AI Article Synopsis
- Cancer metabolism is a key hallmark of cancer, characterized by altered glucose and glutamine metabolism that supports rapid growth and adaptability of cancer cells.
- One-carbon metabolism and nucleotide biosynthesis are crucial components of cancer metabolism, providing essential building blocks for cell growth and providing targets for anti-cancer therapies.
- This review focuses on the biochemical details, enzyme regulation, and potential pharmacological targets within these metabolic pathways, highlighting existing inhibitors and exploring new therapeutic possibilities.
Article Abstract
Cancer-related metabolism has recently emerged as one of the "hallmarks of cancer". It has several important features, including altered metabolism of glucose and glutamine. Importantly, altered cancer metabolism connects different biochemical pathways into the one fine-tuned metabolic network, which stimulates high proliferation rates and plasticity to malignant cells. Among the keystones of cancer metabolism are one-carbon metabolism and nucleotide biosynthesis, which provide building blocks to anabolic reactions. Accordingly, the importance of these metabolic pathways for anticancer therapy has well been documented by more than fifty years of clinical use of specific metabolic inhibitors - methotrexate and nucleotides analogs. In this review we discuss one-carbon metabolism and nucleotide biosynthesis as common and specific features of many, if not all, tumors. The key enzymes involved in these pathways also represent promising anti-cancer therapeutic targets. We review different aspects of these metabolic pathways including their biochemistry, compartmentalization and expression of the key enzymes and their regulation at different levels. We also discuss the effects of known inhibitors of these pathways as well as the recent data on other enzymes of the same pathways as perspective pharmacological targets.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5410357 | PMC |
| http://dx.doi.org/10.18632/oncotarget.15053 | DOI Listing |
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