Engagement of Arginine Finger to ATP Triggers Large Conformational Changes in NtrC1 AAA+ ATPase for Remodeling Bacterial RNA Polymerase

Chen, Baoyu; Sysoeva, Tatyana A.; Chowdhury, Saikat; Guo, Liang; Carlo, Sacha De; Hanson, Jeffrey; Yang, Haw; Nixon, B. Tracy

doi:10.1016/j.str.2010.08.018

Cited by 52 publications

(94 citation statements)

References 37 publications

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“…5). Although it was observed earlier that s54 protein can bind with other oligomeric states of the bEBPs (Rappas et al 2005;Chen et al 2010), we propose that the asymmetric hexamer provides a unique configuration for guiding the protein-protein interaction. Our preliminary EM data for the NtrC1 ATPase in complex with s54-promoter-RNAP suggest the presence of a similarly asymmetric NtrC1 hexamer (S Chowdhury, S DeCarlo, and BT Nixon, unpubl.).…”

Section: The Gap Interface Of the Ntrc1 Atpase As A Nucleotide Releasmentioning

confidence: 53%

“…What does appear certain is that all of the multimeric ATPases need to break rotational symmetry or lower it in order to function efficiently. That requirement may explain inhibition of the ATPase activity by saturating amounts of ATP in the bEBPs PspF and NtrC1 (Schumacher et al 2008;Chen et al 2010).…”

Section: Topologically Open Hexamer As a General Trend?mentioning

confidence: 99%

“…Several bEBPs have been crystallized as hexamers and heptamers, but no mechanism for hydrolysis has yet emerged from those structures (Lee et al 2003;Rappas et al 2005Rappas et al , 2006Sallai and Tucker 2005;Batchelor et al 2008;Chen et al 2010). We showed previously that binding of ATP but not ADP causes large structural changes in the bEBP NtrC1 from the extreme hyperthermophile Aquifex aeolicus (Chen et al 2007.…”

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confidence: 99%

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Nucleotide-induced asymmetry within ATPase activator ring drives σ54–RNAP interaction and ATP hydrolysis

et al. 2013

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It is largely unknown how the typical homomeric ring geometry of ATPases associated with various cellular activities enables them to perform mechanical work. Small-angle solution X-ray scattering, crystallography, and electron microscopy (EM) reconstructions revealed that partial ATP occupancy caused the heptameric closed ring of the bacterial enhancer-binding protein (bEBP) NtrC1 to rearrange into a hexameric split ring of striking asymmetry. The highly conserved and functionally crucial GAFTGA loops responsible for interacting with s54-RNA polymerase formed a spiral staircase. We propose that splitting of the ensemble directs ATP hydrolysis within the oligomer, and the ring's asymmetry guides interaction between ATPase and the complex of s54 and promoter DNA. Similarity between the structure of the transcriptional activator NtrC1 and those of distantly related helicases Rho and E1 reveals a general mechanism in homomeric ATPases whereby complex allostery within the ring geometry forms asymmetric functional states that allow these biological motors to exert directional forces on their target macromolecules.

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Section: The Gap Interface Of the Ntrc1 Atpase As A Nucleotide Releasmentioning

confidence: 53%

Section: Topologically Open Hexamer As a General Trend?mentioning

confidence: 99%

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confidence: 99%

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Nucleotide-induced asymmetry within ATPase activator ring drives σ54–RNAP interaction and ATP hydrolysis

et al. 2013

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“…The altered amino acid is located next to an annotated arginine finger (Arg311) and within an annotated 54 interaction domain. Binding of the arginine finger to ATP triggers a large conformational shift, which is essential for interaction with 54 -RNA polymerase (40). Thus, the mutation of Tyr310 may negatively affect the interaction with 54 -RNA polymerase, resulting in the absence of pxr transcription.…”

Section: Resultsmentioning

confidence: 99%

Spontaneous Reversions of an Evolutionary Trait Loss Reveal Regulators of a Small RNA That Controls Multicellular Development in Myxobacteria

Kleiner

Velicer

2016

J Bacteriol

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Lost traits can reevolve, but the probability of trait reversion depends partly on a trait's genetic complexity. Myxobacterial fruiting body development is a complex trait controlled by the small RNA (sRNA) Pxr, which blocks development under conditions of nutrient abundance. In developmentally proficient strains of Myxococcus xanthus, starvation relaxes the inhibition by Pxr, thereby allowing development to proceed. In contrast, the lab-evolved strain OC does not develop because it fails to relay an early starvation signal that alleviates inhibition by Pxr. A descendant of OC, strain PX, previously reevolved developmental proficiency via a mutation in pxr that inactivates its function. A single-colony screen was used to test whether reversion of OC to developmental proficiency occurs only by mutation of pxr or might also occur through alternative regulatory loci. Five spontaneous mutants of OC that exhibited restored development were isolated, and all five showed defects in Pxr synthesis, structure, or processing, including one that incurred an eight-nucleotide deletion in pxr. Two mutations occurred in the 54 response regulator (RR) gene MXAN_1078 (named pxrR here), immediately upstream of pxr. PxrR was found to positively regulate pxr transcription, presumably via the 54 promoter of pxr. Two other mutations were identified in a histidine kinase (HK) gene (MXAN_1077; named pxrK here) immediately upstream of pxrR. Evolutionarily, the rate of trait restoration documented in this study suggests that reversion of social defects in natural microbial populations may be common. Molecularly, these results suggest a mechanism by which the regulatory functions of an HK-RR two-component signaling system and an sRNA are integrated to control initiation of myxobacterial development. IMPORTANCEMany myxobacteria initiate a process of multicellular fruiting body development upon starvation, but key features of the regulatory network controlling the transition from growth to development remain obscure. Previous work with Myxococcus xanthus identified the first small RNA (sRNA) regulator (Pxr) known to serve as a gatekeeper in this life history transition, as it blocks development when nutrients are abundant. In the present study, a screen for spontaneous mutants of M. xanthus was developed that revealed a two-component system operon (encoding a histidine kinase and a 54 response regulator) associated with the production and processing of Pxr sRNA. This discovery broadens our knowledge of early developmental gene regulation and also represents an evolutionary integration of two-component signaling and sRNA gene regulation to control a bacterial social trait. Functional traits are often lost from evolving populations after selection favoring those traits has been relaxed (1-4). Although Dollo famously asserted that evolutionary losses are irreversible (5), lost traits might be restored evolutionarily, even if infrequently (6). Among animals, some species of dust mites appear to have reevolved host independence from ances...

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“…Such methods include cryo EM and SAXS. Cryo EM has revealed flexibility in the N-domains of E. coli AAA + protein ClpA (Ishikawa et al, 2004) and SAXS experiments have shown large conformational changes in NtrC1 (Chen et al, 2010). Although in some cases conformational changes observed with different methods do not completely agree, it is widely accepted that AAA + proteins undergo dynamic movements during their catalytic cycle.…”

Section: Conformational Changes In Aaa + Proteinsmentioning

confidence: 99%

IBMPFD and p97, the Structural and Molecular Basis for Functional Disruption

Tang¹,

Xia²

2012

Neuromuscular Disorders

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Engagement of Arginine Finger to ATP Triggers Large Conformational Changes in NtrC1 AAA+ ATPase for Remodeling Bacterial RNA Polymerase

Cited by 52 publications

References 37 publications

Nucleotide-induced asymmetry within ATPase activator ring drives σ54–RNAP interaction and ATP hydrolysis

Nucleotide-induced asymmetry within ATPase activator ring drives σ54–RNAP interaction and ATP hydrolysis

Spontaneous Reversions of an Evolutionary Trait Loss Reveal Regulators of a Small RNA That Controls Multicellular Development in Myxobacteria

IBMPFD and p97, the Structural and Molecular Basis for Functional Disruption

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