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自身免疫小鼠狼疮性皮肤病的发病机制。X. 自身免疫小鼠皮肤中组胺 - N - 甲基转移酶活性的评估。

Pathogenesis of lupus dermatoses in autoimmune mice. X. Evaluation of histamine-N-methyltransferase activity in the skin of autoimmune.

作者信息

Furukawa F, Taniguchi S, Tachibana T, Horiguchi Y, Kanauchi H, Ohshio G, Hamashima Y, Imamura S

机构信息

Department of Dermatology, Faculty of Medicine, Kyoto University.

出版信息

Microbiol Immunol. 1988;32(1):83-96. doi: 10.1111/j.1348-0421.1988.tb01368.x.

Abstract

We measured histamine concentration and its metabolizing enzymes in the skin of MRL/Mp-lpr/lpr (MRL/l) and BXSB mice to clarify the contribution of histamine metabolism to the mechanisms of the development of lupus dermatoses. The concentration of histamine seemed to differ with the mouse strain. The activity of histamine-N-methyltransferase (HMT), one of two major metabolizing enzymes, was significantly lower in the tail and back skin of MRL/l mice at the age of 5 months than in the control MRL/Mp-+/+(MRL/n) mice, although there were no characteristic differences among several mouse strains of 1 mo of age. In the back skin of MRL/l mice, an age-dependent decrease of HMT activity was observed along with a corresponding decrease in histamine concentration, whereas an age-dependent increase of both HMT activity and histamine concentration was demonstrated in BXSB mice and other control mouse strains. Autoimmune-prone male BXSB mice and non-autoimmune female BXSB mice at 5 mo of age showed similar HMT activity. Corticosteroid treatment restored HMT activity in the skin of MRL/l mice but not in MRL/n mice. In addition, the change in HMT activity in MRL/l mice treated with corticosteroid appeared earlier than changes in clinicopathological examinations including skin eruptions, dermatopathology and proteinuria. Diamine oxidase (DAO) activity, another major metabolizing enzyme, was not detected in the skin of any autoimmune or control mouse strains. These findings suggest that the low activity of HMT in the skin of MRL/l mice plays a significant pathological role in the development of spontaneous lupus-like eruption. In other mouse strains, it is assumed that HMT activity is regulated by genetic factors.

摘要

我们检测了MRL/Mp-lpr/lpr(MRL/l)和BXSB小鼠皮肤中的组胺浓度及其代谢酶,以阐明组胺代谢在狼疮性皮肤病发病机制中的作用。组胺浓度似乎因小鼠品系而异。5月龄MRL/l小鼠尾巴和背部皮肤中两种主要代谢酶之一的组胺-N-甲基转移酶(HMT)活性显著低于对照MRL/Mp-+/+(MRL/n)小鼠,而1月龄的几种小鼠品系之间没有特征性差异。在MRL/l小鼠的背部皮肤中,观察到HMT活性随年龄下降,同时组胺浓度相应降低,而在BXSB小鼠和其他对照小鼠品系中,HMT活性和组胺浓度均随年龄增加。5月龄的自身免疫易感雄性BXSB小鼠和非自身免疫雌性BXSB小鼠表现出相似的HMT活性。皮质类固醇治疗可恢复MRL/l小鼠皮肤中的HMT活性,但不能恢复MRL/n小鼠的。此外,用皮质类固醇治疗的MRL/l小鼠中HMT活性的变化比包括皮疹、皮肤病理学和蛋白尿在内的临床病理检查变化出现得更早。另一种主要代谢酶二胺氧化酶(DAO)活性在任何自身免疫或对照小鼠品系的皮肤中均未检测到。这些发现表明,MRL/l小鼠皮肤中HMT活性低在自发性狼疮样皮疹的发生中起重要病理作用。在其他小鼠品系中,推测HMT活性受遗传因素调控。

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