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Biosynthetic multitasking facilitates thalassospiramide structural diversity in marine bacteria.


ABSTRACT: Thalassospiramides A and B are immunosuppressant cyclic lipopeptides first reported from the marine ?-proteobacterium Thalassospira sp. CNJ-328. We describe here the discovery and characterization of an extended family of 14 new analogues from four Tistrella and Thalassospira isolates. These potent calpain 1 protease inhibitors belong to six structure classes in which the length and composition of the acylpeptide side chain varies extensively. Genomic sequence analysis of the thalassospiramide-producing microbes revealed related, genus-specific biosynthetic loci encoding hybrid nonribosomal peptide synthetase/polyketide synthases consistent with thalassospiramide assembly. The bioinformatics analysis of the gene clusters suggests that structural diversity, which ranges from the 803.4 Da thalassospiramide C to the 1291.7 Da thalassospiramide F, results from a complex sequence of reactions involving amino acid substrate channeling and enzymatic multimodule skipping and iteration. Preliminary biochemical analysis of the N-terminal nonribosomal peptide synthetase module from the Thalassospira TtcA megasynthase supports a biosynthetic model in which in cis amino acid activation competes with in trans activation to increase the range of amino acid substrates incorporated at the N terminus.

SUBMITTER: Ross AC 

PROVIDER: S-EPMC3563429 | biostudies-literature | 2013 Jan

REPOSITORIES: biostudies-literature

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Biosynthetic multitasking facilitates thalassospiramide structural diversity in marine bacteria.

Ross Avena C AC   Xu Ying Y   Lu Liang L   Kersten Roland D RD   Shao Zongze Z   Al-Suwailem Abdulaziz M AM   Dorrestein Pieter C PC   Qian Pei-Yuan PY   Moore Bradley S BS  

Journal of the American Chemical Society 20130111 3


Thalassospiramides A and B are immunosuppressant cyclic lipopeptides first reported from the marine α-proteobacterium Thalassospira sp. CNJ-328. We describe here the discovery and characterization of an extended family of 14 new analogues from four Tistrella and Thalassospira isolates. These potent calpain 1 protease inhibitors belong to six structure classes in which the length and composition of the acylpeptide side chain varies extensively. Genomic sequence analysis of the thalassospira  ...[more]

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