Heterologous production of new protease inhibitory peptide marinostatin E | Zendy

Kohta Unno | Zendy; Hiroyuki Nakagawa | Zendy; Shinya Kodani | Zendy

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Heterologous production of new protease inhibitory peptide marinostatin E

Author(s) -

Kohta Unno,

Hiroyuki Nakagawa,

Shinya Kodani

Publication year - 2021

Publication title -

bioscience biotechnology and biochemistry

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.509

H-Index - 116

eISSN - 1347-6947

pISSN - 0916-8451

DOI - 10.1093/bbb/zbaa011

Subject(s) - heterologous , heterologous expression , protease , escherichia coli , peptide , biochemistry , recombinant dna , biology , subtilisin , gene cluster , trypsin , gene , chemistry , microbiology and biotechnology , enzyme

Bicyclic peptides, marinostatins, are protease inhibitors derived from the marine bacterium Algicola sagamiensis. The biosynthetic gene cluster of marinostatin was previously identified, although no heterologous production was reported. In this report, the biosynthetic gene cluster of marinostatin (mstA and mstB) was cloned into the expression vector pET-41a(+). As a result of the coexpression experiment, a new analogous peptide named marinostatin E was successfully produced using Escherichia coli BL21(DE3). The structure of marinostatin E was determined by a combination of chemical treatments and tandem mass spectrometry experiments. Marinostatin E exhibited inhibitory activities against chymotrypsin and subtilisin with an IC50 of 4.0 and 39.6 μm, respectively.

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