Bahl Vinay K, Jadhav Uday M, Thacker Hemant P
Department of Cardiology, All India Institute of Medical Sciences, New Delhi, India.
Am J Cardiovasc Drugs. 2009;9(3):135-42. doi: 10.1007/BF03256570.
Current clinical guidelines recognize that the use of more than one agent is necessary to achieve target BP in the majority of patients. The ASCOT-BPLA trial demonstrated that the free combination of amlodipine and perindopril effectively controlled BP and was better than a beta-adrenoceptor antagonist (beta-blocker)/diuretic combination in reducing total mortality and cardiovascular outcomes.
To evaluate the efficacy and tolerability of a fixed combination of perindopril and amlodipine in the clinical setting.
The STRONG (SafeTy & efficacy analysis of coveRsyl amlodipine in uncOntrolled and Newly diaGnosed hypertension) study was a prospective, observational, multicenter trial.
This was a naturalistic, real-world, clinic-based, outpatient study involving 336 general practitioners/primary care physicians in 65 cities in India.
Adults aged 40-70 years with newly diagnosed/untreated stage 2 hypertension (BP >/=160/100 mmHg), hypertension uncontrolled with monotherapy (BP >140/90 mmHg), or hypertension inadequately managed with another combination therapy.
Fixed combination perindopril 4 mg/amlodipine 5 mg once daily for 60 days.
The primary outcomes were the mean change in BP from baseline and the proportion of patients achieving adequate BP control (</=140/90 mmHg, or </=130/80 mmHg in patients with diabetes mellitus) in the intent-to-treat (ITT) population. Secondary analyses included incidence of adverse events (ITT) and treatment adherence rate (completers).
In total, 1250 patients comprised the ITT population: 32.6% with newly diagnosed hypertension; 40.5% with hypertension uncontrolled with monotherapy; and 26.9% with hypertension inadequately managed with another combination therapy. Mean SBP/DBP decreased significantly from baseline (167.4 +/- 15.2/101.4 +/- 9.1 mmHg) over 60 days (-41.9 +/- 34.8/-23.2 +/- 21.8 mmHg; p < 0.0001). Target BP was achieved in 66.1% of patients in the total population, 68.3% of untreated patients, 68.4% of patients uncontrolled with monotherapy, and 59.9% of patients inadequately managed with combination therapy. In 161 patients with SBP >180 mmHg at baseline (newly diagnosed: n = 50; uncontrolled on monotherapy: n = 53; inadequately managed on combination therapy: n = 58), BP was reduced by 63.2 +/- 32.5/29.0 +/- 21.9 mmHg (p < 0.0001) at day 60. The fixed combination was safe and well tolerated. All 1175 patients completing the 60-day study (94%) adhered to their treatment regimen.
Fixed combination perindopril/amlodipine was found to be an effective and well tolerated antihypertensive treatment, with an excellent rate of treatment adherence in the clinical setting. Fixed combination perindopril/amlodipine is expected to be useful in the management of hypertension in primary healthcare, with a positive impact on treatment adherence.
当前临床指南认为,大多数患者需要联合使用多种药物才能达到目标血压。ASCOT - BPLA试验表明,氨氯地平和培哚普利的自由联合能有效控制血压,在降低总死亡率和心血管事件方面优于β - 肾上腺素能受体拮抗剂(β受体阻滞剂)/利尿剂联合用药。
评估培哚普利和氨氯地平固定复方制剂在临床环境中的疗效和耐受性。
STRONG(培哚普利氨氯地平在未控制和新诊断高血压中的安全性与疗效分析)研究是一项前瞻性、观察性、多中心试验。
这是一项基于诊所的自然、真实世界的门诊研究,涉及印度65个城市的336名全科医生/初级保健医生。
年龄在40 - 70岁之间,新诊断/未治疗的2级高血压(血压≥160/100 mmHg)、单药治疗血压未控制(血压>140/90 mmHg)或另一种联合治疗方案血压控制不佳的成年人。
培哚普利4 mg/氨氯地平5 mg固定复方制剂,每日一次,共60天。
主要结局指标为意向性治疗(ITT)人群中血压相对于基线的平均变化以及达到血压充分控制(≤140/90 mmHg,糖尿病患者≤130/80 mmHg)的患者比例。次要分析包括不良事件发生率(ITT)和治疗依从率(完成治疗者)。
ITT人群共1250例患者:32.6%为新诊断高血压;40.5%为单药治疗血压未控制;26.9%为另一种联合治疗方案血压控制不佳。60天内,收缩压/舒张压均值较基线(167.4±15.2/101.4±9.1 mmHg)显著下降(-41.9±34.8/-23.2±21.8 mmHg;p<0.0001)。总人群中66.1%的患者、未治疗患者中68.3%、单药治疗未控制患者中68.4%以及联合治疗控制不佳患者中59.9%达到目标血压。161例基线收缩压>180 mmHg的患者(新诊断:n = 50;单药治疗未控制:n = 53;联合治疗控制不佳:n = 58),第60天时血压下降63.2±32.5/29.0±21.9 mmHg(p<0.0001)。该固定复方制剂安全且耐受性良好。完成60天研究的1175例患者(94%)均坚持治疗方案。
培哚普利/氨氯地平固定复方制剂是一种有效且耐受性良好的抗高血压治疗药物,在临床环境中治疗依从率极高。培哚普利/氨氯地平固定复方制剂有望在基层医疗中用于高血压管理,对治疗依从性产生积极影响。
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