Identification of a cyclic-di-GMP-modulating response regulator that impacts biofilm formation in a model sulfate reducing bacterium

Identification of a cyclic-di-GMP-modulating response regulator that impacts biofilm formation in a model sulfate reducing bacterium

We surveyed the eight putative cyclic-di-GMP-modulating response regulators (RRs) in Desulfovibrio vulgaris Hildenborough that are predicted to function via two-component signaling. Using purified proteins, we examined cyclic-di-GMP production or turnover in vitro of all eight proteins. The two RRs...

Full description

Bibliographic Details
Main Authors: Lara eRajeev, Eric G Luning, Sara eAltenburg, Grant Matthew Zane, Edward E Baidoo, Michela eCatena, Jay D Keasling, Judy D Wall, Matthew W Fields, Aindrila eMukhopadhyay
Format: Article
Language:English
Published: Frontiers Media S.A. 2014-07-01
Series:Frontiers in Microbiology
Subjects:
Desulfovibrio
Biofilm
two-component system
cyclic-di-GMP
HD-GYP
GGDEF
Online Access:http://journal.frontiersin.org/Journal/10.3389/fmicb.2014.00382/full
id doaj-3bd5e0c5f307443ea28d5974c53e57ae
record_format Article
spelling doaj-3bd5e0c5f307443ea28d5974c53e57ae2020-11-24T23:49:23ZengFrontiers Media S.A.Frontiers in Microbiology1664-302X2014-07-01510.3389/fmicb.2014.00382103365Identification of a cyclic-di-GMP-modulating response regulator that impacts biofilm formation in a model sulfate reducing bacteriumLara eRajeev0Eric G Luning1Sara eAltenburg2Grant Matthew Zane3Edward E Baidoo4Michela eCatena5Jay D Keasling6Jay D Keasling7Judy D Wall8Matthew W Fields9Aindrila eMukhopadhyay10Lawrence Berkeley National BerkeleyLawrence Berkeley National BerkeleyMontana State UniversityUniversity of Missouri, ColumbiaLawrence Berkeley National BerkeleyLawrence Berkeley National BerkeleyLawrence Berkeley National BerkeleyUniversity of CaliforniaUniversity of Missouri, ColumbiaMontana State UniversityLawrence Berkeley National BerkeleyWe surveyed the eight putative cyclic-di-GMP-modulating response regulators (RRs) in Desulfovibrio vulgaris Hildenborough that are predicted to function via two-component signaling. Using purified proteins, we examined cyclic-di-GMP production or turnover in vitro of all eight proteins. The two RRs containing only GGDEF domains (DVU2067, DVU0636) demonstrated cyclic-di-GMP production activity in vitro. Of the remaining proteins, three RRs with HD-GYP domains (DVU0722, DVUA0086 and DVU2933) were confirmed to be Mn2+ dependent phosphodiesterases in vitro and converted cyclic-di-GMP to its linear form, pGpG. DVU0408, containing both cyclic-di-GMP production (GGDEF) and degradation domains (EAL), showed cyclic-di-GMP turnover activity in vitro also with production of pGpG. No cyclic-di-GMP related activity could be assigned to the RR DVU0330, containing a metal-dependent phosphohydrolase HD-OD domain, or to the HD-GYP domain RR, DVU1181. Studies included examining the impact of overexpressed cyclic-di-GMP-modulating RRs in the heterologous host E. coli and led to the identification of one RR, DVU0636, with increased cellulose production. Evaluation of a transposon mutant in DVU0636 indicated that the strain was impaired in biofilm formation and demonstrated an altered carbohydrate:protein ratio relative to the D. vulgaris wild type biofilms. However, grown in liquid lactate/sulfate medium, the DVU0636 transposon mutant showed no growth impairment relative to the wild-type strain. Among the eight candidates, only the transposon disruption mutant in the DVU2067 RR presented a growth defect in liquid culture. Our results indicate that, of the two diguanylate cyclases that function as part of two-component signaling, DVU0636 plays an important role in biofilm formation while the function of DVU2067 has pertinence in planktonic growth.http://journal.frontiersin.org/Journal/10.3389/fmicb.2014.00382/fullDesulfovibrioBiofilmtwo-component systemcyclic-di-GMPHD-GYPGGDEF
collection DOAJ
language English
format Article
sources DOAJ
author Lara eRajeev
Eric G Luning
Sara eAltenburg
Grant Matthew Zane
Edward E Baidoo
Michela eCatena
Jay D Keasling
Jay D Keasling
Judy D Wall
Matthew W Fields
Aindrila eMukhopadhyay
spellingShingle Lara eRajeev
Eric G Luning
Sara eAltenburg
Grant Matthew Zane
Edward E Baidoo
Michela eCatena
Jay D Keasling
Jay D Keasling
Judy D Wall
Matthew W Fields
Aindrila eMukhopadhyay
Identification of a cyclic-di-GMP-modulating response regulator that impacts biofilm formation in a model sulfate reducing bacterium
Frontiers in Microbiology
Desulfovibrio
Biofilm
two-component system
cyclic-di-GMP
HD-GYP
GGDEF
author_facet Lara eRajeev
Eric G Luning
Sara eAltenburg
Grant Matthew Zane
Edward E Baidoo
Michela eCatena
Jay D Keasling
Jay D Keasling
Judy D Wall
Matthew W Fields
Aindrila eMukhopadhyay
author_sort Lara eRajeev
title Identification of a cyclic-di-GMP-modulating response regulator that impacts biofilm formation in a model sulfate reducing bacterium
title_short Identification of a cyclic-di-GMP-modulating response regulator that impacts biofilm formation in a model sulfate reducing bacterium
title_full Identification of a cyclic-di-GMP-modulating response regulator that impacts biofilm formation in a model sulfate reducing bacterium
title_fullStr Identification of a cyclic-di-GMP-modulating response regulator that impacts biofilm formation in a model sulfate reducing bacterium
title_full_unstemmed Identification of a cyclic-di-GMP-modulating response regulator that impacts biofilm formation in a model sulfate reducing bacterium
title_sort identification of a cyclic-di-gmp-modulating response regulator that impacts biofilm formation in a model sulfate reducing bacterium
publisher Frontiers Media S.A.
series Frontiers in Microbiology
issn 1664-302X
publishDate 2014-07-01
description We surveyed the eight putative cyclic-di-GMP-modulating response regulators (RRs) in Desulfovibrio vulgaris Hildenborough that are predicted to function via two-component signaling. Using purified proteins, we examined cyclic-di-GMP production or turnover in vitro of all eight proteins. The two RRs containing only GGDEF domains (DVU2067, DVU0636) demonstrated cyclic-di-GMP production activity in vitro. Of the remaining proteins, three RRs with HD-GYP domains (DVU0722, DVUA0086 and DVU2933) were confirmed to be Mn2+ dependent phosphodiesterases in vitro and converted cyclic-di-GMP to its linear form, pGpG. DVU0408, containing both cyclic-di-GMP production (GGDEF) and degradation domains (EAL), showed cyclic-di-GMP turnover activity in vitro also with production of pGpG. No cyclic-di-GMP related activity could be assigned to the RR DVU0330, containing a metal-dependent phosphohydrolase HD-OD domain, or to the HD-GYP domain RR, DVU1181. Studies included examining the impact of overexpressed cyclic-di-GMP-modulating RRs in the heterologous host E. coli and led to the identification of one RR, DVU0636, with increased cellulose production. Evaluation of a transposon mutant in DVU0636 indicated that the strain was impaired in biofilm formation and demonstrated an altered carbohydrate:protein ratio relative to the D. vulgaris wild type biofilms. However, grown in liquid lactate/sulfate medium, the DVU0636 transposon mutant showed no growth impairment relative to the wild-type strain. Among the eight candidates, only the transposon disruption mutant in the DVU2067 RR presented a growth defect in liquid culture. Our results indicate that, of the two diguanylate cyclases that function as part of two-component signaling, DVU0636 plays an important role in biofilm formation while the function of DVU2067 has pertinence in planktonic growth.
topic Desulfovibrio
Biofilm
two-component system
cyclic-di-GMP
HD-GYP
GGDEF
url http://journal.frontiersin.org/Journal/10.3389/fmicb.2014.00382/full
work_keys_str_mv AT laraerajeev identificationofacyclicdigmpmodulatingresponseregulatorthatimpactsbiofilmformationinamodelsulfatereducingbacterium
AT ericgluning identificationofacyclicdigmpmodulatingresponseregulatorthatimpactsbiofilmformationinamodelsulfatereducingbacterium
AT saraealtenburg identificationofacyclicdigmpmodulatingresponseregulatorthatimpactsbiofilmformationinamodelsulfatereducingbacterium
AT grantmatthewzane identificationofacyclicdigmpmodulatingresponseregulatorthatimpactsbiofilmformationinamodelsulfatereducingbacterium
AT edwardebaidoo identificationofacyclicdigmpmodulatingresponseregulatorthatimpactsbiofilmformationinamodelsulfatereducingbacterium
AT michelaecatena identificationofacyclicdigmpmodulatingresponseregulatorthatimpactsbiofilmformationinamodelsulfatereducingbacterium
AT jaydkeasling identificationofacyclicdigmpmodulatingresponseregulatorthatimpactsbiofilmformationinamodelsulfatereducingbacterium
AT jaydkeasling identificationofacyclicdigmpmodulatingresponseregulatorthatimpactsbiofilmformationinamodelsulfatereducingbacterium
AT judydwall identificationofacyclicdigmpmodulatingresponseregulatorthatimpactsbiofilmformationinamodelsulfatereducingbacterium
AT matthewwfields identificationofacyclicdigmpmodulatingresponseregulatorthatimpactsbiofilmformationinamodelsulfatereducingbacterium
AT aindrilaemukhopadhyay identificationofacyclicdigmpmodulatingresponseregulatorthatimpactsbiofilmformationinamodelsulfatereducingbacterium
_version_ 1725482518539403264

Similar Items