Interactions of Bordetella pertussis adenylyl cyclase toxin CyaA with calmodulin mutants and calmodulin antagonists: Comparison with membranous adenylyl cyclase I

Schuler, Dominik; Lübker, Carolin; Lushington, Gerald H.; Tang, Wei-Jen; Shen, Yuequan; Richter, Mark L.; Seifert, Roland

doi:10.1016/j.bcp.2012.01.005

Cited by 7 publications

(9 citation statements)

References 46 publications

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“…The catalytic activity of AC1 was essentially determined as previously described [ 21 , 54 ]. Sf9 membranes expressing AC1 were resuspended using syringes at 4°C and diluted with binding buffer (75 mM Tris-HCl, 12.5 mM MgCl 2 and 1 mM EDTA) to a final protein concentration of 1 μg/μl and a final pH of 7.4.…”

Section: Methodsmentioning

confidence: 99%

“…The three dimensional structure of CaM is modified by binding four Ca 2+ -ions. Ca 2+ -saturated CaM possesses a flexible linker region, connecting a C-terminal and an N-terminal globular region [ 16 ], which affords the interaction with numerous target proteins like myosin light-chain kinase (MLCK), cyclic nucleotide phosphodiesterase (PDE) and Bordetella pertussis AC toxin CyaA (CyaA) and the associated regulation of diverse physiological processes [ 16 – 21 ].…”

Section: Introductionmentioning

confidence: 99%

“…CyaA and sarcoplasmatic/endoplasmatic reticulum Ca 2+ -ATPase (SERCA)), where CDZ acts as a potent inhibitor, it was suggested that the potency of inhibition is correlated with the hydrophobicity and the size of the inhibitor [ 21 , 49 ]. In contrast to most of above CaM-inhibitors, CDZ inhibits many CaM-targets in a CaM-independent manner [ 18 , 21 , 49 – 52 ]. Table 1 summarizes the effects of CaM-inhibitors on CaM-target interactions.…”

Section: Introductionmentioning

confidence: 99%

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Effects of 39 Compounds on Calmodulin-Regulated Adenylyl Cyclases AC1 and Bacillus anthracis Edema Factor

Lübker

Seifert

2015

PLoS ONE

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Adenylyl cyclases (ACs) catalyze the conversion of ATP into the second messenger cAMP. Membranous AC1 (AC1) is involved in processes of memory and learning and in muscle pain. The AC toxin edema factor (EF) of Bacillus anthracis is involved in the development of anthrax. Both ACs are stimulated by the eukaryotic Ca2+-sensor calmodulin (CaM). The CaM-AC interaction could constitute a potential target to enhance or impair the AC activity of AC1 and EF to intervene in above (patho)physiological mechanisms. Thus, we analyzed the impact of 39 compounds including typical CaM-inhibitors, an anticonvulsant, an anticholinergic, antidepressants, antipsychotics and Ca2+-antagonists on CaM-stimulated catalytic activity of AC1 and EF. Compounds were tested at 10 μM, i.e., a concentration that can be reached therapeutically for certain antidepressants and antipsychotics. Calmidazolium chloride decreased CaM-stimulated AC1 activity moderately by about 30%. In contrast, CaM-stimulated EF activity was abrogated by calmidazolium chloride and additionally decreased by chlorpromazine, felodipine, penfluridol and trifluoperazine by about 20–40%. The activity of both ACs was decreased by calmidazolium chloride in the presence and absence of CaM. Thus, CaM-stimulated AC1 activity is more insensitive to inhibition by small molecules than CaM-stimulated EF activity. Inhibition of AC1 and EF by calmidazolium chloride is largely mediated via a CaM-independent allosteric mechanism.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Effects of 39 Compounds on Calmodulin-Regulated Adenylyl Cyclases AC1 and Bacillus anthracis Edema Factor

Lübker

Seifert

2015

PLoS ONE

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“…The crystal structure of the AC enzyme-calmodulin complex with adefovir diphosphate, thereby mimicking the binding of ATP, revealed the mechanism of catalytic activity of CyaA. Both the calmodulin-binding and the catalytic site of the AC enzyme have emerged as targets of inhibitors that can be used to inhibit the catalytic activity of CyaA and may be valuable drugs for the prophylaxis of B. pertussis infection [142][143][144][145][146][147][148][149][150][151].…”

Section: The Cell-invasive Adenylate Cyclase Enzyme Domain Of Cyaamentioning

confidence: 99%

Bordetella protein toxins

Mašín

Osička

Bumba

et al. 2015

The Comprehensive Sourcebook of Bacterial Protein Toxins

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“…Although ExoY shares significant homology in the catalytic domain with CyaA and edema factor, the previously characterized calmodulin-binding domain was absent from ExoY. Calmodulin is required to measure edema factor catalytic activity, and it stimulates CyaA activity over 500-fold (Karst et al 2010; Schuler et al 2012; Selwa et al 2012, 2014). ExoY, however, was not stimulated or activated by calmodulin in the Yahr studies (Yahr et al 1998).…”

Section: Studies On the Discovery Of Exoy And Its Enzymatic Activitymentioning

confidence: 99%

The Pseudomonas aeruginosa Exoenzyme Y: A Promiscuous Nucleotidyl Cyclase Edema Factor and Virulence Determinant

Morrow

Frank

Balczon

et al. 2016

Handbook of Experimental Pharmacology

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Exoenzyme Y (ExoY) was identified as a component of the Pseudomonas aeruginosa type 3 secretion system secretome in 1998. It is a common contributor to the arsenal of type 3 secretion system effectors, as it is present in approximately 90% of Pseudomonas isolates. ExoY has adenylyl cyclase activity that is dependent upon its association with a host cell cofactor. However, recent evidence indicates that ExoY is not just an adenylyl cyclase; rather, it is a promiscuous cyclase capable of generating purine and pyrimidine cyclic nucleotide monophosphates. ExoY’s enzymatic activity causes a characteristic rounding of mammalian cells, due to microtubule breakdown. In endothelium, this cell rounding disrupts cell-to-cell junctions, leading to loss of barrier integrity and an increase in tissue edema. Microtubule breakdown seems to depend upon tau phosphorylation, where the elevation of cyclic nucleotide monophosphates activates protein kinases A and G and causes phosphorylation of endothelial microtubule associated protein tau. Phosphorylation is a stimulus for tau release from microtubules, leading to microtubule instability. Phosphorylated tau accumulates inside endothelium as a high molecular weight, oligomeric form, and is then released from the cell. Extracellular high molecular weight tau causes a transmissible cytotoxicity that significantly hinders cellular repair following infection. Thus, ExoY may contribute to bacterial virulence in at least two ways; first, by microtubule breakdown leading to loss of endothelial cell barrier integrity, and second, by promoting release of a high molecular weight tau cytotoxin that impairs cellular recovery following infection.

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Interactions of Bordetella pertussis adenylyl cyclase toxin CyaA with calmodulin mutants and calmodulin antagonists: Comparison with membranous adenylyl cyclase I

Cited by 7 publications

References 46 publications

Effects of 39 Compounds on Calmodulin-Regulated Adenylyl Cyclases AC1 and Bacillus anthracis Edema Factor

Effects of 39 Compounds on Calmodulin-Regulated Adenylyl Cyclases AC1 and Bacillus anthracis Edema Factor

Bordetella protein toxins

The Pseudomonas aeruginosa Exoenzyme Y: A Promiscuous Nucleotidyl Cyclase Edema Factor and Virulence Determinant

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