大地促进药物开发过程。在这里,我们应用SELDI-TOF技术来建立与PKD的jck小鼠模型中对细胞周期蛋白依赖性激酶(CDK)抑制剂roscovitine的快速治疗反应相关的血清和尿液生物标志物特征。在接受为期5周的慢性治疗的组中,鉴定出一组74个血清和56个尿液标记物。在患有轻度(26天大)和晚期疾病(50天大)的急性(3-5天)治疗的动物中进一步筛选该组的早期功效生物标志物。第三组患有中间疾病(33天龄)的人在给药后4、24或48小时内接受了一次注射以监测蛋白质谱的快速变化。急性治疗组的多因素比较分析确定了一组20种尿液和21种血清功效生物标志物。这种生物标志物的特征为进一步评估CDK抑制剂作为PKD的治疗剂提供了必要的工具。

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