Structure, Function, and Chemical Synthesis of <i>Vaejovis mexicanus</i> Peptide 24: A Novel Potent Blocker of Kv1.3 Potassium Channels of Human T Lymphocytes

Gurrola, Georgina B.; Hernández-López, Rogelio A.; Vega, Ricardo C. Rodrí­guez de la; Varga, Zoltán; Batista, Cesar Vicente Ferreira; Salas-Castillo, Saida P.; Panyi, György; Rı́o-Portilla, Federico del; Possani, Lourival D.

doi:10.1021/bi300060n

Cited by 50 publications

(44 citation statements)

References 73 publications

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“…The a-KTx is the best studied family; its members are small basic peptides (up to 4 kDa) consisting of 23 to 40 amino acids with the structure stabilized by three to four disulfide bridges. To date, the a-KTx family is classified into 27 subfamilies (http://www.uniprot.org/docs/scorpktx) Goudet et al, 2002;Huys et al, 2004;Rodríguez de la Vega and Possani, 2004;Tan et al, 2006;Zhijian et al, 2006;Gurrola et al, 2012) with K 1 channel affinities varying in the micromolar to picomolar range. The a-KTx toxins target mainly the voltage-gated potassium (K v ) channels, especially the K v 1 family members and some Ca 21 -activated K 1 channels ; Rodríguez de la Vega and .…”

Section: Introductionmentioning

confidence: 99%

Structure, Molecular Modeling, and Function of the Novel Potassium Channel Blocker Urotoxin Isolated from the Venom of the Australian Scorpion Urodacus yaschenkoi

et al. 2014

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This communication reports the structural and functional characterization of urotoxin, the first K 1 channel toxin isolated from the venom of the Australian scorpion Urodacus yaschenkoi. It is a basic peptide consisting of 37 amino acids with an amidated C-terminal residue. Urotoxin contains eight cysteines forming four disulfide bridges with sequence similarities resembling the a-potassium channel toxin 6 (a-KTx-6) subfamily of peptides; it was assigned the systematic number of a-KTx-6.21. Urotoxin is a potent blocker of human voltage-gated potassium channel (K v )1.2 channels, with an IC 50 of 160 pM, whereas its affinity for other channels tested was in the nanomolar range (hK v 1

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Section: Introductionmentioning

confidence: 99%

Structure, Molecular Modeling, and Function of the Novel Potassium Channel Blocker Urotoxin Isolated from the Venom of the Australian Scorpion Urodacus yaschenkoi

et al. 2014

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“…This 36-mer peptide consists of α-helix and β-strands, stabilized by four pairs of disulfide bonds (35). It has a K d ∼3 pM for Kv1.3 and >1,500-fold selectivity over Kv1.1, Kv1.2, KCa1.1, and KCa3.1 (36).…”

Section: Resultsmentioning

confidence: 99%

“…Moka1 and Vm24 toxin peptides were synthesized in solid phase by InnoPep. Peptide folding, HPLC purification, and LC-MS validation were performed based on previously published procedures (28,35).…”

Section: Methodsmentioning

confidence: 99%

Rational design of a Kv1.3 channel-blocking antibody as a selective immunosuppressant

Wang

Zhang

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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A variable region fusion strategy was used to generate an immunosuppressive antibody based on a novel "stalk-knob" structural motif in the ultralong complementary-determining region (CDR) of a bovine antibody. The potent Kv1.3 channel inhibitory peptides Moka1-toxin and Vm24-toxin were grafted into different CDRs of the humanized antibodies BVK and Synagis (Syn) using both β-sheet and coiled-coil linkers. Structure-activity relationship efforts led to generation of the fusion protein Syn-Vm24-CDR3L, which demonstrated excellent selectivity and potency against effector human memory T cells (subnanomolar to picomolar EC 50 values). This fusion antibody also had significantly improved plasma half-life and serum stability in rodents compared with the parent Vm24 peptide. Finally, this fusion protein showed potent in vivo efficacy in the delayed type hypersensitivity in rats. These results illustrate the utility of antibody CDR fusions as a general and effective strategy to generate long-acting functional antibodies, and may lead to a selective immunosuppressive antibody for the treatment of autoimmune diseases.antibody | protein engineering | Kv1.3 | autoimmune | immunosuppressive

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“…Inhibit current, ShIR, Xenopus oocytes, 1 mM, (Cerni et al, 2014) Inhibit current, Rat, Xenopus oocytes, 1 mM, (Cerni et al, 2014) Inhibit current, CL1023, Kd ¼ 0.21 nM, (Werkman et al, 1993); Inhibit current, Rat, Xenopus oocytes, 1 mM, (Cerni et al, 2014) Inhibit current, Mouse, Xenopus oocytes, Kd ¼ 3.9 nM, (Rodrigues et al, 2003); Inhibit current, Mouse, L929, Kd ¼ 198 nM, (Rodrigues et al, 2003); Inhibit current, Rat, Xenopus oocytes, 1 mM, (Cerni et al, 2014) Inhibit current, Rat, Xenopus oocytes, 1 mM, (Cerni et al, 2014) Tst26 a-KTx 4.6 Tityus stigmurus Inhibit current, Human, COS7, Kd ¼ 1.9 nM, (Papp et al, 2009) Inhibit current, Human T lymphocyte, Kd ¼ 10.7 nM, (Papp et al, 2009) (Varga et al, 2012) Inhibit current, Human, COS7, Kd ¼ 5e10 nM, (Varga et al, 2012) Inhibit current, Human T lymphocytes, Kd ¼ 3 pM, (Gurrola et al, 2012); Inhibit current, Human T lymphocytes, Kd ¼ 2.9 pM, (Varga et al, 2012) a-KTx 2.14…”

Section: Tityus Serrulatusmentioning

confidence: 99%

Scorpion toxin peptide action at the ion channel subunit level

Housley

Liddell

et al. 2017

Neuropharmacology

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a b s t r a c tThis review categorizes functionally validated actions of defined scorpion toxin (SCTX) neuropeptides across ion channel subclasses, highlighting key trends in this rapidly evolving field. Scorpion envenomation is a common event in many tropical and subtropical countries, with neuropharmacological actions, particularly autonomic nervous system modulation, causing significant mortality. The primary active agents within scorpion venoms are a diverse group of small neuropeptides that elicit specific potent actions across a wide range of ion channel classes. The identification and functional characterisation of these SCTX peptides has tremendous potential for development of novel pharmaceuticals that advance knowledge of ion channels and establish lead compounds for treatment of excitable tissue disorders. This review delineates the unique specificities of 320 individual SCTX peptides that collectively act on 41 ion channel subclasses. Thus the SCTX research field has significant translational implications for pathophysiology spanning neurotransmission, neurohumoral signalling, sensori-motor systems and excitation-contraction coupling.This article is part of the Special Issue entitled 'Venom-derived Peptides as Pharmacological Tools.'

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Structure, Function, and Chemical Synthesis of Vaejovis mexicanus Peptide 24: A Novel Potent Blocker of Kv1.3 Potassium Channels of Human T Lymphocytes

Cited by 50 publications

References 73 publications

Structure, Molecular Modeling, and Function of the Novel Potassium Channel Blocker Urotoxin Isolated from the Venom of the Australian Scorpion Urodacus yaschenkoi

Structure, Molecular Modeling, and Function of the Novel Potassium Channel Blocker Urotoxin Isolated from the Venom of the Australian Scorpion Urodacus yaschenkoi

Rational design of a Kv1.3 channel-blocking antibody as a selective immunosuppressant

Scorpion toxin peptide action at the ion channel subunit level

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