Perspectives of personalized approach to prevention and treatment of anticonvulsant-induced osteoporosis via action on vitamin D exchange and VDR expression

E. Dontseva, V. V. Trefilova, T. Popova, M. Petrova, M. Al-Zamil
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引用次数: 1

Abstract

Anticonvulsant-induced osteoporosis (AIO) and associated pain syndromes and patient disabilities are an important interdisciplinary medical problem generated by various molecular, genetic and pathophysiological mechanisms. AIO are the most important pathological processes associated with chronic pain in adults with epilepsy. Standard approaches to their prevention and treatment do not always solve the problem of the progression of the pathological process and chronicity of AIO. This is the reason for the search for new personalized strategies for the prevention and treatment of AIO. Vitamin D metabolism, expression and specificity of vitamin D receptors (VDRs) may play a key role in the development of AIO and chronic back pain in patients with epilepsy. The aim of the study was to review publications on changes in the vitamin D system in patients with AIO. We searched for articles published in e-Library, PubMed, Oxford Press, Clinical Case, Springer, Elsevier, and Google Scholar. The search was carried out by key-words and their combinations. The role of vitamin D and VDR in the development of AIO and the chronicity of back pain has been demonstrated mainly in animal models and humans. Associative genetic studies have shown that single nucleotide variants (SNVs) of the VDR gene encoding VDR may be associated with the development of osteoporosis of the spine (including those associated with the intake of an anticonvulsants). The prospects for the use of vitamin D preparations for modulating the effect of anticonvulsants used to treat epilepsy are discussed. Genetic association studies of VDR gene SNVs are important for understanding the genetic predictors of AIO and chronic back pain in patients with epilepsy, as well as for developing new personalized pharmacotherapy strategies.
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通过对维生素D交换和VDR表达的作用预防和治疗抗惊厥性骨质疏松症的个性化方法的前景
抗惊厥性骨质疏松症(AIO)及其相关疼痛综合征和患者残疾是一个重要的跨学科医学问题,由多种分子、遗传和病理生理机制引起。AIO是与成人癫痫慢性疼痛相关的最重要的病理过程。标准的预防和治疗方法并不总能解决AIO病理过程的进展和慢性问题。这就是寻求新的个性化策略来预防和治疗AIO的原因。维生素D代谢、维生素D受体(VDRs)的表达和特异性可能在癫痫患者AIO和慢性背痛的发展中起关键作用。这项研究的目的是回顾有关AIO患者体内维生素D系统变化的出版物。我们搜索了发表在e-Library, PubMed, Oxford Press, Clinical Case, Springer, Elsevier和Google Scholar上的文章。搜索是通过关键词及其组合进行的。维生素D和VDR在AIO的发展和背部疼痛的慢性性中的作用主要在动物模型和人类中得到证实。相关遗传学研究表明,编码VDR的VDR基因的单核苷酸变异(SNVs)可能与脊柱骨质疏松症的发生有关(包括与服用抗惊厥药有关的骨质疏松症)。讨论了利用维生素D制剂调节用于治疗癫痫的抗惊厥药的作用的前景。VDR基因snv的遗传关联研究对于了解癫痫患者AIO和慢性背痛的遗传预测因素,以及制定新的个性化药物治疗策略具有重要意义。
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