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L-谷氨酰胺和转化生长因子-α可增强猪缺血后回肠中单酰甘油酰基转移酶和二酰甘油酰基转移酶活性的恢复。

L-glutamine and transforming growth factor-alpha enhance recovery of monoacylglycerol acyltransferase and diacylglycerol acyltransferase activity in porcine postischemic ileum.

作者信息

Ahdieh N, Blikslager A T, Bhat B G, Coleman R A, Argenzio R A, Rhoads J M

机构信息

Department of Nutrition, Center for Gastrointestinal Biology and Disease, University of North Carolina, Chapel Hill 27599-7220, USA.

出版信息

Pediatr Res. 1998 Feb;43(2):227-33. doi: 10.1203/00006450-199802000-00012.

Abstract

Recovery of the ability to digest and absorb lipids is essential to the maintenance of normal nutrition in infants with bowel damage. Two intrinsic microsomal enzymes, monoacylglycerol acyltransferase (MGAT) and diacylglycerol acyltransferase (DGAT), catalyze the major pathway for intestinal triacylglycerol biosynthesis. This study describes the effects of intestinal ischemia on epithelial DGAT and MGAT activities and their recovery in response to two luminal treatments: L-glutamine (Gln), the primary intestinal fuel, and transforming growth factor-alpha (TGF-alpha), a mitogenic hormone similar to epidermal growth factor present in breast milk. Ischemic damage and recovery were analyzed in mucosa from Thiry-Vella loops in the mid-ileum of 7-wk-old pigs. Loops were subjected to 2-h occlusion of local mesenteric arteries, followed by 6 or 72 h of recovery in the presence of luminal glucose (control), Gln, or TGF-alpha. Ischemic tissue followed by 6-h recovery exhibited an approximate 50% decrease in both MGAT and DGAT activities compared with nonischemic loop tissue. At 72 h, MGAT and DGAT recovery in Gln plus TGF-alpha-treated loops was significantly greater than their corresponding 6-h peak damage levels (p < 0.05). From 6 to 72 h, MGAT increased 4-fold and DGAT increased 3.6-fold after Gln plus TGF-alpha treatment. With other treatments, MGAT and DGAT activities increased <2.5-fold from 6 to 72 h. This study shows that intestinal MGAT and DGAT activities decrease after ischemic damage, yet recover rapidly in bowel exposed to Gln and/or TGF-alpha. By stimulating the rate of recovery of the villi and lipid synthesizing enzymes, these treatments could improve the efficacy of enteral feeding in infants recovering from bowel damage.

摘要

消化和吸收脂质能力的恢复对于肠道受损婴儿维持正常营养至关重要。两种内在微粒体酶,单酰甘油酰基转移酶(MGAT)和二酰甘油酰基转移酶(DGAT),催化肠道三酰甘油生物合成的主要途径。本研究描述了肠道缺血对上皮细胞DGAT和MGAT活性的影响,以及它们对两种肠腔处理的反应恢复情况:L-谷氨酰胺(Gln),主要的肠道燃料,以及转化生长因子-α(TGF-α),一种与母乳中存在的表皮生长因子类似的促有丝分裂激素。对7周龄猪回肠中段Thiry-Vella肠袢的黏膜进行缺血损伤和恢复分析。肠袢接受局部肠系膜动脉2小时的闭塞,随后在存在肠腔葡萄糖(对照)、Gln或TGF-α的情况下恢复6或72小时。与非缺血肠袢组织相比,缺血组织恢复6小时后,MGAT和DGAT活性均下降约50%。在72小时时,Gln加TGF-α处理的肠袢中MGAT和DGAT的恢复明显高于其相应的6小时峰值损伤水平(p<0.05)。从6小时到72小时,Gln加TGF-α处理后MGAT增加了4倍,DGAT增加了3.6倍。采用其他处理时,MGAT和DGAT活性从6小时到72小时增加<2.5倍。本研究表明,肠道缺血损伤后MGAT和DGAT活性降低,但在暴露于Gln和/或TGF-α的肠道中恢复迅速。通过刺激绒毛和脂质合成酶的恢复速度,这些处理可以提高肠内喂养对肠道损伤恢复中婴儿的疗效。

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