Folate-Dependent Purine Nucleotide Biosynthesis in Humans

Purine nucleotide biosynthesis de novo (PNB) requires 2 folate-dependent transformylases-5'-phosphoribosyl-glycinamide (GAR) and 5'-phosphoribosyl-5-aminoimidazole-4-carboxamide (AICAR) transformylases-to introduce carbon 8 (C-8) and carbon 2 (C-2) into the purine ring. Both transformylases utilize 10-formyltetrahydrofolate (10-formyl-H(4)folate), where the formyl-carbon sources include ring-2-C of histidine, 3-C of serine, 2-C of glycine, and formate. Our findings in human studies indicate that glycine provides the carbon for GAR transformylase (exclusively C-8), whereas histidine and formate are the predominant carbon sources for AICAR transformylase (C-2). Contrary to the previous notion, these carbon sources may not supply a general 10-formyl-H(4)folate pool, which was believed to equally provide carbons to C-8 and C-2. To explain these phenomena, we postulate that GAR transformylase is in a complex with the trifunctional folate-metabolizing enzyme (TFM) and serine hydroxymethyltransferase to channel carbons of glycine and serine to C-8. There is no evidence for channeling carbons of histidine and formate to AICAR transformylase (C-2). GAR transformylase may require the TFM to furnish 10-formyl-H(4)folate immediately after its production from serine to protect its oxidation to 10-formyldihydrofolate (10-formyl-H(2)folate), whereas AICAR transformylase can utilize both 10-formyl-H(2)folate and 10-formyl-H(4)folate. Human liver may supply AICAR to AICAR transformylase in erythrocytes/erythroblasts. Incorporation of ring-2-C of histidine and formate into C-2 of urinary uric acid presented a circadian rhythm with a peak in the morning, which corresponds to the maximum DNA synthesis in the bone marrow, and it may be useful in the timing of the administration of drugs that block PNB for the treatment of cancer and autoimmune disease.