Cardiovascular Diseases and Metabolic Medications in the Lebanese Population: A Post Hoc Analysis from a Nationwide Cross-Sectional Study.

IF 2 Q3 PHARMACOLOGY & PHARMACY Pharmacy Pub Date : 2024-11-20 DOI:10.3390/pharmacy12060171
Rony M Zeenny, Rachel Abdo, Chadia Haddad, Aline Hajj, Rouba Karen Zeidan, Pascale Salameh, Jean Ferrieres
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Abstract

Objective: This study assesses the association of metabolic drugs (specifically hypoglycemic and hypolipemic agents) with cardiovascular diseases (CVD) among the Lebanese population and patients' subgroups.

Methods: A nationwide cross-sectional retrospective study was carried out in Lebanon. The survey collected information on sociodemographic characteristics, lifestyles, comorbidities, and medication use. Logistic regression models were employed to analyze the data and determine associations between CVD and metabolic drugs. Stratification analyses were performed based on diabetes and dyslipidemia status.

Results: The study found significant associations with CVD among the 2048 participants. Higher scores on the Lebanese Mediterranean Diet Score (LMDS; ORa = 1.06), hypertension (ORa = 1.71), diabetes (ORa = 1.75), dyslipidemia (ORa = 1.89), family history of CVD (ORa = 1.58), and smoking (previous: ORa = 1.63, current: ORa = 2.15) were linked to increased CVD odds. Higher income (intermediate: ORa = 0.64, high: ORa = 0.40) was inversely related to it. A subsequent model that included hypoglycemic and lipid-lowering medications yielded similar results. However, neither hypoglycemic nor lipid-lowering medications demonstrated a significant association with CVD risk. A third regression model was conducted by taking the classes of drugs as an independent variable. Also, the result revealed that all the classes of medication were not associated with the risk of CVD. Stratification by diabetes revealed LMDS and hypertension as risk factors in both groups. Among non-diabetic participants, dyslipidemia (ORa = 2.40), current smoking (ORa = 2.28), and higher income (intermediate: ORa = 0.57, high: ORa = 0.62) were linked to CVD. Among people with diabetes, a family history of CVD (ORa = 2.69) increased the CVD odds, while being an employer (ORa = 0.49) lowered it. Stratification by dyslipidemia showed consistent risk factors, and higher LMDS (ORa = 1.07), diabetes (ORa = 2.14), hypertension (ORa = 1.79), and previous smoking (ORa = 1.95) were linked to CVD without dyslipidemia. Being a female (ORa = 0.52) and having a lower income (ORa = 0.40) were associated with lower CVD odds in those with dyslipidemia. Subgroup analyses showed that medications were not significantly associated with CVD odds among patients with diabetes or hyperlipidemia.

Conclusions: This study's findings highlight the importance of addressing modifiable risk factors and socioeconomic factors to reduce the burden of CVD. Targeted interventions and longitudinal research are necessary to optimize preventive strategies and improve the management of CVD in individuals using hypoglycemic and hypolipemic agents in low- and medium-income countries.

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黎巴嫩人口中的心血管疾病和代谢药物:一项全国性横断面研究的事后分析。
研究目的本研究评估了黎巴嫩人口和患者亚群中代谢药物(特别是降糖药和降脂药)与心血管疾病(CVD)的关系:方法:在黎巴嫩开展了一项全国范围的横断面回顾性研究。调查收集了有关社会人口学特征、生活方式、合并症和药物使用的信息。采用逻辑回归模型分析数据,确定心血管疾病与代谢药物之间的关联。根据糖尿病和血脂异常状况进行了分层分析:研究发现,在 2048 名参与者中,心血管疾病与代谢药物有明显关联。黎巴嫩地中海饮食评分(LMDS;ORa = 1.06)、高血压(ORa = 1.71)、糖尿病(ORa = 1.75)、血脂异常(ORa = 1.89)、心血管疾病家族史(ORa = 1.58)和吸烟(以前:ORa = 1.63,现在:ORa = 2.15)的得分越高,心血管疾病的几率越大。高收入(中等:ORa = 0.64,高:ORa = 0.40)与之成反比。包括降糖药和降脂药的后续模型也得出了类似的结果。然而,降糖药和降脂药均未显示出与心血管疾病风险的显著相关性。第三个回归模型将药物类别作为自变量。结果显示,所有类别的药物均与心血管疾病风险无关。按糖尿病进行分层后发现,低密度脂蛋白胆固醇血症和高血压是两组人群的风险因素。在非糖尿病参与者中,血脂异常(ORa = 2.40)、目前吸烟(ORa = 2.28)和较高收入(中:ORa = 0.57,高:ORa = 0.62)与心血管疾病相关。在糖尿病患者中,有心血管疾病家族史(ORa = 2.69)会增加患心血管疾病的几率,而作为雇主(ORa = 0.49)则会降低患心血管疾病的几率。根据血脂异常进行的分层显示了一致的风险因素,较高的 LMDS(ORa = 1.07)、糖尿病(ORa = 2.14)、高血压(ORa = 1.79)和既往吸烟(ORa = 1.95)与无血脂异常的心血管疾病相关。女性(ORa = 0.52)和收入较低(ORa = 0.40)与血脂异常者发生心血管疾病的几率较低有关。亚组分析表明,药物与糖尿病或高脂血症患者的心血管疾病几率无明显关系:这项研究的结果强调了解决可改变的风险因素和社会经济因素以减轻心血管疾病负担的重要性。有必要采取有针对性的干预措施并开展纵向研究,以优化预防策略并改善中低收入国家使用降糖药和降脂药的人群的心血管疾病管理。
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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来源期刊
Pharmacy
Pharmacy PHARMACOLOGY & PHARMACY-
自引率
9.10%
发文量
141
审稿时长
11 weeks
期刊最新文献
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