Pharmacological characterization of polycation‐induced rat hind‐paw oedema

Antunes, Edson; Mariano, Mário; Cirino, Giuseppe; Levi, Silvio; Nucci, Gilberto De

doi:10.1111/j.1476-5381.1990.tb14193.x

Cited by 41 publications

(19 citation statements)

References 27 publications

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“…Given their lack of selectivity, it is conceivable that systemic administration may also inhibit ecNOS remote from the inflammatory locus, resulting in vasoconstriction, reduced blood delivery to the inflamed site, and, thus, a reduction in inflammation. Indeed, it was shown that the anti-inflammatory effects of L-arginine analogues, given systemically, could be reversed by vasodilators (8,9,24). In agreement with these studies, we also found that when NOS inhibitors were injected i.p., immediately before intrapleural injection of carrageenin, pleural exudates were significantly reduced.…”

Section: Discussionsupporting

confidence: 91%

Nitric Oxide Synthase Inhibitors Have Opposite Effects on Acute Inflammation Depending on Their Route of Administration

Paul-Clark

Gilroy

Willis

et al. 2001

The Journal of Immunology

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The bulk of published data has shown that NO is proinflammatory. However, there also exists the conflicting notion that NO may be protective during an inflammatory insult. In an attempt to resolve this issue, we have compared the effects on inflammation of a range of NO synthase (NOS) inhibitors given either directly to the site of the inflammatory lesion or systemically. It was found that in the carrageenin-induced pleurisy, a single intrapleural injection of the selective inducible NO inhibitors S-(2-aminoethyl) isothiourea (AE-ITU; 3 and 10 mg/kg) and N-(3-(aminomethyl)-benzyl) acetamidine (1400W; 10 mg/kg) or the selective endothelial cell NOS inhibitor l-N5(1-iminoethyl)-ornithine (10 mg/kg) not only exacerbated inflammation at the very early stages of the lesion (1–6 h), but also prevented inflammatory resolution. By contrast, administering NOS inhibitors systemically ameliorated the severity of inflammation throughout the reaction. To elucidate the mechanisms by which inhibition of NO synthesis locally worsened inflammation, we found an increase in histamine, cytokine-induced neutrophil chemoattractant, superoxide, and leukotriene B4 levels at the inflammatory site. In conclusion, this work shows that the local production of NO is protective by virtue of its ability to regulate the release of typical proinflammatory mediators and, importantly, that NOS inhibitors have differential anti-inflammatory effects depending on their route of administration.

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Section: Discussionsupporting

confidence: 91%

Nitric Oxide Synthase Inhibitors Have Opposite Effects on Acute Inflammation Depending on Their Route of Administration

Paul-Clark

Gilroy

Willis

et al. 2001

The Journal of Immunology

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“…Acute administration of L-NAME reduced albumin extravasation and decreased local microvascular blood flow in rat (Hughes et al, 1990;Ialenti et al, 1993), guinea-pig (Teixeira et al, 1993) and rabbit (Mariani-Pedroso et al, 1995) skin, as well as edema formation in the paw (Antunes et al, 1990(Antunes et al, , 1992Ialenti et al, 1993;Giraldelo et al, 1994). Together, these findings indicate that NO is a key element for some relevant aspects of inflammation being most probably largely responsible for edema.…”

Section: Discussionmentioning

confidence: 79%

Diazepam effects on carrageenan-induced inflammatory paw edema in rats: Role of nitric oxide

Lazzarini

Maiorka

et al. 2006

Life Sciences

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“…1986). Heparin has also been shown to inhibit the increased vascular permeability induced by a variety of inflammatory mediators including histamine, bradykinin, prostaglandin El (Carr, 1979) and cationic proteins (Needham et al, 1988;Antunes et al, 1990;Sasaki et al, 1991). Evidence suggests that heparin can inhibit T-lymphocyte activation (Frieri & Metcalfe, 1983), trafficking (Sy et al, 1983;Willenborg & Parish, 1988;Lider et al, 1990) and delayed hypersensitivity responses (Frieri & Metcalfe, 1983;Sy et al, 1983;Lider et al, 1990) via a mechanism unrelated to its anti-coagulant properties.…”

Section: Introductionmentioning

confidence: 99%

Effect of heparin and a low‐molecular weight heparinoid on PAF‐induced airway responses in neonatally immunized rabbits

Sasaki

Herd

Page

1993

British J Pharmacology

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We have investigated the effect of an unfractionated heparin preparation, a low‐molecular weight heparinoid (Org 10172) and the polyanionic molecule polyglutamic acid against PAF‐induced airway hyperresponsiveness and pulmonary cell infiltration in neonatally immunized rabbits in vivo. Exposure of neonatally immunized rabbits to aerosolized platelet activating factor (PAF) (80 μg ml−1 for 60 min) elicited an increase in airway responsiveness to inhaled histamine 24 h and 72 h following challenge which was associated with an infiltration of inflammatory cells into the airways, as assessed by bronchoalveolar lavage (BAL). A significant increase in the total numbers of cells recovered from BAL fluid was associated with significantly increased cell numbers of neutrophils, eosinophils and mononuclear cells 24 h following PAF exposure. The numbers of eosinophils and neutrophils in the airways remained elevated 72 h after challenge. The intravenous administation of an unfractionated preparation of heparin (100 units kg−1) or Org 10172 (100 μg kg−1) 30 min prior to PAF exposure significantly inhibited the airway hyperresponsiveness induced by PAF, 24 h and 72 h following challenge. PAF‐induced hyperresponsiveness was not significantly affected by prior intravenous administration of polyglutamic acid (100 μg kg−1). The intravenous administration of unfractionated heparin (100 units kg−1), Org 10172 (100 μg kg−1) or polyglutamic acid (100 μg kg−1) 30 min prior to PAF exposure significantly inhibited the expected increase in total cell infiltration. This study shows that unfractionated heparin and a low‐molecular weight heparinoid, Org 10172, are capable of inhibiting both the airway hyperresponsiveness and pulmonary cell infiltration induced by PAF in the rabbit.

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Pharmacological characterization of polycation‐induced rat hind‐paw oedema

Cited by 41 publications

References 27 publications

Nitric Oxide Synthase Inhibitors Have Opposite Effects on Acute Inflammation Depending on Their Route of Administration

Nitric Oxide Synthase Inhibitors Have Opposite Effects on Acute Inflammation Depending on Their Route of Administration

Diazepam effects on carrageenan-induced inflammatory paw edema in rats: Role of nitric oxide

Effect of heparin and a low‐molecular weight heparinoid on PAF‐induced airway responses in neonatally immunized rabbits

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