1 Institut für Klinische Forschung und Entwicklung (IKFE) Berlin GmbH , Berlin, Germany .
2 AMCR Institute , Escondido, California.
Diabetes Technol Ther. 2018 Jan;20(1):49-58. doi: 10.1089/dia.2017.0281. Epub 2017 Dec 12.
SAR342434 (SAR-Lis) is a biosimilar (follow-on) of insulin lispro (U100; Humalog; Ly-Lis). This study aimed to show similar efficacy, safety, and immunogenicity of SAR-Lis versus Ly-Lis in adult patients with type 2 diabetes mellitus (T2DM) treated with multiple daily injections, while using insulin glargine (GLA-100; Lantus) as basal insulin.
SORELLA 2 was a 6-month, randomized, open-label, Phase 3 study (NCT02294474). Insulin doses were adjusted to achieve fasting and 2-h postprandial glucose targets according to American Diabetes Association guidelines. Primary endpoint was the HbA change from baseline to week 26 (tested for noninferiority of SAR-Lis vs. Ly-Lis with a margin of 0.3%). Secondary endpoints included fasting plasma glucose (FPG), seven-point self-monitored plasma glucose (SMPG) profiles, hypoglycemic events, treatment-emergent adverse events (TEAEs), and anti-insulin antibodies (AIA).
A total of 505 patients were randomized (1:1) to multiple daily injections of SAR-Lis (n = 253) or Ly-Lis (n = 252) plus once-daily GLA-100. Least square (LS) mean (standard error) change in HbA from baseline to week 26 was similar in both treatment groups (SAR-Lis, -0.92% [0.051] and Ly-Lis, -0.85% [0.051]). Noninferiority at prespecified 0.3% noninferiority margin was demonstrated (LS mean difference of SAR-Lis vs. Ly-Lis: -0.07% [95% CI: -0.215 to 0.067]) as was inverse noninferiority. Similar changes in FPG, seven-point SMPG profiles, including postprandial glucose excursions and mean glucose over 24 h, and insulin dosages were observed in the two groups. Hypoglycemia, TEAEs, and AIA (incidence and prevalence) did not differ between groups.
Results from this controlled study in patients with T2DM also using GLA-100 support similar efficacy and safety (including immunogenicity) of SAR-Lis and Ly-Lis.
SAR342434(SAR-Lis)是胰岛素赖脯氨酸(U100;Humalog;Ly-Lis)的生物类似药(后续产品)。这项研究旨在表明在接受多次每日注射治疗的 2 型糖尿病(T2DM)成年患者中,SAR-Lis 与 Ly-Lis 相比具有相似的疗效、安全性和免疫原性,同时使用甘精胰岛素(GLA-100;Lantus)作为基础胰岛素。
SORELLA 2 是一项为期 6 个月、随机、开放标签、3 期研究(NCT02294474)。根据美国糖尿病协会指南,调整胰岛素剂量以实现空腹和餐后 2 小时血糖目标。主要终点是从基线到 26 周时的 HbA 变化(通过将 SAR-Lis 与 Ly-Lis 的 0.3% 边际进行非劣效性检验进行测试)。次要终点包括空腹血糖(FPG)、七点自我监测血糖(SMPG)谱、低血糖事件、治疗期间出现的不良事件(TEAE)和抗胰岛素抗体(AIA)。
共有 505 名患者被随机分配(1:1)接受 SAR-Lis(n=253)或 Ly-Lis(n=252)联合每日一次 GLA-100 的多次每日注射。从基线到 26 周时,HbA 的最小二乘(LS)平均值(标准误差)变化在两组之间相似(SAR-Lis,-0.92%[0.051];Ly-Lis,-0.85%[0.051])。在预设的 0.3%非劣效性边界证明了非劣效性(SAR-Lis 与 Ly-Lis 的 LS 均值差异:-0.07%[95%CI:-0.215 至 0.067]),并且存在逆非劣效性。两组均观察到 FPG、七点 SMPG 谱(包括餐后血糖波动和 24 小时平均血糖)和胰岛素剂量的相似变化。两组之间低血糖、TEAE 和 AIA(发生率和患病率)无差异。
这项在同时使用 GLA-100 的 T2DM 患者中进行的对照研究结果也支持 SAR-Lis 和 Ly-Lis 具有相似的疗效和安全性(包括免疫原性)。
