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11 results on '"Gruidl, Michael"'

1. Gene expression--based survival prediction in lung adenocarcinoma: a multi-site, blinded validation study

Author

Shedden, Kerby, Taylor, Jeremy M.G., Enkemann, Steven A., Tsao, Ming-Sound, Yeatman, Timothy J., Gerald, William L., Eschrich, Steven, Jurisica, Igor, Giordano, Thomas J., Misek, David E., Chang, Andrew C., Zhu, Chang Qi, Strumpf, Daniel, Hanash, Samir, Shepherd, Frances A., Ding, Keyue, Seymour, Lesley, Naoki, Katsuhiko, Pennell, Nathan, Weir, Barbara, Verhaak, Roel, Ladd-Acosta, Christine, Golub, Todd, Gruidl, Michael, Sharma, Anupama, Szoke, Janos, Zakowski, Maureen, Rusch, Valerie, Kris, Mark, Viale, Agnes, Motoi, Noriko, Travis, William, Conley, Barbara, Seshan, Venkatraman E., Meyerson, Matthew, Kuick, Rork, Dobbin, Kevin K., Lively, Tracy, Jacobson, James W., and Beer, David G.

Subjects
DNA microarrays -- Usage -- Research -- Genetic aspects -- Reports -- Health aspects, Gene expression -- Research -- Reports -- Genetic aspects -- Health aspects -- Usage, Cancer -- Adjuvant treatment, Metastasis -- Research -- Genetic aspects, Lung cancer -- Health aspects -- Reports -- Genetic aspects -- Research, Biological sciences, Health
Abstract

Although prognostic gene expression signatures for survival in early-stage lung cancer have been proposed, for clinical application, it is critical to establish their performance across different subject populations and in different laboratories. Here we report a large, training-testing, multi-site, blinded validation study to characterize the performance of several prognostic models based on gene expression for 442 lung adenocarcinomas. The hypotheses proposed examined whether microarray measurements of gene expression either alone or combined with basic clinical covariates (stage, age, sex) could be used to predict overall survival in lung cancer subjects. Several models examined produced risk scores that substantially correlated with actual subject outcome. Most methods performed better with clinical data, supporting the combined use of clinical and molecular information when building prognostic models for early-stage lung cancer. This study also provides the largest available set of microarray data with extensive pathological and clinical annotation for lung adenocarcinomas., In the United States and in many Western countries, lung cancer represents the leading cause of cancer-related death (1). The 5-year, overall survival rate is 15% and has not improved [...]

Published
2008

4. Phase IIA Chemopreventative Study of Selenium in Persons at Risk for Lung Cancer

Author

UNIVERSITY OF SOUTH FLORIDA TAMPA, Gruidl, Michael E., Walsh, Frank, UNIVERSITY OF SOUTH FLORIDA TAMPA, Gruidl, Michael E., and Walsh, Frank

Abstract

Selenized yeast has also recently been shown to reduce lung cancer incidence and mortality in a population of skin cancer patients. Smokers and survivors of early stage lung and head and neck cancers have had a long period of promotion by carcinogenic agents on the bronchial epithelium resulting in morphologic and molecular alterations. We hypothesize that these morphologic and molecular alterations can be detected and modulated by chemopreventive agents. We have proposed a Phase IIa chemoprevention trial evaluating five different dose levels of selenium administered daily for 3 months in subjects at high risk for lung cancer with bronchoscopically documented dysplasia. Subjects will be entered to determine the effect of dose on the modulation of biomarkers in response to selenium supplementation as well as to measure selenium levels and modulation of glutathione peroxidase as a measure of drug effect. In addition to morphology, the surrogate endpoint biomarkers to be examined include apoptosis, p53 expression, K-ras mutation analysis, p16 methylation, and upregulation of hnRNP A2/B1. Successful completion of this study will support selenium supplementation as potentially beneficial therapy in preventing the progression of lung carcinogenesis as well as identify surrogate endpoint markers that appear to be modulated by selenium supplementation.

Published
2001

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