Literature DB >> 21967810

Antiallodynic effect and side effects of Phα1β, a neurotoxin from the spider Phoneutria nigriventer: comparison with ω-conotoxin MVIIA and morphine.

A H de Souza1, M C Lima, C C Drewes, J F da Silva, K C L Torres, E M R Pereira, C J de Castro Junior, L B Vieira, M N Cordeiro, M Richardson, R S Gomez, M A Romano-Silva, J Ferreira, M V Gomez.   

Abstract

Phα1β is a potent toxin obtained from the spider Phoneutria nigriventer that blocks neuronal voltage-sensitive Ca(2+) channels. This study compared the antiallodynic effects of Phα1β, ω-conotoxin MVIIA and morphine in mice and their side effects in rats. Mechanical allodynia was measured in mice receiving single intrathecal administration of Phα1β, ω-conotoxin MVIIA or morphine before or after the incisional plantar procedure. The effect of the treatments on cardiovascular profile and global neurological were evaluated in rats. The expression of pro or anti-inflammatory cytokines of human polymorph mononuclear cells was also evaluated. Preemptive use of ω-conotoxin MVIIA (1.0 or 10 pmol/site) or morphine (1000 pmol/site) induced shorter antiallodynic effect than Phα1β (100 pmol/site) in mice. Post-incision administration of Phα1β (200 pmol/site) induced longer mechanical antiallodynic effect than ω-conotoxin MVIIA (1.0 or 10 pmol/site) or morphine (1000 pmol/site). Intrathecal injection of Phα1β (200 pmol/site) and morphine (433 pmol/site) did not change while ω-conotoxin MVIIA (100 pmol/site) increased the heart rate in rats 3 h after its administration. Phα1β (200 pmol/site), ω-conotoxin MVIIA (100 pmol/site) and morphine (433 pmol/site) did not change mean arterial pressure 0.5 and 3 h after their administration. The treatments did not alter neurological performance assessed by global neurological evaluation and open-field test. The tested drugs did not induced expression of pro or anti-inflammatory cytokines in CD4 monocytes. In conclusion, preemptive administration Phα1β in mice induced longer antiallodynic effect than ω-conotoxin MVIIA and morphine. Phα1β also induced a longer mechanical antiallodynic effect than ω-conotoxin MVIIA and morphine when used after the surgical incision. The present results suggest that Phα1β has a potential application in the management of postoperative pain with low side effects. Published by Elsevier Ltd.

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Year:  2011        PMID: 21967810     DOI: 10.1016/j.toxicon.2011.09.008

Source DB:  PubMed          Journal:  Toxicon        ISSN: 0041-0101            Impact factor:   3.033


  14 in total

1.  Antinociceptive effect of a novel armed spider peptide Tx3-5 in pathological pain models in mice.

Authors:  Sara M Oliveira; Cássia R Silva; Gabriela Trevisan; Jardel G Villarinho; Marta N Cordeiro; Michael Richardson; Márcia H Borges; Célio J Castro; Marcus V Gomez; Juliano Ferreira
Journal:  Pflugers Arch       Date:  2016-02-22       Impact factor: 3.657

2.  Spinal blockage of P/Q- or N-type voltage-gated calcium channels modulates functional and symptomatic changes related to haemorrhagic cystitis in mice.

Authors:  R B M Silva; N D M Sperotto; E L Andrade; T C B Pereira; C E Leite; A H de Souza; M R Bogo; F B Morrone; M V Gomez; M M Campos
Journal:  Br J Pharmacol       Date:  2014-12-15       Impact factor: 8.739

3.  The peptide Phα1β, from spider venom, acts as a TRPA1 channel antagonist with antinociceptive effects in mice.

Authors:  Raquel Tonello; Camilla Fusi; Serena Materazzi; Ilaria M Marone; Francesco De Logu; Silvia Benemei; Muryel C Gonçalves; Elisabetta Coppi; Celio J Castro-Junior; Marcus Vinicius Gomez; Pierangelo Geppetti; Juliano Ferreira; Romina Nassini
Journal:  Br J Pharmacol       Date:  2016-11-28       Impact factor: 8.739

4.  An evaluation of the antinociceptive effects of Phα1β, a neurotoxin from the spider Phoneutria nigriventer, and ω-conotoxin MVIIA, a cone snail Conus magus toxin, in rat model of inflammatory and neuropathic pain.

Authors:  Alessandra Hubner de Souza; Célio J Castro; Flavia Karine Rigo; Sara Marchesan de Oliveira; Renato Santiago Gomez; Danuza Montijo Diniz; Marcia Helena Borges; Marta Nascimento Cordeiro; Marco Aurélio Romano Silva; Juliano Ferreira; Marcus Vinicius Gomez
Journal:  Cell Mol Neurobiol       Date:  2012-08-07       Impact factor: 5.046

5.  Antinociceptive and genotoxic assessments of the antagonist TRPV1 receptor SB-366791 on morphine-induced tolerance in mice.

Authors:  Thiago Kastell Mazeto; Jaqueline Nascimento Picada; Áurea Pandolfo Correa; Isadora Nunes Rebelo; Magali Terra Ribeiro; Marcus Vinícius Gomez; Alessandra Hubner de Souza
Journal:  Naunyn Schmiedebergs Arch Pharmacol       Date:  2019-10-26       Impact factor: 3.000

6.  A membrane-delimited N-myristoylated CRMP2 peptide aptamer inhibits CaV2.2 trafficking and reverses inflammatory and postoperative pain behaviors.

Authors:  Liberty François-Moutal; Yue Wang; Aubin Moutal; Karissa E Cottier; Ohannes K Melemedjian; Xiaofang Yang; Yuying Wang; Weina Ju; Tally M Largent-Milnes; May Khanna; Todd W Vanderah; Rajesh Khanna
Journal:  Pain       Date:  2015-07       Impact factor: 7.926

7.  Pharmacological Inhibition of Voltage-gated Ca(2+) Channels for Chronic Pain Relief.

Authors:  Seungkyu Lee
Journal:  Curr Neuropharmacol       Date:  2013-12       Impact factor: 7.363

Review 8.  Venom peptides as a rich source of cav2.2 channel blockers.

Authors:  Silmara R Sousa; Irina Vetter; Richard J Lewis
Journal:  Toxins (Basel)       Date:  2013-02-04       Impact factor: 4.546

9.  Postoperative pain-from mechanisms to treatment.

Authors:  Esther M Pogatzki-Zahn; Daniel Segelcke; Stephan A Schug
Journal:  Pain Rep       Date:  2017-03-15

10.  Conotoxin MVIIA improves cell viability and antioxidant system after spinal cord injury in rats.

Authors:  Karen M Oliveira; Nancy S Binda; Mário Sérgio L Lavor; Carla M O Silva; Isabel R Rosado; Endrigo L A Gabellini; Juliana F Da Silva; Camila M Oliveira; Marília M Melo; Marcus Vinícius Gomez; Eliane G Melo
Journal:  PLoS One       Date:  2018-10-04       Impact factor: 3.240
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