4.5 Article

Racial disparity in metabolic regulation of cancer

Journal

FRONTIERS IN BIOSCIENCE-LANDMARK
Volume 22, Issue -, Pages 1221-1246

Publisher

IMR PRESS
DOI: 10.2741/4543

Keywords

Cancer; Metabolism; Race; Ethnic; Mutation; Oncogene; Tumor suppressor; Oncometabolite

Funding

  1. National Institutes of Health [R01 CA163649]
  2. Specialized Programs for Research Excellence (SPORE) [2P50 CA127297]

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Genetic mutations and metabolic reprogramming are two key hallmarks of cancer, required for proliferation, invasion, and metastasis of the disease. While genetic mutations, whether inherited or acquired, are critical for the initiation of tumor development, metabolic reprogramming is an effector mechanism imperative for adaptational transition during the progression of cancer. Recent findings in the literature emphasize the significance of molecular cross-talk between these two cellular processes in regulating signaling and differentiation of cancer cells. Genome-wide sequencing analyses of cancer genomes have highlighted the association of various genic mutations in predicting cancer risk and survival. Oncogenic mutational frequency is heterogeneously distributed among various cancer types in different populations, resulting in varying susceptibility to cancer risk. In this review, we explore and discuss the role of genetic mutations in metabolic enzymes and metabolic oncoregulators to stratify cancer risk in persons of different racial backgrounds.

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