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食物限制可延缓大鼠小肠与年龄相关的组织学变化。

Food restriction retards age-related histological changes in rat small intestine.

作者信息

Heller T D, Holt P R, Richardson A

机构信息

Department of Medicine, St. Luke's/Roosevelt Hospital Center, New York, New York.

出版信息

Gastroenterology. 1990 Feb;98(2):387-91. doi: 10.1016/0016-5085(90)90829-p.

Abstract

Previous studies have reported that small and large intestinal crypt hyperplasia and hyperproliferation occur in senescent rats about 27 mo of age. We have studied duodenal and ileal architecture in ad libitum chow-fed rats and have demonstrated that the increase in duodenal crypt depth and crypt hyperplasia do not develop throughout the life span, but become apparent at 21 and 27 mo of age. These crypt hyperplastic features occur without a change in duodenal villus cell number. Ileal villus cellularity increased throughout the life span, suggesting exposure to a gradually increasing luminal nutrient load. Diet restriction to 60% of the ad libitum feeding rate prolonged the life span of animals from 27 to greater than 33 mo and prevented both the duodenal hyperplasia and the increase in ileal villus cell numbers to the age of 27 mo. Thirty-three-month diet-restricted rats did show evidence of duodenal crypt hyperplasia. We conclude that proximal intestinal hyperplasia is a phenomenon that develops in advanced age, but that ileal villus cellularity increases throughout the ad libitum-fed rodent life span. Diet restriction dramatically retards these intestinal changes that are seen with ad libitum feeding and provides an experimental model for the study of age-related cellular changes of the rodent gastrointestinal tract.

摘要

先前的研究报道,27月龄左右的衰老大鼠会出现小肠和大肠隐窝增生及过度增殖。我们研究了自由采食大鼠的十二指肠和回肠结构,结果表明,十二指肠隐窝深度增加和隐窝增生并非在整个生命周期中都会出现,而是在21月龄和27月龄时才变得明显。这些隐窝增生特征出现时,十二指肠绒毛细胞数量并无变化。回肠绒毛细胞数量在整个生命周期中都有所增加,这表明其受到逐渐增加的肠腔营养负荷的影响。将饮食限制在自由采食速率的60%,可使动物的寿命从27月龄延长至33月龄以上,并可防止十二指肠增生以及回肠绒毛细胞数量在27月龄前增加。33月龄的饮食限制大鼠确实出现了十二指肠隐窝增生的迹象。我们得出结论,近端肠道增生是一种在老年时出现的现象,但回肠绒毛细胞数量在自由采食的啮齿动物整个生命周期中都会增加。饮食限制显著延缓了自由采食时出现的这些肠道变化,并为研究啮齿动物胃肠道与年龄相关的细胞变化提供了一个实验模型。

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