口服igf - 1改变了配方喂养的新生猪的翻译后加工过程,但没有改变乳糖酶-苯二酚水解酶的活性。

D. Burrin, B. Stoll, M. Fan, M. Dudley, S. Donovan, P. Reeds
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引用次数: 29

摘要

为了确定口服胰岛素样生长因子I (IGF-I)增加肠道乳糖酶-苯丙素水解酶(LPH)活性的细胞机制,我们研究了2岁仔猪饲喂牛奶配方奶粉(对照组,n = 5),配方奶粉+低IGF-I (0.5 mg/L;n = 6)或配方+高IGF-I (12.0 mg/L, n = 6),持续15 d。在第15天,通过6小时静脉注射多种稳定同位素(2H(3)-Leu、13C(1)-Leu、13C(1)-Phe、2H(5)-Phe、13C(6)-Phe和13C(9)-Phe),在体内测量肠道蛋白质合成和乳糖酶加工。同时对空肠和回肠进行形态测定和细胞增殖测定。两种剂量的igf - 1均不影响湿组织、蛋白质或DNA的质量,也不影响绒毛高度、细胞增殖或lph特异性活性。口服igf - 1可降低回肠泌乳酶-苯丙醇水解酶(pro-LPH)的合成和丰度,但可增加回肠刷边酶(BB)-LPH的合成。饲喂igf的猪的BB-LPH加工效率是对照组的2 - 3倍。在所有猪中,回肠的绒毛高度、总粘膜和LPH活性比活性均高于空肠,但BB-LPH的合成在回肠显著低于空肠。我们得出结论,口服IGF-I增加了pro-LPH到BB-LPH的加工效率,但不影响LPH活性。此外,BB-LPH在回肠的翻译后加工明显低于空肠。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Oral IGF-I alters the posttranslational processing but not the activity of lactase-phlorizin hydrolase in formula-fed neonatal pigs.
To determine the cellular mechanism whereby oral insulin-like growth factor I (IGF-I) increases intestinal lactase-phlorizin hydrolase (LPH) activity, we studied 2-d-old pigs fed cow's milk formula (control, n = 5), formula + low IGF-I (0.5 mg/L; n = 6) or formula + high IGF-I (12.0 mg/L, n = 6) for 15 d. On d 15, intestinal protein synthesis and lactase processing were measured in vivo in fed pigs using a 6-h intravenous, overlapping infusion of multiple stable isotopes (2H(3)-Leu, 13C(1)-Leu, 13C(1)-Phe, 2H(5)-Phe, 13C(6)-Phe and 13C(9)-Phe). Morphometry and cell proliferation also were measured in the jejunum and ileum. Neither dose of IGF-I affected the masses of wet tissue, protein or DNA, or the villus height, cell proliferation or LPH-specific activity. Oral IGF-I decreased the synthesis and abundance of prolactase-phlorizin hydrolase (pro-LPH), but increased brush-border (BB)-LPH synthesis in the ileum. The BB-LPH processing efficiency was twofold to threefold greater in IGF-fed than in control pigs. In all pigs, villus height and the total mucosal and specific activity of LPH activity were greater in the ileum than in the jejunum, yet the synthesis of BB-LPH were significantly lower in the ileum than in the jejunum. We conclude that oral IGF-I increases the processing efficiency of pro-LPH to BB-LPH but does not affect LPH activity. Moreover, the posttranslational processing of BB-LPH is markedly lower in the ileum than in the jejunum.
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