The Structure of the Antibiotic Deactivating, N-hydroxylating Rifampicin Monooxygenase

Liu, Li Kai; Abdelwahab, Heba; Campo, Julia S. Martín del; Mehra-Chaudhary, Ritcha; Sobrado, Pablo; Tanner, John J.

doi:10.1074/jbc.m116.745315

Cited by 36 publications

(40 citation statements)

References 45 publications

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“…4d) from the C4a of the flavin cofactor. These distances are similar to C11a of chlortetracycline and C4a of FAD in the Tet(X)+chlortetracycline structure 27 , and well within the C4a-reactive atom distances observed for flavin monooxygenases 39 . The C11a in the Tet(50)+chlortetracycline, on the other hand, is on the opposite side of the molecule and 7.9 Å away (Fig.…”

Section: Resultssupporting

confidence: 80%

Plasticity, dynamics, and inhibition of emerging tetracycline resistance enzymes

et al. 2017

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While tetracyclines are an important class of antibiotics in agriculture and the clinic, their efficacy is threatened by increasing resistance. Resistance to tetracyclines can occur through efflux, ribosomal protection, or enzymatic inactivation. Surprisingly, tetracycline enzymatic inactivation has remained largely unexplored despite providing the distinct advantage of antibiotic clearance. The tetracycline destructases are a recently-discovered family of tetracycline-inactivating flavoenzymes from pathogens and soil metagenomes with a high potential for broad dissemination. Here, we show tetracycline destructases accommodate tetracycline-class antibiotics in diverse and novel orientations for catalysis, and antibiotic binding drives unprecedented structural dynamics facilitating tetracycline inactivation. We identify a key inhibitor binding mode that locks the flavin adenine dinucleotide cofactor in an inactive state, functionally rescuing tetracycline activity. Our results reveal the potential of a novel tetracycline/tetracycline destructase inhibitor combination therapy strategy to overcome resistance by enzymatic inactivation and restore the use of an important class of antibiotics.

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Section: Resultssupporting

confidence: 80%

Plasticity, dynamics, and inhibition of emerging tetracycline resistance enzymes

et al. 2017

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“…The 3D Structure of Rox-sv Reveals the FAD Co-factor and Homology to Rox-nf The crystal structures of Rox-sv bound to flavin adenine dinucleotide (FAD; refinement statistics can be found in Table S2) and Rox-sv in complex with both rifampin and FAD were determined to explore active-site similarities between the two homologs (Rox-sv and Rox-nf), which exhibit 74% amino acid sequence identity. The structure of Rox-sv was solved by molecular replacement using Rox-nf (Liu et al, 2016) as a search model. For both the FAD-and rifampin,FAD complexes, the protein crystallized with three molecules in the asymmetric unit; all chains adopted overall similar arrangements (all pairwise rootmean-square deviations [RMSD] less than 0.45 Å ).…”

Section: Rox-sv Is a Rifampin-inactivating Monooxygenasementioning

confidence: 99%

“…The latter have been detected in a variety of bacteria (Nocardia farcinica, Rhodococcus equi) and are associated with decomposition of the antibiotic. The 3D structure of the N. farcinica rifampin monooxygenase (Rox-nf) was recently reported (Liu et al, 2016). A molecular mechanism for rifampin oxidation was proposed (Abdelwahab et al, 2016;Liu et al, 2016) based on the structure of the isolated product (designated rifampin-2 0 -N-oxide) (Hoshino et al, 2010) ( Figure 1A).…”

Section: Introductionmentioning

confidence: 96%

“…The 3D structure of the N. farcinica rifampin monooxygenase (Rox-nf) was recently reported (Liu et al, 2016). A molecular mechanism for rifampin oxidation was proposed (Abdelwahab et al, 2016;Liu et al, 2016) based on the structure of the isolated product (designated rifampin-2 0 -N-oxide) (Hoshino et al, 2010) ( Figure 1A). Here we present the identification of a new rifamycin-inducible rox gene in Streptomyces venezuelae (Rox-sv), determination of its 3D structure by X-ray crystallography, and revision of the molecular mechanism of rifamycin inactivation by Rox enzymes.…”

Section: Introductionmentioning

confidence: 96%

“…Resistance to rifamycin antibiotics in the clinic is predominantly due to point mutations in the target, the b subunit of RNA polymerase (Ramaswamy and Musser, 1998), although a rifampin ADP-ribosyltransferase (Baysarowich et al, 2008) (Arr-2) is found in many Gram-negative resistance plasmids. In contrast to the clinic, environmental bacteria have developed a rich diversity of mechanisms to inactivate the rifamycins including ADP-ribosyltransferases (Baysarowich et al, 2008), glycosyltransferases (Spanogiannopoulos et al, 2012), phosphotransferases (Qi et al, 2016;Spanogiannopoulos et al, 2012;Stogios et al, 2016), and monooxygenases (Andersen et al, 1997;Hoshino et al, 2010;Liu et al, 2016). The latter have been detected in a variety of bacteria (Nocardia farcinica, Rhodococcus equi) and are associated with decomposition of the antibiotic.…”

Section: Introductionmentioning

confidence: 99%

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Rox, a Rifamycin Resistance Enzyme with an Unprecedented Mechanism of Action

Koteva

Cox

Kelso

et al. 2018

Cell Chemical Biology

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Rifamycin monooxygenases (Rox) are present in a variety of environmental bacteria and are associated with decomposition of the clinically utilized antibiotic rifampin. Here we report the structure and function of a drug-inducible rox gene from Streptomyces venezuelae, which encodes a class A flavoprotein monooxygenase that inactivates a broad range of rifamycin antibiotics. Our findings describe a mechanism of rifamycin inactivation initiated by monooxygenation of the 2-position of the naphthyl group, which subsequently results in ring opening and linearization of the antibiotic. The result is an antibiotic that no longer adopts the basket-like structure essential for binding to the RNA exit tunnel of the target RpoB, thereby providing the molecular logic of resistance. This unique mechanism of enzymatic inactivation underpins the broad spectrum of rifamycin resistance mediated by Rox enzymes and presents a new antibiotic resistance mechanism not yet seen in microbial antibiotic detoxification.

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Catalytic Control of Spiroketal Formation in Rubromycin Polyketide Biosynthesis

et al. 2021

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The medically important bacterial aromatic polyketide natural products typically feature a planar, polycyclic core structure. An exception is found for the rubromycins, whose backbones are disrupted by a bisbenzannulated [5,6]‐spiroketal pharmacophore that was recently shown to be assembled by flavin‐dependent enzymes. In particular, a flavoprotein monooxygenase proved critical for the drastic oxidative rearrangement of a pentangular precursor and the installment of an intermediate [6,6]‐spiroketal moiety. Here we provide structural and mechanistic insights into the control of catalysis by this spiroketal synthase, which fulfills several important functions as reductase, monooxygenase, and presumably oxidase. The enzyme hereby tightly controls the redox state of the substrate to counteract shunt product formation, while also steering the cleavage of three carbon‐carbon bonds. Our work illustrates an exceptional strategy for the biosynthesis of stable chroman spiroketals.

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The Structure of the Antibiotic Deactivating, N-hydroxylating Rifampicin Monooxygenase

Cited by 36 publications

References 45 publications

Plasticity, dynamics, and inhibition of emerging tetracycline resistance enzymes

Plasticity, dynamics, and inhibition of emerging tetracycline resistance enzymes

Rox, a Rifamycin Resistance Enzyme with an Unprecedented Mechanism of Action

Catalytic Control of Spiroketal Formation in Rubromycin Polyketide Biosynthesis

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