Wessam El-Sayed, Abdelaziz M Hussein, Ibrahim Elmenshawi, Ghada Helal, Mohammed Abbas, Abdelnaser Badawy, Nedaa A Kiwan, Mahmoud El Tohamy, Ghada Awadalla, Osama A Abulseoud
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In this study, we investigate gene glutamate-ammonia ligase (GLUL) polymorphisms for the glutamine synthetase (GS) enzyme, a key enzyme that catalyzes the removal of ammonia by incorporating it with glutamate to form glutamine, and we investigate whether it has a relationship with the emergence of hyperammonemia during VPA-based therapy.</p><p><strong>Patients and methods: </strong>We enrolled 180 Egyptian epilepsy patients in this study. Patient history, general and neurological examination and blood samples from arm veins were taken. Real time TaqMan PCR polymorphism for three polymorphism SNPs (rs2296521, rs10911021 and rs12136955) of GLUL was done. We assessed the relationship between the patient features, including three GLUL polymorphisms, and the development of hyperammonemia during VPA-based therapy.</p><p><strong>Results: </strong>We found that the ammonia levels showed a positive correlation with VPA treatment duration (p = 0.015) and a negative correlation with carbamazepine total dose per day (p = 0.027) and with WBCs count (p = 0.026). Also, female patients having rs2296521 SNPs with the A allele and patients having rs10911021 SNPs with the C allele were at high risk for elevated plasma ammonia levels. Moreover, patients having rs12136955 SNPs with the A allele or associated hypertension as a co-morbidity were at high risk for elevated plasma ammonia levels.</p><p><strong>Conclusion: </strong>Female patients who have rs2296521 with the A allele, rs10911021 with the C allele, or rs12136955 with the A allele, are independent risk factors for elevated plasma ammonia levels during VPA-based therapy. Moreover, carbamazepine combined therapy may protect against the development of hyperammonemia in VPA-treated patients.</p>","PeriodicalId":19132,"journal":{"name":"Neurologia i neurochirurgia polska","volume":null,"pages":null},"PeriodicalIF":2.9000,"publicationDate":"2024-01-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Association of glutamine synthetase polymorphisms rs2296521, rs10911021 and rs12136955 with plasma ammonia concentration in valproic acid-treated Egyptian epilepsy patients.\",\"authors\":\"Wessam El-Sayed, Abdelaziz M Hussein, Ibrahim Elmenshawi, Ghada Helal, Mohammed Abbas, Abdelnaser Badawy, Nedaa A Kiwan, Mahmoud El Tohamy, Ghada Awadalla, Osama A Abulseoud\",\"doi\":\"10.5603/pjnns.99826\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><strong>Introduction: </strong>The use of valproic acid (VPA) in the treatment of some psychiatric and neurological disorders such as bipolar disorder, migraines, and epilepsy is associated with hyperammonemia. However, the mechanism of this negative effect of VPA is unclear. In this study, we investigate gene glutamate-ammonia ligase (GLUL) polymorphisms for the glutamine synthetase (GS) enzyme, a key enzyme that catalyzes the removal of ammonia by incorporating it with glutamate to form glutamine, and we investigate whether it has a relationship with the emergence of hyperammonemia during VPA-based therapy.</p><p><strong>Patients and methods: </strong>We enrolled 180 Egyptian epilepsy patients in this study. Patient history, general and neurological examination and blood samples from arm veins were taken. Real time TaqMan PCR polymorphism for three polymorphism SNPs (rs2296521, rs10911021 and rs12136955) of GLUL was done. We assessed the relationship between the patient features, including three GLUL polymorphisms, and the development of hyperammonemia during VPA-based therapy.</p><p><strong>Results: </strong>We found that the ammonia levels showed a positive correlation with VPA treatment duration (p = 0.015) and a negative correlation with carbamazepine total dose per day (p = 0.027) and with WBCs count (p = 0.026). Also, female patients having rs2296521 SNPs with the A allele and patients having rs10911021 SNPs with the C allele were at high risk for elevated plasma ammonia levels. Moreover, patients having rs12136955 SNPs with the A allele or associated hypertension as a co-morbidity were at high risk for elevated plasma ammonia levels.</p><p><strong>Conclusion: </strong>Female patients who have rs2296521 with the A allele, rs10911021 with the C allele, or rs12136955 with the A allele, are independent risk factors for elevated plasma ammonia levels during VPA-based therapy. 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引用次数: 0
摘要
简介使用丙戊酸(VPA)治疗双相情感障碍、偏头痛和癫痫等精神和神经疾病与高氨血症有关。然而,VPA 产生这种负面影响的机制尚不清楚。在这项研究中,我们调查了谷氨酰胺合成酶(GS)的基因谷氨酸-氨连接酶(GLUL)多态性,GS酶是催化氨与谷氨酸结合形成谷氨酰胺从而清除氨的一种关键酶,我们还调查了它是否与基于 VPA 治疗期间出现的高氨血症有关:本研究共招募了 180 名埃及癫痫患者。采集了患者病史、全身和神经系统检查以及手臂静脉血样本。对 GLUL 的三个多态性 SNP(rs2296521、rs10911021 和 rs12136955)进行了实时 TaqMan PCR 多态性分析。我们评估了患者特征(包括 GLUL 的三个多态性)与 VPA 治疗期间高氨血症发生之间的关系:结果:我们发现,氨水平与 VPA 治疗时间呈正相关(p = 0.015),与卡马西平每日总剂量呈负相关(p = 0.027),与白细胞计数呈负相关(p = 0.026)。此外,等位基因为 A 的 rs2296521 SNPs 女性患者和等位基因为 C 的 rs10911021 SNPs 患者是血浆氨水平升高的高危人群。此外,等位基因为 A 的 rs12136955 SNPs 患者或合并高血压的患者也是血浆氨水平升高的高危人群:结论:等位基因为 A 的 rs2296521、等位基因为 C 的 rs10911021 或等位基因为 A 的 rs12136955 的女性患者是 VPA 治疗期间血浆氨水平升高的独立风险因素。此外,卡马西平联合疗法可防止 VPA 治疗患者出现高氨血症。
Association of glutamine synthetase polymorphisms rs2296521, rs10911021 and rs12136955 with plasma ammonia concentration in valproic acid-treated Egyptian epilepsy patients.
Introduction: The use of valproic acid (VPA) in the treatment of some psychiatric and neurological disorders such as bipolar disorder, migraines, and epilepsy is associated with hyperammonemia. However, the mechanism of this negative effect of VPA is unclear. In this study, we investigate gene glutamate-ammonia ligase (GLUL) polymorphisms for the glutamine synthetase (GS) enzyme, a key enzyme that catalyzes the removal of ammonia by incorporating it with glutamate to form glutamine, and we investigate whether it has a relationship with the emergence of hyperammonemia during VPA-based therapy.
Patients and methods: We enrolled 180 Egyptian epilepsy patients in this study. Patient history, general and neurological examination and blood samples from arm veins were taken. Real time TaqMan PCR polymorphism for three polymorphism SNPs (rs2296521, rs10911021 and rs12136955) of GLUL was done. We assessed the relationship between the patient features, including three GLUL polymorphisms, and the development of hyperammonemia during VPA-based therapy.
Results: We found that the ammonia levels showed a positive correlation with VPA treatment duration (p = 0.015) and a negative correlation with carbamazepine total dose per day (p = 0.027) and with WBCs count (p = 0.026). Also, female patients having rs2296521 SNPs with the A allele and patients having rs10911021 SNPs with the C allele were at high risk for elevated plasma ammonia levels. Moreover, patients having rs12136955 SNPs with the A allele or associated hypertension as a co-morbidity were at high risk for elevated plasma ammonia levels.
Conclusion: Female patients who have rs2296521 with the A allele, rs10911021 with the C allele, or rs12136955 with the A allele, are independent risk factors for elevated plasma ammonia levels during VPA-based therapy. Moreover, carbamazepine combined therapy may protect against the development of hyperammonemia in VPA-treated patients.
期刊介绍:
Polish Journal of Neurology and Neurosurgery is an official journal of the Polish Society of Neurology and the Polish Society of Neurosurgeons, aimed at publishing high quality articles within the field of clinical neurology and neurosurgery, as well as related subspecialties. For more than a century, the journal has been providing its authors and readers with the opportunity to report, discuss, and share the issues important for every-day practice and research advances in the fields related to neurology and neurosurgery.
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