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乳源性胰岛素样生长因子-I被乳鼠门静脉血吸收。

Absorption of milk-borne insulin-like growth factor-I into portal blood of suckling rats.

作者信息

Philipps A F, Dvorák B, Kling P J, Grille J G, Koldovský O

机构信息

Department of Pediatrics, University of California Davis, Sacramento 95817, USA.

出版信息

J Pediatr Gastroenterol Nutr. 2000 Aug;31(2):128-35. doi: 10.1097/00005176-200008000-00008.

DOI:10.1097/00005176-200008000-00008
PMID:10941963
Abstract

BACKGROUND

Insulin-like growth factors (IGFs) are potent mitogens that have been implicated in control of growth and development during the perinatal period. These hormones are also present in biologically significant quantities in mammalian milks. Although one site of action of these IGFs may be at the intestinal level, current information about whether they pass intact into the circulation is conflicting.

METHODS

To test the hypothesis that milk-borne IGFs are absorbed into blood in receptor-active form, suckling rats were given either recombinant human (rh)125I-IGF-I or -II (4 x 10(6) counts per minute [cpm]), and the activity present in portal and cardiac blood was examined at 5, 10, 20, and 30 minutes after ingestion for presence of appropriate molecular weight peptides in these samples. In selected samples, purified radioactive samples were tested for their ability to bind competitively to crude membranes bearing IGF receptors.

RESULTS

The results of these studies indicate that rh125I-IGF-I is absorbed in receptor-active form into the portal circulation and that maximal amounts are present 20 to 30 minutes after ingestion. Estimation of the presence of intact hormone was made on the basis of the elution profile of samples when run on gel chromatography as well as reversed-phase high-performance liquid chromatography. Isolated samples from portal blood also bound competitively to placental membranes bearing IGF receptors. In contrast, rh125I-IGF-II could not be demonstrated in receptor-active form in portal blood. Chromatography showed appropriate sized peaks with greater activity in portal than cardiac samples, but competitive binding was not appreciated.

CONCLUSIONS

It is likely that at least milk-borne IGF-I is absorbed intact and may exert effects on liver and other peripheral tissues. In addition, this study lends further credence to the possibility of an enterohepatic circulation for IGF-I.

摘要

背景

胰岛素样生长因子(IGFs)是强效的有丝分裂原,与围产期生长发育的调控有关。这些激素在哺乳动物乳汁中也以具有生物学意义的量存在。尽管这些IGFs的一个作用位点可能在肠道水平,但目前关于它们是否完整进入循环的信息相互矛盾。

方法

为了检验乳汁中IGFs以受体活性形式被吸收进入血液这一假说,给哺乳大鼠注射重组人(rh)125I-IGF-I或-II(4×10⁶每分钟计数[cpm]),并在摄入后5、10、20和30分钟检测门静脉血和心脏血中的活性,以检查这些样本中是否存在适当分子量的肽。在选定样本中,测试纯化的放射性样本与携带IGF受体的粗制膜竞争性结合的能力。

结果

这些研究结果表明,rh125I-IGF-I以受体活性形式被吸收进入门静脉循环,摄入后20至30分钟含量最高。根据凝胶色谱和反相高效液相色谱上样本的洗脱图谱估计完整激素的存在情况。从门静脉血中分离的样本也与携带IGF受体的胎盘膜竞争性结合。相比之下,在门静脉血中未检测到rh125I-IGF-II以受体活性形式存在。色谱分析显示门静脉样本中具有适当大小的峰且活性高于心脏样本,但未观察到竞争性结合。

结论

很可能至少乳汁中的IGF-I是完整吸收的,并可能对肝脏和其他外周组织产生影响。此外,这项研究进一步支持了IGF-I存在肠肝循环的可能性。

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