ID   H1A03_CYRHA             Reviewed;          83 AA.
AC   D2Y1X8; P83591;
DT   02-NOV-2010, integrated into UniProtKB/Swiss-Prot.
DT   02-MAR-2010, sequence version 1.
DT   25-MAY-2022, entry version 36.
DE   RecName: Full=Mu-theraphotoxin-Hhn2b 3 {ECO:0000305|PubMed:26429937};
DE            Short=Mu-TRTX-Hhn2b {ECO:0000303|PubMed:26429937};
DE   AltName: Full=Hainantoxin-I {ECO:0000303|PubMed:12727268, ECO:0000303|PubMed:14675784, ECO:0000303|PubMed:20192277};
DE            Short=HnTx-I {ECO:0000303|PubMed:12727268, ECO:0000303|PubMed:14675784, ECO:0000303|PubMed:20192277};
DE   AltName: Full=Peptide F5-19.03;
DE   Flags: Precursor;
OS   Cyriopagopus hainanus (Chinese bird spider) (Haplopelma hainanum).
OC   Eukaryota; Metazoa; Ecdysozoa; Arthropoda; Chelicerata; Arachnida; Araneae;
OC   Mygalomorphae; Theraphosidae; Haplopelma.
OX   NCBI_TaxID=209901;
RN   [1]
RP   NUCLEOTIDE SEQUENCE [LARGE SCALE MRNA], PROTEIN SEQUENCE OF 49-81, AND
RP   IDENTIFICATION BY MASS SPECTROMETRY.
RC   TISSUE=Venom, and Venom gland;
RX   PubMed=20192277; DOI=10.1021/pr1000016;
RA   Tang X., Zhang Y., Hu W., Xu D., Tao H., Yang X., Li Y., Jiang L.,
RA   Liang S.;
RT   "Molecular diversification of peptide toxins from the tarantula Haplopelma
RT   hainanum (Ornithoctonus hainana) venom based on transcriptomic, peptidomic,
RT   and genomic analyses.";
RL   J. Proteome Res. 9:2550-2564(2010).
RN   [2]
RP   PROTEIN SEQUENCE OF 49-81.
RC   TISSUE=Venom;
RX   PubMed=12727268; DOI=10.1016/s0041-0101(02)00280-5;
RA   Xiao Y.-C., Liang S.-P.;
RT   "Purification and characterization of Hainantoxin-V, a tetrodotoxin-
RT   sensitive sodium channel inhibitor from the venom of the spider
RT   Selenocosmia hainana.";
RL   Toxicon 41:643-650(2003).
RN   [3]
RP   SEQUENCE REVISION TO 78-81, FUNCTION, SUBUNIT, SUBCELLULAR LOCATION, MASS
RP   SPECTROMETRY, DISULFIDE BONDS, AMIDATION AT LEU-81, AND STRUCTURE BY NMR OF
RP   48-81.
RC   TISSUE=Venom;
RX   PubMed=14675784; DOI=10.1016/s0014-5793(03)01303-6;
RA   Li D.-L., Xiao Y.-C., Hu W.-J., Xie J.-Y., Bosmans F., Tytgat J.,
RA   Liang S.-P.;
RT   "Function and solution structure of hainantoxin-I, a novel insect sodium
RT   channel inhibitor from the Chinese bird spider Selenocosmia hainana.";
RL   FEBS Lett. 555:616-622(2003).
RN   [4]
RP   STRUCTURE BY NMR OF 48-81 OF WILD-TYPE AND G54W/N71S MUTANT, FUNCTION,
RP   RECOMBINANT EXPRESSION OF 48-81, AND MUTAGENESIS OF LYS-51; GLY-54; ASN-71
RP   AND VAL-79.
RX   PubMed=26429937; DOI=10.1124/mol.115.100784;
RA   Klint J.K., Chin Y.K., Mobli M.;
RT   "Rational engineering defines a molecular switch that is essential for
RT   activity of spider-venom peptides against the analgesics target NaV1.7.";
RL   Mol. Pharmacol. 88:1002-1010(2015).
CC   -!- FUNCTION: Weakly blocks the rat SCN2A/SCN1B (Nav1.2/beta-1) sodium
CC       channel (IC(50)=68 uM) and the insect sodium channel para/tipE
CC       (IC(50)=4.3 uM), without altering the activation or inactivation
CC       kinetics (depressant toxin). {ECO:0000269|PubMed:14675784,
CC       ECO:0000269|PubMed:26429937}.
CC   -!- SUBUNIT: Monomer. {ECO:0000269|PubMed:14675784}.
CC   -!- SUBCELLULAR LOCATION: Secreted {ECO:0000269|PubMed:14675784}.
CC   -!- TISSUE SPECIFICITY: Expressed by the venom gland.
CC       {ECO:0000269|PubMed:14675784}.
CC   -!- DOMAIN: The presence of a 'disulfide through disulfide knot'
CC       structurally defines this protein as a knottin.
CC       {ECO:0000269|PubMed:14675784, ECO:0000269|PubMed:26429937}.
CC   -!- MASS SPECTROMETRY: Mass=3608.02; Method=MALDI;
CC       Evidence={ECO:0000269|PubMed:14675784};
CC   -!- MISCELLANEOUS: Has no effect on mammalian SCN3A/SCN1B (Nav1.3/beta-1),
CC       SCN4A (Nav1.4), SCN5A/SCN1B (Nav1.5/beta-1), and SCN9A/SCN1B
CC       (Nav1.7/beta-1) (PubMed:14675784, PubMed:26429937). Has also no effect
CC       on sodium subtypes in rat DRG neurons containing Nav1.1/SCN1A,
CC       Nav1.6/SCN8A, Nav1.7/SCN9A, Nav1.8/SCN10A and Nav1.9/SCN11A
CC       (PubMed:14675784). {ECO:0000269|PubMed:14675784,
CC       ECO:0000269|PubMed:26429937}.
CC   -!- MISCELLANEOUS: Klint et al., 2015 worked with a recombinant peptide N-
CC       terminally extended by an Ala residue
CC       (AECKGFGKSCVPGKNECCSGYACNSRDKWCKVLL). {ECO:0000305|PubMed:26429937}.
CC   -!- SIMILARITY: Belongs to the neurotoxin 10 (Hwtx-1) family. 14 (Hntx-1)
CC       subfamily. {ECO:0000305}.
CC   ---------------------------------------------------------------------------
CC   Copyrighted by the UniProt Consortium, see https://www.uniprot.org/terms
CC   Distributed under the Creative Commons Attribution (CC BY 4.0) License
CC   ---------------------------------------------------------------------------
DR   EMBL; GU292855; ADB56671.1; -; mRNA.
DR   AlphaFoldDB; D2Y1X8; -.
DR   BMRB; D2Y1X8; -.
DR   SMR; D2Y1X8; -.
DR   ArachnoServer; AS000338; mu-theraphotoxin-Hhn2b.
DR   GO; GO:0005576; C:extracellular region; IEA:UniProtKB-SubCell.
DR   GO; GO:0008200; F:ion channel inhibitor activity; IEA:InterPro.
DR   GO; GO:0017080; F:sodium channel regulator activity; IEA:UniProtKB-KW.
DR   GO; GO:0090729; F:toxin activity; IEA:UniProtKB-KW.
DR   InterPro; IPR011696; Huwentoxin-1.
DR   InterPro; IPR013140; Huwentoxin_CS1.
DR   Pfam; PF07740; Toxin_12; 1.
DR   PROSITE; PS60021; HWTX_1; 1.
PE   1: Evidence at protein level;
KW   Amidation; Direct protein sequencing; Disulfide bond;
KW   Ion channel impairing toxin; Knottin; Neurotoxin; Secreted; Signal; Toxin;
KW   Voltage-gated sodium channel impairing toxin.
FT   SIGNAL          1..21
FT                   /evidence="ECO:0000255"
FT   PROPEP          22..48
FT                   /evidence="ECO:0000305|PubMed:12727268,
FT                   ECO:0000305|PubMed:20192277"
FT                   /id="PRO_0000400498"
FT   PEPTIDE         49..81
FT                   /note="Mu-theraphotoxin-Hhn2b 3"
FT                   /evidence="ECO:0000269|PubMed:12727268,
FT                   ECO:0000269|PubMed:20192277"
FT                   /id="PRO_0000400499"
FT   MOD_RES         81
FT                   /note="Leucine amide"
FT                   /evidence="ECO:0000269|PubMed:14675784"
FT   DISULFID        50..65
FT                   /evidence="ECO:0000269|PubMed:14675784,
FT                   ECO:0000269|PubMed:26429937"
FT   DISULFID        57..70
FT                   /evidence="ECO:0000269|PubMed:14675784,
FT                   ECO:0000269|PubMed:26429937"
FT   DISULFID        64..77
FT                   /evidence="ECO:0000269|PubMed:14675784,
FT                   ECO:0000269|PubMed:26429937"
FT   MUTAGEN         51
FT                   /note="K->L: No gain of activity against hNav1.7/SCN9A."
FT                   /evidence="ECO:0000269|PubMed:26429937"
FT   MUTAGEN         54
FT                   /note="G->W: Low gain of inhibition activity against
FT                   hNav1.7/SCN9A (IC(50)=2.7 uM), and gain of binding to
FT                   anionic POPG liposome. Important gain of inhibition
FT                   activity (IC(50)=440 nM), and gain of binding to anionic
FT                   POPG liposome; when associated with S-71."
FT                   /evidence="ECO:0000269|PubMed:26429937"
FT   MUTAGEN         71
FT                   /note="N->S: Low gain of inhibition activity against
FT                   hNav1.7/SCN9A (IC(50)=4.0 uM) and no change in binding to
FT                   anionic POPG liposome. Important gain of inhibition
FT                   activity (IC(50)=440 nM), and gain of binding to anionic
FT                   POPG liposome; when associated with W-54."
FT                   /evidence="ECO:0000269|PubMed:26429937"
FT   MUTAGEN         79
FT                   /note="V->W: No gain of activity against hNav1.7/SCN9A."
FT                   /evidence="ECO:0000269|PubMed:26429937"
SQ   SEQUENCE   83 AA;  9210 MW;  A72E5B88A8ACCDF2 CRC64;
     MKASMFLALA GLVLLFVVCY ASESEEKEFP RELISKIFAV DDFKGEVREC KGFGKSCVPG
     KNECCSGYAC NSRDKWCKVL LGK