Calitoxin: Difference between revisions

Browse history interactively ← Previous editContent deleted Content addedVisual WikitextInline

Revision as of 03:08, 20 October 2014 editIceKarma (talk \| contribs)Autopatrolled, Administrators6,306 editsm →Structure and chemistry: ce← Previous edit		Latest revision as of 00:18, 23 December 2024 edit undoCitation bot (talk \| contribs)Bots5,439,690 edits Added bibcode. \| Use this bot. Report bugs. \| Suggested by Whoop whoop pull up \| Category:Ion channel toxins \| #UCB_Category 62/201
(58 intermediate revisions by 20 users not shown)
Line 1:		Line 1:
			{{Good article}}
	{{Chembox		{{Chembox
	\| ImageFile =		\| ImageFile =
	\| ImageSize =		\| ImageSize =
	\| ImageAlt =		\| ImageAlt =
	\| IUPACName =		\| IUPACName =
	\| OtherNames =		\| OtherNames =
	\| Section1 = {{Chembox Identifiers		\|Section1={{Chembox Identifiers
	\| CASNo = 118354-83-9		\| CASNo = 118354-83-9
	\| PubChem = <!-- SID = 135330181 -->		\| PubChem = <!-- SID = 135330181 -->
	\| SMILES =		\| SMILES =
	\| Abbreviations = CLX		\| Abbreviations = CLX
			\| ChemSpiderID = none
	}}		}}
	\| Section2 = {{Chembox Properties		\|Section2={{Chembox Properties
			\| Appearance =
	\| C=203\|H=305\|N=55\|O=72\|S=7
	\| ~~Appearance~~ =		\| Density =
	\| ~~Density~~ =		\| MeltingPt =
	\| ~~MeltingPt~~ =		\| BoilingPt =
	\| ~~BoilingPt~~ =		\| Solubility =
	\| Solubility =
	}}		}}
	\| Section3 = {{Chembox Hazards		\|Section3={{Chembox Hazards
	\| MainHazards =		\| MainHazards =
	\| FlashPt =		\| FlashPt =
	\| AutoignitionPt =		\| AutoignitionPt =
	}}		}}
	}}		}}

	{{Infobox nonhuman protein		{{Infobox nonhuman protein
	\| Name = Calitoxin		\| Name = Calitoxin-1
	\| image =		\| image =
	\| width =		\| width =
Line 33:		Line 34:
	\| Organism = ]		\| Organism = ]
	\| TaxID =		\| TaxID =
	\| Symbol = CLX		\| Symbol = CLX-1
	\| AltSymbols =		\| AltSymbols =
	\| EntrezGene =		\| EntrezGene =
Line 40:		Line 41:
	\| RefSeqProtein =		\| RefSeqProtein =
	\| UniProt = P14531		\| UniProt = P14531
			\| ECnumber =
			\| Chromosome =
			\| EntrezChromosome =
			\| GenLoc_start =
			\| GenLoc_end =
			}}
			{{Infobox nonhuman protein
			\| Name = Calitoxin-2
			\| image =
			\| width =
			\| caption =
			\| Organism = ]
			\| TaxID =
			\| Symbol = CLX-2
			\| AltSymbols =
			\| EntrezGene =
			\| PDB =
			\| RefSeqmRNA =
			\| RefSeqProtein =
			\| UniProt = P49127
	\| ECnumber =		\| ECnumber =
	\| Chromosome =		\| Chromosome =
Line 47:		Line 68:
	}}		}}
	{{Pfam_box		{{Pfam_box
	\| Symbol =		\| Symbol = Toxin_4
	\| Name =		\| Name =
	\| image =		\| image =
Line 62:		Line 83:
	}}		}}

			'''Calitoxin''', also known as '''CLX''', is a ] produced by the sea anemone '']''. It targets crabs and octopuses, among other invertebrates. Two ]s (CLX-1 and CLX-2) have been identified, both of which are formed from ] stored in the ]s of the anemone. Once the toxin is activated and released, it causes paralysis by increasing ] at invertebrate ]s. Along with several other toxins derived from anemones, CLX is useful in ] research. Certain structural aspects of calitoxin are dissimilar from sea anemone toxins that also target the ]s. Other toxins resembling calitoxin function in completely different ways.
	'''Calitoxin''', also known as '''CLX''', is a ] toxin which is likely to affect ] in invertebrates.<ref name="car">{{cite journal\|last1=Cariello\|first1=L\|last2=de Santis\|first2=A\|last3=Fiore\|first3=F\|last4=Piccoli\|first4=R\|last5=Spagnuolo\|first5=A\|last6=Zanetti\|first6=L\|last7=Parente\|first7=A\|title=Calitoxin, a neurotoxic peptide from the sea anemone Calliactis parasitica: amino acid sequence and electrophysiological properties.\|journal=Biochemistry\|date= 21 Mar 1989\|volume=28\|issue=6\|pages=2484–9\|pmid=2567180\|accessdate=13 October 2014}}</ref> Two different toxins, namely CLX-1 and CLX-2, can be distinguished.<ref name="spag">{{cite journal\|last1=Spagnuolo\|first1=Antonietta\|last2=Zanetti\|first2=Laura\|last3=Cariello\|first3=Lucio\|last4=Piccoli\|first4=Renata\|title=Isolation and characterization of two genes encoding calitoxins, neurotoxic peptides from Calliactis parasitica (Cnidaria)\|journal=Gene\|volume=138\|issue=1-2\|pages=187–191\|doi=10.1016/0378-1119(94)90805-2}}</ref> It targets invertebrates, among other crabs and octopuses.<ref name="car" />

	== ~~Etymology~~ ==		== Source and discovery ==
			Calitoxin is a highly potent ] produced by the sea anemone '']'', which is stored in the ] of stinging cells (]).<ref name="spag">{{cite journal \| vauthors = Spagnuolo A, Zanetti L, Cariello L, Piccoli R \| title = Isolation and characterization of two genes encoding calitoxins, neurotoxic peptides from Calliactis parasitica (Cnidaria) \| journal = Gene \| volume = 138 \| issue = 1–2 \| pages = 187–91 \| date = January 1994 \| pmid = 7510258 \| doi = 10.1016/0378-1119(94)90805-2 }}</ref> This sea anemone is a species from the ] family and is present along the European coasts of the Atlantic Ocean and in the Mediterranean Sea.<ref name="car">{{cite journal \| vauthors = Cariello L, de Santis A, Fiore F, Piccoli R, Spagnuolo A, Zanetti L, Parente A \| title = Calitoxin, a neurotoxic peptide from the sea anemone ''Calliactis parasitica'': amino acid sequence and electrophysiological properties \| journal = Biochemistry \| volume = 28 \| issue = 6 \| pages = 2484–9 \| date = March 1989 \| pmid = 2567180 \| doi = 10.1021/bi00432a020 }}</ref> The name calitoxin is derived from the organism from which the toxin was isolated. The toxin was isolated by a team of researchers in Naples, Italy from animals collected in the ]. The team isolated the polypeptide through a series of ]s until the ] had lost toxic activity. The resulting pellet was purified using the techniques ], ], and ].<ref name="RappuoliMontecucco1997">{{cite book\|last1=Rappuoli\|first1=Rino\|last2=Montecucco\|first2=Cesare \| name-list-style = vanc \|title=Guidebook to Protein Toxins and Their Use in Cell Biology\|url=https://books.google.com/books?id=ebTwSqbjmXwC&pg=PA139\|date=29 May 1997\|publisher=Oxford University Press, UK\|isbn=978-0-19-154728-7\|pages=139–}}</ref> The team then ] the purified polypeptide chain. They also published details on the toxin's effects '']'' on crustacean tissue preparations, including nerve and muscle. Their findings were published in the journal '']'' in 1989.<ref name="car" />
	''Calitoxin'' (CLX), derives its name from the sea anemone '']''.<ref name="car" />

	== Sources ==
	Calitoxin is a highly potent ], which can be found in the ], organelles in stinging cells, of the ''Calliactis parasitica''.<ref name="spag" /> This sea anemone is a species from the ] family and is present along the European coasts of the Atlantic Ocean and in the Mediterranean Sea.<ref name="car" />

	== Structure and chemistry ==		== Structure and chemistry ==
	~~The~~ ~~formula~~ ~~for~~ ~~calitoxin~~ is ~~C<sub>203~~</~~sub~~>~~H<sub>305</sub>N<sub>55</sub>O<sub>72</sub>S<sub>7</sub>.~~ The amino acid sequence is markedly dissimilar from other known sea anemones toxins. ~~Two~~ genes coding for two highly homologous calitoxins ~~are discovered and analyzed, namely~~ CLX-1 and CLX-2, ~~both~~ ~~consisting~~ ~~of 46 amino acids and originating~~ from a ] of 79 amino acids where the ] determines whether it will be the mature CLX-1 or CLX-2. In ~~the~~ ~~mature~~ ~~CLX,~~ ~~one~~ ~~base-pair~~ ~~substitution~~ is ~~responsible~~ ~~for~~ a ~~single~~ ~~Glu~~ to ~~Lys~~ ~~replacement~~ in the ~~coding~~ ~~region~~ of ~~CLX-2,~~ ~~leading~~ to ~~the~~ ~~difference~~ ~~between~~ the ~~two~~ ~~peptides.~~ ~~The~~ ~~structural~~ ~~organization~~ of ~~these~~ ~~two~~ ~~genes~~ ~~show~~ a ~~high~~ ~~degree~~ of ~~homology~~. ~~This~~ ~~might~~ ~~imply~~ ~~that~~ ~~the~~ ~~two~~ ~~different~~ ~~peptides~~ ~~have~~ the ~~same~~ ~~biological~~ ~~function.~~ ~~This~~ ~~cannot~~ ~~yet~~ be ~~confirmed~~ ~~because~~ ~~only~~ ~~CLX-1~~ ~~has been isolated from ''C.~~ ~~parasitica''~~.<ref name="~~spag~~" />		It has an ] at pH 5.4.<ref name="spag" /> The ] is markedly dissimilar from other known sea anemones toxins. There are two known genes coding for two highly ] calitoxins: CLX-1 and CLX-2. Both originate from a precursor peptide of 79 amino acids where the ] determines whether it will be the mature CLX-1 or CLX-2. The activated toxins consist of 46 amino acids with three ]s.<ref name=Kastin /> Researchers suspect that the toxins are stored as precursors in ]. Under the effects of some triggering stimulus, the precursor is modified and released in the active form. The patterning of cleavage sites targeted during maturation of the peptide suggest that the active ] might be a tetrapeptide.<ref name="RappuoliMontecucco1997" />
			{\| class="wikitable"
			\|+Amino acid sequences of CLX precursors
			!Isoform
			!Sequence
			!Disulfide bridge locations
			\|-
			\| CLX-1 precursor
			\| MKTQVLALFV LCVLFCLAES RTTLNKR'''N'''DI '''E'''KRIECKC'''E'''G DAPDLSHMTG TVYFSCKGGD GSWSKCNTYT AVADCCHQA
			\|{{ubl\|
			*36{{spaced ndash}} 75
			*38{{spaced ndash}} 66
			*56{{spaced ndash}} 76<ref>{{cite web\|title=Calitoxin-1\|url=https://www.uniprot.org/uniprot/P49127\|website=UniProt}}</ref>
			}}
			\|-
			\| CLX-2 precursor
			\| MKTQVLAVFV LCVLFCLAES RTTLNKR'''I'''DI '''A'''KRIECKC'''K'''G DAPDLSHMTG TVYFSCKGGD GSWSKCNTYT AVADCCHQA
			\|{{ubl\|
			*36{{spaced ndash}} 75
			*38{{spaced ndash}} 66
			*56{{spaced ndash}} 76<ref>{{cite web\|title=Calitoxin-2\|url=https://www.uniprot.org/uniprot/P14531\|website=UniProt}}</ref>
			}}
			\|}
			Calitoxin and other sea anemone toxins are used in studying ion channels, with potential applications in biomedical and physiology research.<ref name="Marine Drugs">{{cite journal\|last1=Nagai\|first1=Hiroshi \| name-list-style = vanc \|title=Special Issue "Sea Anemone Toxins"\|journal=Marine Drugs\|year=2012\|url=http://www.mdpi.com/journal/marinedrugs/special_issues/sea-anemone-toxins}}</ref><ref name="RappuoliMontecucco1997" /> In the mature CLX, one ] is responsible for a single ] to ] replacement in the ] of CLX-2, leading to the difference between the two isoforms. The structural organization of these two genes show a high degree of homology. This suggests that the two different peptides have the same biological function. This cannot yet be confirmed because only CLX-1 has been isolated from ''C. parasitica''.<ref name="spag" /> Calitoxin has a very different sequence from another sodium channel binding sea anemone toxin, ], which is produced by the distantly related '']''.<ref>{{cite book \| editor-first= Abba J. \| editor-last = Kastin \| name-list-style = vanc \|url=https://books.google.com/books?id=_kDDZFHdL4UC&pg=PA60 \|title=Neurologic Manifestations—Advances in Research and Treatment \|year=2013 \|author=Q. Ashton Acton \|page=60\|publisher=ScholarlyEditions \|isbn=9781481678049}}</ref> A better understanding of these differences might offer insights about the function of particular amino acid residues.<ref name="spag" /> Despite markedly dissimilar gene sequences, CLX-1 affects crustacean axon potentials similar to two other classes of anemone toxins. Alternatively, certain aspects of the structure of the CLX genes are found in ]s as well as other sea anemone toxins that block ]s.<ref name=Moran>{{cite journal \| vauthors = Moran Y, Gordon D, Gurevitz M \| title = Sea anemone toxins affecting voltage-gated sodium channels--molecular and evolutionary features \| journal = Toxicon \| volume = 54 \| issue = 8 \| pages = 1089–101 \| date = December 2009 \| pmid = 19268682 \| pmc = 2807626 \| doi = 10.1016/j.toxicon.2009.02.028 \| bibcode = 2009Txcn...54.1089M }}</ref>

	== Target and ~~mode of action~~ ==		== Target and activity ==
			Calitoxin causes massive neurotransmitter release from the nerve terminals of the neuromuscular junction, which in turn causes a strong ] and even ]. The exact target of calitoxin has not yet been clarified; since it has a similar action on the neuromuscular junction as ''Anemonia sulcata'' toxins, calitoxin may slow down the inactivation of ]s in motor neurons. Calitoxin has been tested for activity on the crab '']''. Purified toxin was injected into the ] of the crab. The minimum dose of 0.2 ] of toxin triggered muscle contractions in the crab, causing paralysis within 1 minute. The median lethal dose ({{LD50}}) is unknown.<ref name="car" />
	The precise action of calitoxin has not been clarified yet. Calitoxin may influence the activity of voltage-gated sodium channels in motor neurons by inhibiting their inactivation. This leads to prolongation of presynaptic ] and thus massive neurotransmitter release in the nerve terminals, which in turn causes a strong muscle contraction.
	Experimental evidence comes from an experiment with ] (TTX), a blocker of voltage-gated sodium channels. In the presence of TTX in the extracellular medium, no action potentials are recorded in the postsynaptic area of the muscular cells. It seems that in the presence of TTX, calitoxin is not able to exert a postsynaptic effect. Because it is known that TTX engages on the presynaptic voltage-gated sodium channels, it is likely that calitoxin influences the presynaptic voltage-gated sodium channels as well by inhibiting their inactivation.
	In short, calitoxin seems to influence the presynaptic motorneurons resulting in a strong postsynaptic motor response. These muscle contractions create a constant maximal contraction in the muscles, which causes ].<ref name="car" />

	== Function in nature ==		== Function in nature ==
	]]]		]]]
	Sea anemones produce toxins, such as ~~Calitoxin~~, in their stinging cells (]). These cells contain ~~organnelles~~ called ~~nematocysts~~. When triggered, an envenomation response occurs. This can result in injury to target organisms, including capture of prey, defense against predatory organisms, or against aggressors from within their own species.<ref name=Kastin>{{cite book\|last1=Kastin\|first1=~~edited by~~ Abba J.\|title=Handbook of ~~biologically~~ ~~active~~ ~~peptides~~\|date=2006\|publisher=Academic Press\|location=Amsterdam\|isbn=0-12-369442-6\|pages=363–364\|url=~~http~~://books.google.com/books?id=n8SV9iM6kT0C&pg=PA363}}</ref> In a natural setting, ''~~Calliactis~~ parasitica'' ~~establishes~~ a ] relationship with the hermit crab ]. The sea anemone identifies shells inhabited by the hermit crab and attaches. ~~Through stings against potential predators,~~ ''C. parasitica'' provides protection for the hermit crab~~. In return~~, ~~the~~ ~~sea~~ ~~anemone~~ ~~gains~~ an ~~advantage~~ in ~~accessing~~ a ~~broader~~ ~~distribution~~ of ~~food sources, as the crab moves across the ocean floor~~.<ref ~~name="Fish"~~>{{cite book \|~~author~~=~~John~~ ~~Fish~~ & ~~Susan~~ ~~Fish~~ \|~~year~~=~~2011~~ \|~~title~~=A ~~Student's~~ ~~Guide~~ to ~~the~~ ~~Seashore~~ \|~~edition~~=~~3rd~~ \|publisher=] \|isbn=978-0-521-~~72059~~-5 \|chapter=~~''Calliactis~~ ~~parasitica''~~ ~~(Couch)~~ \|~~page~~=96 \|url=~~http~~://books.google.~~co.uk~~/books?id=~~1wD21-DC81YC~~&pg=~~PA96~~}}</ref> ~~]es~~ ~~will~~ ~~avoid~~ ~~shells~~ ~~bearing~~ ~~''C.~~ ~~parasitica''~~.<ref>{{cite book \|~~author~~=~~Roger~~ T. ~~Hanlon~~ & ~~John~~ B. ~~Messenger~~ \|year=~~1998~~ \|title=~~Cephalopod~~ ~~Behaviour~~ \|publisher=] \|isbn=978-0-521-~~64583~~-6 \|chapter=~~Learning~~ ~~and~~ ~~the development of behaviour~~ \|~~pages~~=~~132–148~~ \|url=~~http~~://books.google.~~co.uk~~/books?id=~~Nxfv6xZZ6WYC~~&pg=~~PA140~~}}</ref>		Sea anemones produce toxins, such as calitoxin, in their stinging cells (]). These cells contain organelles called ]s. When triggered, an ] response occurs. This can result in injury to target organisms, including capture of prey, defense against predatory organisms, or against aggressors from within their own species.<ref name=Kastin>{{cite book\|last1=Kastin\|first1=Abba J. \| name-list-style = vanc \|title=Handbook of Biologically Active Peptides\|date=2006\|publisher=Academic Press\|location=Amsterdam\|isbn=0-12-369442-6\|pages=363–364\|url=https://books.google.com/books?id=n8SV9iM6kT0C&pg=PA363}}</ref> In its natural setting, ''C. parasitica'' can establish a ] relationship with the hermit crab '']''. The sea anemone identifies shells inhabited by the hermit crab and attaches. ''C. parasitica'' provides protection for the hermit crab, by stinging or intimidating potential predators. ]es will avoid shells bearing ''C. parasitica''.<ref>{{cite book \| first1 = Roger T. \| last1 = Hanlon \| first2 = John B. \| last2 = Messenger \| name-list-style = vanc \|year=1998 \|title=Cephalopod Behaviour \|publisher=] \|isbn=978-0-521-64583-6 \|chapter=Learning and the development of behaviour \|pages=132–148 \|chapter-url=https://books.google.com/books?id=Nxfv6xZZ6WYC&pg=PA140}}</ref> In return for the protection, the sea anemone gains an advantage in accessing a broader distribution of food sources, as the crab moves across the ocean floor.<ref name="Fish">{{cite book \| first1 = John \| last1 = Fish \| first2 = Susan \| last2 = Fish \|name-list-style = vanc \|year=2011 \|title=A Student's Guide to the Seashore \|edition=3rd \|publisher=] \|isbn=978-0-521-72059-5 \|chapter=''Calliactis parasitica'' (Couch) \|page=96 \|chapter-url=https://books.google.com/books?id=1wD21-DC81YC&pg=PA96}}</ref>

	== Toxicity ==
	Calitoxin has been tested for activity on the crab ''Carcinus mediterraneus'', by injecting a 0.1 mL solution with 0.2 µg lyophilized CLX of into the hemocoel. This revealed that the toxic unit corresponds to this minimum amount of the toxin inducing muscle contractions in the crab causing paralysis within 1 minute from injection. The {{LD50}} is unknown.<ref name="car" />

	== References ==		== References ==
	{{Reflist}}		{{Reflist}}

	]		]
	]		]
			]
			]

Latest revision as of 00:18, 23 December 2024

Calitoxin
Identifiers
CAS Number	118354-83-9
Abbreviations	CLX
ChemSpider	none
CompTox Dashboard (EPA)	DTXSID30897122
Except where otherwise noted, data are given for materials in their standard state (at 25 °C , 100 kPa). Infobox references

Chemical compound

Calitoxin-1

Identifiers

Organism

Calliactis parasitica

Symbol

CLX-1

UniProt

P14531

Search for
Structures	Swiss-model
Domains	InterPro

Calitoxin-2

Identifiers

Organism

Calliactis parasitica

Symbol

CLX-2

UniProt

P49127

Search for
Structures	Swiss-model
Domains	InterPro

Protein family

Identifiers

Symbol

Toxin_4

Available protein structures:
Pfam	structures / ECOD
PDB	RCSB PDB; PDBe; PDBj
PDBsum	structure summary

Calitoxin, also known as CLX, is a sea anemone neurotoxin produced by the sea anemone Calliactis parasitica. It targets crabs and octopuses, among other invertebrates. Two isoforms (CLX-1 and CLX-2) have been identified, both of which are formed from precursors stored in the stinging cells of the anemone. Once the toxin is activated and released, it causes paralysis by increasing neurotransmitter release at invertebrate neuromuscular junctions. Along with several other toxins derived from anemones, CLX is useful in ion channel research. Certain structural aspects of calitoxin are dissimilar from sea anemone toxins that also target the sodium ion channels. Other toxins resembling calitoxin function in completely different ways.

Source and discovery

Calitoxin is a highly potent neurotoxin produced by the sea anemone Calliactis parasitica, which is stored in the nematocysts of stinging cells (cnidocytes). This sea anemone is a species from the Hormathiidae family and is present along the European coasts of the Atlantic Ocean and in the Mediterranean Sea. The name calitoxin is derived from the organism from which the toxin was isolated. The toxin was isolated by a team of researchers in Naples, Italy from animals collected in the Bay of Naples. The team isolated the polypeptide through a series of centrifugations until the supernatant had lost toxic activity. The resulting pellet was purified using the techniques liquid chromatography, gel filtration, and chromatofocusing. The team then sequenced the purified polypeptide chain. They also published details on the toxin's effects in vitro on crustacean tissue preparations, including nerve and muscle. Their findings were published in the journal Biochemistry in 1989.

Structure and chemistry

It has an isoelectric point at pH 5.4. The amino acid sequence is markedly dissimilar from other known sea anemones toxins. There are two known genes coding for two highly homologous calitoxins: CLX-1 and CLX-2. Both originate from a precursor peptide of 79 amino acids where the C-terminus determines whether it will be the mature CLX-1 or CLX-2. The activated toxins consist of 46 amino acids with three disulfide bonds. Researchers suspect that the toxins are stored as precursors in cnidocytes. Under the effects of some triggering stimulus, the precursor is modified and released in the active form. The patterning of cleavage sites targeted during maturation of the peptide suggest that the active quaternary structure might be a tetrapeptide.

Amino acid sequences of CLX precursors
Isoform	Sequence	Disulfide bridge locations
CLX-1 precursor	MKTQVLALFV LCVLFCLAES RTTLNKRNDI EKRIECKCEG DAPDLSHMTG TVYFSCKGGD GSWSKCNTYT AVADCCHQA	36 – 75 38 – 66 56 – 76
CLX-2 precursor	MKTQVLAVFV LCVLFCLAES RTTLNKRIDI AKRIECKCKG DAPDLSHMTG TVYFSCKGGD GSWSKCNTYT AVADCCHQA	36 – 75 38 – 66 56 – 76

Calitoxin and other sea anemone toxins are used in studying ion channels, with potential applications in biomedical and physiology research. In the mature CLX, one base-pair substitution is responsible for a single glutamic acid to lysine replacement in the coding region of CLX-2, leading to the difference between the two isoforms. The structural organization of these two genes show a high degree of homology. This suggests that the two different peptides have the same biological function. This cannot yet be confirmed because only CLX-1 has been isolated from C. parasitica. Calitoxin has a very different sequence from another sodium channel binding sea anemone toxin, ATX-II, which is produced by the distantly related Anemonia sulcata. A better understanding of these differences might offer insights about the function of particular amino acid residues. Despite markedly dissimilar gene sequences, CLX-1 affects crustacean axon potentials similar to two other classes of anemone toxins. Alternatively, certain aspects of the structure of the CLX genes are found in scorpion toxins as well as other sea anemone toxins that block potassium channels.

Target and activity

Calitoxin causes massive neurotransmitter release from the nerve terminals of the neuromuscular junction, which in turn causes a strong muscle contraction and even paralysis. The exact target of calitoxin has not yet been clarified; since it has a similar action on the neuromuscular junction as Anemonia sulcata toxins, calitoxin may slow down the inactivation of voltage-gated sodium channels in motor neurons. Calitoxin has been tested for activity on the crab Carcinus mediterraneus. Purified toxin was injected into the hemocoel of the crab. The minimum dose of 0.2 μg of toxin triggered muscle contractions in the crab, causing paralysis within 1 minute. The median lethal dose (LD₅₀) is unknown.

Function in nature

Sea anemones produce toxins, such as calitoxin, in their stinging cells (cnidocytes). These cells contain organelles called nematocysts. When triggered, an envenomation response occurs. This can result in injury to target organisms, including capture of prey, defense against predatory organisms, or against aggressors from within their own species. In its natural setting, C. parasitica can establish a mutualistic relationship with the hermit crab Pagurus bernhardus. The sea anemone identifies shells inhabited by the hermit crab and attaches. C. parasitica provides protection for the hermit crab, by stinging or intimidating potential predators. Octopuses will avoid shells bearing C. parasitica. In return for the protection, the sea anemone gains an advantage in accessing a broader distribution of food sources, as the crab moves across the ocean floor.

References

^ Spagnuolo A, Zanetti L, Cariello L, Piccoli R (January 1994). "Isolation and characterization of two genes encoding calitoxins, neurotoxic peptides from Calliactis parasitica (Cnidaria)". Gene. 138 (1–2): 187–91. doi:10.1016/0378-1119(94)90805-2. PMID 7510258.
^ Cariello L, de Santis A, Fiore F, Piccoli R, Spagnuolo A, Zanetti L, Parente A (March 1989). "Calitoxin, a neurotoxic peptide from the sea anemone Calliactis parasitica: amino acid sequence and electrophysiological properties". Biochemistry. 28 (6): 2484–9. doi:10.1021/bi00432a020. PMID 2567180.
^ Rappuoli R, Montecucco C (29 May 1997). Guidebook to Protein Toxins and Their Use in Cell Biology. Oxford University Press, UK. pp. 139–. ISBN 978-0-19-154728-7.
^ Kastin AJ (2006). Handbook of Biologically Active Peptides. Amsterdam: Academic Press. pp. 363–364. ISBN 0-12-369442-6.
"Calitoxin-1". UniProt.
"Calitoxin-2". UniProt.
Nagai H (2012). "Special Issue "Sea Anemone Toxins"". Marine Drugs.
Q. Ashton Acton (2013). Kastin AJ (ed.). Neurologic Manifestations—Advances in Research and Treatment. ScholarlyEditions. p. 60. ISBN 9781481678049.
Moran Y, Gordon D, Gurevitz M (December 2009). "Sea anemone toxins affecting voltage-gated sodium channels--molecular and evolutionary features". Toxicon. 54 (8): 1089–101. Bibcode:2009Txcn...54.1089M. doi:10.1016/j.toxicon.2009.02.028. PMC 2807626. PMID 19268682.
Hanlon RT, Messenger JB (1998). "Learning and the development of behaviour". Cephalopod Behaviour. Cambridge University Press. pp. 132–148. ISBN 978-0-521-64583-6.
Fish J, Fish S (2011). "Calliactis parasitica (Couch)". A Student's Guide to the Seashore (3rd ed.). Cambridge University Press. p. 96. ISBN 978-0-521-72059-5.

Categories: