Identification and Biochemical Characterization of Small-Molecule Inhibitors of
            <i>Clostridium botulinum</i>
            Neurotoxin Serotype A

Roxas-Duncan, Virginia; Enyedy, Istvan; Montgomery, Vicki A.; Eccard, Vanessa S.; Carrington, Marco A.; Lai, Huiguo; Gul, Nizamettin; Yang, David C.H.; Smith, Leonard A.

doi:10.1128/aac.00141-09

Cited by 68 publications

(101 citation statements)

References 48 publications

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“…Inhibitors capable of delaying the onset of botulism by blocking BoNT-Lc activity have also been described (8,69). Although these compounds generally work better in vitro (69,70), some have led to 60% of treated mice surviving 3-fold longer than controls (8). One pitfall of these molecules is that they are only effective against a specific serotype.…”

Section: Discussionmentioning

confidence: 99%

Dynamin Inhibition Blocks Botulinum Neurotoxin Type A Endocytosis in Neurons and Delays Botulism

Harper

Martin

Nguyen

et al. 2011

Journal of Biological Chemistry

144

149

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The botulinum neurotoxins (BoNTs) are di-chain bacterial proteins responsible for the paralytic disease botulism. Following binding to the plasma membrane of cholinergic motor nerve terminals, BoNTs are internalized into an endocytic compartment. Although several endocytic pathways have been characterized in neurons, the molecular mechanism underpinning the uptake of BoNTs at the presynaptic nerve terminal is still unclear. Here, a recombinant BoNT/A heavy chain binding domain (Hc) was used to unravel the internalization pathway by fluorescence and electron microscopy. BoNT/A-Hc initially enters cultured hippocampal neurons in an activity-dependent manner into synaptic vesicles and clathrin-coated vesicles before also entering endosomal structures and multivesicular bodies. We found that inhibiting dynamin with the novel potent Dynasore analog, Dyngo-4a TM , was sufficient to abolish BoNT/ A-Hc internalization and BoNT/A-induced SNAP25 cleavage in hippocampal neurons. Dyngo-4a also interfered with BoNT/ A-Hc internalization into motor nerve terminals. Furthermore, Dyngo-4a afforded protection against BoNT/A-induced paralysis at the rat hemidiaphragm. A significant delay of >30% in the onset of botulism was observed in mice injected with Dyngo-4a. Dynamin inhibition therefore provides a therapeutic avenue for the treatment of botulism and other diseases caused by pathogens sharing dynamin-dependent uptake mechanisms.

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Section: Discussionmentioning

confidence: 99%

Dynamin Inhibition Blocks Botulinum Neurotoxin Type A Endocytosis in Neurons and Delays Botulism

Harper

Martin

Nguyen

et al. 2011

Journal of Biological Chemistry

144

149

View full text Add to dashboard Cite

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“…BoNT antagonist development has been largely limited to studies of small sets of compounds or peptides chosen through rational design, computer-assisted, or other methods [54][55][56][57][58][59]. Although these studies have provided a considerable amount of information about BoNT catalytic mechanism and substrate requirements, few of the small molecule inhibitors that have emerged from these studies have sufficient potency to be effective BoNT therapeutics.…”

Section: Discussionmentioning

confidence: 99%

Detection of six serotypes of botulinum neurotoxin using fluorogenic reporters

Ruge

Dunning

Piazza

et al. 2011

Analytical Biochemistry

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a b s t r a c tMethods that do not require animal sacrifice to detect botulinum neurotoxins (BoNTs) are critical for BoNT antagonist discovery and the advancement of quantitative assays for biodefense and pharmaceutical applications. Here we describe the development and optimization of fluorogenic reporters that detect the proteolytic activity of BoNT/A, B, D, E, F, and G serotypes in real time with femtomolar to picomolar sensitivity. Notably, the reporters can detect femtomolar concentrations of BoNT/A in 4 h and BoNT/E in 20 h, sensitivity that equals that of animal-based methods. The reporters can be used to determine the specific activity of BoNT preparations with intra-and inter-assay coefficients of variation of approximately 10%. Finally, we find that the greater sensitivity of our reporters compared with those used in other commercially available assays makes the former attractive candidates for high-throughput screening of BoNT antagonists.Ó 2011 Elsevier Inc. All rights reserved.Botulinum neurotoxins (BoNTs), 1 produced by the bacteria of the genus Clostridium, are the most lethal substances known. The zinc-dependent endopeptidases act by entering neurons and cleaving soluble N-ethylmaleimide-sensitive factor attachment protein receptors (SNAREs) and, thus, compromise the protein machinery responsible for neurotransmitter release [1][2][3][4][5][6][7][8]. Failure to promptly treat a victim of BoNT poisoning can result in flaccid paralysis, respiratory failure, or death [9]. The combination of extreme potency and a lack of medical treatments other than antitoxin administration and intensive care has made BoNT a biodefense priority requiring the discovery and development of assays to quantify toxins and to identify antagonists to counteract intoxication [10][11][12][13]. Despite their lethality, BoNTs are widely used for cosmetic and pharmaceutical applications due in part to their exquisite specificity for the neuromuscular junction. BoNTs provide relief of muscle tension and pain by inhibiting neurons that cause excessive muscle contractions. Therapeutic preparations of BoNT/A and B serotypes are Food and Drug Administration (FDA) approved for treating glabellar lines, strabismus, cervical dystonia, blepharospasm, cranial nerve VII disorders, and primary axillary hyperhidrosis. Dozens of ''off-label'' BoNT clinical applications have also been documented [14][15][16][17].The mouse bioassay, or lethality test, has been the standard for testing BoNT-containing samples for the past 30 years [18][19][20]. Government agencies use this method for testing food and serum samples for the presence of BoNT, whereas the pharmaceutical industry uses it for quality control and to quantify ''for human use'' BoNT preparations. The test is carried out by injecting mice intraperitoneally with approximately 0.5 ml of sample per mouse and recording the number of deaths over a 1-to 7-day period. The assay is very sensitive, with a detection limit of 5-10 pg for BoNT/A [21,22]. Results for the mouse bioassay are reported in...

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“…Pharmacological treatments that could mitigate the toxicity of the toxin once it has been internalized would be important adjuncts to existing therapeutic procedures and will be invaluable in the event of an attack by serving as antidotes to those already exposed to the toxin to prevent progression and hasten recovery. Small molecule non-peptidic inhibitors (SMNPI) are being developed [12][13][14][15][16][17][18]. Synthetic molecule based high-throughput drug discovery is also in progress [19].…”

Section: Introductionmentioning

confidence: 99%

Structure Based Discovery of Pan Active Botulinum Neurotoxin Inhibitors

Vieni¹,

McGillick²,

Kumaran³

et al. 2018

J Infect Dis Ther

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Clostridium botulinum neurotoxins (BoNTs) released by the bacterium Clostridium botulinum are the most potent toxins causing the fatal disease called botulism. There are seven distinct serotypes of BoNTs (A to G) released by various strains of botulinum. They all have high sequence homology and similar three-dimensional structure. The toxicity of BoNT follows a four-step process-binding, internalization, translocation, and cleavage of its target protein, one of the three components of the SNARE complex (Soluble N-ethylmaleimde-sensitive factor attachment protein receptor) required for membrane docking and neurotransmitter release. Cleavage of one of the three proteins causes blockage of neurotransmitter release leading to flaccid paralysis. Though anyone of the above four steps could be a target for developing antidotes for botulism, the catalytic domain is the most suitable target for post exposure treatment. Of the seven serotypes BoNT/A, B, E and probably F affect humans, with BoNT/A considered to be the most potent. Development of drugs for botulism is focused on serotype specific inhibitors, but pan-active inhibitor acting on several serotypes is preferable since it is difficult to identify the serotype before the treatment, especially since there is at least a 36 h window before botulism can be diagnosed. Using structure-based drug discovery, we have developed three heptapeptides based on the SNARE proteins which inhibit BoNT/A, B and E equally well. Probable reasons for pan-activity of these peptides are discussed.

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Identification and Biochemical Characterization of Small-Molecule Inhibitors of Clostridium botulinum Neurotoxin Serotype A

Cited by 68 publications

References 48 publications

Dynamin Inhibition Blocks Botulinum Neurotoxin Type A Endocytosis in Neurons and Delays Botulism

Dynamin Inhibition Blocks Botulinum Neurotoxin Type A Endocytosis in Neurons and Delays Botulism

Detection of six serotypes of botulinum neurotoxin using fluorogenic reporters

Structure Based Discovery of Pan Active Botulinum Neurotoxin Inhibitors

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