作者
Harald Mischak, Günter Allmaier, Rolf Apweiler, Teresa Attwood, Marc Baumann, Ariela Benigni, Samuel E Bennett, Rainer Bischoff, Erik Bongcam-Rudloff, Giovambattista Capasso, Joshua J Coon, Patrick D’Haese, Anna F Dominiczak, Mohammed Dakna, Hassan Dihazi, Jochen H Ehrich, Patricia Fernandez-Llama, Danilo Fliser, Jorgen Frokiaer, Jerome Garin, Mark Girolami, William S Hancock, Marion Haubitz, Denis Hochstrasser, Rury R Holman, John PA Ioannidis, Joachim Jankowski, Bruce A Julian, Jon B Klein, Walter Kolch, Theo Luider, Ziad Massy, William B Mattes, Franck Molina, Bernard Monsarrat, Jan Novak, Karlheinz Peter, Peter Rossing, Marta Sánchez-Carbayo, Joost P Schanstra, O John Semmes, Goce Spasovski, Dan Theodorescu, Visith Thongboonkerd, Raymond Vanholder, Timothy D Veenstra, Eva Weissinger, Tadashi Yamamoto, Antonia Vlahou
发表日期
2010/8/25
来源
Science translational medicine
卷号
2
期号
46
页码范围
46ps42-46ps42
出版商
American Association for the Advancement of Science
简介
Clinical proteomics has yielded some early positive results—the identification of potential disease biomarkers—indicating the promise for this analytical approach to improve the current state of the art in clinical practice. However, the inability to verify some candidate molecules in subsequent studies has led to skepticism among many clinicians and regulatory bodies, and it has become evident that commonly encountered shortcomings in fundamental aspects of experimental design mainly during biomarker discovery must be addressed in order to provide robust data. In this Perspective, we assert that successful studies generally use suitable statistical approaches for biomarker definition and confirm results in independent test sets; in addition, we describe a brief set of practical and feasible recommendations that we have developed for investigators to properly identify and qualify proteomic biomarkers, which could …
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H Mischak, G Allmaier, R Apweiler, T Attwood… - Science translational medicine, 2010