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Pharmacogenomic testing and outcome among depressed patients in a tertiary care outpatient psychiatric consultation practice

机译:三级门诊精神科咨询实践中抑郁症患者的药物基因组学测试和结果

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The authors tested the hypothesis that pharmacogenomic genotype knowledge is associated with better clinical and cost outcomes in depressed patients, after controlling for other factors that might differentiate tested and non-tested patients. Medical records of 251 patients, seen in the Mayo Clinic Rochester outpatient psychiatric practice, who had patient health questionnaire-9 (PHQ-9) scores before and after consultation, were reviewed. Comparisons of differences in pre-consultation and post-consultation depression scores and slopes between tested and non-tested patients and between genotype categories of tested patients, were evaluated, along with healthcare cost and utilization comparisons between tested and non-tested patients, using Kruskal–Wallis tests, Wilcoxon rank-sum tests and group mean comparisons, controlling for significant univariate demographic and clinical differences. Tested patients had significantly higher depression diagnosis frequency, baseline PHQ-9 scores, family history of depression, psychiatric hospitalization history, and higher numbers of antidepressant, mood stabilizer and antipsychotic medication trials. After controlling for these differences, there were no differences between tested and non-tested patients in post-baseline depression scores or slopes for CYP genotype categories. For patients with 5-HTTLPR testing, there was significantly more depression score improvement for patients with the long/long genotype at time 4 (N=55, χ2-value=8.0492, P=0.018) and at time 5 (N=44, χ2-value=6.1492, P=0.046). For a subgroup (n=46) with two pre- and two post-baseline PHQ-9 scores, the mean difference between pre-baseline and post-baseline PHQ-9 score slopes for tested patients was ?0.08 (median ?0.01; range ?1.20 to 0.15) compared with 0.13 (median 0.02; range ?0.18 to 2.16) for non-tested patients (P=0.03). Among genotype categories, mean differences between pre-consultation and post-consultation slopes were significantly better for poor CYP2D6 metabolizers than intermediate or extensive metabolizers (P=0.04); there was a trend for slope differences to be better for 5-HTTLPR long/long genotype patients (P=0.06). Subsets of local tested and consultant-adjusted non-tested controls (n=19), who had 8 years of longitudinal care within the health system, had similar overall mean healthcare costs before and after testing; however, tested patients on average had significantly fewer time-adjusted post-baseline psychiatric admissions (0.8 vs 3.8, P=0.04) and fewer time-adjusted psychiatric consultations and comprehensive mental health-specialty evaluations (4.2 vs 9.9, P=0.03). Prospective study is indicated as to whether and how pharmacogenomic testing in a psychiatric consultation practice may improve clinical and cost outcomes.. ? 2011 Macmillan Publishers Limited
机译:在控制了可能使被测患者与未测患者区别开来的其他因素之后,作者检验了以下假设:在抑郁症患者中,药物基因组学基因型知识与更好的临床和成本结果相关。回顾了在梅奥诊所罗切斯特门诊精神病学实践中见到的251例患者的医疗记录,这些患者在咨询前后均进行了患者健康问卷9(PHQ-9)评分。使用Kruskal评估了接受测试的和未接受测试的患者之间以及接受测试的患者的基因型类别之间的咨询前和咨询后抑郁评分和斜率的差异,并进行了医疗成本和利用率的比较。 –Wallis检验,Wilcoxon秩和检验和组均值比较,以控制显着的单变量人口统计学和临床​​差异。受测患者的抑郁症诊断频率,基线PHQ-9得分,抑郁症家族史,精神病住院史以及抗抑郁药,情绪稳定剂和抗精神病药物试验的次数均明显更高。在控制了这些差异之后,测试后和未测试的患者在基线后抑郁评分或CYP基因型类别的斜率方面没有差异。对于具有5-HTTLPR测试的患者,具有长基因型/长基因型的患者在第4时的抑郁评分改善显着更多(N = 55,χ 2 -值= 8.0492,P = 0.018),并且在时间5(N = 44,χ 2 -值= 6.1492,P = 0.046)。对于基线水平前两个和基线后两个水平的QQ-9得分的亚组(n = 46),被测患者基线前和基线后PHQ-9得分斜率的平均差为±0.08(中位数为0.01) ;未经测试的患者为(1.20至0.15),而未经测试的患者为0.13(中位数0.02;范围为0.18至2.16)(P = 0.03)。在基因型类别中,不良CYP2D6代谢者的咨询前和咨询后斜率之间的平均差异明显优于中度或广泛代谢者(P = 0.04); 5-HTTLPR长/长基因型患者的斜率差异有改善的趋势(P = 0.06)。在卫生系统内进行了8年纵向护理的本地经过测试和经顾问调整的未经测试的对照组(n = 19)的子集在测试前后的总体平均医疗保健费用相似;然而,接受测试的患者平均而言,经过时间调整的基线后精神科入院人数明显减少(0.8 vs 3.8,P = 0.04),经过时间调整的精神科咨询和全面的心理健康专业评估(4.2 vs 9.9,P = 0.03)更少。对精神科咨询实践中的药物基因组学测试是否以及如何改善临床和成本结果进行了前瞻性研究。 2011 Macmillan Publishers Limited

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