首页> 外文期刊>Toxicon: An International Journal Devoted to the Exchange of Knowledge on the Poisons Derived from Animals, Plants and Microorganisms >Mast cells and histamine play an important role in edema and leukocyte recruitment induced by Potamotrygon motoro stingray venom in mice
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Mast cells and histamine play an important role in edema and leukocyte recruitment induced by Potamotrygon motoro stingray venom in mice

机译:肥大细胞和组胺在小鼠角斑病毒引起的水肿和白细胞募集中起重要作用

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This work aimed to investigate mechanisms underlying the inflammatory response caused by Potamotrygon motoro stingray venom (PmV) in mouse paws. Pre-treatment of animals with a mast cell degranulation inhibitor (cromolyn) diminished edema (62% of inhibition) and leukocyte influx into the site of PmV injection. Promethazine (histamine type 1 receptor antagonist) or thioperamide (histamine type 3 and 4 receptor antagonist) also decreased edema (up to 30%) and leukocyte numbers, mainly neutrophils (40-50 %). Cimetidine (histamine type 2 receptor antagonist) had no effect on PmV-induced inflammation. In the RBL-2H3 lineage of mast cells, PmV caused proper cell activation, in a dose-dependent manner, with release of PGD(2) and PGE(2). In addition, the role of COXs products on PmV inflammatory response was evaluated. Indomethacin (COX-1/COX-2 inhibitor) or etoricoxib (COX-2 inhibitor) partially diminished edema (around 20%) in PmV-injected mice. Indomethacin, but not etoricoxib, modulated neutrophil influx into the site of venom injection. In conclusion, mast cell degranulation and histamine, besides COXs products, play an important role in PmV-induced reaction. Since PmV mechanism of action remains unknown, hindering accurate treatment, clinical studies can be performed to validate the prescription of antihistaminic drugs, besides NSAIDs, to patients injured by freshwater stingrays. (C) 2015 Elsevier Ltd. All rights reserved.
机译:这项工作旨在调查潜在的机制,由小鼠爪中的马铃薯角斑病毒(PmV)引起的炎症反应。用肥大细胞脱粒抑制剂(cromolyn)预处理动物可减少水肿(抑制作用的62%)和白细胞流入PmV注射部位。异丙嗪(组胺1型受体拮抗剂)或硫代过酰胺(组胺3和4型受体拮抗剂)也可减少水肿(最多30%)和白细胞数量,主要是中性粒细胞(40-50%)。西咪替丁(2型组胺受体拮抗剂)对PmV诱导的炎症没有影响。在肥大细胞的RBL-2H3谱系中,PmV以剂量依赖性方式引起适当的细胞活化,并释放PGD(2)和PGE(2)。此外,还评估了COXs产品对PmV炎症反应的作用。消炎痛(COX-1 / COX-2抑制剂)或依托考昔(COX-2抑制剂)可部分减轻注射PmV的小鼠的水肿(约20%)。消炎痛而不是依托昔布调节嗜中性粒细胞流入毒液注射部位。总之,肥大细胞脱粒和组胺除COXs产物外,在PmV诱导的反应中也起重要作用。由于PmV的作用机理仍然未知,阻碍了准确的治疗,因此可以进行临床研究,以验证除NSAID以外的抗组胺药物对淡水黄貂鱼受伤的患者的处方。 (C)2015 Elsevier Ltd.保留所有权利。

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