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组胺超敏反应及β肾上腺素能阻滞剂所致小鼠全身性过敏反应:核苷酸的保护作用

Hypersensitivity to histamine and systemic anaphylaxis in mice with pharmacologic beta adrenergic blockade: protection by nucleotides.

作者信息

Matsumura Y, Tan E M, Vaughan J H

出版信息

J Allergy Clin Immunol. 1976 Sep;58(3):387-94. doi: 10.1016/0091-6749(76)90119-6.

Abstract

The effects of exogenous nucleotides on the histamine hypersensitivity of pharmacologically beta-blocked mice were investigated. Female HLA-SW (ICR) mice, 27-29 gm, were injected intraperitoneally with 20 to 100 mug of propranolol 45 min before intraperitoneal challenge with 1 mg histamine. These animals had a mortality which averaged approximately 80%. At various time intervals before histamine, doses of from 0.5 to 12 mumoles of nucleotides were administered intravenously. Noncyclic nucleotides, adenosine, adenosine 5'-monophosphate (AMP), and guanosine 5'-monophosphate (GMP) showed clear, dose-response protection against histamine death of propranolol-treated mice when they were given 45 to 90 min before histamine. Cyclic AMP showed significant protection only when it was given at a dose of 8 mumoles 45 to 90 min before histamine, and lower or higher doses gave equivocal or no protection. Cyclic GMP WAS Not protective at any dose tested. Propranolol treatment also produced enhanced sensitivity to passive systemic anaphylaxis. Mice were passively sensitized by intraperitoneal injection of mouse anti-egg albumin antibody 6 hr before intravenous challenge with 0.5 mg egg albumin. The mortality from anaphylaxis in the group treated with 20 mug propranolol 45 min before antigen challenge increased to 83%, while that of the group not given propranolol was only 10%. Nucleotides were given intravenously 45 min before antigen challenge. The nucleotides that protected mice from death due to histamine challenge also protected them from death due to systemic anaphylaxis. These protective nucleotides were the same nucleotides that had been reported previously to be protective against Bordetella pertussis-induced hypersensitivity to histamine and anaphylaxis.

摘要

研究了外源性核苷酸对药理学β受体阻滞剂处理小鼠组胺超敏反应的影响。选用体重27 - 29克的雌性HLA - SW(ICR)小鼠,在腹腔注射1毫克组胺前45分钟,腹腔注射20至100微克普萘洛尔。这些动物的死亡率平均约为80%。在组胺攻击前的不同时间间隔,静脉注射0.5至12微摩尔的核苷酸。非环状核苷酸,腺苷、腺苷5'-单磷酸(AMP)和鸟苷5'-单磷酸(GMP),在组胺攻击前45至90分钟给予时,对普萘洛尔处理小鼠的组胺致死表现出明显的剂量反应性保护作用。环磷腺苷仅在组胺攻击前45至90分钟以8微摩尔的剂量给予时显示出显著的保护作用,较低或较高剂量的保护作用不明确或无保护作用。环磷鸟苷在任何测试剂量下均无保护作用。普萘洛尔处理还导致对被动全身性过敏反应的敏感性增强。在静脉注射0.5毫克卵清蛋白前6小时,通过腹腔注射小鼠抗卵清蛋白抗体使小鼠被动致敏。在抗原攻击前45分钟用20微克普萘洛尔处理的组中,过敏反应的死亡率增加到83%,而未给予普萘洛尔的组仅为10%。在抗原攻击前45分钟静脉给予核苷酸。能保护小鼠免于组胺攻击致死的核苷酸,也能保护它们免于全身性过敏反应致死。这些具有保护作用的核苷酸与先前报道的对百日咳博德特氏菌诱导的组胺超敏反应和过敏反应具有保护作用的核苷酸相同。

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