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经肠腔给予胰岛素样生长因子-I对胎羊胃肠道生长的调节作用。

Regulation of gastrointestinal growth in fetal sheep by luminally administered insulin-like growth factor-I.

作者信息

Trahair J F, Wing S J, Quinn K J, Owens P C

机构信息

Department of Anatomy and Histology, University of Adelaide, Australia.

出版信息

J Endocrinol. 1997 Jan;152(1):29-38. doi: 10.1677/joe.0.1520029.

DOI:10.1677/joe.0.1520029
PMID:9014837
Abstract

Fetuses swallow large volumes of amniotic fluid. Absence of swallowing results in gastrointestinal tract (GIT) growth deficits. While it is not yet known to what extent the growth factors present in amniotic fluid are involved in GIT ontogeny, milk-derived growth factors are considered to be important for neonatal growth. Our experiment tested the hypothesis that a luminal growth factor (insulin-like growth factor-I, IGF-I) can sustain or promote GIT growth in utero in a model of gastrointestinal tract growth retardation. Ten-day infusion of either human recombinant IGF-I or vehicle into twin fetal sheep at 80 days gestation via an indwelling esophageal catheter resulted in altered GIT growth. Weight of the forestomach and small intestine increased. Significant histological changes were noted in the proximal small intestine, i.e. the region most exposed to the luminal infusion. Mucosal tissues were reduced in size. While the enterocytes in the proximal small intestine were generally more mature with regard to the ontogeny of the apical endocytic complex (which is responsible for uptake and transport of whole peptides), there were also many abnormal cytological features present. These included the development of large lysosomal-like inclusion bodies and many surfactant-like particles within the apical cytoplasm. Plasma IGF-I levels were on average 20% higher in treated siblings, suggesting that luminal IGF-I crossed the fetal gut and entered blood. IGF-II levels were not significantly affected. These observations are consistent with the suggestion that growth factors, which are present in swallowed amniotic fluid, influence fetal ontogeny.

摘要

胎儿会吞咽大量羊水。无法吞咽会导致胃肠道(GIT)生长发育迟缓。虽然目前尚不清楚羊水中存在的生长因子在多大程度上参与胃肠道个体发育,但源自乳汁的生长因子被认为对新生儿生长很重要。我们的实验检验了这样一个假设:在胃肠道生长发育迟缓模型中,一种腔内生长因子(胰岛素样生长因子-I,IGF-I)能够维持或促进子宫内胃肠道的生长。在妊娠80天时,通过留置食管导管向双胎胎羊体内输注人重组IGF-I或赋形剂,持续10天,结果导致胃肠道生长发生改变。前胃和小肠的重量增加。在近端小肠(即最暴露于腔内输注的区域)观察到显著的组织学变化。黏膜组织尺寸减小。虽然近端小肠中的肠上皮细胞在顶端内吞复合体(负责摄取和转运完整肽段)的个体发育方面总体上更成熟,但也存在许多异常细胞学特征。这些特征包括顶端细胞质中出现大的溶酶体样包涵体和许多表面活性剂样颗粒。接受治疗的胎羊的血浆IGF-I水平平均高出20%,这表明腔内IGF-I穿过胎儿肠道并进入血液。IGF-II水平未受到显著影响。这些观察结果与以下观点一致:吞咽的羊水中存在的生长因子会影响胎儿个体发育。

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Regulation of gastrointestinal growth in fetal sheep by luminally administered insulin-like growth factor-I.经肠腔给予胰岛素样生长因子-I对胎羊胃肠道生长的调节作用。
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