Title of article
Formation of β-Hydroxy Histidine in the Biosynthesis of Nikkomycin Antibiotics Original Research Article
Author/Authors
Huawei Chen، نويسنده , , Brian K Hubbard، نويسنده , , Sarah E OʹConnor، نويسنده , , Christopher T Walsh، نويسنده ,
Issue Information
ماهنامه با شماره پیاپی سال 2002
Pages
10
From page
103
To page
112
Abstract
Nikkomycins, a group of peptidyl nucleoside antibiotics produced Streptomyces tendae Tü901, are potent competitive inhibitors of chitin synthase. In this study, three nikkomycin biosynthetic enzymes, NikP1, NikQ, and NikP2, were overexpressed, purified, and characterized. The NikP1 activated L-His and transferred it to the carrier protein domain to form L-His-S-NikP1, which served as the β-hydroxylation substrate of NikQ. The β-OH-His was then hydrolytically released from NikP1 by NikP2. The results reported here substantiate our earlier proposal that the covalent tethering of an amino acid onto a carrier protein domain prior to downstream modification is a general strategy for diverting a fraction of the amino acid into secondary metabolism.
Journal title
Chemistry and Biology
Serial Year
2002
Journal title
Chemistry and Biology
Record number
1158445
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