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首页> 外文期刊>Reproduction, fertility, and development >Fetal organ growth in response to oesophageal infusion of amniotic fluid, colostrum, milk or gastrin-releasing peptide: a study in fetal sheep
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Fetal organ growth in response to oesophageal infusion of amniotic fluid, colostrum, milk or gastrin-releasing peptide: a study in fetal sheep

机译:食道输注羊水,初乳,牛奶或释放胃泌素的胎儿器官的生长:在胎羊中的一项研究

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摘要

The hypothesis of the present study was that the infusion of the biological fluids to which the developing gut is normally exposed (i.e. amniotic fluid, colostrum, milk) and a single growth factor (gastrin-releasing peptide), which is found in high concentrations in fetal fluids and milk, could ameliorate the altered growth induced by the elimination of swallowed input secondary to ligation of the oesophagus. At 108-110 days of gestation the fetal oesophagus was ligated and a catheter inserted towards the stomach (32 fetuses). At 117-119 days of gestation saline (n = 5), amniotic fluid (n = 5), colostral whey (n = 5), milk whey (n = 5) or gastrin-releasing peptide (3.6 nmol day~(-1), n = 6), was infused for 7 days (4 X 20 mL day~(-1)), or no infusion was given (ligated group, n = 6). A further 15 fetuses were not ligated (normal group, n = 15). All fetuses had carotid artery and/or jugular vein catheters implanted. At 124-126 days of gestation the fetus was delivered and fetal body and organ weights recorded. Analysing the results by ANOVA, there were no effects of either ligation alone or infusion after ligation on fetal weight, crown-rump length, or weight relative to bodyweight of heart, adrenal, pancreas, large intestine and cecum. There were significant differences between the infusion groups for lungs, kidney, pancreas, total gut, abomasum, small intestine, spleen, chest and neck thymus, and mesenteric lymph nodes. Ligation alone significantly reduced small intestinal growth and increased kidney and spleen growth. Colostrum infusion enhanced growth of most organs. Gastrin- releasing peptide significantly increased growth of all the immune organs studied. It was concluded that at an age when premature delivery could be encountered, the fetal gut is capable of significant adaptive growth, to varying degrees, depending on the enteral diet. Growth effects in organs distant to the gut suggest that either gastrointestinal uptake and transport of growth factors or altered nutrient uptake and/or availability can affect the growth of other major fetal organs.
机译:本研究的假设是,输注发育中的肠道通常所接触的生物液体(例如羊水,初乳,牛奶)和单一生长因子(释放胃泌素的肽),其浓度很高。胎液和牛奶可以减轻因食管结扎引起的吞咽输入消除而引起的生长改变。在妊娠108-110天时结扎胎儿食道,并向胃内插入导管(32胎)。妊娠117-119天时,生理盐水(n = 5),羊水(n = 5),初乳(n = 5),乳清(n = 5)或释放胃泌素的肽(3.6 nmol day〜(-1) )(n = 6),输注7天(4 X 20 mL day〜(-1)),或不输注(结扎组,n = 6)。未结扎另外15个胎儿(正常组,n = 15)。所有胎儿均植入了颈动脉和/或颈静脉导管。妊娠124-126天时,胎儿已分娩并记录了胎儿的体重和器官重量。通过ANOVA分析结果,单独结扎或结扎后输注对胎儿体重,冠状臀围长度或相对于心脏,肾上腺,胰腺,大肠和盲肠的体重而言均无影响。输液组之间在肺,肾,胰腺,全肠,厌恶,小肠,脾脏,胸颈部和胸腺以及肠系膜淋巴结之间存在显着差异。单独结扎可明显减少小肠生长,并增加肾脏和脾脏的生长。初乳注入促进大多数器官的生长。释放胃泌素的肽显着增加了所有研究的免疫器官的生长。结论是,在可能遇到早产的年龄,根据肠道饮食的不同,胎儿的肠道能够在不同程度上显着适应性生长。在远离肠道的器官中的生长效应表明,胃肠道对生长因子的摄取和运输或营养素摄取和/或利用率的改变都可能影响其他主要胎儿器官的生长。

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