Gastric cancer pharmacogenetics: progress or old tripe?

Author:

Patel Jai N12,Fuchs Charles S3,Owzar Kouros4,Chen Zihua5,McLeod Howard L26

Affiliation:

1. UNC Institute for Pharmacogenomics & Individualized Therapy, University of North Carolina, 120 Mason Farm Road, CB #7361, Room 1010, Chapel Hill, NC 27599-7361, USA

2. University of North Carolina, Eshelman School of Pharmacy, NC, USA

3. Dana-Farber Cancer Institute, Boston, MA, USA

4. Duke Department of Biostatistics & Bioinformatics, Durham, NC, USA

5. Xiang Ya Hospital, Changsha, China

6. UNC Institute for Pharmacogenomics & Individualized Therapy, University of North Carolina, 120 Mason Farm Road, CB #7361, Room 1010, Chapel Hill, NC 27599-7361, USA. .

Abstract

Gastric cancer remains the second most frequent cause of cancer-related mortality. While surgery is traditionally the initial treatment for early-stage disease, the addition of chemotherapy has been shown to significantly increase overall survival and progression-free survival in advanced and metastatic stages of disease. However, despite the incorporation of newer chemotherapies and regimens into gastric cancer clinical trials, the response rate and median overall survival for treated patients has not significantly improved throughout the years; therefore, newer therapeutic approaches to improve upon the medication selection process are warranted. Treatment and dose selection based on patient factors, such as genetic variation, may provide a more rational and potentially more powerful means of personalizing chemotherapy. This review provides an update on the current status of pharmacogenetic studies regarding germline DNA mutations that may alter response to chemotherapeutic agents used to treat gastric cancer, including perspectives on clinical translation and future work.

Publisher

Future Medicine Ltd

Subject

Pharmacology,Genetics,Molecular Medicine

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