Botulinum toxins--cause of botulism and systemic diseases?

Toxins ofClostridium botulinum (types A-G) are known as neurotoxins, causing the clinically well-known picture of flaccid muscular paralysis. The molecular biological background is the blocking of acetylcholine secretion in neuromuscular junctions by enzymatic cleavage of molecules forming the machi...

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Veröffentlicht in:Veterinary research communications 2005-06, Vol.29 (4), p.313-345
Hauptverfasser: Bohnel, H, Gessler, F
Format: Artikel
Sprache:eng
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Zusammenfassung:Toxins ofClostridium botulinum (types A-G) are known as neurotoxins, causing the clinically well-known picture of flaccid muscular paralysis. The molecular biological background is the blocking of acetylcholine secretion in neuromuscular junctions by enzymatic cleavage of molecules forming the machinery of exocytosis. Two non-neurotoxins (types C2, C3) are produced by some strains ofC. botulinum types C and D. These affect the cytoskeleton by ribosylating actin filaments. All these toxins are used as cell biological tools for the study of specific actions and effects in different eukaryotic cells. Pharmaceutical and molecular biological research has shown their influence on several crucial organs (or cell cultures thereof) of humans and animals (brain and spinal cord, cerebellum, hippocampus, hypophysis, pancreas, adrenal glands, salivary glands and others). Under natural conditions, botulinum toxins may pass the intestinal barrier and circulate in the bloodstream for a certain time. Carriers occurring naturally in food, such as wheat germ agglutinin, digitonin or saponin, and bacterial toxins such as streptolysin O, perfringolysins, C2 toxin or botulinolysin may also form pores in cell walls. They facilitate the entry of botulinum toxins into cells that may not have natural binding receptors. It is concluded that in vivo actions of different botulinum toxins after their entry into the organism may contribute to the onset of different diseases of hitherto cryptogenic origin. Some examples are given and future problems are discussed.
ISSN:0165-7380
1573-7446
DOI:10.1023/B:VERC.0000048489.45634.32