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哺乳期结束时使用溴隐亭治疗可预防成年期早期断奶大鼠出现食欲亢进、内脏脂肪增加和肝脏甘油三酯升高的情况。

Bromocriptine treatment at the end of lactation prevents hyperphagia, higher visceral fat and liver triglycerides in early-weaned rats at adulthood.

作者信息

Peixoto-Silva Nayara, Moura Egberto G, Carvalho Janaine C, Nobre Jéssica L, Quitete Fernanda T, Pinheiro Cintia R, Santos-Silva Ana Paula, de Oliveira Elaine, Lisboa Patricia C

机构信息

Laboratory of Endocrine Physiology, Department of Physiological Sciences, Roberto Alcantara Gomes Biology Institute, State University of Rio de Janeiro, Rio de Janeiro, RJ, Brazil.

出版信息

Clin Exp Pharmacol Physiol. 2017 Apr;44(4):488-499. doi: 10.1111/1440-1681.12724.

Abstract

Non-pharmacological early weaning (NPEW) leads offspring to obesity, higher liver oxidative stress and microsteatosis in adulthood. Pharmacological EW (PEW) by maternal treatment with bromocriptine (BRO) causes obesity in the adult progeny but precludes hepatic injury. To test the hypothesis that BRO prevents the deleterious changes of NPEW, we injected BRO into the pups from the NPEW model in late lactation. Lactating rats were divided into two groups: dams with an adhesive bandage around the body to prevent breastfeeding on the last 3 days of lactation and dams whose pups had free suckling (C). Offspring from both groups were subdivided into two groups: pups treated with BRO (intraperitoneal (i.p.) 4 mg/kg per day) on the last 3 days of lactation (NPEW/BRO and C/BRO) or pups treated with the vehicle (NPEW and C). At PN120, offspring were challenged with a high fat diet (HFD), and food intake was recorded after 30 minutes and 12 hours. Rats were killed at PN120 and PN200. At PN120, adipocyte size was greater in the NPEW group but was normal in the NPEW/BRO group. At PN200, the NPEW group presented hyperphagia, higher adiposity, adipocyte hypertrophy, hyperleptinaemia, glucose intolerance and increased hepatic triglycerides. These parameters were normalized in the NPEW/BRO group. In the feeding test, BRO groups showed lower HFD intake at 30 minutes than did their controls; however, at 12 hours, the NPEW group ate more HFD. The treatment with BRO can preclude some deleterious effects of the NPEW model, which prevented the development of overweight and its comorbidities.

摘要

非药物性早期断奶(NPEW)会导致子代成年后肥胖、肝脏氧化应激增加和微脂肪变性。通过母体使用溴隐亭(BRO)进行药物性早期断奶(PEW)会导致成年子代肥胖,但可预防肝脏损伤。为了验证BRO可预防NPEW有害变化的假设,我们在哺乳期后期向NPEW模型的幼崽注射BRO。哺乳期大鼠分为两组:在哺乳期最后3天用粘性绷带缠绕身体以防止哺乳的母鼠,以及幼崽可自由哺乳的母鼠(对照组)。两组的子代再细分为两组:在哺乳期最后3天接受BRO治疗(腹腔注射(i.p.),每天4mg/kg)的幼崽(NPEW/BRO和C/BRO)或接受赋形剂治疗的幼崽(NPEW和C)。在出生后第120天(PN120),给子代喂食高脂饮食(HFD),并在30分钟和12小时后记录食物摄入量。在PN120和PN200处死大鼠。在PN120时,NPEW组的脂肪细胞大小更大,但NPEW/BRO组正常。在PN200时,NPEW组出现食欲亢进、肥胖增加、脂肪细胞肥大、高瘦素血症、葡萄糖不耐受和肝脏甘油三酯增加。这些参数在NPEW/BRO组中恢复正常。在喂食试验中,BRO组在30分钟时的HFD摄入量低于其对照组;然而,在12小时时,NPEW组摄入的HFD更多。BRO治疗可预防NPEW模型的一些有害影响,从而防止超重及其合并症的发生。

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