Division of Endocrinology, Diabetes and Metabolism, Department of Internal Medicine, Boston VA Healthcare System and Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, Massachusetts, USA.
First Department of Propaedeutic Internal Medicine, Laiko General Hospital, National and Kapodistrian University of Athens School of Medicine, Athens, Greece.
Diabetes Obes Metab. 2023 Sep;25(9):2561-2574. doi: 10.1111/dom.15141. Epub 2023 May 29.
To investigate the changes of circulating levels of all proglucagon-derived peptides (PGDPs) in individuals with overweight or obesity receiving liraglutide (3 mg) or naltrexone/bupropion (32/360 mg), and to explore the association between induced changes in postprandial PGDP levels and body composition, as well as metabolic variables, after 3 and 6 months on treatment.
Seventeen patients with obesity or with overweight and co-morbidities, but without diabetes, were assigned to receive once-daily oral naltrexone/bupropion 32/360 mg (n = 8) or once-daily subcutaneous liraglutide 3 mg (n = 9). Participants were assessed before treatment initiation and after 3 and 6 months on treatment. At the baseline and 3-month visits, participants underwent a 3-hour mixed meal tolerance test to measure fasting and postprandial levels of PGDPs, C-peptide, hunger and satiety. Clinical and biochemical indices of metabolic function, magnetic resonance-assessed liver steatosis and ultrasound-assessed liver stiffness were measured at each visit.
Both medications improved body weight and composition, carbohydrate and lipid metabolism, and liver fat and function. Naltrexone/bupropion produced a weight-independent increase in the levels of proglucagon (P < .001) and decreases in glucagon-like peptide-2 (GLP-2), glucagon and the major proglucagon fragment (P ≤ .01), whereas liraglutide markedly upregulated total glucagon-like peptide-1 (GLP-1) levels in a weight-independent manner (P = .04), and similarly downregulated the major proglucagon fragment, GLP-2 and glucagon (P < .01). PGDP levels at the 3-month visit were positively and independently correlated with improvements in fat mass, glycaemia, lipaemia and liver function, and negatively with reductions in fat-free mass, at both the 3- and 6-month visits.
PGDP levels in response to liraglutide and naltrexone/bupropion are associated with improvements in metabolism. Our study provides support for the administration of the downregulated members of the PGDP family as replacement therapy (e.g. glucagon), in addition to the medications currently in use that induced their downregulation (e.g. GLP-1), and future studies should explore whether the addition of other PGDPs (e.g. GLP-2) could offer additional benefits.
研究超重或肥胖个体接受利拉鲁肽(3mg)或纳曲酮/安非他酮(32/360mg)治疗时,所有胰高血糖素原衍生肽(PGDPs)循环水平的变化,并探讨治疗 3 个月和 6 个月后,餐后 PGDP 水平的诱导变化与体重组成以及代谢变量之间的关系。
将 17 名肥胖或超重伴合并症但无糖尿病的患者分配接受每日一次口服纳曲酮/安非他酮 32/360mg(n=8)或每日一次皮下注射利拉鲁肽 3mg(n=9)治疗。在治疗开始前和治疗后 3 个月和 6 个月评估参与者。在基线和 3 个月访视时,参与者接受了 3 小时混合餐耐量试验,以测量空腹和餐后 PGDPs、C 肽、饥饿和饱腹感。每次就诊时均测量代谢功能的临床和生化指标、磁共振评估的肝脂肪变性和超声评估的肝硬度。
两种药物均改善了体重和组成、碳水化合物和脂质代谢以及肝脂肪和功能。纳曲酮/安非他酮导致胰高血糖素原水平升高(P<0.001),而胰高血糖素-2(GLP-2)、胰高血糖素和主要胰高血糖素片段降低(P≤0.01),而利拉鲁肽则以独立于体重的方式显著上调总胰高血糖素样肽-1(GLP-1)水平(P=0.04),并同样下调主要胰高血糖素片段、GLP-2 和胰高血糖素(P<0.01)。3 个月时 PGDP 水平与脂肪量、血糖、血脂和肝功能的改善呈正相关,与 3 个月和 6 个月时去脂体重的减少呈负相关。
利拉鲁肽和纳曲酮/安非他酮的 PGDP 水平与代谢改善相关。我们的研究支持使用下调的 PGDP 家族成员作为替代治疗(例如,胰高血糖素),除了目前诱导其下调的药物(例如 GLP-1),未来的研究应探讨是否添加其他 PGDPs(例如 GLP-2)会带来额外的益处。
