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Apamin

March 12, 2024

Apamin is an 18 amino acid globular peptide neurotoxin found in apitoxin (bee venom).[2] Dry bee venom consists of 2–3% of apamin.[3] Apamin selectively blocks SK channels, a type of Ca2+-activated K+ channel expressed in the central nervous system. Toxicity is caused by only a few amino acids, in particular cysteine1, lysine4, arginine13, arginine14 and histidine18. These amino acids are involved in the binding of apamin to the Ca2+-activated K+ channel. Due to its specificity for SK channels, apamin is used as a drug in biomedical research to study the electrical properties of SK channels and their role in the afterhyperpolarizations occurring immediately following an action potential.[4]

Apamin[1]
Identifiers
  • 24345-16-2 Y
3D model (JSmol)
  • Interactive image
ChEMBL
  • ChEMBL525408 N
ChemSpider
  • 23975893 Y
ECHA InfoCard 100.041.969
  • 2311
  • 16129677
UNII
  • X644P85KUR Y
  • DTXSID70897227
  • InChI=1S/C79H131N31O24S4/c1-35(2)26-49-70(127)107-51-31-136-135-30-41(81)63(120)105-50(28-57(84)114)71(128)108-53(73(130)99-42(12-7-8-22-80)64(121)96-38(5)77(134)110-25-11-15-54(110)75(132)102-47(18-21-58(115)116)69(126)109-59(39(6)111)76(133)95-37(4)62(119)104-49)33-138-137-32-52(106-66(123)44(14-10-24-92-79(88)89)98-65(122)43(13-9-23-91-78(86)87)97-61(118)36(3)94-72(51)129)74(131)101-45(16-19-55(82)112)67(124)100-46(17-20-56(83)113)68(125)103-48(60(85)117)27-40-29-90-34-93-40/h29,34-39,41-54,59,111H,7-28,30-33,80-81H2,1-6H3,(H2,82,112)(H2,83,113)(H2,84,114)(H2,85,117)(H,90,93)(H,94,129)(H,95,133)(H,96,121)(H,97,118)(H,98,122)(H,99,130)(H,100,124)(H,101,131)(H,102,132)(H,103,125)(H,104,119)(H,105,120)(H,106,123)(H,107,127)(H,108,128)(H,109,126)(H,115,116)(H4,86,87,91)(H4,88,89,92)/t36?,37-,38-,39+,41-,42-,43-,44?,45-,46-,47-,48-,49-,50-,51-,52-,53-,54-,59?/m0/s1 Y
    Key: YVIIHEKJCKCXOB-WNKOHBQLSA-N Y
  • InChI=1S/C79H131N31O24S4/c1-35(2)26-49-70(127)107-51-31-136-135-30-41(81)63(120)105-50(28-57(84)114)71(128)108-53(73(130)99-42(12-7-8-22-80)64(121)96-38(5)77(134)110-25-11-15-54(110)75(132)102-47(18-21-58(115)116)69(126)109-59(39(6)111)76(133)95-37(4)62(119)104-49)33-138-137-32-52(106-66(123)44(14-10-24-92-79(88)89)98-65(122)43(13-9-23-91-78(86)87)97-61(118)36(3)94-72(51)129)74(131)101-45(16-19-55(82)112)67(124)100-46(17-20-56(83)113)68(125)103-48(60(85)117)27-40-29-90-34-93-40/h29,34-39,41-54,59,111H,7-28,30-33,80-81H2,1-6H3,(H2,82,112)(H2,83,113)(H2,84,114)(H2,85,117)(H,90,93)(H,94,129)(H,95,133)(H,96,121)(H,97,118)(H,98,122)(H,99,130)(H,100,124)(H,101,131)(H,102,132)(H,103,125)(H,104,119)(H,105,120)(H,106,123)(H,107,127)(H,108,128)(H,109,126)(H,115,116)(H4,86,87,91)(H4,88,89,92)/t36?,37-,38-,39+,41-,42-,43-,44?,45-,46-,47-,48-,49-,50-,51-,52-,53-,54-,59?/m0/s1
  • Key: YVIIHEKJCKCXOB-WNKOHBQLSA-N
  • C[C@H]1C(=O)N[C@H](C(=O)N[C@H](C(=O)N[C@@H](CSSC[C@H]2C(=O)N[C@H](C(=O)N[C@H](C(=O)N3CCC[C@H]3C(=O)N[C@H](C(=O)NC(C(=O)N[C@H](C(=O)N[C@H](C(=O)N[C@@H](CSSC[C@@H](C(=O)N[C@H](C(=O)N2)CC(=O)N)N)C(=O)N1)CC(C)C)C)[C@@H](C)O)CCC(=O)O)C)CCCCN)C(=O)N[C@@H](CCC(=O)N)C(=O)N[C@@H](CCC(=O)N)C(=O)N[C@@H](Cc4cnc[nH]4)C(=O)N)CCCNC(=N)N)CCCNC(=N)N
Properties
C79H131N31O24S4
Molar mass 2027.33874 g/mol
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).
N verify (what is YN ?)
Apamin Preproprotein
Identifiers
SymbolApamin
CAS number24345-16-2
NCBI gene406135
UniProtP01500
Search for
StructuresSwiss-model
DomainsInterPro

Origin edit

The first symptoms of apitoxin (bee venom), that are now thought to be caused by apamin, were described back in 1936 by Hahn and Leditschke. Apamin was first isolated by Habermann in 1965 from Apis mellifera, the Western honey bee. Apamin was named after this bee. Bee venom contains many other compounds, like histamine, phospholipase A2, hyaluronidase, MCD peptide, and the main active component melittin. Apamin was separated from the other compounds by gel filtration and ion exchange chromatography.[2]

Structure and active site edit

Apamin is a polypeptide possessing an amino acid sequence of H-Cys-Asn-Cys-Lys-Ala-Pro-Glu-Thr-Ala-Leu-Cys-Ala-Arg-Arg-Cys-Gln-Gln-His-NH2 (one-letter sequence CNCKAPETALCARRCQQH-NH2, with disulfide bonds between Cys1-Cys11 and Cys3-Cys15). Apamin is very rigid because of the two disulfide bridges and seven hydrogen bonds. The three-dimensional structure of apamin has been studied with several spectroscopical techniques: HNMR, Circular Dichroism, Raman spectroscopy, FT-IR. The structure is presumed to consist of an alpha-helix and beta-turns, but the exact structure is still unknown.[5]

By local alterations it is possible to find the amino acids that are involved in toxicity of apamin. It was found by Vincent et al. that guanidination of the ε-amino group of lysine4 does not decrease toxicity. When the ε-amino group of lysine4 and the α-amino group of cysteine1 are acetylated or treated with fluorescamine, toxicity decreases with a factor of respectively 2.5 and 2.8. This is only a small decrease, which indicates that neither the ε-amino group of lysine4 nor the α-amino group of cysteine1 is essential for the toxicity of apamin. Glutamine7 was altered by formation of an amide bond with glycine ethyl ester, this resulted in a decrease in toxicity of a factor 2.0. Glutamine7 also doesn't appear to be essential for toxicity. When histidine18 is altered by carbethoxylation, toxicity decreases only by a factor 2.6. But when histidine18, the ε-amino group of lysine4 and the α-amino group of cysteine1 all are carbethoxylated and acetylated toxicity decreases drastically. This means that these three amino acids are not essential for toxicity on their own, but the three of them combined are. Chemical alteration of arginine13 and arginine14 by treatment of 1,2-cyclohexanedione and cleavage by trypsin decreases toxicity by a factor greater than 10. The amino acids that cause toxicity of apamin are cysteine1, lysine4, arginine13, arginine14 and histidine18.[6]

Toxicodynamics edit

Apamin is the smallest neurotoxin polypeptide known, and the only one that passes the blood-brain barrier.[6] Apamin thus reaches its target organ, the central nervous system. Here it inhibits small-conductance Ca2+-activated K+ channels (SK channels) in neurons. These channels are responsible for the afterhyperpolarizations that follow action potentials, and therefore regulate the repetitive firing frequency.[7] Three different types of SK channels show different characteristics. Only SK2 and SK3 are blocked by apamin, whereas SK1 is apamin insensitive. SK channels function as a tetramer of subunits. Heteromers have intermediate sensitivity.[7] SK channels are activated by the binding of intracellular Ca2+ to the protein calmodulin, which is constitutively associated to the channel.[8] Transport of potassium ions out of the cell along their concentration gradient causes the membrane potential to become more negative. The SK channels are present in a wide range of excitable and non-excitable cells, including cells in the central nervous system, intestinal myocytes, endothelial cells, and hepatocytes.

Binding of apamin to SK channels is mediated by amino acids in the pore region as well as extracellular amino acids of the SK channel.[9] It is likely that the inhibition of SK channels is caused by blocking of the pore region, which hinders the transport of potassium ions. This will increase the neuronal excitability and lower the threshold for generating an action potential. Other toxins that block SK channels are tamapin and scyllatoxin.

Toxicokinetics edit

The kinetics of labeled derivatives of apamin were studied in vitro and in vivo in mice by Cheng-Raude et al. This shed some light on the kinetics of apamin itself. The key organ for excretion is likely to be the kidney, since enrichment of the labeled derivatives was found there. The peptide apamin is small enough to pass the glomerular barrier, facilitating renal excretion. The central nervous system, contrarily, was found to contain only very small amounts of apamin. This is unexpected, as this is the target organ for neurotoxicity caused by apamin. This low concentration thus appeared to be sufficient to cause the toxic effects.[10]

However, these results disagree with a study of Vincent et al. After injection of a supralethal dose of radioactive acetylated apamin in mice, enrichment was found in the spinal cord, which is part of the target organ. Some other organs, including kidney and brain, contained only small amounts of the apamin derivative.[6]

Symptoms edit

Symptoms following bee sting may include:

Patients poisoned with bee venom can be treated with anti-inflammatory medication, antihistamines and oral prednisolone.[11]

Apamin is an element in bee venom. You can come into contact with apamin through bee venom, so the symptoms that are known are not caused by apamin directly, but by the venom as a whole. Apamin is the only neurotoxin acting purely on the central nervous system. The symptoms of apamin toxicity are not well known, because people are not easily exposed to the toxin alone.[12]

Through research about the neurotoxicity of apamin some symptoms were discovered. In mice, the injection of apamin produces convulsions and long-lasting spinal spasticity. Also, it is known that the polysynaptic spinal reflexes are disinhibited in cats.[12] Polysynaptic reflex is a reflex action that transfers an impulse from a sensory neuron to a motor neuron via an interneuron in the spinal cord.[13] In rats, apamin was found to cause tremor and ataxia, as well as dramatic haemorrhagic effects in the lungs.[14]

Furthermore, apamin has been found to be 1000 times more efficient when applied into the ventricular system instead of the peripheral nervous system. The ventricular system is a set of structures in the brain containing cerebrospinal fluid. The peripheral nervous system contains the nerves and ganglia outside of the brain and spinal cord.[12] This difference in efficiency can easily be explained. Apamin binds to the SK channels, which differ slightly in different tissues. So apamin binding is probably stronger in SK channels in the ventricular system than in other tissues.

Toxicity rates edit

In earlier years it was thought that apamin was a rather nontoxic compound (LD50 = 15 mg/kg in mice) compared to the other compounds in bee venom.[15] The current lethal dose values of apamin measured in mice are given below.[16] There are no data known specific for humans.

Intraperitoneal (mouse) LD50: 3.8 mg/kg

Subcutaneous (mouse) LD50: 2.9 mg/kg

Intravenous (mouse) LD50: 4 mg/kg

Intracerebral (mouse) LD50: 1800 ng/kg

Parenteral (mouse) LD50: 600 mg/kg

Therapeutic use edit

Recent studies have shown that SK channels do not only regulate afterhyperpolarization, they also have an effect on synaptic plasticity. This is the activity-dependent adaptation of the strength of synaptic transmission. Synaptic plasticity is an important mechanism underlying learning and memory processes. Apamin is expected to influence these processes by inhibiting SK channels. It has been shown that apamin enhances learning and memory in rats and mice.[7][17] This may provide a basis for the use of apamin as a treatment for memory disorders and cognitive dysfunction. However, due to the risk of toxic effects, the therapeutic window is very narrow.[17]

SK channel blockers may have a therapeutic effect on Parkinson's disease. Dopamine, which is depleted in this disease, will be released from midbrain dopaminergic neurons when these SK channels are inhibited. SK channels have also been proposed as targets for the treatment of epilepsy, emotional disorders and schizophrenia.[17]

References edit

  1. ^ Apamin - Compound Summary, PubChem.
  2. ^ a b Habermann E (1984). "Apamin". Pharmacology & Therapeutics. 25 (2): 255–70. doi:10.1016/0163-7258(84)90046-9. PMID 6095335.
  3. ^ Son DJ, Lee JW, Lee YH, Song HS, Lee CK, Hong JT (Aug 2007). "Therapeutic application of anti-arthritis, pain-releasing, and anti-cancer effects of bee venom and its constituent compounds". Pharmacology & Therapeutics. 115 (2): 246–70. doi:10.1016/j.pharmthera.2007.04.004. PMID 17555825.
  4. ^ Castle NA, Haylett DG, Jenkinson DH (Feb 1989). "Toxins in the characterization of potassium channels". Trends in Neurosciences. 12 (2): 59–65. doi:10.1016/0166-2236(89)90137-9. PMID 2469212. S2CID 22356085.
  5. ^ Kastin AJ. "Apamin". Handbook of Biologically Active Peptides (2013 ed.): 417–418.
  6. ^ a b c Vincent JP, Schweitz H, Lazdunski M (Jun 1975). "Structure-function relationships and site of action of apamin, a neurotoxic polypeptide of bee venom with an action on the central nervous system". Biochemistry. 14 (11): 2521–5. doi:10.1021/bi00682a035. PMID 1138869.
  7. ^ a b c M. Stocker; M. Krause; P. Pedarzani (1999). "An apamin-sentisitive Ca2+-activated K+ current in hippocampal pyramidal neurons". PNAS. 96 (8): 4662–4667. Bibcode:1999PNAS...96.4662S. doi:10.1073/pnas.96.8.4662. PMC 16389. PMID 10200319.
  8. ^ Stocker M (Oct 2004). "Ca(2+)-activated K+ channels: molecular determinants and function of the SK family". Nature Reviews. Neuroscience. 5 (10): 758–70. doi:10.1038/nrn1516. PMID 15378036. S2CID 22211829.
  9. ^ Nolting A, Ferraro T, D'hoedt D, Stocker M (Feb 2007). "An amino acid outside the pore region influences apamin sensitivity in small conductance Ca2+-activated K+ channels". The Journal of Biological Chemistry. 282 (6): 3478–86. doi:10.1074/jbc.M607213200. PMC 1849974. PMID 17142458.
  10. ^ Cheng-Raude D, Treloar M, Habermann E (1976). "Preparation and pharmacokinetics of labeled derivatives of apamin". Toxicon. 14 (6): 467–76. doi:10.1016/0041-0101(76)90064-7. PMID 1014036.
  11. ^ a b Saravanan R, King R, White J (Apr 2004). "Transient claw hand owing to a bee sting. A report of two cases". The Journal of Bone and Joint Surgery. British Volume. 86 (3): 404–5. doi:10.1302/0301-620x.86b3.14311. PMID 15125129.
  12. ^ a b c Habermann E (Nov 1977). "Neurotoxicity of apamin and MCD peptide upon central application". Naunyn-Schmiedeberg's Archives of Pharmacology. 300 (2): 189–91. doi:10.1007/bf00505050. PMID 593441. S2CID 11709787.
  13. ^ "polysynaptic reflex".
  14. ^ Lallement G, Fosbraey P, Baille-Le-Crom V, Tattersall JE, Blanchet G, Wetherell JR, Rice P, Passingham SL, Sentenac-Roumanou H (Dec 1995). "Compared toxicity of the potassium channel blockers, apamin and dendrotoxin". Toxicology. 104 (1–3): 47–52. doi:10.1016/0300-483X(95)03120-5. PMID 8560501.
  15. ^ department of the army Edgewood Arsenal biodemical laboratory (1972). . Archived from the original on April 9, 2013. {{cite journal}}: Cite journal requires |journal= (help)
  16. ^ "Apamin" (PDF). Material Safety Data Sheet.
  17. ^ a b c Faber ES, Sah P (Oct 2007). "Functions of SK channels in central neurons". Clinical and Experimental Pharmacology & Physiology. 34 (10): 1077–83. doi:10.1111/j.1440-1681.2007.04725.x. PMID 17714097. S2CID 5553791.

External links edit

March 12, 2024
apamin, amino, acid, globular, peptide, neurotoxin, found, apitoxin, venom, venom, consists, apamin, selectively, blocks, channels, type, activated, channel, expressed, central, nervous, system, toxicity, caused, only, amino, acids, particular, cysteine1, lysi. Apamin is an 18 amino acid globular peptide neurotoxin found in apitoxin bee venom 2 Dry bee venom consists of 2 3 of apamin 3 Apamin selectively blocks SK channels a type of Ca2 activated K channel expressed in the central nervous system Toxicity is caused by only a few amino acids in particular cysteine1 lysine4 arginine13 arginine14 and histidine18 These amino acids are involved in the binding of apamin to the Ca2 activated K channel Due to its specificity for SK channels apamin is used as a drug in biomedical research to study the electrical properties of SK channels and their role in the afterhyperpolarizations occurring immediately following an action potential 4 Apamin 1 IdentifiersCAS Number 24345 16 2 Y3D model JSmol Interactive imageChEMBL ChEMBL525408 NChemSpider 23975893 YECHA InfoCard 100 041 969IUPHAR BPS 2311PubChem CID 16129677UNII X644P85KUR YCompTox Dashboard EPA DTXSID70897227InChI InChI 1S C79H131N31O24S4 c1 35 2 26 49 70 127 107 51 31 136 135 30 41 81 63 120 105 50 28 57 84 114 71 128 108 53 73 130 99 42 12 7 8 22 80 64 121 96 38 5 77 134 110 25 11 15 54 110 75 132 102 47 18 21 58 115 116 69 126 109 59 39 6 111 76 133 95 37 4 62 119 104 49 33 138 137 32 52 106 66 123 44 14 10 24 92 79 88 89 98 65 122 43 13 9 23 91 78 86 87 97 61 118 36 3 94 72 51 129 74 131 101 45 16 19 55 82 112 67 124 100 46 17 20 56 83 113 68 125 103 48 60 85 117 27 40 29 90 34 93 40 h29 34 39 41 54 59 111H 7 28 30 33 80 81H2 1 6H3 H2 82 112 H2 83 113 H2 84 114 H2 85 117 H 90 93 H 94 129 H 95 133 H 96 121 H 97 118 H 98 122 H 99 130 H 100 124 H 101 131 H 102 132 H 103 125 H 104 119 H 105 120 H 106 123 H 107 127 H 108 128 H 109 126 H 115 116 H4 86 87 91 H4 88 89 92 t36 37 38 39 41 42 43 44 45 46 47 48 49 50 51 52 53 54 59 m0 s1 YKey YVIIHEKJCKCXOB WNKOHBQLSA N YInChI 1S C79H131N31O24S4 c1 35 2 26 49 70 127 107 51 31 136 135 30 41 81 63 120 105 50 28 57 84 114 71 128 108 53 73 130 99 42 12 7 8 22 80 64 121 96 38 5 77 134 110 25 11 15 54 110 75 132 102 47 18 21 58 115 116 69 126 109 59 39 6 111 76 133 95 37 4 62 119 104 49 33 138 137 32 52 106 66 123 44 14 10 24 92 79 88 89 98 65 122 43 13 9 23 91 78 86 87 97 61 118 36 3 94 72 51 129 74 131 101 45 16 19 55 82 112 67 124 100 46 17 20 56 83 113 68 125 103 48 60 85 117 27 40 29 90 34 93 40 h29 34 39 41 54 59 111H 7 28 30 33 80 81H2 1 6H3 H2 82 112 H2 83 113 H2 84 114 H2 85 117 H 90 93 H 94 129 H 95 133 H 96 121 H 97 118 H 98 122 H 99 130 H 100 124 H 101 131 H 102 132 H 103 125 H 104 119 H 105 120 H 106 123 H 107 127 H 108 128 H 109 126 H 115 116 H4 86 87 91 H4 88 89 92 t36 37 38 39 41 42 43 44 45 46 47 48 49 50 51 52 53 54 59 m0 s1Key YVIIHEKJCKCXOB WNKOHBQLSA NSMILES C C H 1C O N C H C O N C H C O N C H CSSC C H 2C O N C H C O N C H C O N3CCC C H 3C O N C H C O NC C O N C H C O N C H C O N C H CSSC C H C O N C H C O N2 CC O N N C O N1 CC C C C C H C O CCC O O C CCCCN C O N C H CCC O N C O N C H CCC O N C O N C H Cc4cnc nH 4 C O N CCCNC N N CCCNC N NPropertiesChemical formula C79H131N31O24S4Molar mass 2027 33874 g molExcept where otherwise noted data are given for materials in their standard state at 25 C 77 F 100 kPa N verify what is Y N Infobox references Apamin PreproproteinIdentifiersSymbolApaminCAS number24345 16 2NCBI gene406135UniProtP01500Search forStructuresSwiss modelDomainsInterPro Contents 1 Origin 2 Structure and active site 3 Toxicodynamics 4 Toxicokinetics 5 Symptoms 6 Toxicity rates 7 Therapeutic use 8 References 9 External linksOrigin editThe first symptoms of apitoxin bee venom that are now thought to be caused by apamin were described back in 1936 by Hahn and Leditschke Apamin was first isolated by Habermann in 1965 from Apis mellifera the Western honey bee Apamin was named after this bee Bee venom contains many other compounds like histamine phospholipase A2 hyaluronidase MCD peptide and the main active component melittin Apamin was separated from the other compounds by gel filtration and ion exchange chromatography 2 Structure and active site editApamin is a polypeptide possessing an amino acid sequence of H Cys Asn Cys Lys Ala Pro Glu Thr Ala Leu Cys Ala Arg Arg Cys Gln Gln His NH2 one letter sequence CNCKAPETALCARRCQQH NH2 with disulfide bonds between Cys1 Cys11 and Cys3 Cys15 Apamin is very rigid because of the two disulfide bridges and seven hydrogen bonds The three dimensional structure of apamin has been studied with several spectroscopical techniques HNMR Circular Dichroism Raman spectroscopy FT IR The structure is presumed to consist of an alpha helix and beta turns but the exact structure is still unknown 5 By local alterations it is possible to find the amino acids that are involved in toxicity of apamin It was found by Vincent et al that guanidination of the e amino group of lysine4 does not decrease toxicity When the e amino group of lysine4 and the a amino group of cysteine1 are acetylated or treated with fluorescamine toxicity decreases with a factor of respectively 2 5 and 2 8 This is only a small decrease which indicates that neither the e amino group of lysine4 nor the a amino group of cysteine1 is essential for the toxicity of apamin Glutamine7 was altered by formation of an amide bond with glycine ethyl ester this resulted in a decrease in toxicity of a factor 2 0 Glutamine7 also doesn t appear to be essential for toxicity When histidine18 is altered by carbethoxylation toxicity decreases only by a factor 2 6 But when histidine18 the e amino group of lysine4 and the a amino group of cysteine1 all are carbethoxylated and acetylated toxicity decreases drastically This means that these three amino acids are not essential for toxicity on their own but the three of them combined are Chemical alteration of arginine13 and arginine14 by treatment of 1 2 cyclohexanedione and cleavage by trypsin decreases toxicity by a factor greater than 10 The amino acids that cause toxicity of apamin are cysteine1 lysine4 arginine13 arginine14 and histidine18 6 Toxicodynamics editApamin is the smallest neurotoxin polypeptide known and the only one that passes the blood brain barrier 6 Apamin thus reaches its target organ the central nervous system Here it inhibits small conductance Ca2 activated K channels SK channels in neurons These channels are responsible for the afterhyperpolarizations that follow action potentials and therefore regulate the repetitive firing frequency 7 Three different types of SK channels show different characteristics Only SK2 and SK3 are blocked by apamin whereas SK1 is apamin insensitive SK channels function as a tetramer of subunits Heteromers have intermediate sensitivity 7 SK channels are activated by the binding of intracellular Ca2 to the protein calmodulin which is constitutively associated to the channel 8 Transport of potassium ions out of the cell along their concentration gradient causes the membrane potential to become more negative The SK channels are present in a wide range of excitable and non excitable cells including cells in the central nervous system intestinal myocytes endothelial cells and hepatocytes Binding of apamin to SK channels is mediated by amino acids in the pore region as well as extracellular amino acids of the SK channel 9 It is likely that the inhibition of SK channels is caused by blocking of the pore region which hinders the transport of potassium ions This will increase the neuronal excitability and lower the threshold for generating an action potential Other toxins that block SK channels are tamapin and scyllatoxin Toxicokinetics editThe kinetics of labeled derivatives of apamin were studied in vitro and in vivo in mice by Cheng Raude et al This shed some light on the kinetics of apamin itself The key organ for excretion is likely to be the kidney since enrichment of the labeled derivatives was found there The peptide apamin is small enough to pass the glomerular barrier facilitating renal excretion The central nervous system contrarily was found to contain only very small amounts of apamin This is unexpected as this is the target organ for neurotoxicity caused by apamin This low concentration thus appeared to be sufficient to cause the toxic effects 10 However these results disagree with a study of Vincent et al After injection of a supralethal dose of radioactive acetylated apamin in mice enrichment was found in the spinal cord which is part of the target organ Some other organs including kidney and brain contained only small amounts of the apamin derivative 6 Symptoms editSymptoms following bee sting may include Local effects burning or stinging pain swelling redness Severe systemic reactions swelling of the tongue and throat difficulty breathing and shock Development of optic neuritis and atrophy Atrial fibrillation cerebral infarction acute myocardial infarction Fisher s syndrome acute inflammatory polyradiculopathy Guillain Barre syndrome claw hand through a central action of apamin on the spinal cord and a peripheral action in the form of median and ulnar neuritis causing spasms of the long flexors in the forearm 11 Patients poisoned with bee venom can be treated with anti inflammatory medication antihistamines and oral prednisolone 11 Apamin is an element in bee venom You can come into contact with apamin through bee venom so the symptoms that are known are not caused by apamin directly but by the venom as a whole Apamin is the only neurotoxin acting purely on the central nervous system The symptoms of apamin toxicity are not well known because people are not easily exposed to the toxin alone 12 Through research about the neurotoxicity of apamin some symptoms were discovered In mice the injection of apamin produces convulsions and long lasting spinal spasticity Also it is known that the polysynaptic spinal reflexes are disinhibited in cats 12 Polysynaptic reflex is a reflex action that transfers an impulse from a sensory neuron to a motor neuron via an interneuron in the spinal cord 13 In rats apamin was found to cause tremor and ataxia as well as dramatic haemorrhagic effects in the lungs 14 Furthermore apamin has been found to be 1000 times more efficient when applied into the ventricular system instead of the peripheral nervous system The ventricular system is a set of structures in the brain containing cerebrospinal fluid The peripheral nervous system contains the nerves and ganglia outside of the brain and spinal cord 12 This difference in efficiency can easily be explained Apamin binds to the SK channels which differ slightly in different tissues So apamin binding is probably stronger in SK channels in the ventricular system than in other tissues Toxicity rates editIn earlier years it was thought that apamin was a rather nontoxic compound LD50 15 mg kg in mice compared to the other compounds in bee venom 15 The current lethal dose values of apamin measured in mice are given below 16 There are no data known specific for humans Intraperitoneal mouse LD50 3 8 mg kgSubcutaneous mouse LD50 2 9 mg kgIntravenous mouse LD50 4 mg kgIntracerebral mouse LD50 1800 ng kgParenteral mouse LD50 600 mg kgTherapeutic use editRecent studies have shown that SK channels do not only regulate afterhyperpolarization they also have an effect on synaptic plasticity This is the activity dependent adaptation of the strength of synaptic transmission Synaptic plasticity is an important mechanism underlying learning and memory processes Apamin is expected to influence these processes by inhibiting SK channels It has been shown that apamin enhances learning and memory in rats and mice 7 17 This may provide a basis for the use of apamin as a treatment for memory disorders and cognitive dysfunction However due to the risk of toxic effects the therapeutic window is very narrow 17 SK channel blockers may have a therapeutic effect on Parkinson s disease Dopamine which is depleted in this disease will be released from midbrain dopaminergic neurons when these SK channels are inhibited SK channels have also been proposed as targets for the treatment of epilepsy emotional disorders and schizophrenia 17 References edit Apamin Compound Summary PubChem a b Habermann E 1984 Apamin Pharmacology amp Therapeutics 25 2 255 70 doi 10 1016 0163 7258 84 90046 9 PMID 6095335 Son DJ Lee JW Lee YH Song HS Lee CK Hong JT Aug 2007 Therapeutic application of anti arthritis pain releasing and anti cancer effects of bee venom and its constituent compounds Pharmacology amp Therapeutics 115 2 246 70 doi 10 1016 j pharmthera 2007 04 004 PMID 17555825 Castle NA Haylett DG Jenkinson DH Feb 1989 Toxins in the characterization of potassium channels Trends in Neurosciences 12 2 59 65 doi 10 1016 0166 2236 89 90137 9 PMID 2469212 S2CID 22356085 Kastin AJ Apamin Handbook of Biologically Active Peptides 2013 ed 417 418 a b c Vincent JP Schweitz H Lazdunski M Jun 1975 Structure function relationships and site of action of apamin a neurotoxic polypeptide of bee venom with an action on the central nervous system Biochemistry 14 11 2521 5 doi 10 1021 bi00682a035 PMID 1138869 a b c M Stocker M Krause P Pedarzani 1999 An apamin sentisitive Ca2 activated K current in hippocampal pyramidal neurons PNAS 96 8 4662 4667 Bibcode 1999PNAS 96 4662S doi 10 1073 pnas 96 8 4662 PMC 16389 PMID 10200319 Stocker M Oct 2004 Ca 2 activated K channels molecular determinants and function of the SK family Nature Reviews Neuroscience 5 10 758 70 doi 10 1038 nrn1516 PMID 15378036 S2CID 22211829 Nolting A Ferraro T D hoedt D Stocker M Feb 2007 An amino acid outside the pore region influences apamin sensitivity in small conductance Ca2 activated K channels The Journal of Biological Chemistry 282 6 3478 86 doi 10 1074 jbc M607213200 PMC 1849974 PMID 17142458 Cheng Raude D Treloar M Habermann E 1976 Preparation and pharmacokinetics of labeled derivatives of apamin Toxicon 14 6 467 76 doi 10 1016 0041 0101 76 90064 7 PMID 1014036 a b Saravanan R King R White J Apr 2004 Transient claw hand owing to a bee sting A report of two cases The Journal of Bone and Joint Surgery British Volume 86 3 404 5 doi 10 1302 0301 620x 86b3 14311 PMID 15125129 a b c Habermann E Nov 1977 Neurotoxicity of apamin and MCD peptide upon central application Naunyn Schmiedeberg s Archives of Pharmacology 300 2 189 91 doi 10 1007 bf00505050 PMID 593441 S2CID 11709787 polysynaptic reflex Lallement G Fosbraey P Baille Le Crom V Tattersall JE Blanchet G Wetherell JR Rice P Passingham SL Sentenac Roumanou H Dec 1995 Compared toxicity of the potassium channel blockers apamin and dendrotoxin Toxicology 104 1 3 47 52 doi 10 1016 0300 483X 95 03120 5 PMID 8560501 department of the army Edgewood Arsenal biodemical laboratory 1972 Beta adrenergic and antiarrhythmic effect of apamin a component of bee venom Archived from the original on April 9 2013 a href Template Cite journal html title Template Cite journal cite journal a Cite journal requires journal help Apamin PDF Material Safety Data Sheet a b c Faber ES Sah P Oct 2007 Functions of SK channels in central neurons Clinical and Experimental Pharmacology amp Physiology 34 10 1077 83 doi 10 1111 j 1440 1681 2007 04725 x PMID 17714097 S2CID 5553791 External links editApamin at the U S National Library of Medicine Medical Subject Headings MeSH Retrieved from https en wikipedia org w index php title Apamin amp oldid 1187501057, wikipedia, wiki, book, books, library,

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