Conserved inhibitory mechanism and competent ATP binding mode for adenylyltransferases with Fic fold.

Conserved inhibitory mechanism and competent ATP binding mode for adenylyltransferases with Fic fold.

The ubiquitous FIC domain is evolutionarily conserved from bacteria to human and has been shown to catalyze AMP transfer onto protein side-chain hydroxyl groups. Recently, it was predicted that most catalytically competent Fic proteins are inhibited by the presence of an inhibitory helix αinh that i...

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Main Authors: Arnaud Goepfert, Frédéric V Stanger, Christoph Dehio, Tilman Schirmer
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3667792?pdf=render
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spelling doaj-34f9849263614d3fb58c49661bc3eaad2020-11-25T01:10:08ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0185e6490110.1371/journal.pone.0064901Conserved inhibitory mechanism and competent ATP binding mode for adenylyltransferases with Fic fold.Arnaud GoepfertFrédéric V StangerChristoph DehioTilman SchirmerThe ubiquitous FIC domain is evolutionarily conserved from bacteria to human and has been shown to catalyze AMP transfer onto protein side-chain hydroxyl groups. Recently, it was predicted that most catalytically competent Fic proteins are inhibited by the presence of an inhibitory helix αinh that is provided by a cognate anti-toxin (class I), or is part of the N- or C-terminal part of the Fic protein itself (classes II and III). In vitro, inhibition is relieved by mutation of a conserved glutamate of αinh to glycine. For the class III bacterial Fic protein NmFic from Neisseria meningitidis, the inhibitory mechanism has been elucidated. Here, we extend above study by including bacterial class I and II Fic proteins VbhT from Bartonella schoenbuchensis and SoFic from Shewanella oneidensis, respectively, and the respective E->G mutants. Comparative enzymatic and crystallographic analyses show that, in all three classes, the ATP substrate binds to the wild-type FIC domains, but with the α-phosphate in disparate and non-competent orientations. In the E->G mutants, however, the tri-phosphate moiety is found reorganized to the same tightly bound structure through a unique set of hydrogen bonds with Fic signature motif residues. The γ-phosphate adopts the location that is taken by the inhibitory glutamate in wild-type resulting in an α-phosphate orientation that can be attacked in-line by a target side-chain hydroxyl group. The latter is properly registered to the Fic active center by main-chain β-interactions with the β-hairpin flap. These data indicate that the active site motif and the exposed edge of the flap are both required to form an adenylylation-competent Fic protein.http://europepmc.org/articles/PMC3667792?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Arnaud Goepfert
Frédéric V Stanger
Christoph Dehio
Tilman Schirmer
spellingShingle Arnaud Goepfert
Frédéric V Stanger
Christoph Dehio
Tilman Schirmer
Conserved inhibitory mechanism and competent ATP binding mode for adenylyltransferases with Fic fold.
PLoS ONE
author_facet Arnaud Goepfert
Frédéric V Stanger
Christoph Dehio
Tilman Schirmer
author_sort Arnaud Goepfert
title Conserved inhibitory mechanism and competent ATP binding mode for adenylyltransferases with Fic fold.
title_short Conserved inhibitory mechanism and competent ATP binding mode for adenylyltransferases with Fic fold.
title_full Conserved inhibitory mechanism and competent ATP binding mode for adenylyltransferases with Fic fold.
title_fullStr Conserved inhibitory mechanism and competent ATP binding mode for adenylyltransferases with Fic fold.
title_full_unstemmed Conserved inhibitory mechanism and competent ATP binding mode for adenylyltransferases with Fic fold.
title_sort conserved inhibitory mechanism and competent atp binding mode for adenylyltransferases with fic fold.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description The ubiquitous FIC domain is evolutionarily conserved from bacteria to human and has been shown to catalyze AMP transfer onto protein side-chain hydroxyl groups. Recently, it was predicted that most catalytically competent Fic proteins are inhibited by the presence of an inhibitory helix αinh that is provided by a cognate anti-toxin (class I), or is part of the N- or C-terminal part of the Fic protein itself (classes II and III). In vitro, inhibition is relieved by mutation of a conserved glutamate of αinh to glycine. For the class III bacterial Fic protein NmFic from Neisseria meningitidis, the inhibitory mechanism has been elucidated. Here, we extend above study by including bacterial class I and II Fic proteins VbhT from Bartonella schoenbuchensis and SoFic from Shewanella oneidensis, respectively, and the respective E->G mutants. Comparative enzymatic and crystallographic analyses show that, in all three classes, the ATP substrate binds to the wild-type FIC domains, but with the α-phosphate in disparate and non-competent orientations. In the E->G mutants, however, the tri-phosphate moiety is found reorganized to the same tightly bound structure through a unique set of hydrogen bonds with Fic signature motif residues. The γ-phosphate adopts the location that is taken by the inhibitory glutamate in wild-type resulting in an α-phosphate orientation that can be attacked in-line by a target side-chain hydroxyl group. The latter is properly registered to the Fic active center by main-chain β-interactions with the β-hairpin flap. These data indicate that the active site motif and the exposed edge of the flap are both required to form an adenylylation-competent Fic protein.
url http://europepmc.org/articles/PMC3667792?pdf=render
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AT fredericvstanger conservedinhibitorymechanismandcompetentatpbindingmodeforadenylyltransferaseswithficfold
AT christophdehio conservedinhibitorymechanismandcompetentatpbindingmodeforadenylyltransferaseswithficfold
AT tilmanschirmer conservedinhibitorymechanismandcompetentatpbindingmodeforadenylyltransferaseswithficfold
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