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胆囊收缩素-A(-1)、-B(-2)受体缺陷型小鼠在禁食时缺乏胃饥饿素分泌。

Lack of ghrelin secretion in response to fasting in cholecystokinin-A (-1), -B (-2) receptor-deficient mice.

作者信息

Sakurai Chihiro, Ohta Minoru, Kanai Setsuko, Uematsu Hiroshi, Funakoshi Akihiro, Miyasaka Kyoko

机构信息

Department of Clinical Physiology, Tokyo Metropolitan Institute of Gerontology, Tokyo, 173-0015 Japan.

出版信息

J Physiol Sci. 2006 Dec;56(6):441-7. doi: 10.2170/physiolsci.RP003306. Epub 2006 Dec 1.

Abstract

Cholecystokinin receptors (CCK-Rs) have been classified into two subtypes: CCK-AR (1R) and -BR (2R). We generated CCK-AR(-/-), CCK-BR(-/-), and CCK-AR(-/-)BR(-/-) mice and found that the gastric emptying of a liquid meal was increased in CCK-BR(-/-) and AR(-/-)BR(-/-) mice, compared with wild-type and CCK-AR(-/-) mice. Given that enhanced gastric emptying leads to eating, food intake after overnight fasting was examined, as was the effect of CCK-8S on food intake. Male mice 6-8 months of age were deprived of food for 16 h with free access to water, after which they were injected intraperitoneally (0.1 ml/mouse) with either vehicle or CCK-8 (0.3, 1.0, or 3.0 nmol/mouse), and their food intake was monitored for 4 h. CCK-8S inhibited food intake in wild-type and CCK-BR(-/-) mice, but not in CCK-AR(-/-) or AR(-/-)BR(-/-) mice. Unexpectedly, we observed a lower food intake in CCK-AR(-/-)BR (-/-) mice treated with vehicle than in mice of the other genotypes. To examine the mechanism of decrease in food intake in CCK-AR(-/-)BR(-/-) mice, the involvement of ghrelin was determined in wild-type and CCK-AR(-/-)BR(-/-) mice. Fasting plasma ghrelin levels were significantly lower in CCK-AR (-/-)BR(-/-) mice than in wild-type mice, and no increase in response to fasting was observed in CCK-AR(-/-)BR(-/-) mice. An administration of acyl-ghrelin produced a small increase in food intake in CCK-AR(-/-)BR(-/-) mice, but not to the levels of wild-type mice. In conclusion, CCK-AR(-/-)BR(-/-) mice showed lower food intake as well as lower response to exogenous ghrelin, and a lower plasma ghrelin level after fasting, though which receptor is more important is unknown.

摘要

胆囊收缩素受体(CCK-Rs)已被分为两种亚型:CCK-AR(1R)和-BR(2R)。我们培育出了CCK-AR(-/-)、CCK-BR(-/-)和CCK-AR(-/-)BR(-/-)小鼠,并发现与野生型和CCK-AR(-/-)小鼠相比,CCK-BR(-/-)和AR(-/-)BR(-/-)小鼠的流食胃排空有所增加。鉴于胃排空增强会导致进食,我们检测了禁食过夜后的食物摄入量以及CCK-8S对食物摄入量的影响。6至8月龄的雄性小鼠禁食16小时,可自由饮水,之后腹腔注射(0.1毫升/只)溶剂或CCK-8(0.3、1.0或3.0纳摩尔/只),并监测其4小时的食物摄入量。CCK-8S抑制野生型和CCK-BR(-/-)小鼠的食物摄入,但不抑制CCK-AR(-/-)或AR(-/-)BR(-/-)小鼠的食物摄入。出乎意料的是,我们观察到注射溶剂的CCK-AR(-/-)BR(-/-)小鼠的食物摄入量低于其他基因型的小鼠。为了研究CCK-AR(-/-)BR(-/-)小鼠食物摄入量减少的机制,我们在野生型和CCK-AR(-/-)BR(-/-)小鼠中确定了胃饥饿素的作用。CCK-AR(-/-)BR(-/-)小鼠的空腹血浆胃饥饿素水平显著低于野生型小鼠,且CCK-AR(-/-)BR(-/-)小鼠对禁食无反应增加。给予酰基胃饥饿素使CCK-AR(-/-)BR(-/-)小鼠的食物摄入量略有增加,但未达到野生型小鼠的水平。总之,CCK-AR(-/-)BR(-/-)小鼠表现出较低的食物摄入量、对外源性胃饥饿素的较低反应以及禁食后较低的血浆胃饥饿素水平,不过哪种受体更重要尚不清楚。

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