Ethanol consumption during gestation promotes placental alterations in IGF-1 deficient mouse placentas.

Q2 Pharmacology, Toxicology and Pharmaceutics F1000Research Pub Date : 2024-10-31 eCollection Date: 2021-01-01 DOI:10.12688/f1000research.75116.1
Irene Martín-Estal, Oscar R Fajardo-Ramírez, Mario Bermúdez De León, Carolina Zertuche-Mery, Diego Rodríguez-Mendoza, Patricio Gómez-Álvarez, Marcela Galindo-Rangel, Andrea Leal López, Inma Castilla-Cortázar, Fabiola Castorena-Torres
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Abstract

Background: During pregnancy, the placenta is an extremely important organ as it secretes its own hormones, e.g. insulin-like growth factor 1 (IGF-1), to ensure proper intrauterine fetal growth and development. Ethanol, an addictive and widely used drug, has numerous adverse effects during pregnancy, including fetal growth restriction (FGR). To date, the molecular mechanisms by which ethanol triggers its toxic effects during pregnancy, particularly in the placenta, are not entirely known. For this reason, a murine model of partial IGF-1 deficiency was used to determine ethanol alterations in placental morphology and aspartyl/asparaginyl β-hydroxylase (AAH) expression.

Methods: Wild type (WT, Igf1 +/+) and heterozygous (HZ, Igf1 +/-) female mice were given 10% ethanol in water during 14 days as an acclimation period and throughout pregnancy. WT and HZ female mice given water were used as controls. At gestational day 19, pregnant dams were sacrificed, placentas were collected and genotyped for subsequent studies.

Results: IGF-1 deficiency and ethanol consumption during pregnancy altered placental morphology, and decreased placental efficiency and AAH expression in placentas from all genotypes. No differences were found in Igf1, Igf2, Igf1r and Igf2r mRNA expression in placentas from all groups.

Conclusions: IGF-1 deficiency and ethanol consumption throughout gestation altered placental development, suggesting the crucial role of IGF-1 in the establishment of an adequate intrauterine environment that allows fetal growth. However, more studies are needed to study the precise mechanism to stablish the relation between both insults.

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妊娠期间的乙醇消耗促进了IGF-1缺陷小鼠胎盘的改变
背景:在怀孕期间,胎盘是一个极其重要的器官,因为它会分泌自己的激素,如胰岛素样生长因子1(IGF-1),以确保胎儿在宫内正常生长发育。乙醇是一种成瘾且广泛使用的药物,在怀孕期间会产生许多不良反应,包括胎儿生长受限(FGR)。到目前为止,乙醇在怀孕期间,特别是在胎盘中引发毒性作用的分子机制尚不完全清楚。出于这个原因,使用部分IGF-1缺乏的小鼠模型来确定胎盘形态和AAH表达的乙醇改变。方法:在14天的驯化期和整个妊娠期给杂合(HZ,Igf1+/-)雌性小鼠10%乙醇。给予水的HZ雌性小鼠用作对照。在妊娠第19天,处死怀孕的母鼠,收集胎盘并进行基因分型,以进行后续研究。结果:妊娠期IGF-1缺乏和乙醇消耗改变了胎盘形态,降低了胎盘效率和所有基因型胎盘中天冬氨酰/天冬酰胺基β-羟化酶(AAH)的表达。各组胎盘中Igf1、Igf2、Igf1r和Igf2r mRNA表达均无差异。结论:IGF-1缺乏和整个妊娠期的乙醇消耗改变了胎盘发育,表明IGF-1在建立允许胎儿生长的适当宫内环境中发挥着至关重要的作用。然而,还需要更多的研究来研究建立这两种侮辱之间关系的确切机制。
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来源期刊
F1000Research
F1000Research Pharmacology, Toxicology and Pharmaceutics-Pharmacology, Toxicology and Pharmaceutics (all)
CiteScore
5.00
自引率
0.00%
发文量
1646
审稿时长
1 weeks
期刊介绍: F1000Research publishes articles and other research outputs reporting basic scientific, scholarly, translational and clinical research across the physical and life sciences, engineering, medicine, social sciences and humanities. F1000Research is a scholarly publication platform set up for the scientific, scholarly and medical research community; each article has at least one author who is a qualified researcher, scholar or clinician actively working in their speciality and who has made a key contribution to the article. Articles must be original (not duplications). All research is suitable irrespective of the perceived level of interest or novelty; we welcome confirmatory and negative results, as well as null studies. F1000Research publishes different type of research, including clinical trials, systematic reviews, software tools, method articles, and many others. Reviews and Opinion articles providing a balanced and comprehensive overview of the latest discoveries in a particular field, or presenting a personal perspective on recent developments, are also welcome. See the full list of article types we accept for more information.
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