How Botulinum Neurotoxin Light Chain A1 Maintains Stable Association with the Intracellular Neuronal Plasma Membrane

被引:3
作者
Gardner, Alexander P. [1 ]
Barbieri, Joseph T. [1 ]
Pellett, Sabine [2 ]
机构
[1] Med Coll, Microbiol & Immunol, Wisconsin 8701 Watertown Plank Rd, Milwaukee, WI 53226 USA
[2] Univ Wisconsin Madison, Dept Bacteriol, Microbial Sci Bldg,1550 Linden Dr, Madison, WI 53706 USA
基金
英国科研创新办公室; 美国国家卫生研究院;
关键词
botulinum toxin; bacterial toxins; SNAP-25; intracellular trafficking; protein modeling; TOXIN TYPE-A; SUBSTRATE RECOGNITION; SNARE; IDENTIFICATION; SEROTYPES; MECHANISM; PROTEINS; DURATION; TETANUS; SNAP-25;
D O I
10.3390/toxins14120814
中图分类号
TS2 [食品工业];
学科分类号
0832 ;
摘要
Botulinum neurotoxin serotype A (BoNT/A) is the most potent protein toxin for humans and is utilized as a therapy for numerous neurologic diseases. BoNT/A comprises a catalytic Light Chain (LC/A) and a Heavy Chain (HC/A) and includes eight subtypes (BoNT/A1-/A8). Previously we showed BoNT/A potency positively correlated with stable localization on the intracellular plasma membrane and identified a low homology domain (amino acids 268-357) responsible for LC/A1 stable co-localization with SNAP-25 on the plasma membrane, while LC/A3 was present in the cytosol of Neuro2A cells. In the present study, steady-state- and live-imaging of a cytosolic LC/A3 derivative (LC/A3V) engineered to contain individual structural elements of the A1 LDH showed that a 59 amino acid region (275-334) termed the MLD was sufficient to direct LC/A3V from the cytosol to the plasma membrane co-localized with SNAP-25. Informatics and experimental validation of the MLD-predicted R1 region (an alpha-helix, residues 275-300) and R2 region (a loop, alpha-helix, loop, residues 302-334) both contribute independent steps to the stable co-localization of LC/A1 with SNAP-25 on the plasma membrane of Neuro-2A cells. Understanding how these structural elements contribute to the overall association of LC/A1 on the plasma membrane may identify the molecular basis for the LC contribution of BoNT/A1 to high potency.
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页数:16
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