The Impact of Pharmacogenomic CYP3A5 Variants on Calcineurin Inhibitor Metabolism and SLCO1B1 Variants on Methotrexate in Adult Allogeneic BMT Patients

Q4 Medicine
Mary Thoma, Kimberly Langer, Patricia McLean, David Dingli
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Abstract

Allogeneic blood and marrow transplant (BMT) is used to transplant a new immune system in patients with hematologic malignancies or immune-mediated disease. BMT patients require initial immune suppression to prevent graft rejection and graft versus host disease (GVHD). Tacrolimus and cyclosporine are calcineurin inhibitors (CNI) and methotrexate is an antimetabolite used to mitigate this immune response. Tacrolimus has data supporting oral dose variation based on pharmacogenomic (PGx) studies for Intermediate Metabolizers (IM) and Poor Metabolizers (PM) on studies done in kidney transplant patients. There are fewer studies on BMT patients in this field, and even less on the variability of IV to oral conversion dosing and first pass metabolism effect based on PGx profiles. Methotrexate has been shown to have PGx mutations affecting its metabolism at higher dosing used for chemotherapy, but its impact on BMT patient dosing is not well-defined. Based on our study, we found statistically significant variability in Tacrolimus concentration based on drug assay levels compared with dosing for Intravenous (IV) and oral formulation based on PGx predicted phenotypes. We further noted a profound effect on first pass metabolism when transitioning between IV and oral dosing of Tacrolimus based on PGx predicted phenotypes. The average oral dose in predicted IM phenotypes divided by the IV dose was 2.68. For the predicted PM phenotype, the average oral dose divided by the IV dose was 1.18. The p-value in a two-tailed nonparametric T-test with equal variance assessing the conversion factor from IV to oral dosing in predicted IM versus PM phenotypes was significant with a p-value of 0.002. Methotrexate metabolism did not seem to be affected by PGx mutations at the doses used for BMT GVHD prevention.

药物基因组学CYP3A5变异对钙调磷酸酶抑制剂代谢的影响以及SLCO1B1变异对成人异基因BMT患者甲氨蝶呤的影响
同种异体血液和骨髓移植(BMT)用于移植新的免疫系统的患者血液恶性肿瘤或免疫介导的疾病。BMT患者需要初始免疫抑制来预防移植物排斥和移植物抗宿主病(GVHD)。他克莫司和环孢素是钙调磷酸酶抑制剂(CNI),甲氨蝶呤是一种用于减轻这种免疫反应的抗代谢物。他克莫司有数据支持基于药物基因组学(PGx)研究的中间代谢物(IM)和差代谢物(PM)在肾移植患者中的口服剂量变化。该领域对BMT患者的研究较少,基于PGx谱的静脉到口服转换剂量的变异性和首过代谢效应的研究更少。甲氨蝶呤已被证明在化疗中使用高剂量时,PGx突变会影响其代谢,但其对BMT患者剂量的影响尚不明确。根据我们的研究,我们发现基于药物检测水平的他克莫司浓度与基于PGx预测表型的静脉注射(IV)和口服制剂的剂量相比具有统计学上显著的差异。我们进一步注意到,根据PGx预测的表型,他克莫司在IV和口服剂量之间转换时对首过代谢的深远影响。预测IM表型的平均口服剂量除以静脉剂量为2.68。对于预测的PM表型,平均口服剂量除以静脉剂量为1.18。双尾非参数t检验的等方差评估从静脉给药到口服给药在预测IM与PM表型中的转换因子的p值显著,p值为0.002。在用于BMT GVHD预防的剂量下,甲氨蝶呤代谢似乎不受PGx突变的影响。
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来源期刊
Transplantation Reports
Transplantation Reports Medicine-Transplantation
CiteScore
0.60
自引率
0.00%
发文量
24
审稿时长
101 days
期刊介绍: To provide to national and regional audiences experiences unique to them or confirming of broader concepts originating in large controlled trials. All aspects of organ, tissue and cell transplantation clinically and experimentally. Transplantation Reports will provide in-depth representation of emerging preclinical, impactful and clinical experiences. -Original basic or clinical science articles that represent initial limited experiences as preliminary reports. -Clinical trials of therapies previously well documented in large trials but now tested in limited, special, ethnic or clinically unique patient populations. -Case studies that confirm prior reports but have occurred in patients displaying unique clinical characteristics such as ethnicities or rarely associated co-morbidities. Transplantation Reports offers these benefits: -Fast and fair peer review -Rapid, article-based publication -Unrivalled visibility and exposure for your research -Immediate, free and permanent access to your paper on Science Direct -Immediately citable using the article DOI
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