生化和血液参数在预测心血管风险中的作用

W. K. T. Nuwanthika, D. I. K. Welivitigoda, S. P. N. N. Senadeera, D. U. Kottahachchi, C. B. Ranaweera, N. Wijesighe
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摘要

导言心血管疾病(CVDs)是指任何影响心脏或血管的疾病。心血管疾病是全球最常见的死亡原因,在 20 世纪初,10% 的死亡是由心血管疾病造成的。这些心血管疾病可表现为心肌梗死或缺血性心脏病、中风和充血性心力衰竭。诊断心血管疾病需要进行体格检查、放射学检查以及心肌酶和血脂的实验室检查。在临床实践中,心血管风险预测模型对心血管疾病的识别、预防和严重程度分期非常重要。弗雷明汉风险评分-冠心病、弗雷明汉风险评分-心血管疾病、QRESEARCH-心血管风险算法、英国联合学会风险计算器-3、WHO/ISH 心血管疾病风险预测图和动脉粥样硬化性心血管疾病风险估算器是一些可用的心血管疾病风险估算器。然而,其中许多估算器只能用于评估 40 岁以上的个体和 10 年的风险。 因此,需要新的风险估算器来克服现有风险估算器的不足。新的研究方向是常规血液和生化实验室参数的比率,如中性粒细胞与淋巴细胞比率(NLR)、血小板与淋巴细胞比率(PLR)和天门冬氨酸氨基转移酶与丙氨酸氨基转移酶比率(AST/ALT)。结果表明,上述比率与心血管疾病风险之间存在关系。 结论:有鉴于此,本综述阐述了通过合并一些生化和血液学参数(包括 NLR、PLR 和 AST/ALT 比值)来开发心血管疾病风险评估工具的重要性,旨在克服现有的不足之处。
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Role Played by Biochemical and Hematological Parameters in the Prediction of Cardiovascular Risk
Introduction: The term “cardiovascular diseases” (CVDs) refers to any disease affecting the heart or blood vessels. CVDs are the most common cause of death worldwide and the most responsible reason for 10% of deaths in the early 20th century. These CVDs can emerge as myocardial infarction or ischemic heart disease, stroke, and congestive heart failure. For diagnosing CVDs, physical, radiological investigations, and laboratory investigations for cardiac enzymes and lipid profile are used. In clinical practices, cardiovascular risk prediction models are very important in the identification, prevention, and staging of the severity of CVDs. Framingham Risk Score-coronary heart disease, Framingham Risk Score-cardiovascular disease, QRESEARCH-cardiovascular risk algorithm, Joint British Society risk-calculator-3, WHO/ISH CVD risk prediction charts, and Atherosclerotic Cardiovascular Disease risk-estimator are some of the available CVD risk estimators. However, many of these estimators can be used only to evaluate individuals more than 40 years and to assess the risk for 10-years.  Therefore, new risk estimators are needed to overcome the deficiencies of the available risk estimators. Research have been done in novel directions; on ratios of routinely performing hematological and biochemical laboratory parameters such as Neutrophil to Lymphocyte Ratio (NLR), Platelet to Lymphocyte Ratio (PLR), and Aspartate aminotransferase to Alanine aminotransferase ratio (AST/ALT). The outcomes indicate a relationship between the above-said ratios and the risk for CVDs.  Conclusion: On such grounds, this review describes the importance of developing a CVD risk estimator by amalgamating some of the biochemical and hematological parameters, including NLR, PLR, and AST/ALT ratios, aiming to overcome the existing shortcomings.
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