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BSSL and PLRP2: key enzymes for lipid digestion in the newborn examined using the Caco-2 cell line

机译:BSSL和PLRP2:使用Caco-2细胞系检测新生儿脂质消化的关键酶

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摘要

In rodents, bile salt-stimulated lipase (BSSL) and pancreatic lipase-related protein 2 (PLRP2) are the dominant lipases expressed in the exocrine pancreas in early life when milk is the main food. The aim of the present study was to evaluate whether BSSL and PLRP2 are also key enzymes in neonatal intestinal fat digestion. Using Caco-2 cells as a model for the small intestinal epithelium, purified human enzymes were incubated in the apical compartment with substrates, bile salt composition and concentrations physiologic to newborn infants. Both BSSL and PLRP2 hydrolyzed triglycerides (TG) to free FA and glycerol. Released FA were absorbed by the cells and reesterfied to TG. Together, BSSL and PLRP2 had a synergistic effect, increasing cellular uptake and reesterification 4-fold compared with the sum of each lipase alone. A synergistic effect was also observed with retinyl ester as a substrate. PLRP2 hydrolyzed cholesteryl ester but not as efficiently as BSSL, and the two had an additive rather than synergistic effect. We conclude the key enzymes in intestinal fat digestion are different in newborns than later in life. Further studies are needed to fully understand this difference and its implication for designing optimal neonatal nutrition.
机译:在啮齿动物中,以牛奶为主要食物的胆汁盐刺激脂肪酶(BSSL)和胰腺脂肪酶相关蛋白2(PLRP2)是早期分泌在胰腺中的主要脂肪酶。本研究的目的是评估BSSL和PLRP2是否也是新生儿肠道脂肪消化中的关键酶。使用Caco-2细胞作为小肠上皮的模型,将纯化的人类酶与底物,胆汁盐组成和新生婴儿生理浓度一起在根尖区温育。 BSSL和PLRP2都将甘油三酸酯(TG)水解成游离的FA和甘油。释放的FA被细胞吸收并重新酯化为TG。与单独的每种脂肪酶的总和相比,BSSL和PLRP2共同具有协同作用,使细胞摄取和酯化增加4倍。以视黄酯为底物也观察到协同作用。 PLRP2水解胆甾醇酯,但不如BSSL高效,并且两者具有加成作用而不是协同作用。我们得出结论,新生儿肠道脂肪消化中的关键酶与生命后期不同。需要进一步研究以充分理解这种差异及其对设计最佳新生儿营养的意义。

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