TY - JOUR

T1 - Exploiting substrate diversity of NRPS Led to the generation of new sansanmycin analogs

AU - Wang, Shan Shan

AU - Zhang, Ning Ning

AU - He, Ning

AU - Guo, Wen Qiang

AU - Lei, Xuan

AU - Cai, Qiang

AU - Hong, Bin

AU - Xie, Yun Ying

PY - 2017/5

Y1 - 2017/5

N2 - Further exploration of substrate diversity of the sansanmycin biosynthetic pathway using available halogen- and methyl-phenylalanines led to the generation of diverse sansanmycin derivatives, either at the single C- or N-terminus alone or at both C- and N-termini. The structures of all of these derivatives were determined by MS/MS spectra, and amongst them, the structures of [2-Cl-Phe]-sansanmycin H (1) and [2-Cl-Phe]-sansanmycin A (2) were further identified by NMR. Both the C-terminal derivative 1 and the N-terminal derivative 2 were assayed for their antibacterial activities, and compound 1 exhibited moderate activity against P. aeruginosa and ΔtolC mutant E. coli.

AB - Further exploration of substrate diversity of the sansanmycin biosynthetic pathway using available halogen- and methyl-phenylalanines led to the generation of diverse sansanmycin derivatives, either at the single C- or N-terminus alone or at both C- and N-termini. The structures of all of these derivatives were determined by MS/MS spectra, and amongst them, the structures of [2-Cl-Phe]-sansanmycin H (1) and [2-Cl-Phe]-sansanmycin A (2) were further identified by NMR. Both the C-terminal derivative 1 and the N-terminal derivative 2 were assayed for their antibacterial activities, and compound 1 exhibited moderate activity against P. aeruginosa and ΔtolC mutant E. coli.

KW - Antibacterial activity

KW - NRPS

KW - Sansanmycin

KW - Substrate diversity

UR - http://www.scopus.com/inward/record.url?scp=85019771271&partnerID=8YFLogxK

U2 - 10.1177/1934578x1701200524

DO - 10.1177/1934578x1701200524

M3 - Article

AN - SCOPUS:85019771271

VL - 12

SP - 781

EP - 783

JO - Natural product communications

JF - Natural product communications

SN - 1934-578X

IS - 5

ER -