DNA连接酶
生物化学
生物
酶
化学
计算生物学
作者
M. Gordon,Melisa S. Gonzalez,Priya,Rongrong Yu,Elijah Abraham,Xiang Li,Dilip V. Prajapati,Rebecca A. Butcher
标识
DOI:10.1021/acschembio.5c00237
摘要
mutant worm strain does not produce the nemamides but accumulates a β-amino-containing polyketide, named nematide A, which is made by PKS-1 and is potentially loaded by PKAL-1 onto NRPS-1. Here, however, we show that PKAL-1 does not accept β-amino-containing substrates. Furthermore, phylogenetic and structural analyses of PKAL-1 indicate that it is likely missing key residues in its active site for binding to a β-amino group. By analyzing a panel of alternative substrates in biochemical assays, we show that PKAL-1 prefers α,β-unsaturated substrates. Our work potentially suggests an alternative model for nemamide biosynthesis whereby PKAL-1 loads an α,β-unsaturated substrate onto NRPS-1 and the β-amino group is installed later in the biosynthetic pathway. Furthermore, our data could indicate that nematide A is separate from the biosynthetic intermediates that are passed between PKS-1 and NRPS-1 in the construction of the nemamides and may have its own signaling function. Thus, PKAL-1 may help to regulate what is made by the PKS-1-NRPS-1 assembly line, either nematide A or the nemamides.
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