使用胰高血糖素样肽-1(GLP-1)受体激动剂进行治疗可减少体重减轻维持期间游离血浆瘦素的下降。
Treatment with a GLP-1 receptor agonist diminishes the decrease in free plasma leptin during maintenance of weight loss.
作者信息
Iepsen E W, Lundgren J, Dirksen C, Jensen J-Eb, Pedersen O, Hansen T, Madsbad S, Holst J J, Torekov S S
机构信息
1] Department of Biomedical Sciences and NNF Center for Basic Metabolic Research, Faculty of Health Sciences, University of Copenhagen, Copenhagen, Denmark [2] Department of Endocrinology, Hvidovre University Hospital, Hvidovre, Denmark.
Department of Endocrinology, Hvidovre University Hospital, Hvidovre, Denmark.
出版信息
Int J Obes (Lond). 2015 May;39(5):834-41. doi: 10.1038/ijo.2014.177. Epub 2014 Oct 7.
BACKGROUND
Recent studies indicate that glucagon-like peptide (GLP)-1 inhibits appetite in part through regulation of soluble leptin receptors. Thus, during weight loss maintenance, GLP-1 receptor agonist (GLP-1RA) administration may inhibit weight loss-induced increases in soluble leptin receptors thereby preserving free leptin levels and preventing weight regain.
METHODS
In a randomized controlled trial, 52 healthy obese individuals were, after a diet-induced 12% body weight loss, randomized to treatment with or without administration of the GLP-1RA liraglutide (1.2 mg per day). In case of weight gain, low-calorie diet products were allowed to replace up to two meals per day to achieve equal weight maintenance. Glucose tolerance and hormone responses were investigated before and after weight loss and after 52 weeks weight maintenance. Primary end points: increase in soluble leptin receptor plasma levels and decrease in free leptin index after 52 weeks weight loss maintenance.
RESULTS
Soluble leptin receptor increase was 59% lower; 2.1±0.7 vs 5.1±0.8 ng ml(-1) (-3.0 (95% confidence interval (CI)=-0.5 to -5.5)), P<0.001 and free leptin index decrease was 43% smaller; -62±15 vs -109±20 (-47 (95% CI=-11 to -83)), P<0.05 with administration of GLP-1RA compared with control group. The 12% weight loss was successfully maintained in both the groups with no significant change in weight after 52 weeks follow-up. The GLP-1RA group had greater weight loss during the weight maintenance period (-2.3 kg (95% CI=-0.6 to -4.0)), and had fewer meal replacements per day compared with the control group (minus one meal per day (95% CI=-0.6 to -1)), P<0.001. Fasting glucose was decreased by an additional -0.2±0.1 mmol l(-1) in the GLP-1RA group in contrast to the control group, where glucose increased 0.3±0.1 mmol l(-1) to the level before weight loss (-0.5mmol l(-1) (95% CI=-0.1 to -0.9)), P<0.005. Meal response of peptide PYY3-36 was higher at week 52 in the GLP-1RA group compared with the control group, P<0.05.
CONCLUSIONS
The weight maintaining effect of GLP-1RAs may be mediated by smaller decrease in free leptin and higher PYY3-36 response. Low dose GLP-1RA therapy maintained 12% weight loss for 1 year and may prevent pre-diabetes in obesity.
背景
近期研究表明,胰高血糖素样肽(GLP)-1部分通过调节可溶性瘦素受体来抑制食欲。因此,在维持体重减轻期间,给予GLP-1受体激动剂(GLP-1RA)可能会抑制体重减轻引起的可溶性瘦素受体增加,从而维持游离瘦素水平并防止体重反弹。
方法
在一项随机对照试验中,52名健康肥胖个体在通过节食使体重减轻12%后,被随机分为接受或不接受GLP-1RA利拉鲁肽(每日1.2毫克)治疗的两组。若体重增加,允许使用低热量饮食产品替代每日最多两餐以维持体重。在体重减轻前后以及体重维持52周后,对葡萄糖耐量和激素反应进行了研究。主要终点:体重维持52周后可溶性瘦素受体血浆水平的增加以及游离瘦素指数的降低。
结果
与对照组相比,接受GLP-1RA治疗组的可溶性瘦素受体增加降低了59%;分别为2.1±0.7与5.1±0.8纳克/毫升(-3.0(95%置信区间(CI)=-0.5至-5.5)),P<0.001,游离瘦素指数降低减少了43%;分别为-62±15与-109±20(-47(95%CI=-11至-83)),P<0.05。两组均成功维持了12%的体重减轻,52周随访后体重无显著变化。GLP-1RA组在体重维持期体重减轻更多(-2.3千克(95%CI=-0.6至-4.0)),且与对照组相比,每日的餐食替代次数更少(每日少一餐(95%CI=-0.6至-1)),P<0.001。与对照组相比,GLP-1RA组的空腹血糖额外降低了-0.2±0.1毫摩尔/升,而对照组的血糖增加了0.3±0.1毫摩尔/升,恢复到体重减轻前的水平(-0.5毫摩尔/升(95%CI=-0.1至-0.9)),P<0.005。与对照组相比,GLP-1RA组在第52周时肽YY3-36的餐后反应更高,P<0.05。
结论
GLP-1RA的体重维持作用可能是通过游离瘦素的较小降低和较高的PYY3-36反应介导的。低剂量GLP-1RA治疗可维持12%的体重减轻达1年,并可能预防肥胖患者的糖尿病前期。
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