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首页> 外文期刊>The AAPS Journal >Translational Biomarkers: from Preclinical to Clinical a Report of 2009 AAPS/ACCP Biomarker Workshop
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Translational Biomarkers: from Preclinical to Clinical a Report of 2009 AAPS/ACCP Biomarker Workshop

机译:转化型生物标志物:从临床前到临床,2009 AAPS / ACCP生物标志物研讨会报告

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摘要

There have been some successes in qualifying biomarkers and applying them to drug development and clinical treatment of various diseases. A recent success is illustrated by a collaborative effort among the US Food and Drug Administration, the European Medicines Agency, and the pharmaceutical industry to provide a set of seven preclinical kidney toxicity biomarkers for drug development. Other successes include, but are not limited to, clinical biomarkers for cancer treatment and clinical management of heart transplant patients. The value of fully qualified surrogate endpoints in facilitating successful drug development is undisputed, especially for diseases in which the traditional clinical outcome can only be assessed in large, multi-year trials. Emerging biomarkers, including chemical genomic or imaging biomarkers, and measurement of circulating tumor cells hold great promise for early diagnosis of disease and as prognostic tests for managing treatment of chronic diseases such as osteoarthritis, Alzheimer disease, cardiovascular disease, and cancer. To advance the success of treating and managing these diseases, efforts are needed to establish the temporal relationship between changes in inflammatory or imaging biomarkers with the progression of the chronic disease, and in the case of cancer, between the extent of circulating cancer cells and tumor progression or remission.
机译:在鉴定生物标志物并将其应用于药物开发和各种疾病的临床治疗方面取得了一些成功。美国食品药品监督管理局,欧洲药品管理局和制药行业之间的合作努力表明了最近的成功,该合作为药物开发提供了一套七种临床前肾毒性生物标志物。其他成功包括但不限于用于癌症治疗和心脏移植患者临床管理的临床生物标志物。毫无疑问,完全合格的替代终点在促进药物开发成功方面的价值是无可争议的,特别是对于那些只能在大型,多年试验中评估传统临床结果的疾病。新兴的生物标志物,包括化学基因组或成像生物标志物,以及对循环肿瘤细胞的测量,对于疾病的早期诊断和作为治疗慢性疾病(如骨关节炎,阿尔茨海默病,心血管疾病和癌症)的预后测试具有广阔的前景。为了促进治疗和控制这些疾病的成功,需要努力建立炎性或成像生物标志物的变化与慢性疾病进展之间的时间关系,在癌症的情况下,在循环癌细胞和肿瘤的程度之间建立时间关系。进展或缓解。

著录项

  • 来源
    《The AAPS Journal》 |2011年第2期|274-283|共10页
  • 作者单位

    Office of Clinical Pharmacology Office of Translational Science Center for Drug Evaluation and Research US Food and Drug Administration Silver Spring Maryland USA;

    Drug ampamp Biotechnology Development LLC Clearwater Florida USA;

    Office of Translational Science Center for Drug Evaluation and Research US Food and Drug Administration Silver Spring Maryland 20993 USA;

    Office of Clinical Pharmacology Office of Translational Science Center for Drug Evaluation and Research US Food and Drug Administration Silver Spring Maryland USA;

    EMEA Canary Wharf London UK;

    XDx Expression Diagnostics Brisbane California USA;

    Office of Clinical Pharmacology Office of Translational Science Center for Drug Evaluation and Research US Food and Drug Administration Silver Spring Maryland USA;

    University of Buffalo State University of New York Buffalo New York USA;

    Office of Clinical Pharmacology Office of Translational Science Center for Drug Evaluation and Research US Food and Drug Administration Silver Spring Maryland USA;

    University of Tennessee Memphis Tennessee USA;

    Amgen Inc Thousand Oaks California USA;

    Merck ampamp Co Inc. Rahway New Jersey USA;

    University of Michigan Ann Arbor Michigan USA;

    Washington University in St. Louis St. Louis Missouri USA;

    Merck ampamp Co Inc. Rahway New Jersey USA;

    Hospital of the University of Pennsylvania Philadelphia Pennsylvania USA;

    Office of Translational Science Center for Drug Evaluation and Research US Food and Drug Administration Silver Spring Maryland 20993 USA;

    Bristol-Myers Squibb Lawrenceville New Jersey USA;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    biomarkers; diagnostic; diseases; gene expression; imaging;

    机译:生物标志物;诊断;疾病;基因表达;成像;

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