Cytochrome bd biosynthesis in Escherichia coli: the sequences of the cydC and cydD genes suggest that they encode the components of an ABC membrane transporter

Poole, Robert K.; Hatch, L; Cleeter, M. W. J.; Gibson, F.; Cox, G B; Wu, Guanghui

doi:10.1111/j.1365-2958.1993.tb02673.x

Cited by 87 publications

(92 citation statements)

References 33 publications

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“…This family may also include YojI, which has a similar domain organization and a TMD closely related to the TMDs of the other members of the family, although the ABC domain of YojI is either of different origin or has diverged faster than the other members of the subfamily. No clear function for any of these proteins has been defined, although CydCD is required for biogenesis of cytochrome oxidase b (Poole et al, 1993). However, members of this family are the E. coli proteins most closely related to the mammalian multidrug resistance P-glycoprotein and the multidrug resistance protein of Lactococcus lactis, LmrA (van Veen et al, 1998).…”

Section: Function/substrate Specificitymentioning

confidence: 99%

The Escherichia coli ATP‐binding cassette (ABC) proteins

Linton

Higgins

1998

Molecular Microbiology

390

278

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SummaryThe recent completion of the Escherichia coli genome sequence (Blattner et al., 1997) has permitted an analysis of the complement of genomically encoded ATPbinding cassette (ABC) proteins. A total of 79 ABC proteins makes this the largest paralogous family of proteins in E. coli. These 79 proteins include 97 ABC domains (as some proteins include more than one ABC domain) and are components of 69 independent functional systems (as many systems involve more than one ABC domain). The ABC domains are often, but not exclusively, the energy-generating domains of multicomponent membrane-bound transporters. Thus, 57 of the 69 systems are ABC transporters, of which 44 are periplasmic-binding protein-dependent uptake systems and 13 are presumed exporters. The genes encoding these ABC transporters occupy almost 5% of the genome. Of the 12 systems that are not obviously transport related, the function of only one, the excision repair protein UvrA, is known. A phylogenetic analysis suggests that the majority of ABC proteins can be assigned to 10 subfamilies. Together with statistical and, importantly, biological evidence, this analysis provides insight into the evolution and function of the ABC proteins.

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Section: Function/substrate Specificitymentioning

confidence: 99%

The Escherichia coli ATP‐binding cassette (ABC) proteins

Linton

Higgins

1998

Molecular Microbiology

390

278

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“…First, mutants defective in cydC or cydD encoding the polypeptides of the heterodimer, exhibit several defects of the periplasm, namely a hyperoxidized redox state and failure to assemble periplasmic cytochromes b and c (40,41). Second, cydDC mutants fail to assemble the cytochrome bd-type oxidase complex (25,41); in such mutants, the CydA and CydB subunits are detectable but the hemes are not incorporated into the subunits (42). Interestingly, both the hemes and the oxygen-reactive site (43) are thought to be close to the periplasmic side of the cytoplasmic membrane.…”

Section: Gsh Is Transported By Cyddc In An Atp-dependent Manner-the Ementioning

confidence: 99%

“…DTT was therefore first removed by solvent extraction with ethyl acetate, and the GSH was then oxidized to GSSG by exposure to air for 24 h. To determine whether the oxidation was complete, we employed DTNB, which undergoes oxidation in the presence of sulfhydryl groups. The transport assay conditions used to determine [ 35 (25) and periplasmic cytochromes c (41). Because GSH is a substrate of the CydDC transporter, it may be directly required in cytochrome bd assembly.…”

Section: Gsh Complements Bacterial Motility Defects In a Cydd Mutant-wementioning

confidence: 99%

“…Recently, we demonstrated that an ABC-type transporter, CydDC, originally identified by its requirement for assembly of the cytochrome bd-type terminal oxidase of E. coli (23)(24)(25), is a transporter of cysteine outwards across the cytoplasmic membrane (26). Given the established roles of GSH in redox buffering in eukaryotic cells (7), we hypothesized that GSH is also a substrate of CydDC.…”

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confidence: 99%

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A Bacterial Glutathione Transporter (Escherichia coli CydDC) Exports Reductant to the Periplasm

Pittman

Robinson

Poole

2005

Journal of Biological Chemistry

Self Cite

165

138

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Glutathione (GSH), a major biological antioxidant, maintains redox balance in prokaryotes and eukaryotic cells and forms exportable conjugates with compounds of pharmacological and agronomic importance. However, no GSH transporter has been characterized in a prokaryote. We show here that a heterodimeric ATP-binding cassette-type transporter, CydDC, mediates GSH transport across the Escherichia coli cytoplasmic membrane. In everted membrane vesicles, GSH is imported via an ATP-driven, protonophore-insensitive, orthovanadate-sensitive mechanism, equating with export to the periplasm in intact cells. GSH transport and cytochrome bd quinol oxidase assembly are abolished in the cydD1 mutant. Glutathione disulfide (GSSG) was not transported in either Cyd ؉ or Cyd ؊ strains. Exogenous GSH restores defective swarming motility and benzylpenicillin sensitivity in a cydD mutant and also benzylpenicillin sensitivity in a gshA mutant defective in GSH synthesis. Overexpression of the cydDC operon in dsbD mutants defective in disulfide bond formation restores dithiothreitol tolerance and periplasmic cytochrome b assembly, revealing redundant pathways for reductant export to the periplasm. These results identify the first prokaryotic GSH transporter and indicate a key role for GSH in periplasmic redox homeostasis.

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“…Deletion analysis indicated that an intact leucine-rich repeat (residues 345-470) of CCR4 was required for its interaction with both CAF4 and CAF16 (Table II, to encode a novel protein (yeast protein YKR036c) containing seven WD40 repeats in its C terminus (residues 320 -659). CAF16 when sequenced in its entirety was found to encode a protein (now designated YFL028c) that shares significant homology to the ABC ATPase family of proteins (31,32). ABC ATPases are principally found to play roles in transport across membranes and as membrane receptors (33).…”

Section: Ccr4mentioning

confidence: 99%

Characterization of CAF4 and CAF16 Reveals a Functional Connection between the CCR4-NOT Complex and a Subset of SRB Proteins of the RNA Polymerase II Holoenzyme

Liu

Chiang

Pan

et al. 2001

Journal of Biological Chemistry

101

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The CCR4-NOT transcriptional regulatory complex affects transcription both positively and negatively and consists of the following two complexes: a core 1 ؋ 10 6 dalton (1 MDa) complex consisting of CCR4, CAF1, and the five NOT proteins and a larger, less defined 1.9-MDa complex. We report here the identification of two new factors that associate with the CCR4-NOT proteins as follows: CAF4, a WD40-containing protein, and CAF16, a putative ABC ATPase. Whereas neither CAF4 nor CAF16 was part of the core CCR4-NOT complex, both CAF16 and CAF4 appeared to be present in the 1.9-MDa complex. CAF4 also displayed physical interactions with multiple CCR4-NOT components and with DBF2, a likely component of the 1.9-MDa complex. In addition, both CAF4 and CAF16 were found to interact in a CCR4-dependent manner with SRB9, a component of the SRB complex that is part of the yeast RNA polymerase II holoenzyme. The three related SRB proteins, SRB9, SRB10, and SRB11, were found to interact with and to coimmunoprecipitate DBF2, CAF4, CCR4, NOT2, and NOT1. Defects in SRB9 and SRB10 also affected processes at the ADH2 locus known to be controlled by components of the CCR4-NOT complex; an srb9 mutation was shown to reduce ADH2 derepression and either an srb9 or srb10 allele suppressed spt10-enhanced expression of ADH2. In addition, srb9 and srb10 alleles increased ADR1 c -dependent ADH2 expression; not4 and not5 deletions are the only other known defects that elicit this phenotype. These results suggest a close physical and functional association between components of the CCR4-NOT complexes and the SRB9, -10, and -11 components of the holoenzyme.

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Cytochrome bd biosynthesis in Escherichia coli: the sequences of the cydC and cydD genes suggest that they encode the components of an ABC membrane transporter

Cited by 87 publications

References 33 publications

The Escherichia coli ATP‐binding cassette (ABC) proteins

The Escherichia coli ATP‐binding cassette (ABC) proteins

A Bacterial Glutathione Transporter (Escherichia coli CydDC) Exports Reductant to the Periplasm

Characterization of CAF4 and CAF16 Reveals a Functional Connection between the CCR4-NOT Complex and a Subset of SRB Proteins of the RNA Polymerase II Holoenzyme

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