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Cardiovascular risk assessment of dyslipidemic children: analysis of biomarkers to identify monogenic dyslipidemia

机译:血脂异常儿童的心血管风险评估:生物标志物分析以鉴定单基因血脂异常

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The distinction between a monogenic dyslipidemia and a polygenic/environmental dyslipidemia is important for the cardiovascular risk assessment, counseling, and treatment of these patients. The present work aims to perform the cardiovascular risk assessment of dyslipidemic children to identify useful biomarkers for clinical criteria improvement in clinical settings. Main cardiovascular risk factors were analyzed in a cohort of 237 unrelated children with clinical diagnosis of familial hypercholesterolemia (FH). About 40% carried at least two cardiovascular risk factors and 37.6% had FH, presenting mutations in LDLR and APOB. FH children showed significant elevated atherogenic markers and lower concentration of antiatherogenic particles. Children without a molecular diagnosis of FH had higher levels of TGs, apoC2, apoC3, and higher frequency of BMI and overweight/obesity, suggesting that environmental factors can be the underlying cause of their hypercholesterolem[≥]ia. An apoB/apoA1 ratio [≥]0.68 was identified as the best biomarker (area under the curve = 0.835) to differentiate FH from other dyslipidemias. The inclusion in clinical criteria of a higher cut-off point for LDL cholesterol or an apoB/apoA1 ratio [≥]0.68 optimized the criteria sensitivity and specificity. The correct identification, at an early age, of all children at-risk is of great importance so that specific interventions can be implemented. apoB/apoA1 can improve the identification of FH patients.
机译:单基因血脂异常和多基因/环境血脂异常之间的区别对于这些患者的心血管风险评估,咨询和治疗很重要。本工作旨在对血脂异常儿童进行心血管风险评估,以鉴定有用的生物标记物,以改善临床环境中的临床标准。在一项临床诊断为家族性高胆固醇血症(FH)的237名无关儿童中分析了主要的心血管危险因素。大约40%的人携带至少两种心血管危险因素,而37.6%的人患有FH,表现出LDLR和APOB突变。跳频儿童表现出明显的动脉粥样硬化标志物升高和较低的抗动脉粥样硬化颗粒浓度。未进行FH分子诊断的儿童的TG,apoC2,apoC3含量较高,BMI发生频率较高,并且超重/肥胖,这表明环境因素可能是其高胆固醇血症[≥] ia的根本原因。 apoB / apoA1比[≥] 0.68被认为是区分FH与其他血脂异常的最佳生物标志物(曲线下面积= 0.835)。在临床标准中纳入较高的LDL胆固醇临界值或apoB / apoA1比[≥] 0.68可优化标准的敏感性和特异性。正确识别所有处于危险之中的儿童,在早期就非常重要,因此可以实施特定的干预措施。 apoB / apoA1可以改善FH患者的识别。

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