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Cancer Pharmacogenomics and Pharmacoepidemiology: Setting a Research Agenda to Accelerate Translation

Recent advances in genomic research have demonstrated a substantial role for genomic factors in predicting response to cancer therapies. Researchers in the fields of cancer pharmacogenomics and pharmacoepidemiology seek to understand why individuals respond differently to drug therapy, in terms of b...

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Autores principales: Freedman, Andrew N., Sansbury, Leah B., Figg, William D., Potosky, Arnold L., Weiss Smith, Sheila R., Khoury, Muin J., Nelson, Stefanie A., Weinshilboum, Richard M., Ratain, Mark J., McLeod, Howard L., Epstein, Robert S., Ginsburg, Geoffrey S., Schilsky, Richard L., Liu, Geoffrey, Flockhart, David A., Ulrich, Cornelia M., Davis, Robert L., Lesko, Lawrence J., Zineh, Issam, Randhawa, Gurvaneet, Ambrosone, Christine B., Relling, Mary V., Rothman, Nat, Xie, Heng, Spitz, Margaret R., Ballard-Barbash, Rachel, Doroshow, James H., Minasian, Lori M.
Formato: Texto
Lenguaje:English
Publicado: Oxford University Press 2010
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2982809/
https://www.ncbi.nlm.nih.gov/pubmed/20944079
http://dx.doi.org/10.1093/jnci/djq390
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author Freedman, Andrew N.
Sansbury, Leah B.
Figg, William D.
Potosky, Arnold L.
Weiss Smith, Sheila R.
Khoury, Muin J.
Nelson, Stefanie A.
Weinshilboum, Richard M.
Ratain, Mark J.
McLeod, Howard L.
Epstein, Robert S.
Ginsburg, Geoffrey S.
Schilsky, Richard L.
Liu, Geoffrey
Flockhart, David A.
Ulrich, Cornelia M.
Davis, Robert L.
Lesko, Lawrence J.
Zineh, Issam
Randhawa, Gurvaneet
Ambrosone, Christine B.
Relling, Mary V.
Rothman, Nat
Xie, Heng
Spitz, Margaret R.
Ballard-Barbash, Rachel
Doroshow, James H.
Minasian, Lori M.
author_facet Freedman, Andrew N.
Sansbury, Leah B.
Figg, William D.
Potosky, Arnold L.
Weiss Smith, Sheila R.
Khoury, Muin J.
Nelson, Stefanie A.
Weinshilboum, Richard M.
Ratain, Mark J.
McLeod, Howard L.
Epstein, Robert S.
Ginsburg, Geoffrey S.
Schilsky, Richard L.
Liu, Geoffrey
Flockhart, David A.
Ulrich, Cornelia M.
Davis, Robert L.
Lesko, Lawrence J.
Zineh, Issam
Randhawa, Gurvaneet
Ambrosone, Christine B.
Relling, Mary V.
Rothman, Nat
Xie, Heng
Spitz, Margaret R.
Ballard-Barbash, Rachel
Doroshow, James H.
Minasian, Lori M.
author_sort Freedman, Andrew N.
collection PubMed
description Recent advances in genomic research have demonstrated a substantial role for genomic factors in predicting response to cancer therapies. Researchers in the fields of cancer pharmacogenomics and pharmacoepidemiology seek to understand why individuals respond differently to drug therapy, in terms of both adverse effects and treatment efficacy. To identify research priorities as well as the resources and infrastructure needed to advance these fields, the National Cancer Institute (NCI) sponsored a workshop titled “Cancer Pharmacogenomics: Setting a Research Agenda to Accelerate Translation” on July 21, 2009, in Bethesda, MD. In this commentary, we summarize and discuss five science-based recommendations and four infrastructure-based recommendations that were identified as a result of discussions held during this workshop. Key recommendations include 1) supporting the routine collection of germline and tumor biospecimens in NCI-sponsored clinical trials and in some observational and population-based studies; 2) incorporating pharmacogenomic markers into clinical trials; 3) addressing the ethical, legal, social, and biospecimen- and data-sharing implications of pharmacogenomic and pharmacoepidemiologic research; and 4) establishing partnerships across NCI, with other federal agencies, and with industry. Together, these recommendations will facilitate the discovery and validation of clinical, sociodemographic, lifestyle, and genomic markers related to cancer treatment response and adverse events, and they will improve both the speed and efficiency by which new pharmacogenomic and pharmacoepidemiologic information is translated into clinical practice.
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spelling pubmed-29828092010-11-17 Cancer Pharmacogenomics and Pharmacoepidemiology: Setting a Research Agenda to Accelerate Translation Freedman, Andrew N. Sansbury, Leah B. Figg, William D. Potosky, Arnold L. Weiss Smith, Sheila R. Khoury, Muin J. Nelson, Stefanie A. Weinshilboum, Richard M. Ratain, Mark J. McLeod, Howard L. Epstein, Robert S. Ginsburg, Geoffrey S. Schilsky, Richard L. Liu, Geoffrey Flockhart, David A. Ulrich, Cornelia M. Davis, Robert L. Lesko, Lawrence J. Zineh, Issam Randhawa, Gurvaneet Ambrosone, Christine B. Relling, Mary V. Rothman, Nat Xie, Heng Spitz, Margaret R. Ballard-Barbash, Rachel Doroshow, James H. Minasian, Lori M. J Natl Cancer Inst Commentary Recent advances in genomic research have demonstrated a substantial role for genomic factors in predicting response to cancer therapies. Researchers in the fields of cancer pharmacogenomics and pharmacoepidemiology seek to understand why individuals respond differently to drug therapy, in terms of both adverse effects and treatment efficacy. To identify research priorities as well as the resources and infrastructure needed to advance these fields, the National Cancer Institute (NCI) sponsored a workshop titled “Cancer Pharmacogenomics: Setting a Research Agenda to Accelerate Translation” on July 21, 2009, in Bethesda, MD. In this commentary, we summarize and discuss five science-based recommendations and four infrastructure-based recommendations that were identified as a result of discussions held during this workshop. Key recommendations include 1) supporting the routine collection of germline and tumor biospecimens in NCI-sponsored clinical trials and in some observational and population-based studies; 2) incorporating pharmacogenomic markers into clinical trials; 3) addressing the ethical, legal, social, and biospecimen- and data-sharing implications of pharmacogenomic and pharmacoepidemiologic research; and 4) establishing partnerships across NCI, with other federal agencies, and with industry. Together, these recommendations will facilitate the discovery and validation of clinical, sociodemographic, lifestyle, and genomic markers related to cancer treatment response and adverse events, and they will improve both the speed and efficiency by which new pharmacogenomic and pharmacoepidemiologic information is translated into clinical practice. Oxford University Press 2010-11-17 2010-10-13 /pmc/articles/PMC2982809/ /pubmed/20944079 http://dx.doi.org/10.1093/jnci/djq390 Text en Published by Oxford University Press 2010. This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/2.5), which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Commentary
Freedman, Andrew N.
Sansbury, Leah B.
Figg, William D.
Potosky, Arnold L.
Weiss Smith, Sheila R.
Khoury, Muin J.
Nelson, Stefanie A.
Weinshilboum, Richard M.
Ratain, Mark J.
McLeod, Howard L.
Epstein, Robert S.
Ginsburg, Geoffrey S.
Schilsky, Richard L.
Liu, Geoffrey
Flockhart, David A.
Ulrich, Cornelia M.
Davis, Robert L.
Lesko, Lawrence J.
Zineh, Issam
Randhawa, Gurvaneet
Ambrosone, Christine B.
Relling, Mary V.
Rothman, Nat
Xie, Heng
Spitz, Margaret R.
Ballard-Barbash, Rachel
Doroshow, James H.
Minasian, Lori M.
Cancer Pharmacogenomics and Pharmacoepidemiology: Setting a Research Agenda to Accelerate Translation
title Cancer Pharmacogenomics and Pharmacoepidemiology: Setting a Research Agenda to Accelerate Translation
title_full Cancer Pharmacogenomics and Pharmacoepidemiology: Setting a Research Agenda to Accelerate Translation
title_fullStr Cancer Pharmacogenomics and Pharmacoepidemiology: Setting a Research Agenda to Accelerate Translation
title_full_unstemmed Cancer Pharmacogenomics and Pharmacoepidemiology: Setting a Research Agenda to Accelerate Translation
title_short Cancer Pharmacogenomics and Pharmacoepidemiology: Setting a Research Agenda to Accelerate Translation
title_sort cancer pharmacogenomics and pharmacoepidemiology: setting a research agenda to accelerate translation
topic Commentary
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2982809/
https://www.ncbi.nlm.nih.gov/pubmed/20944079
http://dx.doi.org/10.1093/jnci/djq390
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