Structural and functional analysis of two SHMT8 variants associated with soybean cyst nematode resistance

大豆孢囊线虫 丝氨酸羟甲基转移酶 甘氨酸 丝氨酸 酶动力学 生物化学 生物 化学 氨基酸 活动站点 基因
作者
David A. Korasick,Luckio F Owuocha,Pramod Kaitheri Kandoth,John J. Tanner,Melissa G. Mitchum,Lesa J. Beamer
出处
期刊:FEBS Journal [Wiley]
标识
DOI:10.1111/febs.16971
摘要

Two amino acid variants in soybean serine hydroxymethyltransferase 8 (SHMT8) are associated with resistance to the soybean cyst nematode (SCN), a devastating agricultural pathogen with worldwide economic impacts for soybean production. SHMT8 is a cytoplasmic enzyme that catalyzes the PLP-dependent conversion of serine and tetrahydrofolate (THF) to glycine and 5,10-methylenetetrahydrofolate. A previous study of the P130R/N358Y double variant of SHMT8, identified in the SCN-resistant soybean cultivar (cv.) Forrest, showed profound impairment of folate binding affinity and reduced THF-dependent enzyme activity, relative to the highly active SHMT8 in cv. Essex, which is susceptible to SCN. Given the importance of SCN-resistance in soybean agriculture, we report here biochemical and structural characterization of the P130R and N358Y single variants to elucidate their individual effects on soybean SHMT8. We find that both single variants have reduced THF-dependent catalytic activity relative to Essex SHMT8 (10 to 50-fold decrease in kcat /Km ) but are significantly more active than the P130R/N368Y double variant. The kinetic data also show that the single variants lack THF-substrate inhibition as found in Essex SHMT8, an observation with implications for regulation of the folate cycle. Five crystal structures of the P130R and N358Y variants in complex with various ligands (resolutions from 1.49 to 2.30 Å) reveal distinct structural impacts of the mutations and provide new insights into allosterism. Our results support the notion that the P130R/N358Y double variant in Forrest SHMT8 produces unique and unexpected effects on the enzyme, which cannot be easily predicted from the behavior of the individual variants.

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