Abstract

Botulinum toxins (BoNTs) are among the most potent toxins known, thus defining it as a Class A bio-terrorism threat by NIAID. Intoxication with BoNT leads to flaccid paralysis, respiratory arrest, and death by blocking acetylcholine release at neuromuscular junctions. BoNTs mediate paralysis by cleaving molecules found in synaptic terminals, synaptosomal-associated protein of 25 kD (SNAP-25), vesicle-associated membrane protein (VAMP), or syntaxin. Early treatment with humanized antibodies can prevent progression and death by BoNT intoxication. However, many surviving patients exhibit a persistent or chronic fatigue syndrome. Unfortunately, not much is known about the cellular and molecular mechanism of this fatigue syndrome. A prime hypothesis here is that this disabling fatigue syndrome is caused by cell injury and death of motoneurons and that different BoNT serotypes have differential effects in mediating this newly recognized neurodegenerative disorder. Thus the goal of this project will be to gain new insight into how BoNTs mediate motoneuron cell death. To achieve this goal, primary motoneurons will be analyzed using approaches such as cell biology, immunocytochemistry, time-lapse deconvolution microscopy, electron microscopy, and gene and peptide transfer. Among the specific questions that will be addressed are: (1) How does BoNT/C but not BoNT/A induce damage to synaptic endings and neurites, eventually resulting in motoneuron degeneration? (2) What are the real-time changes in synaptic endings and neurites, cytoskeleton, and mitochondria linked to BoNT-induced motoneuron cell death? (3) Does cleavage of SNAP-25, syntaxin, or synaptobrevin/VAMP suffice to induce motoneuron damage and cell death initiated by BoNTs? Results obtained here will in general lead to a better understanding of the mode of action of BoNTs. Most importantly, new insights gained here will set the foundation to treat and prevent long-term, devastating neurological effects linked to BoNT-mediated intoxication after a bioterrorism attack.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI055789-04
Application #
7455746
Study Section
Special Emphasis Panel (ZAI1)
Project Start
Project End
Budget Start
2007-07-01
Budget End
2008-06-30
Support Year
4
Fiscal Year
2007
Total Cost
$372,924
Indirect Cost

  Institution

Name
Sanford-Burnham Medical Research Institute
Department
Type
DUNS #
020520466
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Aleshin, Alexander E; DiScipio, Richard G; Stec, Boguslaw et al. (2012) Crystal structure of C5b-6 suggests structural basis for priming assembly of the membrane attack complex. J Biol Chem 287:19642-52
Shiryaev, Sergey A; Chernov, Andrei V; Shiryaeva, Tatiana N et al. (2011) The acidic sequence of the NS4A cofactor regulates ATP hydrolysis by the HCV NS3 helicase. Arch Virol 156:313-8
Stranzl, Gudrun R; Santelli, Eugenio; Bankston, Laurie A et al. (2011) Structural insights into inhibition of Bacillus anthracis sporulation by a novel class of non-heme globin sensor domains. J Biol Chem 286:8448-58
Low, Lieh Yoon; Yang, Chen; Perego, Marta et al. (2011) Role of net charge on catalytic domain and influence of cell wall binding domain on bactericidal activity, specificity, and host range of phage lysins. J Biol Chem 286:34391-403
Zhai, Dayong; Yu, Eric; Jin, Chaofang et al. (2010) Vaccinia virus protein F1L is a caspase-9 inhibitor. J Biol Chem 285:5569-80
Zhao, Li-Chun; Yang, Bo; Wang, Rengang et al. (2010) Type C botulinum toxin causes degeneration of motoneurons in vivo. Neuroreport 21:14-18
Shiryaev, Sergey A; Radichev, Ilian A; Ratnikov, Boris I et al. (2010) Isolation and characterization of selective and potent human Fab inhibitors directed to the active-site region of the two-component NS2B-NS3 proteinase of West Nile virus. Biochem J 427:369-76
Remacle, Albert G; Gawlik, Katarzyna; Golubkov, Vladislav S et al. (2010) Selective and potent furin inhibitors protect cells from anthrax without significant toxicity. Int J Biochem Cell Biol 42:987-95
Chan, Siew Leong; Mukasa, Takashi; Santelli, Eugenio et al. (2010) The crystal structure of a TIR domain from Arabidopsis thaliana reveals a conserved helical region unique to plants. Protein Sci 19:155-61
Shiryaev, Sergey A; Strongin, Alex Y (2010) Structural and functional parameters of the flaviviral protease: a promising antiviral drug target. Future Virol 5:593-606

Showing the most recent 10 out of 48 publications