癌症患者中环磷酰胺毒性与 CYP2B6 药物遗传学缺乏关联。

Lack of association of CYP2B6 pharmacogenetics with cyclophosphamide toxicity in patients with cancer.

机构信息

Department of Clinical Pharmacy, University of Michigan College of Pharmacy, Room 2560C, 428 Church St., Ann Arbor, MI, 48109-1065, USA.

Department of Biostatistics, University of Michigan School of Public Health, Ann Arbor, MI, 48109-2029, USA.

出版信息

Support Care Cancer. 2022 Sep;30(9):7355-7363. doi: 10.1007/s00520-022-07118-y. Epub 2022 May 24.

DOI:10.1007/s00520-022-07118-y

PMID:35606478

Abstract

PURPOSE

Cyclophosphamide is a commonly used cancer agent that is metabolically activated by polymorphic enzymes. This study aims to investigate the association between predicted activity of candidate pharmacogenes with severe toxicity during cyclophosphamide treatment.

METHODS

Genome-wide genetic data was collected from an institutional genetic data repository for CYP2B6, CYP3A4, CYP2C9, CYP2C19, GSTA1, GSTP1, ALDH1A1, ALDH3A1, ABCC1, ABCB1, and ERCC1. Treatment and toxicity data were retrospectively collected from the patient's medical record. The a priori selected primary hypothesis was that patients who have CYP2B6 reduced metabolizer activity (poor or intermediate (PM/IM) vs. normal (NM) metabolizer) have lower risk of severe toxicity or cyclophosphamide treatment modification due to toxicity.

RESULTS

In the primary analysis of 510 cyclophosphamide-treated patients with available genetic data, there was no difference in the odds of severe toxicity or treatment modification due to toxicity in CYP2B6 PM/IM vs. NM (odds ratio = 0.97, 95% Confidence Interval: 0.62-1.50, p = 0.88). In an exploratory, statistically uncorrected secondary analysis, carriers of the ALDH1A1 rs8187996 variant had a lower risk of the primary toxicity endpoint compared with wild-type homozygous patients (odds ratio = 0.31, 95% Confidence Interval: 0.09-0.78, p = 0.028). None of the other tested phenotypes or genotypes was associated with the primary or secondary endpoints in unadjusted analysis (all p > 0.05).

CONCLUSION

The finding that patients who carry ALDH1A1 rs8187996 may have a lower risk of cyclophosphamide toxicity than wild-type patients contradicts a prior finding for this variant and should be viewed with skepticism. We found weak evidence that any of these candidate pharmacogenetic predictors of cyclophosphamide toxicity may be useful to personalize cyclophosphamide dosing to optimize therapeutic outcomes in patients with cancer.

摘要

目的

环磷酰胺是一种常用的癌症治疗药物，其代谢活性由多态性酶所激活。本研究旨在探讨候选药物代谢基因的预测活性与环磷酰胺治疗期间严重毒性之间的关联。

方法

从机构遗传数据存储库中收集 CYP2B6、CYP3A4、CYP2C9、CYP2C19、GSTA1、GSTP1、ALDH1A1、ALDH3A1、ABCC1、ABCB1 和 ERCC1 的全基因组遗传数据。从患者的病历中回顾性收集治疗和毒性数据。预先选择的主要假设是，具有 CYP2B6 低代谢活性（弱代谢或中间代谢（PM/IM）与正常代谢（NM））的患者由于毒性而发生严重毒性或环磷酰胺治疗改变的风险较低。

结果

在对 510 名接受环磷酰胺治疗且具有可用遗传数据的患者进行的主要分析中，CYP2B6 PM/IM 与 NM 相比，严重毒性或因毒性而改变治疗的可能性没有差异（比值比=0.97，95%置信区间：0.62-1.50，p=0.88）。在未经统计学校正的探索性次要分析中，ALDH1A1 rs8187996 变异携带者与野生型纯合子患者相比，主要毒性终点的风险较低（比值比=0.31，95%置信区间：0.09-0.78，p=0.028）。在未调整分析中，未发现其他测试表型或基因型与主要或次要终点相关（均 p>0.05）。

结论

携带 ALDH1A1 rs8187996 的患者发生环磷酰胺毒性的风险可能低于野生型患者的这一发现与先前该变异的发现相矛盾，应持怀疑态度。我们发现，这些候选药物代谢基因预测环磷酰胺毒性的指标中，任何一个都可能有助于为癌症患者个性化环磷酰胺剂量，以优化治疗效果，但证据较弱。

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癌症患者中环磷酰胺毒性与 CYP2B6 药物遗传学缺乏关联。

Lack of association of CYP2B6 pharmacogenetics with cyclophosphamide toxicity in patients with cancer.

机构信息

出版信息

PURPOSE

METHODS

RESULTS

CONCLUSION

目的

方法

结果

结论

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