Initiation of the pharmacogenetics of capecitabine in Morocco

IF 0.4 Q4 ONCOLOGY
Khalid Zouine, Meryem Abassi, L. Bouguenouch, Ismail Mouhrach, Kettani Oussama, Souleimani Abdellah, Ouldim Karim, M. Nawfel
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引用次数: 1

Abstract

The pharmacogenetics of anticancer drugs is of paramount importance in minimizing their side effects and increasin their efficacy. When applied to capecitabine, the result is that variation in patient responses has been largely linked to different genetic polymorphisms of dihydropyrimidine dehydrogenase (DPD) and this variation explains in many cases the onset of toxicity of this medication in patients. Failure of this enzyme is known to be responsible for a high incidence of serious or even fatal side effects. In this study conducted on Moroccan patients under treatment with capecitabine at usual doses at the Fez University Hospital, the first in Africa and Morocco, we are looking for the presence of four variants of DPD gene (DPYD): T486A on exon 5 (rs666523971), c.1679T> G (p.I560S; rs55886062; allele DPYD * 13) on exon 13, c.1905 + 1G> A (IVS14 + 1G> A; rs3918290; allele DPYD * 2A) on the splice site near exon 14 and the c.2846A> T mutation (p.D949V; rs67376798) on exon 22. We will therefore seek to establish the cause-and-effect relationship between this toxicity and the presence of these variants in his patients, which will allow us to avoid the dangerous prescription of capecitabine in patients carrying these polymorphisms. This is a prospective study which is carried out at the Laboratory of Medical Genetics of the CHU Hassan II Fez and spread over a period of 3 years. Patient recruitment was carried out from the oncology department of CHU Hassan II-Fès. All recruited patients are treated with capecitabine A total of 64 patients were tested. Blood samples (5 ml) were obtained from each one of them after their consent and DNA was extracted. The study of these four polymorphisms was carried out by PCR sequencing. We have studied 64 patients taking capecitabine. Their median age was 50 years and the mean age of 50,79 years with extremes of 25 and 78 years. The sex ratio F / M was 0,60. Different levels of toxicity have been developed in patients ranging from simple vomiting to IV degree hand and foot syndrome and second degree neuropathy involving total discontinuation of treatment. These mutations were not found in the patients. Thus it would be interesting to enlarge the sample size, to look for these polymorphisms and others on other exons of the DPYD gene and to try to understand the cause of this increased incidence of capecitabine toxicity in the Moroccan population. Capecitabine-based chemotherapy caused adverse effects with varying levels in its patients. The SNPs on the DPYD gene sought were not found in this Moroccan sample. It is desirable to screen more patients and to search for other SNPs to understand the toxicity of capecitabine in relation to the DPYD gene. This will make it possible to adjust the dosage of this drug, increase its effectiveness and minimize its toxicity.
摩洛哥卡培他滨药物遗传学研究的开始
抗癌药物的药物遗传学对减少其副作用和提高其疗效至关重要。当应用于卡培他滨时,结果是患者反应的变化在很大程度上与二氢嘧啶脱氢酶(DPD)的不同遗传多态性有关,这种变异在许多情况下解释了该药物在患者中的毒性发作。众所周知,这种酶的失效是造成严重甚至致命副作用的原因。在非斯大学医院(Fez University Hospital)对接受卡培他滨常规剂量治疗的摩洛哥患者进行的这项研究中,我们正在寻找DPD基因(DPYD)的四种变体的存在:外显子5上的T486A (rs666523971), c.1679T> G (p.I560S;rs55886062;外显子13的等位基因DPYD * 13, c.1905 + 1G> A (IVS14 + 1G> A);rs3918290;等位基因DPYD * 2A)和c.2846A> T突变(p.D949V;Rs67376798)外显子22。因此,我们将寻求建立这种毒性与他的患者中这些变异的存在之间的因果关系,这将使我们能够避免对携带这些多态性的患者使用卡培他滨的危险处方。这是在朱哈桑二世非斯医学遗传学实验室进行的一项前瞻性研究,为期3年。患者招募从CHU Hassan ii - f的肿瘤科进行。所有招募的患者都接受卡培他滨治疗,总共64名患者接受了测试。经同意后,每人抽取血液样本(5ml)并提取DNA。对这4个多态性进行PCR测序研究。我们研究了64例服用卡培他滨的患者。他们的中位年龄为50岁,平均年龄为50岁,79岁,极端年龄为25岁和78岁。性别比F / M为0.60。不同程度的毒性已在患者中发展,从单纯呕吐到IV度手足综合征和涉及完全停止治疗的二度神经病变。这些突变在患者中未被发现。因此,扩大样本量,在DPYD基因的其他外显子上寻找这些多态性和其他多态性,并试图了解摩洛哥人群中卡培他滨毒性发生率增加的原因,将是很有趣的。以卡培他滨为基础的化疗在患者中引起不同程度的不良反应。在这个摩洛哥样本中没有发现DPYD基因上的snp。希望筛选更多的患者,并寻找其他snp,以了解卡培他滨与DPYD基因相关的毒性。这样就有可能调整这种药物的剂量,增加其效力并尽量减少其毒性。
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来源期刊
CiteScore
1.00
自引率
0.00%
发文量
50
期刊介绍: Current Cancer Therapy Reviews publishes frontier reviews on all the latest advances in clinical oncology, cancer therapy and pharmacology. The journal"s aim is to publish the highest quality review articles dedicated to clinical research in the field. The journal is essential reading for all researchers and clinicians in cancer therapy.
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