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激肽释放酶、一氧化氮与热暴露大鼠颌下腺的血管反应

Kallikrein, nitric oxide and the vascular responses of the submaxillary glands in rats exposed to heat.

作者信息

Damas J

机构信息

Department of human Physiology, University of Liège, Belgium.

出版信息

Arch Int Physiol Biochim Biophys. 1994 Mar-Apr;102(2):139-46. doi: 10.3109/13813459408996122.

Abstract

During exposure of normal rats to an ambient temperature of 36 degrees C or 40 degrees C, body temperature increases; thermolytic processes are set up and saliva is spread on the skin. In Wistar rats, thermolytic salivation started when body temperature was above 39 degrees C. This water loss was associated with a loss of body weight. A 10% reduction of plasma volume was observed in animals exposed to 40 degrees C but no change was observed in those exposed to 36 degrees C. Body weight loss was reduced by hexamethonium, atropine, prazosin, HOE 140, a bradykinin-antagonist, and NG-nitro-L-arginine (NOARG), a NO synthase inhibitor. The weight and blood content of the submaxillary glands, which are the main effectors of the thermolytic processes, increased as a function of the ambient temperature. The increase of blood content was enhanced by hexamethonium but reduced by atropine and NOARG. The weight increase was inhibited by hexamethonium, prazosin, HOE 140 and NOARG. At an ambient temperature of 40 degrees C, a large swelling developed around the submaxillary glands, resulting in a distention of the surrounding soft tissues. This local oedema fluid contained low levels of endogenous proteins but accumulated exogenous labelled albumin. This swelling was enhanced by atropine but decreased by hexamethonium, trasylol, HOE 140, NOARG, ketoprofen, a cyclooxygenase inhibitor, and prazosin. In kininogen deficient rats, the blood content of submaxillary glands increased as a function of ambient temperature. No increase in glandular weight and no swelling of the of the soft tissues were observed. After atropine, the weight of the glands increased and a swelling of the soft tissues appeared.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

将正常大鼠置于36摄氏度或40摄氏度的环境温度下时,体温会升高;会启动散热过程,唾液会散布在皮肤上。在Wistar大鼠中,当体温高于39摄氏度时开始出现散热性流涎。这种水分流失与体重减轻有关。在暴露于40摄氏度的动物中观察到血浆量减少了10%,但在暴露于36摄氏度的动物中未观察到变化。六甲铵、阿托品、哌唑嗪、HOE 140(一种缓激肽拮抗剂)和NG-硝基-L-精氨酸(NOARG,一种一氧化氮合酶抑制剂)可减轻体重减轻。作为散热过程的主要效应器,颌下腺的重量和血液含量随环境温度的升高而增加。六甲铵可增强血液含量的增加,但阿托品和NOARG可使其降低。六甲铵、哌唑嗪、HOE 140和NOARG可抑制重量增加。在40摄氏度的环境温度下,颌下腺周围出现大量肿胀,导致周围软组织扩张。这种局部水肿液中内源性蛋白质含量低,但积聚了外源性标记白蛋白。阿托品可增强这种肿胀,但六甲铵、抑肽酶、HOE 140、NOARG、酮洛芬(一种环氧化酶抑制剂)和哌唑嗪可使其减轻。在激肽原缺乏的大鼠中,颌下腺的血液含量随环境温度的升高而增加。未观察到腺体重量增加和软组织肿胀。给予阿托品后,腺体重量增加,软组织出现肿胀。(摘要截取自250字)

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