在患有或不患有2型糖尿病的超重和肥胖患者中,高剂量口服赛马鲁肽可显著减轻体重和/或降低Hba1c水平

Iskandar Idris DM
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引用次数: 0

摘要

Semagulide是一种GLP-1类似肽,多年来一直被用于治疗超重、肥胖或2型糖尿病,每周皮下注射一次。赛马鲁肽(Rybelsius)的口服制剂也已上市,目前批准的最大剂量为14 mg/天。然而,在之前的2期剂量范围研究中,在高于14的剂量下观察到额外的体重减轻 mg/天。因此,进行了两项试验——OASIS,针对超重或肥胖但没有2型糖尿病的患者,以及PIONEER PLUS,针对控制不足的2型糖尿病患者,以评估在25岁和50岁时更高剂量的口服赛姆鲁肽的疗效和安全性 mg/天,以诱导体重减轻和其他代谢参数的改善。这两项3期研究都在美国糖尿病协会(ADA)第83届科学会议上发表,并同时发表在《柳叶刀》上。OASIS-1[1]显示口服赛马鲁肽50 mg的平均%体重减轻了15.1%,而安慰剂组为-2.4%。口服赛马鲁肽的不良事件发生率略高,主要由胃肠道副作用(口服赛马鲁肽为80%,安慰剂为46%)以及胆囊和胆道相关疾病(口服赛马鲁肽为11.1%,安慰剂为3.6%)引起。同时,PIONER PLUS试验[2]显示,血糖控制和体重减轻效果良好,心脏代谢危险因素改善,每天口服一次的塞马鲁肽剂量更高(25和50 mg),而目前[最高]批准的14mg剂量。口服赛马鲁肽14、25和50可使Hba1c降低−1.5%、−1.8%和−2.0% mg。因此,这两项研究表明口服赛马鲁肽治疗肥胖和2型糖尿病的安全性和有效性,其结果与注射赛马鲁素的使用相当。2.4 mg,每周一次。由于全球范围内缺乏注射用赛马鲁肽,人们认为,有效的“药丸”的可用性可能会在全球范围内扩大,增加获得护理的机会,并为个体化护理提供机会,尤其是为难以使用注射疗法的人提供机会。然而,它对减少心血管后果的影响尚不清楚。目前正在进行研究,以澄清这一重要的临床和研究问题。
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Higher dose oral semaglutide shown to produce remarkable weight loss and/or reduce Hba1c levels in overweight and obese patients with or without type 2 diabetes

Semaglutide is a GLP-1 analogue peptide which has been used and approved to treat overweight, obesity or type 2 diabetes for many years as a once weekly subcutaneous injections. The oral formulation of semaglutide (Rybelsius) is also now available and currently approved at a maximum dose of 14 mg/day. In a previous phase 2 dose ranging studies however, additional weight loss was observed at doses higher than 14 mg/day. Two trials—the OASIS, in patients with overweight or obesity without type 2 diabetes and PIONEER PLUS in patients with inadequately controlled type 2 diabetes, were therefore conducted to evaluate the efficacy and safety of higher doses of oral semglutide at 25 and 50 mg/day to induce weight loss and improvement of other metabolic parameters. Both phase-3 studies were presented at the American Diabetes Association (ADA) 83rd Scientific Sessions and simultaneously published in The Lancet. OASIS-1[1] showed that oral semaglutide 50 mg produced a mean % weight reduction of 15.1% compared with −2.4% with placebo. Adverse events were marginally more frequent with oral semaglutide, driven by largely gastrointestinal side effects (80% with oral semaglutide vs. 46% with placebo) and gall bladder and biliary related disorders (11.1% with oral semaglutide vs. 3.6% with placebo). The PIONEER PLUS trial[2] meanwhile showed superior glycemic control and body-weight loss and improvement in cardiometabolic risk factors, with higher doses of once-daily oral semaglutide (25 and 50 mg) compared with the currently [highest] approved 14-mg dose. Hba1c reduction was reduced by −1.5%, −1.8% and −2.0% with oral semaglutide 14, 25 and 50 mg, respectively. These two studies therefore showed the safety and efficacy of oral semaglutide to treat obesity and type 2 diabetes, with results comparable to the use of injectable semaglutide 2.4 mg once weekly. Due to the lack of availability of injectable semaglutide worldwide, it is thought that availability of an efficacious ‘pill’ might have a larger global reach and increase access to care as well as provide opportunities to individualized care especially for individuals who struggle with the use of injectable therapies. However, its effect on reducing cardiovascular outcomes remains unclear. Studies are ongoing to clarify this important clinical and research question.

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Issue Information Precision medicine approach to detect obese people who are at high risk of developing diabetes Increasing excess to weight loss injection shown to save thousands of lives a year Semaglutide shown to improve cardiovascular outcomes among patients with type 2 diabetes with any forms of heart failure Real world study provided reassurance of the safety of GLP-1 therapy on mental health and suicide risk
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