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Serine Hydroxymethyltransferase As a Potential Target of Antibacterial Agents Acting Synergistically with One-Carbon Metabolism-Related Inhibitors

Communications biology(2022)

Cited 5|Views16
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Abstract
Serine hydroxymethyltransferase (SHMT) produces 5,10-methylenetetrahydrofolate (CH 2 -THF) from tetrahydrofolate with serine to glycine conversion. SHMT is a potential drug target in parasites, viruses and cancer. (+)-SHIN-1 was developed as a human SHMT inhibitor for cancer therapy. However, the potential of SHMT as an antibacterial target is unknown. Here, we show that (+)-SHIN-1 bacteriostatically inhibits the growth of Enterococcus faecium at a 50% effective concentration of 10 –11 M and synergistically enhances the antibacterial activities of several nucleoside analogues. Our results, including crystal structure analysis, indicate that (+)-SHIN-1 binds tightly to E. faecium SHMT ( efm SHMT). Two variable loops in SHMT are crucial for inhibitor binding, and serine binding to efm SHMT enhances the affinity of (+)-SHIN-1 by stabilising the loop structure of efm SHMT. The findings highlight the potency of SHMT as an antibacterial target and the possibility of developing SHMT inhibitors for treating bacterial, viral and parasitic infections and cancer.
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Key words
Target identification,X-ray crystallography,Life Sciences,general
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