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The impact of pharmacogenomic factors on steroid dependency in pediatric heart transplant patients using logistic regression analysis.

机译:使用Logistic回归分析,药物基因组学因素对小儿心脏移植患者类固醇依赖性的影响。

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Zheng HX, Webber SA, Zeevi A, Schuetz E, Zhang J, Lamba J, Boyle GJ, Wilson JW, Burckart GJ. The impact of pharmacogenomic factors on steroid dependency in pediatric heart transplant patients using logistic regression analysis. Pediatr Transplantation 2004. (c) 2004 Blackwell MunksgaardAbstract: Many pharmacogenomic predictors of drug response are now available, and include both drug metabolism-disposition factors and drug targets. Information on statistical approaches to analyzing large clinical data sets in relation to genetic polymorphisms is limited. The objective of this study was to evaluate whether logistic regression could identify pharmacogenomic predictors of outcome in a large data set in a complex transplant patient population. Seventy pediatric heart transplant patients were studied. Patients were followed for at least 1 yr post-transplantation as outpatients, and weaned from corticosteroids if clinically appropriate. Logistic regression analysis was used to identify the predictors of steroid dependency. The dependent variable was the presence or absence of steroid therapy at 1 yr post-transplantation. The independent variables were the patients' transplant age, gender, MDR1 C3435T and G2677T, CYP3A53B and cytokine polymorphisms. By chi-square test for the MDR1 C3435T polymorphism, 12 of 18 (67%) patients in the CC group were still on prednisone, whereas only 18 of 47 (38%) of the CT/TT group were still receiving prednisone (p = 0.04). For the IL-10 groups, two of 15 patients with the high producer genotype (13.3%) remained on prednisone, in comparison with 16 of 28 patients with the intermediate producer genotype (57.1%) and 15 of 26 patients with the low producer genotype (57.7%, p = 0.01). Logistic regression analysis confirmed MDR1 C3435T (p = 0.021), and IL-10 polymorphisms (intermediate producer genotype p = 0.015; low producer genotype p = 0.013) as independent risk factors for steroid dependency at 1 yr after transplantation. This approach identifies pharmacogenomic factors, which can be studied more extensively in larger data sets, and used in prospective studies to individualize immunosuppressive therapy following solid organ transplantation.
机译:Zheng HX,Webber SA,Zeevi A,Schuetz E,Zhang J,Lamba J,Boyle GJ,Wilson JW,Burckart GJ。使用Logistic回归分析,药物基因组学因素对小儿心脏移植患者类固醇依赖性的影响。 Pediatr Transplantation2004。(c)2004 Blackwell Munksgaard摘要:现在可以找到许多药物反应的药物基因组学预测因子,包括药物代谢处​​置因子和药物靶标。关于与遗传多态性有关的分析大型临床数据集的统计方法的信息有限。这项研究的目的是评估逻辑回归是否可以在复杂的移植患者群体的大量数据中确定药物基因组学预测结果的指标。研究了70名小儿心脏移植患者。门诊患者在移植后至少随访1年,并在临床上适当的情况下停用皮质类固醇激素。 Logistic回归分析用于确定类固醇依赖的预测因子。因变量是移植后1年是否存在类固醇治疗。自变量是患者的移植年龄,性别,MDR1 C3435T和G2677T,CYP3A53B和细胞因子多态性。通过对MDR1 C3435T多态性的卡方检验,CC组的18名患者中有12名(67%)仍在接受泼尼松治疗,而CT / TT组的47名患者中只有18名(38%)仍在接受泼尼松治疗(p = 0.04)。对于IL-10组,泼尼松仍保留15例高生产者基因型患者中的2例(13.3%),而28例中等生产者基因型患者中的16例(57.1%)和26例低生产者基因型患者中的15例(57.7%,p = 0.01)。 Logistic回归分析证实了MDR1 C3435T(p = 0.021)和IL-10多态性(中间生产者基因型p = 0.015;低生产者基因型p = 0.013)是移植后1年类固醇依赖的独立危险因素。这种方法确定了药物基因组学因素,可以在更大的数据集中进行更广泛的研究,并将其用于前瞻性研究中,以对实体器官移植后的免疫抑制疗法进行个体化。

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