Acylation of Streptomyces type II polyketide synthase acyl carrier proteins

John Crosby; Kate J. Byrom; Timothy S. Hitchman; Russell J. Cox; Matthew P. Crump; I. Stuart C. Findlow; Maureen J. Bibb; Thomas J. Simpson

doi:10.1016/S0014-5793(98)00840-0

Acylation of Streptomyces type II polyketide synthase acyl carrier proteins

John Crosby
, Kate J. Byrom
, Timothy S. Hitchman
, Russell J. Cox
, Matthew P. Crump
, I. Stuart C. Findlow
, Maureen J. Bibb
, Thomas J. Simpson^*

^*Korrespondierende*r Autor*in für diese Arbeit

Publikation: Beitrag in Fachzeitschrift › Artikel › Forschung › Peer-Review

Abstract

Acyl derivatives of type II PKS ACPs are required for in vitro studies of polyketide biosynthesis. The presence of an exposed cysteine residue prevented specific chemical acylation of the phosphopantetheine thiol of the actinorhodin PKS holo ACP. Acylation studies were further complicated by intramolecular disulphide formation between cysteine 17 and the phosphopantetheine. The presence of this intramolecular disulphide was confirmed by tryptic digestion of the ACP followed by ESMS analysis of the fragments. An act Cys17Ser ACP was engineered by site-directed mutagenesis. S-Acyl adducts of act C17S, oxytetracycline and griseusin holo ACPs were rapidly formed by reaction with hexanoyl, 5-ketohexanoyl and protected acetoacetyl imidazolides. Comparisons with type II FAS ACPs were made. Copyright (C) 1998 Federation of European Biochemical Societies.

Originalsprache	Englisch
Seiten (von - bis)	132-138
Seitenumfang	7
Fachzeitschrift	FEBS letters
Jahrgang	433
Ausgabenummer	1-2
DOIs	https://doi.org/10.1016/S0014-5793(98)00840-0
Publikationsstatus	Veröffentlicht - 14 Aug. 1998
Extern publiziert	Ja

ASJC Scopus Sachgebiete

Biophysik
Strukturelle Biologie
Biochemie
Molekularbiologie
Genetik
Zellbiologie

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10.1016/S0014-5793(98)00840-0

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title = "Acylation of Streptomyces type II polyketide synthase acyl carrier proteins",

abstract = "Acyl derivatives of type II PKS ACPs are required for in vitro studies of polyketide biosynthesis. The presence of an exposed cysteine residue prevented specific chemical acylation of the phosphopantetheine thiol of the actinorhodin PKS holo ACP. Acylation studies were further complicated by intramolecular disulphide formation between cysteine 17 and the phosphopantetheine. The presence of this intramolecular disulphide was confirmed by tryptic digestion of the ACP followed by ESMS analysis of the fragments. An act Cys17Ser ACP was engineered by site-directed mutagenesis. S-Acyl adducts of act C17S, oxytetracycline and griseusin holo ACPs were rapidly formed by reaction with hexanoyl, 5-ketohexanoyl and protected acetoacetyl imidazolides. Comparisons with type II FAS ACPs were made. Copyright (C) 1998 Federation of European Biochemical Societies.",

keywords = "Acyl carrier protein, Acylation, Fatty acid synthase, Polyketide synthase",

author = "John Crosby and Byrom, \{Kate J.\} and Hitchman, \{Timothy S.\} and Cox, \{Russell J.\} and Crump, \{Matthew P.\} and Findlow, \{I. Stuart C.\} and Bibb, \{Maureen J.\} and Simpson, \{Thomas J.\}",

note = "Funding information: This work was supported by the Engineering and Physical Sciences Research Council (EPSRC), the Biotechnology and Biological Sciences Research Council (BBSRC) and the John Innes Foundation. Studentships from the EPSRC (I.S.C.F., T.S.H. and M.P.C.) and School of Chemistry (K.J.B.) are gratefully acknowledged. R.J.C. gratefully acknowledges the receipt of a Royal Society equipment grant.",

year = "1998",

month = aug,

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doi = "10.1016/S0014-5793(98)00840-0",

language = "English",

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journal = "FEBS letters",

issn = "0014-5793",

publisher = "John Wiley and Sons Inc.",

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T1 - Acylation of Streptomyces type II polyketide synthase acyl carrier proteins

AU - Crosby, John

AU - Byrom, Kate J.

AU - Hitchman, Timothy S.

AU - Cox, Russell J.

AU - Crump, Matthew P.

AU - Findlow, I. Stuart C.

AU - Bibb, Maureen J.

AU - Simpson, Thomas J.

N1 - Funding information: This work was supported by the Engineering and Physical Sciences Research Council (EPSRC), the Biotechnology and Biological Sciences Research Council (BBSRC) and the John Innes Foundation. Studentships from the EPSRC (I.S.C.F., T.S.H. and M.P.C.) and School of Chemistry (K.J.B.) are gratefully acknowledged. R.J.C. gratefully acknowledges the receipt of a Royal Society equipment grant.

PY - 1998/8/14

Y1 - 1998/8/14

N2 - Acyl derivatives of type II PKS ACPs are required for in vitro studies of polyketide biosynthesis. The presence of an exposed cysteine residue prevented specific chemical acylation of the phosphopantetheine thiol of the actinorhodin PKS holo ACP. Acylation studies were further complicated by intramolecular disulphide formation between cysteine 17 and the phosphopantetheine. The presence of this intramolecular disulphide was confirmed by tryptic digestion of the ACP followed by ESMS analysis of the fragments. An act Cys17Ser ACP was engineered by site-directed mutagenesis. S-Acyl adducts of act C17S, oxytetracycline and griseusin holo ACPs were rapidly formed by reaction with hexanoyl, 5-ketohexanoyl and protected acetoacetyl imidazolides. Comparisons with type II FAS ACPs were made. Copyright (C) 1998 Federation of European Biochemical Societies.

AB - Acyl derivatives of type II PKS ACPs are required for in vitro studies of polyketide biosynthesis. The presence of an exposed cysteine residue prevented specific chemical acylation of the phosphopantetheine thiol of the actinorhodin PKS holo ACP. Acylation studies were further complicated by intramolecular disulphide formation between cysteine 17 and the phosphopantetheine. The presence of this intramolecular disulphide was confirmed by tryptic digestion of the ACP followed by ESMS analysis of the fragments. An act Cys17Ser ACP was engineered by site-directed mutagenesis. S-Acyl adducts of act C17S, oxytetracycline and griseusin holo ACPs were rapidly formed by reaction with hexanoyl, 5-ketohexanoyl and protected acetoacetyl imidazolides. Comparisons with type II FAS ACPs were made. Copyright (C) 1998 Federation of European Biochemical Societies.

KW - Acyl carrier protein

KW - Acylation

KW - Fatty acid synthase

KW - Polyketide synthase

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