Neurotoxicity of clostridium toxins (Homo sapiens)

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3, 15, 20, 26, 36...1, 33, 36, 553613, 17, 495120, 233636201, 36, 39, 556, 7, 4322, 33, 36, 4640, 45, 5045, 47, 507, 16, 35910, 20, 238, 24, 524, 5, 33, 364, 22, 33, 36, 4614, 4825, 382033, 34, 3633, 34, 3633, 36, 49, 5319, 21, 33, 34, 3652, 54252, 27205, 32, 33, 3610, 20, 233619, 21, 33, 34, 363610, 20, 23, 30363631, 45, 5010, 20, 23clathrin-coated endocytic vesiclecytosolsynaptic vesicle lumensynaptic vesicle lumencytosolendocytic vesicleSV2A SV2C SV2A,B,CGD2SNAP25(198-206)NTNHA botD HC disulfide bonded Zn2+ VAMP1(1-83)GM1aZn2+ SV2A SV2C VAMP1(61-118)SV2C GD3botA LC disulfide bonded BoNT/G LC disulfide bonded SNAP25(199-206)SV2A TeNT LC disulfide bonded botF HC disulfide bonded SV2A Zn2+ botD LC disulfide bonded VAMP2(2-59)STX1A(?-288) GT1b Zn2+ SNAP25(1-198)GT1bH+SNAP25ha70 Zn2+ Zn2+ tetX HCTeNT HC disulfide bonded BoNT/G HCZn2+ botF LC:Zn2+SV2C botC:GT1bbotG LC:Zn2+BoNT/G LC disulfide bonded H+botB HC disulfide bonded SV2A,BbotC LC disulfide bonded botD LC disulfide bonded GT1bZn2+ GT1b TeNT LC disulfide bonded SV2B botD LC disulfide bonded SV2C Zn2+ VAMP1SV2C botD HC disulfide bonded H+SV2A botC HCSTX1B(?-288) SV2B botB HC disulfide bonded SYT1 SV2B botF LC disulfide bonded Zn2+ SYT2 STX1B(1-?) GT1b SV2B botD:SV2:GD2SV2A,B,CSV2A,B,CSV2A VAMP2VAMP2GT1bTeNT LC disulfide bonded botE LC SV2C botD:SV2:GD2TeNT HC disulfide bonded GT1b GT1b SV2A BoNT/G HC disulfide bonded VAMP2(82-116)botC:GT1bVAMP1(62-118)GM1a SNAP25botA HCSYT2 botB LC disulfide bonded SV2A VAMP1tetX:gangliosidesBoNT/G LC disulfide bonded botE:SV2:GT1bSV2C Zn2+ botE HC disulfide bonded GM1a botB HC disulfide bonded SNAP25(1-197)H+ha70 GT1bVAMP2(60-116)botE HC:LCdimer:NTNHAGT1b Zn2+ NTNHA Zn2+ GD3 GT1bSYT1 botD HC disulfide bonded tetX LC:Zn2+VAMP1(1-61)botC LC Zn2+ VAMP2(2-76)GD2 botF:SV2:GT1bSTX1(?-288)GT1b ha17NTNHAtetX HC:LC dimerZn2+ SV2A botE:SV2:GT1bGT1bbotG HC:LC dimerNTNHA VAMP2(2-58)TeNT LC disulfide bonded botE LC disulfide bonded SV2A Zn2+ SYT1 ha33 botE HC:LC dimerbotF HC disulfide bonded Zn2+ SV2C SYT1SV2B botE LC disulfide bonded SYT1 GT1bVAMP2(77-116)SYT1H+Zn2+ SV2B Zn2+ botA HC disulfide bonded botC LC:Zn2+Zn2+ GT1b GD2botC HC disulfide bonded Zn2+ botC LC disulfide bonded botF LC disulfide bonded botA HC disulfide bonded botE LC disulfide bonded STX1NTNHAbotF HC:LC dimerSV2A,B,CVAMP2(2-81)SYT1 SV2B Zn2+ STX1A GD3 Zn2+ botD HC:LC dimerbotD HCSYT2 SV2C BoNT/G HC disulfide bonded botA HC disulfide bonded SV2B Zn2+ SNAP25(1-198)GM1abotD LC:Zn2+SNAP25botA LC GT1b ha33 botB HC disulfide bonded botB LC:Zn2+VAMP2(77-116)ha70tetX:gangliosidesbotB HC:LCdimer:NTNHA:HASV2A,B,CZn2+ botF:SV2:GT1bbotE LC disulfide bonded SV2C SYT1,2Zn2+ H+Zn2+ botB HC:LC dimerTeNT HC disulfide bonded botB HC:LC:SYT:GT1bbotA HC:LC dimerGT1b botE LC:Zn2+SV2B botA LC disulfide bonded VAMP2(59-116)VAMP2SV2B SV2A SV2B SYT1,2GT1bSV2A SV2A,BSNAP25(199-206)ha33botA LC disulfide bonded botB LC Zn2+ Zn2+ SYT1 Zn2+ GD3STX1A(1-?) Zn2+ SV2A,B,CVAMP1(84-118)ha17 tetX:gangliosidesbotB LC disulfide bonded H+TeNT LC botE HC disulfide bonded Zn2+ STX1(1-?)botE HCBoNT/G HC disulfide bonded botD LC botA HC:LCdimer:SV2:GT1bSV2B GT1bbotF LC botE HC disulfide bonded botB HCbotC HC:LC dimerGT1bbotA LC disulfide bonded VAMP2(2-76)botA HC disulfide bonded VAMP1(1-60)GT1b SV2A botA HC:LCdimer:NTNHA:HAbotB LC disulfide bonded botB LC disulfide bonded GD2 botB HC:LCdimer:SYT:GT1bSV2A SV2B SV2C GM1a Zn2+ Zn2+ SV2A botC HC disulfide bonded H+GT1b SV2B botA LC:Zn2+botC HC disulfide bonded botA HC:LCdimer:SV2:GT1bSTX1B SYT2 botG:SYT1:GT1bbotE HC disulfide bonded botF LC disulfide bonded GD3 BoNT/G LC SV2B SV2A botG:SYT1:GT1bVAMP2botF HC disulfide bonded TeNT HC disulfide bonded botF HCbotC LC disulfide bonded SV2B Zn2+ ha17 Zn2+ GT1b3137112037114424234195, 3211474049, 53161642421124, 423717, 38, 44288344212, 18426, 7443749, 5316443737372, 2712, 1812, 1817, 444, 227, 353712, 182942373734, 544217, 25, 38, 4444344115, 3242437374441117, 38, 443712, 1817, 29344242114314, 481112, 1819, 341112, 181, 55191, 554, 2212, 1844949, 5312, 18444449, 531, 55371, 553419, 3491144


Description

Clostridial neurotoxins, when taken up by human neurons, block synaptic transmission by cleaving proteins required for the fusion of synaptic vesicles with the plasma membrane. They are remarkably efficient so that very small doses cause paralysis of an affected person (Lalli et al. 2003; Turton et al. 2002). All characterized clostridial neurotoxins are synthesized as products of chromosomal, plasmid or prophage-borne bacterial genes. The nascent toxin may be cleaved into light (LC) and heavy (HC) chain moieties that remain attached by noncovalent interactions and a disulfide bond (Turton et al. 2002).

Strains of Clostridium botulinum produce seven serologically distinct toxins, BoNT/A, B, C, D, E, F, and G. An eighth toxin, BoNT/H has recently been identified (Barash & Arnon 2014) but its molecular properties have not yet been described. Human poisoning most commonly result from ingestion of toxin contaminated food. More rarely, it is due to wound infection or clostridial colonization of the gut of an infant whose own gut flora have not yet developed or of an older individual whose flora have been suppressed. While all seven characterized toxins can cleave human target proteins, three, BoNT/A, B, and E, are most commonly associated with human disease (Hatheway 1995; Sakaguchi 1982). BoNT/F is also able to cause human botulism.<p>Once ingested, the botulinum toxin must be taken up from the gut lumen into the circulation, a process mediated by four accessory proteins. These proteins form a complex that mediates transcytosis of the toxin molecule across the gut epithelium, allowing its entry into the circulation. The accessory proteins produced by different C. botulinum strains differ in their affinities for polarized epithelia of different species (e.g., human versus canine), and may thus be a key factor in human susceptibility to the toxins of strains A, B, and E and resistance to the others (Simpson 2004).<p>Clostridium tetani produces TeNT toxin. Human poisoning is the result of toxin secretion by bacteria growing in an infected wound and the toxin is released directly into the circulation.<p>Circulating clostridial toxins are taken up by neurons at neuromuscular junctions. They bind to specific gangliosides (BoNT/C, TeNT) or to both gangliosides and synaptic vesicle proteins (BoNT/A, B, D G) exposed on the neuronal plasma membrane during vesicle exocytosis (Montal 2010). All seven characterized forms of BoNT are thought to be taken up into synaptic vesicles as these re-form at the neuromuscular junction. These vesicles remain close to the site of uptake and are rapidly re-loaded with neurotransmitter and acidified (Sudhoff 2004). TeNT, in contrast, is taken up into clathrin coated vesicles that reach the neuron cell body by retrograde transport and then possibly other neurons before undergoing acidification. Vesicle acidification causes a conformational change in the toxin, allowing its HC part to function as a channel through which its LC part is extruded into the neuronal cytosol. The HC - LC disulfide bond is cleaved and the cytosolic LC functions as a zinc metalloprotease to cleave specific bonds in proteins on the cytosolic faces of synaptic vesicles and plasma membranes that normally mediate exocytosis (Lalli et al. 2003; Montal 2010). View original pathway at Reactome.</div>

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Bibliography

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  1. Schiavo G, Malizio C, Trimble WS, Polverino de Laureto P, Milan G, Sugiyama H, Johnson EA, Montecucco C.; ''Botulinum G neurotoxin cleaves VAMP/synaptobrevin at a single Ala-Ala peptide bond.''; PubMed Europe PMC Scholia
  2. Kroken AR, Karalewitz AP, Fu Z, Kim JJ, Barbieri JT.; ''Novel ganglioside-mediated entry of botulinum neurotoxin serotype D into neurons.''; PubMed Europe PMC Scholia
  3. Barash JR, Arnon SS.; ''A novel strain of Clostridium botulinum that produces type B and type H botulinum toxins.''; PubMed Europe PMC Scholia
  4. Vaidyanathan VV, Yoshino K, Jahnz M, Dörries C, Bade S, Nauenburg S, Niemann H, Binz T.; ''Proteolysis of SNAP-25 isoforms by botulinum neurotoxin types A, C, and E: domains and amino acid residues controlling the formation of enzyme-substrate complexes and cleavage.''; PubMed Europe PMC Scholia
  5. Foran P, Lawrence GW, Shone CC, Foster KA, Dolly JO.; ''Botulinum neurotoxin C1 cleaves both syntaxin and SNAP-25 in intact and permeabilized chromaffin cells: correlation with its blockade of catecholamine release.''; PubMed Europe PMC Scholia
  6. Dong M, Richards DA, Goodnough MC, Tepp WH, Johnson EA, Chapman ER.; ''Synaptotagmins I and II mediate entry of botulinum neurotoxin B into cells.''; PubMed Europe PMC Scholia
  7. Kozaki S, Kamata Y, Watarai S, Nishiki T, Mochida S.; ''Ganglioside GT1b as a complementary receptor component for Clostridium botulinum neurotoxins.''; PubMed Europe PMC Scholia
  8. Dong M, Liu H, Tepp WH, Johnson EA, Janz R, Chapman ER.; ''Glycosylated SV2A and SV2B mediate the entry of botulinum neurotoxin E into neurons.''; PubMed Europe PMC Scholia
  9. Karalewitz AP, Fu Z, Baldwin MR, Kim JJ, Barbieri JT.; ''Botulinum neurotoxin serotype C associates with dual ganglioside receptors to facilitate cell entry.''; PubMed Europe PMC Scholia
  10. Sun S, Tepp WH, Johnson EA, Chapman ER.; ''Botulinum neurotoxins B and E translocate at different rates and exhibit divergent responses to GT1b and low pH.''; PubMed Europe PMC Scholia
  11. Dasgupta BR, Datta A.; ''Botulinum neurotoxin type B (strain 657): partial sequence and similarity with tetanus toxin.''; PubMed Europe PMC Scholia
  12. Sathyamoorthy V, Dasgupta BR, Foley J, Niece RL.; ''Botulinum neurotoxin type A: cleavage of the heavy chain into two halves and their partial sequences.''; PubMed Europe PMC Scholia
  13. Link E, Edelmann L, Chou JH, Binz T, Yamasaki S, Eisel U, Baumert M, Südhof TC, Niemann H, Jahn R.; ''Tetanus toxin action: inhibition of neurotransmitter release linked to synaptobrevin proteolysis.''; PubMed Europe PMC Scholia
  14. Willjes G, Mahrhold S, Strotmeier J, Eichner T, Rummel A, Binz T.; ''Botulinum neurotoxin G binds synaptotagmin-II in a mode similar to that of serotype B: tyrosine 1186 and lysine 1191 cause its lower affinity.''; PubMed Europe PMC Scholia
  15. Sakaguchi G.; ''Clostridium botulinum toxins.''; PubMed Europe PMC Scholia
  16. Lacy DB, Tepp W, Cohen AC, DasGupta BR, Stevens RC.; ''Crystal structure of botulinum neurotoxin type A and implications for toxicity.''; PubMed Europe PMC Scholia
  17. Schiavo G, Poulain B, Rossetto O, Benfenati F, Tauc L, Montecucco C.; ''Tetanus toxin is a zinc protein and its inhibition of neurotransmitter release and protease activity depend on zinc.''; PubMed Europe PMC Scholia
  18. Schmidt JJ, Sathyamoorthy V, DasGupta BR.; ''Partial amino acid sequence of the heavy and light chains of botulinum neurotoxin type A.''; PubMed Europe PMC Scholia
  19. Schiavo G, Rossetto O, Catsicas S, Polverino de Laureto P, DasGupta BR, Benfenati F, Montecucco C.; ''Identification of the nerve terminal targets of botulinum neurotoxin serotypes A, D, and E.''; PubMed Europe PMC Scholia
  20. Montal M.; ''Botulinum neurotoxin: a marvel of protein design.''; PubMed Europe PMC Scholia
  21. Arndt JW, Chai Q, Christian T, Stevens RC.; ''Structure of botulinum neurotoxin type D light chain at 1.65 A resolution: repercussions for VAMP-2 substrate specificity.''; PubMed Europe PMC Scholia
  22. Binz T, Blasi J, Yamasaki S, Baumeister A, Link E, Südhof TC, Jahn R, Niemann H.; ''Proteolysis of SNAP-25 by types E and A botulinal neurotoxins.''; PubMed Europe PMC Scholia
  23. Koriazova LK, Montal M.; ''Translocation of botulinum neurotoxin light chain protease through the heavy chain channel.''; PubMed Europe PMC Scholia
  24. Kumaran D, Eswaramoorthy S, Furey W, Navaza J, Sax M, Swaminathan S.; ''Domain organization in Clostridium botulinum neurotoxin type E is unique: its implication in faster translocation.''; PubMed Europe PMC Scholia
  25. Deinhardt K, Berninghausen O, Willison HJ, Hopkins CR, Schiavo G.; ''Tetanus toxin is internalized by a sequential clathrin-dependent mechanism initiated within lipid microdomains and independent of epsin1.''; PubMed Europe PMC Scholia
  26. Turton K, Chaddock JA, Acharya KR.; ''Botulinum and tetanus neurotoxins: structure, function and therapeutic utility.''; PubMed Europe PMC Scholia
  27. Peng L, Tepp WH, Johnson EA, Dong M.; ''Botulinum neurotoxin D uses synaptic vesicle protein SV2 and gangliosides as receptors.''; PubMed Europe PMC Scholia
  28. Agarwal R, Eswaramoorthy S, Kumaran D, Binz T, Swaminathan S.; ''Structural analysis of botulinum neurotoxin type E catalytic domain and its mutant Glu212-->Gln reveals the pivotal role of the Glu212 carboxylate in the catalytic pathway.''; PubMed Europe PMC Scholia
  29. Mochida S, Poulain B, Weller U, Habermann E, Tauc L.; ''Light chain of tetanus toxin intracellularly inhibits acetylcholine release at neuro-neuronal synapses, and its internalization is mediated by heavy chain.''; PubMed Europe PMC Scholia
  30. Sun S, Suresh S, Liu H, Tepp WH, Johnson EA, Edwardson JM, Chapman ER.; ''Receptor binding enables botulinum neurotoxin B to sense low pH for translocation channel assembly.''; PubMed Europe PMC Scholia
  31. Lee K, Gu S, Jin L, Le TT, Cheng LW, Strotmeier J, Kruel AM, Yao G, Perry K, Rummel A, Jin R.; ''Structure of a bimodular botulinum neurotoxin complex provides insights into its oral toxicity.''; PubMed Europe PMC Scholia
  32. Blasi J, Chapman ER, Yamasaki S, Binz T, Niemann H, Jahn R.; ''Botulinum neurotoxin C1 blocks neurotransmitter release by means of cleaving HPC-1/syntaxin.''; PubMed Europe PMC Scholia
  33. Südhof TC, De Camilli P, Niemann H, Jahn R.; ''Membrane fusion machinery: insights from synaptic proteins.''; PubMed Europe PMC Scholia
  34. Yamasaki S, Baumeister A, Binz T, Blasi J, Link E, Cornille F, Roques B, Fykse EM, Südhof TC, Jahn R.; ''Cleavage of members of the synaptobrevin/VAMP family by types D and F botulinal neurotoxins and tetanus toxin.''; PubMed Europe PMC Scholia
  35. Dong M, Yeh F, Tepp WH, Dean C, Johnson EA, Janz R, Chapman ER.; ''SV2 is the protein receptor for botulinum neurotoxin A.''; PubMed Europe PMC Scholia
  36. Sudhof TC.; ''The synaptic vesicle cycle.''; PubMed Europe PMC Scholia
  37. Henderson I, Whelan SM, Davis TO, Minton NP.; ''Genetic characterisation of the botulinum toxin complex of Clostridium botulinum strain NCTC 2916.''; PubMed Europe PMC Scholia
  38. Chen C, Fu Z, Kim JJ, Barbieri JT, Baldwin MR.; ''Gangliosides as high affinity receptors for tetanus neurotoxin.''; PubMed Europe PMC Scholia
  39. Montecucco C, Schiavo G.; ''Mechanism of action of tetanus and botulinum neurotoxins.''; PubMed Europe PMC Scholia
  40. Benefield DA, Dessain SK, Shine N, Ohi MD, Lacy DB.; ''Molecular assembly of botulinum neurotoxin progenitor complexes.''; PubMed Europe PMC Scholia
  41. Hatheway CL.; ''Botulism: the present status of the disease.''; PubMed Europe PMC Scholia
  42. Giménez JA, DasGupta BR.; ''Botulinum neurotoxin type E fragmented with endoproteinase Lys-C reveals the site trypsin nicks and homology with tetanus neurotoxin.''; PubMed Europe PMC Scholia
  43. Swaminathan S, Eswaramoorthy S.; ''Structural analysis of the catalytic and binding sites of Clostridium botulinum neurotoxin B.''; PubMed Europe PMC Scholia
  44. Krieglstein K, Henschen A, Weller U, Habermann E.; ''Arrangement of disulfide bridges and positions of sulfhydryl groups in tetanus toxin.''; PubMed Europe PMC Scholia
  45. Simpson LL.; ''Identification of the major steps in botulinum toxin action.''; PubMed Europe PMC Scholia
  46. Schiavo G, Santucci A, Dasgupta BR, Mehta PP, Jontes J, Benfenati F, Wilson MC, Montecucco C.; ''Botulinum neurotoxins serotypes A and E cleave SNAP-25 at distinct COOH-terminal peptide bonds.''; PubMed Europe PMC Scholia
  47. Amatsu S, Sugawara Y, Matsumura T, Kitadokoro K, Fujinaga Y.; ''Crystal structure of Clostridium botulinum whole hemagglutinin reveals a huge triskelion-shaped molecular complex.''; PubMed Europe PMC Scholia
  48. Peng L, Berntsson RP, Tepp WH, Pitkin RM, Johnson EA, Stenmark P, Dong M.; ''Botulinum neurotoxin D-C uses synaptotagmin I and II as receptors, and human synaptotagmin II is not an effective receptor for type B, D-C and G toxins.''; PubMed Europe PMC Scholia
  49. Foran P, Shone CC, Dolly JO.; ''Differences in the protease activities of tetanus and botulinum B toxins revealed by the cleavage of vesicle-associated membrane protein and various sized fragments.''; PubMed Europe PMC Scholia
  50. Fujinaga Y, Sugawara Y, Matsumura T.; ''Uptake of botulinum neurotoxin in the intestine.''; PubMed Europe PMC Scholia
  51. Lalli G, Bohnert S, Deinhardt K, Verastegui C, Schiavo G.; ''The journey of tetanus and botulinum neurotoxins in neurons.''; PubMed Europe PMC Scholia
  52. Rummel A, Häfner K, Mahrhold S, Darashchonak N, Holt M, Jahn R, Beermann S, Karnath T, Bigalke H, Binz T.; ''Botulinum neurotoxins C, E and F bind gangliosides via a conserved binding site prior to stimulation-dependent uptake with botulinum neurotoxin F utilising the three isoforms of SV2 as second receptor.''; PubMed Europe PMC Scholia
  53. Schiavo G, Benfenati F, Poulain B, Rossetto O, Polverino de Laureto P, DasGupta BR, Montecucco C.; ''Tetanus and botulinum-B neurotoxins block neurotransmitter release by proteolytic cleavage of synaptobrevin.''; PubMed Europe PMC Scholia
  54. Fu Z, Chen C, Barbieri JT, Kim JJ, Baldwin MR.; ''Glycosylated SV2 and gangliosides as dual receptors for botulinum neurotoxin serotype F.''; PubMed Europe PMC Scholia
  55. Yamasaki S, Binz T, Hayashi T, Szabo E, Yamasaki N, Eklund M, Jahn R, Niemann H.; ''Botulinum neurotoxin type G proteolyses the Ala81-Ala82 bond of rat synaptobrevin 2.''; PubMed Europe PMC Scholia

History

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114691view16:16, 25 January 2021ReactomeTeamReactome version 75
113137view11:20, 2 November 2020ReactomeTeamReactome version 74
112368view15:30, 9 October 2020ReactomeTeamReactome version 73
101270view11:16, 1 November 2018ReactomeTeamreactome version 66
100808view20:44, 31 October 2018ReactomeTeamreactome version 65
100349view19:21, 31 October 2018ReactomeTeamreactome version 64
99894view16:04, 31 October 2018ReactomeTeamreactome version 63
99451view14:38, 31 October 2018ReactomeTeamreactome version 62 (2nd attempt)
99115view12:40, 31 October 2018ReactomeTeamreactome version 62
93784view13:36, 16 August 2017ReactomeTeamreactome version 61
93317view11:20, 9 August 2017ReactomeTeamreactome version 61
87757view09:56, 25 July 2016RyanmillerOntology Term : 'disease pathway' added !
87755view09:56, 25 July 2016RyanmillerOntology Term : 'infectious disease pathway' added !
87752view09:53, 25 July 2016RyanmillerOntology Term : 'bacterial infectious disease' added !
86402view09:17, 11 July 2016ReactomeTeamreactome version 56
83321view10:46, 18 November 2015ReactomeTeamVersion54
81748view09:47, 26 August 2015ReactomeTeamVersion53
76848view08:07, 17 July 2014ReactomeTeamFixed remaining interactions
76552view11:53, 16 July 2014ReactomeTeamFixed remaining interactions
75885view09:54, 11 June 2014ReactomeTeamRe-fixing comment source
75585view10:42, 10 June 2014ReactomeTeamReactome 48 Update
74940view13:46, 8 May 2014AnweshaFixing comment source for displaying WikiPathways description
74584view08:37, 30 April 2014ReactomeTeamNew pathway

External references

DataNodes

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NameTypeDatabase referenceComment
BoNT/G HC disulfide bonded ProteinQ60393 (Uniprot-TrEMBL)
BoNT/G HCProteinQ60393 (Uniprot-TrEMBL)
BoNT/G LC ProteinQ60393 (Uniprot-TrEMBL)
BoNT/G LC disulfide bonded ProteinQ60393 (Uniprot-TrEMBL)
GD2 MetaboliteCHEBI:28648 (ChEBI)
GD2MetaboliteCHEBI:28648 (ChEBI)
GD3 MetaboliteCHEBI:28424 (ChEBI)
GD3MetaboliteCHEBI:28424 (ChEBI)
GM1a MetaboliteCHEBI:18216 (ChEBI)
GM1aMetaboliteCHEBI:18216 (ChEBI)
GT1b MetaboliteCHEBI:60913 (ChEBI)
GT1bMetaboliteCHEBI:60913 (ChEBI)
H+MetaboliteCHEBI:15378 (ChEBI)
NTNHA ProteinQ9LBS8 (Uniprot-TrEMBL)
NTNHAProteinQ9LBS8 (Uniprot-TrEMBL)
SNAP25(1-197)ProteinP60880 (Uniprot-TrEMBL)
SNAP25(1-198)ProteinP60880 (Uniprot-TrEMBL)
SNAP25(198-206)ProteinP60880 (Uniprot-TrEMBL)
SNAP25(199-206)ProteinP60880 (Uniprot-TrEMBL)
SNAP25ProteinP60880 (Uniprot-TrEMBL)
STX1(1-?)ComplexR-HSA-5250515 (Reactome)
STX1(?-288)ComplexR-HSA-5250513 (Reactome)
STX1A ProteinQ16623 (Uniprot-TrEMBL)
STX1A(1-?) ProteinQ16623 (Uniprot-TrEMBL)
STX1A(?-288) ProteinQ16623 (Uniprot-TrEMBL)
STX1B ProteinP61266 (Uniprot-TrEMBL)
STX1B(1-?) ProteinP61266 (Uniprot-TrEMBL)
STX1B(?-288) ProteinP61266 (Uniprot-TrEMBL)
STX1ComplexR-HSA-5250514 (Reactome)
SV2A ProteinQ7L0J3 (Uniprot-TrEMBL)
SV2A,B,CComplexR-HSA-5324682 (Reactome)
SV2A,B,CComplexR-HSA-5324684 (Reactome)
SV2A,BComplexR-HSA-5324689 (Reactome)
SV2A,BComplexR-HSA-5324690 (Reactome)
SV2B ProteinQ7L1I2 (Uniprot-TrEMBL)
SV2C ProteinQ496J9 (Uniprot-TrEMBL)
SYT1 ProteinP21579 (Uniprot-TrEMBL)
SYT1,2ComplexR-HSA-5324683 (Reactome)
SYT1,2ComplexR-HSA-5324686 (Reactome)
SYT1ProteinP21579 (Uniprot-TrEMBL)
SYT2 ProteinQ8N9I0 (Uniprot-TrEMBL)
TeNT HC disulfide bonded ProteinP04958 (Uniprot-TrEMBL)
TeNT LC ProteinP04958 (Uniprot-TrEMBL)
TeNT LC disulfide bonded ProteinP04958 (Uniprot-TrEMBL)
VAMP1(1-60)ProteinP23763 (Uniprot-TrEMBL)
VAMP1(1-61)ProteinP23763 (Uniprot-TrEMBL)
VAMP1(1-83)ProteinP23763 (Uniprot-TrEMBL)
VAMP1(61-118)ProteinP23763 (Uniprot-TrEMBL)
VAMP1(62-118)ProteinP23763 (Uniprot-TrEMBL)
VAMP1(84-118)ProteinP23763 (Uniprot-TrEMBL)
VAMP1ProteinP23763 (Uniprot-TrEMBL)
VAMP2(2-58)ProteinP63027 (Uniprot-TrEMBL)
VAMP2(2-59)ProteinP63027 (Uniprot-TrEMBL)
VAMP2(2-76)ProteinP63027 (Uniprot-TrEMBL)
VAMP2(2-81)ProteinP63027 (Uniprot-TrEMBL)
VAMP2(59-116)ProteinP63027 (Uniprot-TrEMBL)
VAMP2(60-116)ProteinP63027 (Uniprot-TrEMBL)
VAMP2(77-116)ProteinP63027 (Uniprot-TrEMBL)
VAMP2(82-116)ProteinP63027 (Uniprot-TrEMBL)
VAMP2ProteinP63027 (Uniprot-TrEMBL)
Zn2+ MetaboliteCHEBI:29105 (ChEBI)
botA HC disulfide bonded ProteinP0DPI0 (Uniprot-TrEMBL)
botA HC:LC dimer:NTNHA:HAComplexR-CBO-5228604 (Reactome)
botA HC:LC dimer:SV2:GT1bComplexR-HSA-5244411 (Reactome)
botA HC:LC dimer:SV2:GT1bComplexR-HSA-5244507 (Reactome)
botA HC:LC dimerComplexR-CBO-5228590 (Reactome)
botA HCProteinP0DPI0 (Uniprot-TrEMBL)
botA LC ProteinP0DPI0 (Uniprot-TrEMBL)
botA LC disulfide bonded ProteinP0DPI0 (Uniprot-TrEMBL)
botA LC:Zn2+ComplexR-CBO-190017 (Reactome)
botB HC disulfide bonded ProteinP10844 (Uniprot-TrEMBL)
botB HC:LC dimer:NTNHA:HAComplexR-CBO-5228681 (Reactome)
botB HC:LC dimer:SYT:GT1bComplexR-HSA-5244408 (Reactome)
botB HC:LC dimerComplexR-CBO-5228599 (Reactome)
botB HC:LC:SYT:GT1bComplexR-HSA-5244502 (Reactome)
botB HCProteinP10844 (Uniprot-TrEMBL)
botB LC ProteinP10844 (Uniprot-TrEMBL)
botB LC disulfide bonded ProteinP10844 (Uniprot-TrEMBL)
botB LC:Zn2+ComplexR-CBO-190016 (Reactome)
botC HC disulfide bonded ProteinP18640 (Uniprot-TrEMBL)
botC HC:LC dimerComplexR-CBO-5246516 (Reactome)
botC HCProteinP18640 (Uniprot-TrEMBL)
botC LC ProteinP18640 (Uniprot-TrEMBL)
botC LC disulfide bonded ProteinP18640 (Uniprot-TrEMBL)
botC LC:Zn2+ComplexR-CBO-190018 (Reactome)
botC:GT1bComplexR-CBO-5246508 (Reactome)
botC:GT1bComplexR-CBO-5246513 (Reactome)
botD HC disulfide bonded ProteinP19321 (Uniprot-TrEMBL)
botD HC:LC dimerComplexR-CBO-5250523 (Reactome)
botD HCProteinP19321 (Uniprot-TrEMBL)
botD LC ProteinP19321 (Uniprot-TrEMBL)
botD LC disulfide bonded ProteinP19321 (Uniprot-TrEMBL)
botD LC:Zn2+ComplexR-CBO-190038 (Reactome)
botD:SV2:GD2ComplexR-HSA-5250603 (Reactome)
botD:SV2:GD2ComplexR-HSA-5250612 (Reactome)
botE HC disulfide bonded ProteinQ00496 (Uniprot-TrEMBL)
botE HC:LC dimer:NTNHAComplexR-CBO-5228688 (Reactome)
botE HC:LC dimerComplexR-CBO-5228686 (Reactome)
botE HCProteinQ00496 (Uniprot-TrEMBL)
botE LC ProteinQ00496 (Uniprot-TrEMBL)
botE LC disulfide bonded ProteinQ00496 (Uniprot-TrEMBL)
botE LC:Zn2+ComplexR-CBO-190047 (Reactome)
botE:SV2:GT1bComplexR-HSA-5244509 (Reactome)
botE:SV2:GT1bComplexR-HSA-5244512 (Reactome)
botF HC disulfide bonded ProteinP30996 (Uniprot-TrEMBL)
botF HC:LC dimerComplexR-CBO-5250693 (Reactome)
botF HCProteinP30996 (Uniprot-TrEMBL)
botF LC ProteinP30996 (Uniprot-TrEMBL)
botF LC disulfide bonded ProteinP30996 (Uniprot-TrEMBL)
botF LC:Zn2+ComplexR-CBO-190042 (Reactome)
botF:SV2:GT1bComplexR-HSA-5250879 (Reactome)
botF:SV2:GT1bComplexR-HSA-5250883 (Reactome)
botG HC:LC dimerComplexR-CBO-5250691 (Reactome)
botG LC:Zn2+ComplexR-CBO-190032 (Reactome)
botG:SYT1:GT1bComplexR-HSA-5250975 (Reactome)
botG:SYT1:GT1bComplexR-HSA-5250976 (Reactome)
ha17 ProteinQ45878 (Uniprot-TrEMBL)
ha17ProteinQ45878 (Uniprot-TrEMBL)
ha33 ProteinQ57230 (Uniprot-TrEMBL)
ha33ProteinQ57230 (Uniprot-TrEMBL)
ha70 ProteinQ45877 (Uniprot-TrEMBL)
ha70ProteinQ45877 (Uniprot-TrEMBL)
tetX HC:LC dimerComplexR-CTE-5228372 (Reactome)
tetX HCProteinP04958 (Uniprot-TrEMBL)
tetX LC:Zn2+ComplexR-CTE-5228371 (Reactome)
tetX:gangliosidesComplexR-CTE-5228368 (Reactome)
tetX:gangliosidesComplexR-CTE-5228374 (Reactome)
tetX:gangliosidesComplexR-CTE-5228403 (Reactome)

Annotated Interactions

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SourceTargetTypeDatabase referenceComment
BoNT/G HCArrowR-HSA-5250972 (Reactome)
GD2ArrowR-HSA-5250616 (Reactome)
GD2R-HSA-5250607 (Reactome)
GD3ArrowR-HSA-5228406 (Reactome)
GD3R-HSA-5228407 (Reactome)
GM1aArrowR-HSA-5228406 (Reactome)
GM1aR-HSA-5228407 (Reactome)
GT1bArrowR-HSA-5244404 (Reactome)
GT1bArrowR-HSA-5244428 (Reactome)
GT1bArrowR-HSA-5244506 (Reactome)
GT1bArrowR-HSA-5246514 (Reactome)
GT1bArrowR-HSA-5250884 (Reactome)
GT1bArrowR-HSA-5250972 (Reactome)
GT1bR-HSA-5244397 (Reactome)
GT1bR-HSA-5244415 (Reactome)
GT1bR-HSA-5244503 (Reactome)
GT1bR-HSA-5246506 (Reactome)
GT1bR-HSA-5250880 (Reactome)
GT1bR-HSA-5250986 (Reactome)
H+ArrowR-HSA-5228406 (Reactome)
H+ArrowR-HSA-5244404 (Reactome)
H+ArrowR-HSA-5244428 (Reactome)
H+ArrowR-HSA-5244506 (Reactome)
H+ArrowR-HSA-5246514 (Reactome)
H+ArrowR-HSA-5250616 (Reactome)
H+ArrowR-HSA-5250884 (Reactome)
H+ArrowR-HSA-5250972 (Reactome)
NTNHAArrowR-HSA-5228940 (Reactome)
NTNHAArrowR-HSA-5228941 (Reactome)
NTNHAArrowR-HSA-5228943 (Reactome)
R-HSA-181567 (Reactome) Botulinum toxin type C light chain (botC LC), in the cytosol of a target cell, catalyzes the removal of an aminoterminal peptide from syntaxin 1 (STX1). botC LC is a zinc metalloprotease (Blasi et al. 1993; Foran et al. 1994). STX1 is associated with the cytosolic face of the target cell plasma membrane where it forms part of a complex required for synaptic vesicle docking and exocytosis. Its cleavage by botulinum toxin blocks synaptic vesicle fusion with the plasma membrane and neurotransmitter release (Sudhof et al, 1993; Sudhof 2004).
R-HSA-194793 (Reactome) Botulinum toxin type C light chain (botC LC), in the cytosol of a target cell, catalyzes the removal of a carboxyterminal peptide from synaptosomal associated protein 25 (SNAP25). botC LC is a zinc metalloprotease (Foran et al. 1994; Vaidyanathan et al. 1999). SNAP25 is associated with the cytosolic face of the target cell plasma membrane where it forms part of a complex required for synaptic vesicle docking and exocytosis. Its cleavage by botulinum toxin blocks synaptic vesicle fusion with the plasma membrane and neurotransmitter release (Sudhof et al, 1993; Sudhof 2004).
R-HSA-194796 (Reactome) Botulinum toxin type B light chain (botB LC), in the cytosol of a target cell, catalyzes the removal of an aminoterminal peptide from vesicle-associated membrane protein 2 (VAMP2). botB LC is a zinc metalloprotease (Foran et al. 1994; Schiavo et al. 1992). VAMP2 is associated with the cytosolic face of the target cell synaptic vesicle and is required for vesicle docking and exocytosis. Its cleavage by botulinum toxin blocks synaptic vesicle fusion with the plasma membrane and neurotransmitter release and in vivo leads to a long lasting flaccid paralysis (Sudhof et al, 1993; Sudhof 2004).
R-HSA-194800 (Reactome) Botulinum toxin type E light chain (botE LC), in the cytosol of a target cell, catalyzes the removal of a carboxyterminal peptide from synaptosomal-associated protein 25 (SNAP25). botE LC is a zinc metalloprotease (Binz et al. 1994; Schiavo et al. 1993; Vaidyanathan et al. 1999). SNAP25 is associated with the cytosolic face of the target cell plasma membrane where it forms part of a complex required for synaptic vesicle docking and exocytosis. Its cleavage by botulinum toxin blocks synaptic vesicle fusion with the plasma membrane and neurotransmitter release and in vivo leads to a long lasting flaccid paralysis (Sudhof et al, 1993; Sudhof 2004).
R-HSA-194808 (Reactome) Botulinum toxin type F light chain (botF LC), in the cytosol of a target cell, catalyzes the removal of an aminoterminal peptide from vesicle-associated membrane protein 1 (VAMP1). botF LC is a zinc metalloprotease (Yamasaki et al. 1994). VAMP1 is associated with the cytosolic face of the target cell synaptic vesicle and is required for vesicle docking and exocytosis. Its cleavage by botulinum toxin blocks synaptic vesicle fusion with the plasma membrane and neurotransmitter release (Sudhof et al, 1993; Sudhof 2004).
R-HSA-194809 (Reactome) Botulinum toxin type D light chain (botD LC), in the cytosol of a target cell, catalyzes the removal of an aminoterminal peptide from vesicle-associated membrane protein 1 (VAMP1). botD LC is a zinc metalloprotease (Arndt et al. 2006; Schiavo et al. 1993; Yamasaki et al. 1994). VAMP1 is associated with the cytosolic face of the target cell synaptic vesicle and is required for vesicle docking and exocytosis. Its cleavage by botulinum toxin blocks synaptic vesicle fusion with the plasma membrane and neurotransmitter release (Sudhof et al, 1993; Sudhof 2004).
R-HSA-194818 (Reactome) Botulinum toxin type A light chain (botA LC), in the cytosol of a target cell, catalyzes the removal of a carboxyterminal peptide from synaptosomal-associated protein 25 (SNAP25). botA LC is a zinc metalloprotease (Binz et al. 1994; Schiavo et al. 1993). SNAP25 is associated with the cytosolic face of the target cell plasma membrane where it forms part of a complex required for synaptic vesicle docking and exocytosis. Its cleavage by botulinum toxin blocks synaptic vesicle fusion with the plasma membrane and neurotransmitter release and in vivo leads to a long lasting flaccid paralysis (Sudhof et al, 1993; Sudhof 2004).
R-HSA-5228406 (Reactome) Acidification of the vesicle containing tetanus toxin disulfide-bonded heavy chain - light chain dimer (tetX HC:LC) is inferred to cause a conformational change in the toxin dimer, allowing the HC part of the toxin to function as a channel through which its LC part is extruded into the neuronal cytosol (Montal 2010).
R-HSA-5228407 (Reactome) Tetanus toxin disulfide-bonded heavy chain - light chain dimer (tetX HC:LC) binds gangliosides on the plasma membrane of a human target cell (Chen et al. 2009; Deinhardt et al. 2006).
R-HSA-5228408 (Reactome) Vesicles containing ganglioside-bound tetanus toxin disulfide-bonded heavy chain - light chain dimer (tetX HC:LC) are transported in a retrograde fashion away from the target cell synapse where they were formed into the cell body (Lalli et al. 2003).
R-HSA-5228411 (Reactome) Ganglioside-bound tetanus toxin disulfide-bonded heavy chain - light chain dimer (tetX HC:LC) is taken up into the target cell by clathrin-mediated endocytosis (Deinhardt et al. 2006).
R-HSA-5228578 (Reactome) Tetanus toxin light chain (tetX LC), in the cytosol of a target cell, catalyzes the removal of an aminoterminal peptide from vesicle-associated membrane protein 2 (VAMP2). tetX LC is a zinc metalloprotease (Foran et al. 1994; Schiavo et al. 1992). VAMP2 is associated with the cytosolic face of the target cell synaptic vesicle and is required for vesicle docking and exocytosis. Its cleavage by botulinum toxin blocks exocytosis and in vivo leads to a long-lasting spastic paralysis (Link et al. 1992).
R-HSA-5228940 (Reactome) The bacterial botB:NTNHA:HA (BoNT/B:NTNHA:HA) complex,, consisting of a Botulinum toxin type B (botB) disulfide bonded heavy chain (HC) - light chain (LC) dimer associated with nontoxic nonhemagglutinin protein (NTNHA), three molecules of hemagglutinin (ha) 17, six of ha33, and three of ha70 (Amatsu et al. 2013), associates with the plasma membrane of a human cell (in vivo, the apical surface of a gut epithelial cell) and undergoes transcytosis. While the molecular details of transcytosis remain to be established definitively, the process enables the toxin heterodimer to cross the epithelial cell layer and enter the circulation (Fujinaga et al. 2013; Simpson 2004).
R-HSA-5228941 (Reactome) The bacterial botE:NTNHA complex, consisting of a Botulinum toxin type E (botE, also known as BoNT/E) disulfide bonded heavy chain (HC) - light chain (LC) heterodimer (“dichain�) associated with nontoxic nonhemagglutinin protein (NTNHA) (Benefield et al. 2013), associates with the plasma membrane of a human cell (in vivo, the apical surface of a gut epithelial cell) and undergoes transcytosis. While the molecular details of transcytosis remain to be established definitively, the process enables the toxin heterodimer to cross the epithelial cell layer and enter the circulation (Fujinaga et al. 2013; Simpson 2004).
R-HSA-5228943 (Reactome) The bacterial botA:NTNHA:HA (BoNT/A:NTNHA:HA) complex, consisting of a Botulinum toxin type A (botA) disulfide bonded heavy chain (HC) - light chain (LC) heterodimer ("dichain") associated with nontoxic nonhemagglutinin protein (NTNHA), three molecules of hemagglutinin (ha) 17, six of ha33, and three of ha70 (Lee et al. 2013), associates with the plasma membrane of a human cell (in vivo, the apical surface of a gut epithelial cell) and undergoes transcytosis. While the molecular details of transcytosis remain to be established definitively, the process enables the toxin heterodimer to cross the epithelial cell layer and enter the circulation (Fujinaga et al. 2013; Simpson 2004).
R-HSA-5244397 (Reactome) The Botulinum toxin type B disulfide-bonded heavy chain - light chain dimer (botB HC:LC, encoded by the C. botulinum botB gene) (Swaminathan & Eswaramoorthy 2000) binds ganglioside GT1b and syntagmin 1 or 2 (SYT1 or 2) on the plasma membrane of a human target cell. In vivo, this process specifically targets synapses at neuromuscular junctions, where toxin association with ganglioside may position it to bind efficiently to SYT1 or 2 when those proteins are exposed at the cell surface by exocytosis (Dong et al. 2003). In vitro, botB HC:LC can bind gangliosides in addition to GT1b but with lower affinity (Kozaki et al. 1998). Only GT1b binding is annotated here.
R-HSA-5244402 (Reactome) Synaptic vesicles re-form rapidly after exocytosis, carrying vesicle membrane proteins that had been exposed on the cell surface by exocytosis back into the cell (Sudhoff 2004). The botulinum toxin type B disulfide bonded heavy chain - light chain heterodimer (botB HC:LC dimer) bound to ganglioside GT1b and syntagmin 1 or 2 (SYT) is inferred to be taken up as well, delivering it to the re-formed synaptic vesicle.
R-HSA-5244404 (Reactome) By analogy to the process described for botulinum toxin type A (Koriazova and Montal 2003; Montal 2010), acidification, a normal step in synaptic vesicle recycling, is inferred to cause a conformational change in the botulinum toxin type B disulfide bonded heavy chain - light chain dimer (botB HC:LC) it contains, allowing the HC part of the toxin to function as a channel through which its LC part is extruded into the neuronal cytosol. The HC - LC disulfide bond is cleaved. Recent studies in vitro suggest that GT1b ganglioside associated with the toxin may play a role in this process (Sun et al. 2011, 2012).
R-HSA-5244415 (Reactome) The Botulinum toxin type A disulfide bonded heavy chain - light chain heterodimer (botA HC:LC, encoded by the C. botulinum botA gene) (Lacy et al. 1998) binds ganglioside GT1b and synaptic vesicle protein 2A (SV2A) on the plasma membrane of a human target cell. In vivo, this process specifically targets synapses at neuromuscular junctions, where toxin association with ganglioside may position it to bind efficiently to SV2A, SV2B, or SV2C when those proteins are exposed at the cell surface by exocytosis (Dong et al. 2006). In vitro, botA HC:LC can bind gangliosides in addition to GT1b but with lower affinity (Kozaki et al. 1998). Only GT1b binding is annotated here.
R-HSA-5244424 (Reactome) Synaptic vesicles re-form rapidly after exocytosis, carrying vesicle membrane proteins that had been exposed on the cell surface by exocytosis back into the cell (Sudhoff 2004). The botulinum toxin type A disulfide bonded heavy chain - light chain heterodimer (“dichain�) (botA HC:LC) bound to ganglioside GT1b and synaptic vesicle protein 2A, 2B, or 2C (SV2A, B, or C) is inferred to be taken up as well, delivering it to the re-formed synaptic vesicle.
R-HSA-5244428 (Reactome) Acidification, a normal step in endocytosis causes a conformational change in the botulinum toxin type A disulfide bonded heavy chain - light chain heterodimer (“dichain�) (botA HC:LC) it contains, allowing the HC part of the toxin to function as a channel through which its LC part is extruded into the neuronal cytosol. The HC - LC disulfide bond is cleaved (Koriazova & Montal 2003; Montal 2010). Recent studies in vitro suggest that GT1b ganglioside associated with the toxin may play a role in this process (Sun et al. 2012).
R-HSA-5244500 (Reactome) Synaptic vesicles re-form rapidly after exocytosis, carrying vesicle membrane proteins that had been exposed on the cell surface by exocytosis back into the cell (Sudhoff 2004). The botulinum toxin type E disulfide bonded heavy chain - light chain heterodimer (botE HC:LC) bound to ganglioside GT1b and synaptic vesicle protein 2A (SV2A) or 2B (SV2B) is inferred to be taken up as well, delivering it to the re-formed synaptic vesicle.
R-HSA-5244503 (Reactome) The Botulinum toxin type E disulfide bonded heavy chain - light chain heterodimer (botE HC:LC, encoded by the C. botulinum botE gene) (Kumaran et al. 2009) binds ganglioside GT1b and synaptic vesicle protein 2A (SV2A) or 2B (SV2B) on the plasma membrane of a human target cell. In vivo, this process specifically targets synapses at neuromuscular junctions, where toxin association with ganglioside may position it to bind efficiently to SV2A or B when those proteins are exposed at the cell surface by exocytosis (Dong et al. 2008; Rummel et al. 2009).
R-HSA-5244506 (Reactome) By analogy to the process described for botulinum toxin type A (Koriazova and Montal 2003; Montal 2010), acidification, a normal step in synaptic vesicle recycling, is inferred to cause a conformational change in the botulinum toxin type E disulfide bonded heavy chain - light chain dimer (botE HC:LC) it contains, allowing the HC part of the toxin to function as a channel through which its LC part is extruded into the neuronal cytosol. The HC - LC disulfide bond is cleaved. Recent studies in vitro suggest that GT1b ganglioside associated with the toxin may play a role in this process (Sun et al. 2012).
R-HSA-5246506 (Reactome) The botulinum toxin type C disulfide-bonded heavy chain - light chain heterodimer (“dichain�) (botC HC:LC, encoded by the C. botulinum botC1 gene) binds two molecules of GT1b ganglioside on the plasma membrane of a human target cell (Karalewitz et al. 2012).
R-HSA-5246509 (Reactome) Synaptic vesicles re-form rapidly after exocytosis, carrying vesicle membrane proteins that had been exposed on the cell surface by exocytosis back into the cell (Sudhoff 2004). The botulinum toxin type C disulfide-bonded heavy chain - light chain heterodimer (botC HC:LC) bound to ganglioside GT1b is inferred to be taken up as well, delivering it to the re-formed synaptic vesicle.
R-HSA-5246514 (Reactome) By analogy to the process described for botulinum toxin type A (Koriazova and Montal 2003; Montal 2010), acidification, a normal step in synaptic vesicle recycling, is inferred to cause a conformational change in the botulinum toxin type C disulfide-bonded heavy chain - light chain dimer (botC HC:LC) it contains, allowing the HC part of the toxin to function as a channel through which its LC part is extruded into the neuronal cytosol. The HC - LC disulfide bond is cleaved. Recent studies in vitro suggest that GT1b ganglioside associated with the toxin may play a role in this process (Sun et al. 2012).
R-HSA-5250600 (Reactome) Synaptic vesicles re-form rapidly after exocytosis, carrying vesicle membrane proteins that had been exposed on the cell surface by exocytosis back into the cell (Sudhoff 2004). The botulinum toxin type D disulfide-bonded heavy chain - light chain heterodimer (botD HC:LC) bound to ganglioside GD2 and synaptic vesicle protein 2A, 2B, or 2C (SV2A, B, or C) is inferred to be taken up as well, delivering it to the re-formed synaptic vesicle.
R-HSA-5250606 (Reactome) Botulinum toxin type D light chain (botD LC), in the cytosol of a target cell, catalyzes the removal of an aminoterminal peptide from vesicle-associated membrane protein 2 (VAMP2). botD LC is a zinc metalloprotease (Arndt et al. 2006; Schiavo et al. 1993; Yamasaki et al. 1994). VAMP2 is associated with the cytosolic face of the target cell synaptic vesicle and is required for vesicle docking and exocytosis. Its cleavage by botulinum toxin blocks synaptic vesicle fusion with the plasma membrane and neurotransmitter release (Sudhof et al, 1993; Sudhof 2004).
R-HSA-5250607 (Reactome) The botulinum toxin type D disulfide-bonded heavy chain - light chain heterodimer ("dichain") (botD HC:LC, encoded by the C. botulinum botD gene) binds ganglioside GD2 and synaptic vesicle proteins 2A (SV2A), 2B (SV2B), or 2C (SV2C) on the plasma membrane of a human target cell. In vivo, this process specifically targets synapses at neuromuscular junctions, where toxin association with ganglioside may position it to bind efficiently to SV2A, SV2B, or SV2C when those proteins are exposed at the cell surface by exocytosis (Kroken et al. 2011; Peng et al. 2011).
R-HSA-5250616 (Reactome) By analogy to the process described for botulinum toxin type A (Koriazova and Montal 2003; Montal 2010), acidification, a normal step in synaptic vesicle recycling, is inferred to cause a conformational change in the botulinum toxin type D disulfide-bonded heavy chain - light chain dimer (botD HC:LC) it contains, allowing the HC part of the toxin to function as a channel through which its LC part is extruded into the neuronal cytosol where the HC - LC disulfide bond is cleaved.
R-HSA-5250875 (Reactome) Synaptic vesicles re-form rapidly after exocytosis, carrying vesicle membrane proteins that had been exposed on the cell surface by exocytosis back into the cell (Sudhoff 2004). The botulinum toxin type F disulfide-bonded heavy chain - light chain heterodimer ("dichain") (botF HC:LC) bound to ganglioside GT1b and synaptic vesicle protein 2A (SV2A), 2B (SV2B), or 2C (SV2C) is inferred to be taken up as well, delivering it to the re-formed synaptic vesicle.
R-HSA-5250880 (Reactome) The botulinum toxin type F disulfide-bonded heavy chain - light chain heterodimer ("dichain") (botF HC:LC, encoded by the C. botulinum botF gene) binds ganglioside GT1b and synaptic vesicle protein 2A (SV2A), B (SV2B), or C (SV2C) on the plasma membrane of a human target cell. In vivo, this process specifically targets synapses at neuromuscular junctions, where toxin association with ganglioside may position it to bind efficiently to SV2A, B, or C when those proteins are exposed at the cell surface by exocytosis (Fu et al. 2009; Rummel et al. 2009).
R-HSA-5250884 (Reactome) By analogy to the process described for botulinum toxin type A (Koriazova and Montal 2003; Montal 2010), acidification, a normal step in synaptic vesicle recycling, is inferred to cause a conformational change in the botulinum toxin type F disulfide-bonded heavy chain - light chain heterodimer (botF HC:LC) it contains, allowing the HC part of the toxin to function as a channel through which its LC part is extruded into the neuronal cytosol.The HC - LC disulfide bond is cleaved. Recent studies in vitro suggest that GT1b ganglioside associated with the toxin may play a role in this process (Sun et al. 2012).
R-HSA-5250892 (Reactome) Botulinum toxin type F light chain (botF LC), in the cytosol of a target cell, catalyzes the removal of an aminoterminal peptide from vesicle-associated membrane protein 2 (VAMP2). botF LC is a zinc metalloprotease (Yamasaki et al. 1994). VAMP2 is associated with the cytosolic face of the target cell synaptic vesicle and is required for vesicle docking and exocytosis. Its cleavage by botulinum toxin blocks synaptic vesicle fusion with the plasma membrane and neurotransmitter release (Sudhof et al, 1993; Sudhof 2004).
R-HSA-5250962 (Reactome) Botulinum toxin type G light chain (botG LC), in the cytosol of a target cell, catalyzes the removal of an aminoterminal peptide from vesicle-associated membrane protein 2 (VAMP2). botG LC is a zinc metalloprotease (Schiavo et al. 1994; Yamasaki et al. 1994). VAMP2 is associated with the cytosolic face of the target cell synaptic vesicle and is required for vesicle docking and exocytosis. Its cleavage by botulinum toxin blocks synaptic vesicle fusion with the plasma membrane and neurotransmitter release (Sudhof et al, 1993; Sudhof 2004).
R-HSA-5250972 (Reactome) By analogy to the process described for botulinum toxin type A (Koriazova and Montal 2003; Montal 2010), acidification, a normal step in synaptic vesicle recycling, is inferred to cause a conformational change in the botulinum toxin type G disulfide-bonded heavy chain - light chain dimer (BoNT/G HC:LC) it contains, allowing the HC part of the toxin to function as a channel through which its LC part is extruded into the neuronal cytosol. The HC - LC disulfide bond is cleaved. Recent studies in vitro suggest that GT1b ganglioside associated with the toxin may play a role in this process (Sun et al. 2012).
R-HSA-5250978 (Reactome) Botulinum toxin type G light chain (botG LC), in the cytosol of a target cell, catalyzes the removal of an aminoterminal peptide from vesicle-associated membrane protein 1 (VAMP1). botG LC is a zinc metalloprotease (Schiavo et al. 1994; Yamasaki et al. 1994). VAMP1 is associated with the cytosolic face of the target cell synaptic vesicle and is required for vesicle docking and exocytosis.Its cleavage by botulinum toxin blocks synaptic vesicle fusion with the plasma membrane and neurotransmitter release (Sudhof et al, 1993; Sudhof 2004).
R-HSA-5250979 (Reactome) Synaptic vesicles re-form rapidly after exocytosis, carrying vesicle membrane proteins that had been exposed on the cell surface by exocytosis back into the cell (Sudhoff 2004). The botulinum toxin type G disulfide-bonded heavy chain - light chain heterodimer (botG HC:LC) bound to ganglioside GT1b and syntagmin 1 (SYT1) is inferred to be taken up as well, delivering it to the re-formed synaptic vesicle.
R-HSA-5250986 (Reactome) The botulinum toxin type G disulfide-bonded heavy chain - light chain heterodimer ("dichain") (botG HC:LC) binds ganglioside GT1b and synaptotagmin-1 (SYT1) on the plasma membrane of a human target cell. In vivo, this process specifically targets synapses at neuromuscular junctions, where toxin association with ganglioside may position it to bind efficiently to SYT1 when that protein is exposed at the cell surface by exocytosis (Peng et al. 2012; Willjes et al. 2013).
SNAP25(1-197)ArrowR-HSA-194818 (Reactome)
SNAP25(1-198)ArrowR-HSA-194793 (Reactome)
SNAP25(1-198)ArrowR-HSA-194800 (Reactome)
SNAP25(198-206)ArrowR-HSA-194818 (Reactome)
SNAP25(199-206)ArrowR-HSA-194793 (Reactome)
SNAP25(199-206)ArrowR-HSA-194800 (Reactome)
SNAP25R-HSA-194793 (Reactome)
SNAP25R-HSA-194800 (Reactome)
SNAP25R-HSA-194818 (Reactome)
STX1(1-?)ArrowR-HSA-181567 (Reactome)
STX1(?-288)ArrowR-HSA-181567 (Reactome)
STX1R-HSA-181567 (Reactome)
SV2A,B,CArrowR-HSA-5244428 (Reactome)
SV2A,B,CArrowR-HSA-5250616 (Reactome)
SV2A,B,CArrowR-HSA-5250884 (Reactome)
SV2A,B,CR-HSA-5244415 (Reactome)
SV2A,B,CR-HSA-5250607 (Reactome)
SV2A,B,CR-HSA-5250880 (Reactome)
SV2A,BArrowR-HSA-5244506 (Reactome)
SV2A,BR-HSA-5244503 (Reactome)
SYT1,2ArrowR-HSA-5244404 (Reactome)
SYT1,2R-HSA-5244397 (Reactome)
SYT1ArrowR-HSA-5250972 (Reactome)
SYT1R-HSA-5250986 (Reactome)
VAMP1(1-60)ArrowR-HSA-194808 (Reactome)
VAMP1(1-61)ArrowR-HSA-194809 (Reactome)
VAMP1(1-83)ArrowR-HSA-5250978 (Reactome)
VAMP1(61-118)ArrowR-HSA-194808 (Reactome)
VAMP1(62-118)ArrowR-HSA-194809 (Reactome)
VAMP1(84-118)ArrowR-HSA-5250978 (Reactome)
VAMP1R-HSA-194808 (Reactome)
VAMP1R-HSA-194809 (Reactome)
VAMP1R-HSA-5250978 (Reactome)
VAMP2(2-58)ArrowR-HSA-5250892 (Reactome)
VAMP2(2-59)ArrowR-HSA-5250606 (Reactome)
VAMP2(2-76)ArrowR-HSA-194796 (Reactome)
VAMP2(2-76)ArrowR-HSA-5228578 (Reactome)
VAMP2(2-81)ArrowR-HSA-5250962 (Reactome)
VAMP2(59-116)ArrowR-HSA-5250892 (Reactome)
VAMP2(60-116)ArrowR-HSA-5250606 (Reactome)
VAMP2(77-116)ArrowR-HSA-194796 (Reactome)
VAMP2(77-116)ArrowR-HSA-5228578 (Reactome)
VAMP2(82-116)ArrowR-HSA-5250962 (Reactome)
VAMP2R-HSA-194796 (Reactome)
VAMP2R-HSA-5228578 (Reactome)
VAMP2R-HSA-5250606 (Reactome)
VAMP2R-HSA-5250892 (Reactome)
VAMP2R-HSA-5250962 (Reactome)
botA HC:LC dimer:NTNHA:HAR-HSA-5228943 (Reactome)
botA HC:LC dimer:SV2:GT1bArrowR-HSA-5244415 (Reactome)
botA HC:LC dimer:SV2:GT1bArrowR-HSA-5244424 (Reactome)
botA HC:LC dimer:SV2:GT1bR-HSA-5244424 (Reactome)
botA HC:LC dimer:SV2:GT1bR-HSA-5244428 (Reactome)
botA HC:LC dimer:SV2:GT1bmim-catalysisR-HSA-5244428 (Reactome)
botA HC:LC dimerArrowR-HSA-5228943 (Reactome)
botA HC:LC dimerR-HSA-5244415 (Reactome)
botA HCArrowR-HSA-5244428 (Reactome)
botA LC:Zn2+ArrowR-HSA-5244428 (Reactome)
botA LC:Zn2+mim-catalysisR-HSA-194818 (Reactome)
botB HC:LC dimer:NTNHA:HAR-HSA-5228940 (Reactome)
botB HC:LC dimer:SYT:GT1bArrowR-HSA-5244397 (Reactome)
botB HC:LC dimer:SYT:GT1bR-HSA-5244402 (Reactome)
botB HC:LC dimerArrowR-HSA-5228940 (Reactome)
botB HC:LC dimerR-HSA-5244397 (Reactome)
botB HC:LC:SYT:GT1bArrowR-HSA-5244402 (Reactome)
botB HC:LC:SYT:GT1bR-HSA-5244404 (Reactome)
botB HC:LC:SYT:GT1bmim-catalysisR-HSA-5244404 (Reactome)
botB HCArrowR-HSA-5244404 (Reactome)
botB LC:Zn2+ArrowR-HSA-5244404 (Reactome)
botB LC:Zn2+mim-catalysisR-HSA-194796 (Reactome)
botC HC:LC dimerR-HSA-5246506 (Reactome)
botC HCArrowR-HSA-5246514 (Reactome)
botC LC:Zn2+ArrowR-HSA-5246514 (Reactome)
botC LC:Zn2+mim-catalysisR-HSA-181567 (Reactome)
botC LC:Zn2+mim-catalysisR-HSA-194793 (Reactome)
botC:GT1bArrowR-HSA-5246506 (Reactome)
botC:GT1bArrowR-HSA-5246509 (Reactome)
botC:GT1bR-HSA-5246509 (Reactome)
botC:GT1bR-HSA-5246514 (Reactome)
botC:GT1bmim-catalysisR-HSA-5246514 (Reactome)
botD HC:LC dimerR-HSA-5250607 (Reactome)
botD HCArrowR-HSA-5250616 (Reactome)
botD LC:Zn2+ArrowR-HSA-5250616 (Reactome)
botD LC:Zn2+mim-catalysisR-HSA-194809 (Reactome)
botD LC:Zn2+mim-catalysisR-HSA-5250606 (Reactome)
botD:SV2:GD2ArrowR-HSA-5250600 (Reactome)
botD:SV2:GD2ArrowR-HSA-5250607 (Reactome)
botD:SV2:GD2R-HSA-5250600 (Reactome)
botD:SV2:GD2R-HSA-5250616 (Reactome)
botD:SV2:GD2mim-catalysisR-HSA-5250616 (Reactome)
botE HC:LC dimer:NTNHAR-HSA-5228941 (Reactome)
botE HC:LC dimerArrowR-HSA-5228941 (Reactome)
botE HC:LC dimerR-HSA-5244503 (Reactome)
botE HCArrowR-HSA-5244506 (Reactome)
botE LC:Zn2+ArrowR-HSA-5244506 (Reactome)
botE LC:Zn2+mim-catalysisR-HSA-194800 (Reactome)
botE:SV2:GT1bArrowR-HSA-5244500 (Reactome)
botE:SV2:GT1bArrowR-HSA-5244503 (Reactome)
botE:SV2:GT1bR-HSA-5244500 (Reactome)
botE:SV2:GT1bR-HSA-5244506 (Reactome)
botE:SV2:GT1bmim-catalysisR-HSA-5244506 (Reactome)
botF HC:LC dimerR-HSA-5250880 (Reactome)
botF HCArrowR-HSA-5250884 (Reactome)
botF LC:Zn2+ArrowR-HSA-5250884 (Reactome)
botF LC:Zn2+mim-catalysisR-HSA-194808 (Reactome)
botF LC:Zn2+mim-catalysisR-HSA-5250892 (Reactome)
botF:SV2:GT1bArrowR-HSA-5250875 (Reactome)
botF:SV2:GT1bArrowR-HSA-5250880 (Reactome)
botF:SV2:GT1bR-HSA-5250875 (Reactome)
botF:SV2:GT1bR-HSA-5250884 (Reactome)
botF:SV2:GT1bmim-catalysisR-HSA-5250884 (Reactome)
botG HC:LC dimerR-HSA-5250986 (Reactome)
botG LC:Zn2+ArrowR-HSA-5250972 (Reactome)
botG LC:Zn2+mim-catalysisR-HSA-5250962 (Reactome)
botG LC:Zn2+mim-catalysisR-HSA-5250978 (Reactome)
botG:SYT1:GT1bArrowR-HSA-5250979 (Reactome)
botG:SYT1:GT1bArrowR-HSA-5250986 (Reactome)
botG:SYT1:GT1bR-HSA-5250972 (Reactome)
botG:SYT1:GT1bR-HSA-5250979 (Reactome)
botG:SYT1:GT1bmim-catalysisR-HSA-5250972 (Reactome)
ha17ArrowR-HSA-5228940 (Reactome)
ha17ArrowR-HSA-5228943 (Reactome)
ha33ArrowR-HSA-5228940 (Reactome)
ha33ArrowR-HSA-5228943 (Reactome)
ha70ArrowR-HSA-5228940 (Reactome)
ha70ArrowR-HSA-5228943 (Reactome)
tetX HC:LC dimerR-HSA-5228407 (Reactome)
tetX HCArrowR-HSA-5228406 (Reactome)
tetX LC:Zn2+ArrowR-HSA-5228406 (Reactome)
tetX LC:Zn2+mim-catalysisR-HSA-5228578 (Reactome)
tetX:gangliosidesArrowR-HSA-5228407 (Reactome)
tetX:gangliosidesArrowR-HSA-5228408 (Reactome)
tetX:gangliosidesArrowR-HSA-5228411 (Reactome)
tetX:gangliosidesR-HSA-5228406 (Reactome)
tetX:gangliosidesR-HSA-5228408 (Reactome)
tetX:gangliosidesR-HSA-5228411 (Reactome)
tetX:gangliosidesmim-catalysisR-HSA-5228406 (Reactome)

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