Liraglutide Enhances the Activity of the ACE-2/Ang(1–7)/Mas Receptor Pathway in Lungs of Male Pups from Food-Restricted Mothers and Prevents the Reduction of SP-A

J. Fandi?o; A. A. Vaz; L. Toba; M. Romaní-Pérez; L. González-Matías; F. Mallo; Y. Diz-Chaves; Silvia Monticone

首页> 外文期刊>International journal of endocrinology >Liraglutide Enhances the Activity of the ACE-2/Ang(1–7)/Mas Receptor Pathway in Lungs of Male Pups from Food-Restricted Mothers and Prevents the Reduction of SP-A

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Liraglutide Enhances the Activity of the ACE-2/Ang(1–7)/Mas Receptor Pathway in Lungs of Male Pups from Food-Restricted Mothers and Prevents the Reduction of SP-A

机译：Liraglutide增强了来自食品受限制母亲的雄性幼犬肺肺肺（1-7）/ MAS受体途径的活性，并防止了SP-A的减少

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In utero growth restriction and being born small for gestational age are risk factors for respiratory morbidity. IUGR (in utero growth retardation) is associated to overall reduction in lung weight, surfactant content and activity, impaired maturation of the alveolar type II cells, and decreased alveolar formation. The renin-angiotensin system (RAS) may be a key target underlying pathophysiological lung alterations. GLP-1 and agonists of its receptor modulate the expression levels of different components of RAS and also are very important for lung maturation and the production of surfactant proteins. The aim of this study was to elucidate the effects of IUGR induced by perinatal food restriction of the mother in the lung function of pups at early stages of life (PD21) and to determine if liraglutide had any effect during gestational period. Sprague-Dawley pregnant rats were randomly assigned to 50% food restriction (MPFR) or ad libitum control (CT) groups at day of pregnancy 12 (GD12). From GD14 to parturition, pregnant MPFR and CT rats were treated with liraglutide or vehicle. At postnatal day 21 and before weaning, 20 CT and 20 FR male pups were sacrificed and lungs were analyzed by RT-PCR. Liraglutide restored surfactant protein A (SP-A) mRNA expression in pup lungs from food-restricted mothers. Surfactant protein B (SP-B) mRNA expression is not affected by neither IUGR nor liraglutide treatment. Moreover, liraglutide modulated different elements of RAS, increasing angiotensin-converting enzyme 2 (ACE2) and MasR mRNA expression only in pups from food-restricted mothers (MPFR), despite food restriction had not any direct effect at this early stage. Liraglutide also increased endothelial nitric oxide synthase (eNOS) expression in MPFR lungs, reflecting the activation of MasR by angiotensin 1–7. In conclusion, liraglutide prevented the alteration in lung function induced by IUGR and promoted the positive effects of ACE2-Ang(1–7)-MasR in restoring lung function.

机译：在子宫生长限制和出生较小的胎龄中是呼吸发病率的危险因素。 IUGR（在子宫生长迟滞中）与肺重量，表面活性剂含量和活性的总体降低相关，肺泡II型细胞的成熟受损，降低肺泡形成。肾素 - 血管紧张素系统（RAS）可以是潜在病理生理肺改变的关键目标。其受体的GLP-1和激动剂调节RA的不同组分的表达水平，对肺成熟和表面活性剂蛋白的产生也非常重要。本研究的目的是阐明IUGR在寿命早期阶段（PD21）的幼崽肺功能的围类血液中血液的肺功能诱导的影响，并确定在妊娠期期间的丽菌蛋白质是否有任何效果。 Sprague-Dawley怀孕孕大鼠在怀孕当天随机分配到50％的食物限制（MPFR）或AD Libitum对照（CT）组（GD12）。从GD14到分娩，怀孕的MPFR和CT大鼠用Liraglutide或载体处理。在后期21天和断奶前，处死20ct和20 fr雄性幼崽，通过RT-PCR分析肺。 Liraglutide恢复了食物受限制母亲的幼崽肺中的表面活性剂蛋白A（SP-A）mRNA表达。表面活性剂蛋白B（SP-B）mRNA表达不受IUGR和Liraglutide治疗的影响。此外，黎勒肽调节了Ras的不同元素，仅在食品受限母亲（MPFR）的幼崽中增加了血管紧张素转换酶2（ACE2）和MasR mRNA表达，尽管食物限制在此早期没有任何直接效果。 Liraglutide还增加了MPFR肺中的内皮型一氧化氮合酶（Enos）表达，反映了血管紧张素1-7的激活MasR。总之，黎棱捷人阻止了IUGR诱导的肺功能的改变，并促进了ACE2-Ang（1-7）-MASR在恢复肺功能中的积极作用。

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来源
《International journal of endocrinology》 |2018年第3期|共9页
作者
J. Fandi?o; A. A. Vaz; L. Toba; M. Romaní-Pérez; L. González-Matías; F. Mallo; Y. Diz-Chaves; Silvia Monticone;
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作者单位

Laboratory Endocrinology;

Laboratory Endocrinology;

Laboratory Endocrinology;

Laboratory Endocrinology;

Laboratory Endocrinology;

Laboratory Endocrinology;

Laboratory Endocrinology;

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正文语种 eng
中图分类内分泌腺疾病及代谢病;
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3. Liraglutide Enhances the Activity of the ACE-2/Ang(1–7)/Mas Receptor Pathway in Lungs of Male Pups from Food-Restricted Mothers and Prevents the Reduction of SP-A [J] . J. Fandio, A. A. Vaz, L. Toba, International journal of endocrinology . 2018,第3期

机译：利拉鲁肽增强了受食物限制的母亲的雄性幼崽肺中ACE-2 / Ang（1-7）/ Mas受体途径的活性，并防止SP-A的降低
4. The ACE-2/Ang1-7/Mas cascade enhances bone structure and metabolism following angiotensin-II type 1 receptor blockade [J] . Abuohashish Hatem M., Ahmed Mohammed M., Sabry Dina, European Journal of Pharmacology: An International Journal . 2017,第期

机译：ACE-2 / Ang1-7 / MAS级联增强了血管紧张素-II型1受体封锁后的骨骼结构和代谢
5. GLP-1 Analogue Liraglutide Enhances SP-A Expression in LPS-Induced Acute Lung Injury through the TTF-1 Signaling Pathway [J] . Tao Zhu, Changyi Li, Xue Zhang, Mediators of inflammation . 2018,第12期

机译：GLP-1类似物利拉鲁肽通过TTF-1信号通路增强LPS诱导的急性肺损伤中SP-A表达
6. Liraglutide Enhances the Activity of the ACE-2/Ang(1–7)/Mas Receptor Pathway in Lungs of Male Pups from Food-Restricted Mothers and Prevents the Reduction of SP-A [O] . J. Fandiño, A. A. Vaz, L. Toba, 2018

机译：利拉鲁肽增强了受食物限制的母亲的雄性幼仔肺中ACE-2 / Ang（1-7）/ Mas受体途径的活性并阻止了SP-A的降低
7. Liraglutide Enhances the Activity of the ACE-2/Ang(1–7)/Mas Receptor Pathway in Lungs of Male Pups from Food-Restricted Mothers and Prevents the Reduction of SP-A [O] . J. Fandiño, A. A. Vaz, L. Toba, 2018

机译：Liraglutide增强了来自食品受限制母亲的雄性幼犬肺肺肺的ACE-2 / Ang（1-7）/ MAS受体途径的活性，防止SP-A的减少

Liraglutide Enhances the Activity of the ACE-2/Ang(1–7)/Mas Receptor Pathway in Lungs of Male Pups from Food-Restricted Mothers and Prevents the Reduction of SP-A

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