Identification of Rv3230c as the NADPH Oxidoreductase of a Two-Protein DesA3 Acyl-CoA Desaturase in<i>Mycobacterium tuberculosis</i>H37Rv

Chen, Yong; Fox, Brian G.

doi:10.1021/bi0615285

Cited by 25 publications

(29 citation statements)

References 69 publications

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“…Among them, at least three copies of IS6110 interrupt different described operons, i.e., Rv2349c (plcB and plcC), Rv2823c (Rv2824c and Rv2819c), and Rv3229c (Rv3230c and Rv3229c) (41)(42)(43), and the potential transcriptional influence on these operons is an interesting point to be studied.…”

Section: Discussionmentioning

confidence: 99%

“…Its product is a stearoyl-coenzyme A desaturase (DesA3) implicated in the synthesis of oleic acid and considered to be essential for intracellular growth in macrophages (44,45). In addition, DesA3 is a target of the secondline antituberculosis drug isoxyl, which was used together with isoniazid in multiple-drug therapy in the 1960s (43,44). Isoxyl inhibits the synthesis of oleic and mycolic acids (43) and was demonstrated to be effective against various clinical isolates of multidrug-resistant strains of M. tuberculosis (46).…”

Section: Discussionmentioning

confidence: 99%

“…In addition, DesA3 is a target of the secondline antituberculosis drug isoxyl, which was used together with isoniazid in multiple-drug therapy in the 1960s (43,44). Isoxyl inhibits the synthesis of oleic and mycolic acids (43) and was demonstrated to be effective against various clinical isolates of multidrug-resistant strains of M. tuberculosis (46). The finding of the insertion of IS6110 in the desA3 (Rv3229c) gene suggests that isoxyl would not be effective against the Zaragoza strain.…”

Section: Discussionmentioning

confidence: 99%

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Global Study of IS 6110 in a Successful Mycobacterium tuberculosis Strain: Clues for Deciphering Its Behavior and for Its Rapid Detection

et al. 2013

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eThe Mycobacterium tuberculosis insertion sequence IS6110, besides being a very useful tool in molecular epidemiology, seems to have an impact on the biology of bacilli. In the present work, we mapped the 12 points of insertion of IS6110 in the genome of a successful strain named M. tuberculosis Zaragoza (which has been referred to as the MTZ strain). This strain, belonging to principal genetic group 3, caused a large unsuspected tuberculosis outbreak involving 85 patients in Zaragoza, Spain, in 2001 to 2004. The mapping of the points of insertion of IS6110 in the genome of the Zaragoza strain offers clues for a better understanding of the adaptability and virulence of M. tuberculosis. Surprisingly, the presence of one copy of IS6110 was found in Rv2286c, as was recently described for a successful Beijing sublineage. As a result of this analysis, a rapid method for detecting this particular M. tuberculosis strain has been designed.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Global Study of IS 6110 in a Successful Mycobacterium tuberculosis Strain: Clues for Deciphering Its Behavior and for Its Rapid Detection

et al. 2013

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“…The X-ray structure of phthalate dioxygenase reductase is the representative structure for this clade and domain arrangement (PDB ID 2PIA, [25]). In one example reported so far, catalytic cross-reactivity was not observed across the clades, i.e., T4moF did not substitute for Rv3230c [26]. The crossreactivity within the clades has not been explicitly tested.…”

Section: Characterization Of T4mofmentioning

confidence: 96%

“…The X-ray structure of BZD is the representative structure for this clade and domain arrangement (PDB ID 1KRH, [24]). The other clade, with representatives phthalate dioxygenase reductase [25] and Rv3230c [26], has N-terminal flavinand NAD-binding domains and a C-terminal [2Fe-2S] domain. The X-ray structure of phthalate dioxygenase reductase is the representative structure for this clade and domain arrangement (PDB ID 2PIA, [25]).…”

Section: Characterization Of T4mofmentioning

confidence: 99%

Soluble expression and purification of the oxidoreductase component of toluene 4-monooxygenase

Bailey

Elsen

Pierce

et al. 2008

Protein Expression and Purification

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Toluene 4-monooxygenase (T4MO) is a member of the bacterial multicomponent monooxygenases, an enzyme family that utilizes a soluble diiron hydroxylase to oxidize a variety of hydrocarbons as the initial step in their metabolism. The hydroxylases obtain reducing equivalents from NAD(P)H via an electron transfer chain that is initiated by an oxidoreductase containing an N-terminal ferredoxin domain and C-terminal flavin-and NAD-binding domains. T4moF, the NADH oxidoreductase of T4MO, was expressed as a soluble protein in Escherichia coli BL21(DE3) from the pUC-derived expression vector pRS205. This vector contains a lac promoter instead of a T7 promoter. A three step purification from the soluble cell lysate yielded ∼1 mg of T4moF per gram of wet cell paste with greater than 90% purity. The purified protein contained 1 mol of FAD and 2 mol of Fe per mol of T4moF; quantitiative EPR spectroscopy showed ∼1 mol of the S = ½ signal from the reduced [2Fe-2S] cluster per mol of T4moF. Steady state kinetic analysis of p-cresol formation activity treating T4moF as the variable substrate while all other proteins and substrates were held constant gave apparent K M -and apparent k cat -values of 0.15 μM and 3.0 s -1 , respectively. This expression system and purification allows for the recovery of the soluble oxidoreductase in yields that facilitate further biochemical and structural characterizations.

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One‐plasmid tunable coexpression for mycobacterial protein–protein interaction studies

et al. 2009

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A single plasmid that allows controlled coexpression has been developed for use in mycobacteria. The tetracycline inducible promoter, PtetO, was used to provide tetracyclinedependent induction of one gene, while the Psmyc, Pimyc, or Phsp promoters were used to provide three different levels of constitutive expression of a second gene. The functions of these four individual promoters were established using green fluorescent protein (GFP) and a newly identified red fluorescence inducible protein from Geobacillus sterothermophilus strain G1.13 (RFIP) as reporters. The tandem use of GFP and RFIP as reporter genes allowed optimization of the tunable coexpression in Mycobacterium smegmatis; either time at a fixed inducer concentration or changes in inducer concentration could be used to control the protein:protein ratio. This single vector system was used to coexpress the two-protein Mycobacterium tuberculosis stearoyl-CoA D 9 desaturase complex (integral membrane desaturase Rv3229c and NADPH oxidoreductase Rv3230c) in M. smegmatis. The catalytic activity was found to increase in a manner corresponding to increasing the level of Rv3230c relative to a fixed level of Rv3229c. This system, which can yield finely tuned coexpression of the fatty acid desaturase complex in mycobacteria, may be useful for study of other multicomponent complexes. Furthermore, the tunable coexpression strategy used herein should also be applicable in other species with minor modifications.

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Identification of Rv3230c as the NADPH Oxidoreductase of a Two-Protein DesA3 Acyl-CoA Desaturase inMycobacterium tuberculosisH37Rv

Cited by 25 publications

References 69 publications

Global Study of IS 6110 in a Successful Mycobacterium tuberculosis Strain: Clues for Deciphering Its Behavior and for Its Rapid Detection

Global Study of IS 6110 in a Successful Mycobacterium tuberculosis Strain: Clues for Deciphering Its Behavior and for Its Rapid Detection

Soluble expression and purification of the oxidoreductase component of toluene 4-monooxygenase

One‐plasmid tunable coexpression for mycobacterial protein–protein interaction studies

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