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咪唑斯汀对实验性结肠炎期间内脏感觉传入敏感性和炎症的影响。

Effect of mizolastine on visceral sensory afferent sensitivity and inflammation during experimental colitis.

作者信息

Goldhill J, Pichat P, Roome N, Angel I, Arbilla S

机构信息

Synthélabo Recherche, Rueil-Malmaison France.

出版信息

Arzneimittelforschung. 1998 Feb;48(2):179-84.

PMID:9541730
Abstract

In the present study the effect of mizolastine (CAS 108612-45-9, SL85.0324-00) a novel potent histamine H1-receptor antagonist, on 2,4,6-trinitrobenzene sulphonic acid (TNBS)-induced colitis, a rat model of inflammatory bowel disease, was investigated to determine whether mizolastine has anti-inflammatory properties. Treatment with TNBS resulted in increased nociception in response to rectal balloon distension and caused intestinal damage, tissue oedema and inflammation. Oral mizolastine (0.03-3.00 mg/kg given 1 h before and once daily for 3 days after TNBS treatment) significantly (p < 0.05) reduced nociception (49% at 0.3 mg/kg), gross intestinal damage (78% at 3.0 mg/kg), histological damage (54% at 3.0 mg/kg), intestinal tissue weight (69% at 3.0 mg/kg) and myeloperoxidase activity (66% at 3.0 mg/kg). In contrast, the H1-receptor antagonist terfenadine tested under the same experimental conditions at 3-30 mg/kg was without significant effect. It is concluded that, in addition to its antiallergic properties, mizolastine possesses anti-inflammatory actions that may not be related to its H1-receptor blocking properties, reducing sensory afferent hypersensitivity, damage and neutrophil infiltration observed during colitis.

摘要

在本研究中,考察了新型强效组胺H1受体拮抗剂咪唑斯汀(CAS 108612-45-9,SL85.0324-00)对2,4,6-三硝基苯磺酸(TNBS)诱导的结肠炎(一种炎症性肠病大鼠模型)的影响,以确定咪唑斯汀是否具有抗炎特性。用TNBS处理导致对直肠气囊扩张的伤害感受增加,并引起肠道损伤、组织水肿和炎症。口服咪唑斯汀(在TNBS处理前1小时给予0.03 - 3.00 mg/kg,并在处理后每天一次,共3天)显著(p < 0.05)降低了伤害感受(0.3 mg/kg时降低49%)、大体肠道损伤(3.0 mg/kg时降低78%)、组织学损伤(3.0 mg/kg时降低54%)、肠道组织重量(3.0 mg/kg时降低69%)和髓过氧化物酶活性(3.0 mg/kg时降低66%)。相比之下,在相同实验条件下以3 - 30 mg/kg测试的H1受体拮抗剂特非那定没有显著效果。得出的结论是,除了其抗过敏特性外,咪唑斯汀还具有抗炎作用,这可能与其H1受体阻断特性无关,可减轻结肠炎期间观察到的感觉传入超敏反应、损伤和中性粒细胞浸润。

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