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- Title:
- Formyl-peptide receptor is not involved in the protection afforded by annexin 1 in murine acute myocardial infarct
- Barts & London
- Univ Naples 2
- Universidade Estadual Paulista (UNESP)
- 0892-6638
- Recent interest in the annexin 1 field has come from the notion that specific G-protein-coupled receptors, members of the formyl-peptide receptor (FPR) family, appear to mediate the anti-inflammatory actions of this endogenous mediator. Administration of the annexin 1 N-terminal derived peptide Ac2-26 to mice after 25 min ischemia significantly attenuated the extent of acute myocardial injury as assessed 60 min postreperfusion. Evident at the dose of 1 mg/kg (similar to9 nmol per animal), peptide Ac2-26 cardioprotection was intact in FPR null mice. Similarly, peptide Ac2-26 inhibition of specific markers of heart injury (specifically myeloperoxidase activity, CXC chemokine KC contents, and endogenous annexin 1 protein expression) was virtually identical in heart samples collected from wild-type and FPR null mice. Mouse myocardium expressed the mRNA for FPR and the structurally related lipoxin A(4) receptor, termed ALX; thus, comparable equimolar doses of two ALX agonists (W peptide and a stable lipoxin A4 analog) exerted cardioprotection in wild-type and FPR null mice to an equal extent. Curiously, marked (>95%) blood neutropenia produced by an anti-mouse neutrophil serum did not modify the extent of acute heart injury, whereas it prevented the protection afforded by peptide Ac2-26. Thus, this study sheds light on the receptor mechanism(s) mediating annexin 1-induced cardioprotection and shows a pivotal role for ALX and circulating neutrophil, whereas it excludes any functional involvement of mouse FPR. These mechanistic data can help in developing novel therapeutics for acute cardioprotection.
- 1-Oct-2004
- Faseb Journal. Bethesda: Federation Amer Soc Exp Biol, v. 18, n. 13, p. 100-+, 2004.
- 100-+
- Federation Amer Soc Exp Biol
- FPR
- ischemia/reperfusion
- PMN
- http://dx.doi.org/10.1096/fj.04-2178fje
- Acesso restrito
- outro
- http://repositorio.unesp.br/handle/11449/21352
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