一种长效 PYY 类似物在非人灵长类动物中具有强大的厌食疗效,且恶心副作用最小。
A Long-Acting PYY Analog Mediates Robust Anorectic Efficacy with Minimal Emesis in Nonhuman Primates.
机构信息
Discovery Biology, Cardiovascular and Metabolic Therapeutic Areas, Janssen Research and Development, Spring House, PA, USA.
Discovery Biology, Cardiovascular and Metabolic Therapeutic Areas, Janssen Research and Development, Spring House, PA, USA.
出版信息
Cell Metab. 2019 Apr 2;29(4):837-843.e5. doi: 10.1016/j.cmet.2019.01.017. Epub 2019 Feb 14.
Abstract
The gut hormone PYY reduces food intake in humans and exhibits at least additive efficacy in combination with GLP-1. However, the utility of PYY analogs as anti-obesity agents has been severely limited by emesis and rapid proteolysis, a profile similarly observed with native PYY in obese rhesus macaques. Here, we found that antibody conjugation of a cyclized PYY analog achieved high NPY2R selectivity, unprecedented in vivo stability, and gradual infusion-like exposure. These properties permitted profound reduction of food intake when administered to macaques for 23 days without a single emetic event in any animal. Co-administration with the GLP-1 receptor agonist liraglutide for an additional 5 days further reduced food intake with only one animal experiencing a single bout of emesis. This antibody-conjugated PYY analog therefore may enable the long-sought potential of GLP-1/PYY-based combination treatment to achieve robust, well-tolerated weight reduction in obese patients.
摘要
肠激素 PYY 可减少人体的食物摄入量,并与 GLP-1 联合使用时至少具有相加的疗效。然而,PYY 类似物作为抗肥胖药物的应用受到严重限制,因为其会引起呕吐和快速蛋白水解,这一特性与肥胖恒河猴中的天然 PYY 类似。在这里,我们发现,一种环化 PYY 类似物的抗体缀合可实现高 NPY2R 选择性、前所未有的体内稳定性和逐渐输注样暴露。当将其连续给恒河猴给药 23 天时,该特性可显著减少食物摄入量,而没有一只动物出现呕吐。与 GLP-1 受体激动剂利拉鲁肽联合使用额外 5 天,仅使一只动物经历一次呕吐,进一步减少了食物摄入量。因此,这种抗体缀合的 PYY 类似物可能使人们长期以来期望的基于 GLP-1/PYY 的联合治疗能够在肥胖患者中实现稳健、耐受良好的体重减轻。
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