Comparison of baseline clinical characteristics among people with type 2 diabetes on second-line therapy previously added with dapagliflozin or another oral glucose-lowering drug: AGORA study

Vicente Pallarés-Carratalá , Antonio Ruiz-García , Adalberto Serrano-Cumplido , Antonio Segura Fragoso , Verónica Fernández-Pascual , Beatriz Sánchez-Sánchez , María Inmaculada Cervera-Pérez , Francisco Javier Alonso-Moreno , Ezequiel Arranz-Martínez , Alfonso Barquilla-García , Daniel Rey-Aldana , José Polo García , Sergio Cinza-Sanjurjo , on behalf of the Investigators of the AGORA study, of the Spanish Society of Primary Care Physicians SEMERGEN Foundation
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Abstract

Introduction

Type 2 diabetes mellitus (T2D) has acquired epidemic proportions worldwide. In recent years, new oral glucose-lowering drugs (OGLD) have emerged that improve the cardiovascular–kidney–metabolic control in T2D people.

Objectives

To compare the baseline clinical–biological characteristics among T2D people to whom had added-on dapagliflozin (DAPA group) or another OGLD (SOC group) second-line hypoglycaemic therapies among the AGORA study population.

Methods

This is a multicentre cross-sectional observational study of the baseline characteristics of T2D people recruited through competitive sampling among 46 primary care health centres in Spain for the AGORA study. The inclusion and exclusion criteria of participants, and justification of the sample size are reported. After verifying the data necessary to be evaluated and informed consent, 317 subjects were included to the DAPA group and 288 to the SOC group. Both categorical and continuous variables were analysed and compared with the usual statistics. Cohen's d was used to assess the standardised difference in means.

Results

Six hundred and five patients with T2D were assessed (mean age 63.5 [SD ± 8.1] years, 61.8% men), whom 17.4% were smokers, 47.6% had obesity, 74.8% hypertension, 87.3% dyslipidaemia, and 41.7% reported physical inactivity, with no significant differences between both comparison groups. The mean (SD) evolution time of T2D was 10.1 (5.6) years. Most baseline clinical–biological characteristics at recruitment were similar in both groups. However, DAPA group was younger (2.9 years), and had lower systolic blood pressure (SBP) (2.8 mmHg), higher body weight (BW) (3.7 kg), and higher glycated haemoglobin A1c (HbA1c) (0.3%) than SOC group. Only 11.5% of participants had poor glycaemic control (HbA1c > 8%) at recruitment, 54.9% had good glycaemic control (HbA1c < 7%), being significantly lower in the DAPA group (47.3%) than in the SOC group (63.4%). The percentage of T2D patients with high vascular risk (VR) was 46.3%, and 53.7% with very high VR, being significantly higher in the DAPA group (57.4%) than in the SOC group (49.6%).

Conclusions

Most baseline cardiovascular–kidney–metabolic characteristics were similar in T2D patients whom had added dapagliflozin on second-line hypoglycaemic therapy as those whom had added-on another OGLD. However, patients whom had added-on dapagliflozin had higher VR, lower SBP, higher BW, and slightly worse HbA1c control. Future research is necessary to explain the causes of these differences in cardiometabolic control.
AGORA研究:先前加用达格列净或另一种口服降糖药物的二线治疗的2型糖尿病患者的基线临床特征比较
2型糖尿病(T2D)已在世界范围内流行。近年来,新的口服降糖药物(OGLD)出现,改善了t2dm患者的心血管-肾脏代谢控制。目的比较AGORA研究人群中接受加用达格列净(DAPA组)或另一种OGLD (SOC组)二线降糖治疗的t2dm患者的基线临床生物学特性。方法:这是一项多中心横断面观察性研究,通过竞争性抽样在西班牙46个初级保健卫生中心招募T2D患者进行AGORA研究。报告了受试者的纳入和排除标准,以及样本量的合理性。在验证了评估所需的数据和知情同意后,317名受试者被纳入DAPA组,288名受试者被纳入SOC组。对分类变量和连续变量进行分析,并与通常的统计数据进行比较。使用Cohen’s d来评估标准化均值差。结果共纳入665例T2D患者(平均年龄63.5 [SD±8.1]岁,男性占61.8%),其中吸烟占17.4%,肥胖占47.6%,高血压占74.8%,血脂异常占87.3%,缺乏运动占41.7%,两组间差异无统计学意义。T2D的平均(SD)演化时间为10.1(5.6)年。两组招募时的大多数基线临床生物学特征相似。然而,DAPA组更年轻(2.9岁),收缩压(SBP)更低(2.8 mmHg),体重(BW)更高(3.7 kg),糖化血红蛋白A1c (HbA1c)更高(0.3%)。只有11.5%的参与者血糖控制不良(HbA1c >;8%), 54.9%的人血糖控制良好(HbA1c和lt;7%), DAPA组(47.3%)明显低于SOC组(63.4%)。T2D患者血管高危(VR)比例为46.3%,高危(VR)比例为53.7%,其中DAPA组(57.4%)明显高于SOC组(49.6%)。结论:在二线降糖治疗中添加达格列净的t2dm患者与添加另一种OGLD的t2dm患者的大多数基线心血管-肾脏代谢特征相似。然而,加用达格列净的患者有更高的VR、更低的收缩压、更高的BW和稍差的HbA1c控制。未来的研究有必要解释这些心脏代谢控制差异的原因。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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