Autologous cell using for the restoration of functional defects in patients with ischemic cerebrovascular accident

E. Pedachenko, V. Moroz, V. Yatsyk, U. I. Malyar, L. Liubich, D. Egorova
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引用次数: 3

Abstract

Stroke is a global medical and socio-economic problem and a great demand for alternative therapies, the leading one being stem cell (SC) therapy. Pathogenetic processes in ischemic stroke (II) trigger the mechanisms of necrotic and apoptotic death of neurons with the formation of the central infarct zone («core of ischemia») and the ischemic «penumbra» zone; the severity and reversibility of the injury directly depends on the duration of ischemia. In parallel with pathogenetic processes, endogenous neurogenesis occurs – the proliferation of neurogenic stem and progenitor cells (NSC/NPC) and their migration into the ischemic focus; however, most NSCs and newly formed neurons undergo apoptosis and recovery of lost functions does not occur. Significant efforts are being made to find ways to control neurogenesis, in particular through the transplantation of exogenous SCs. The main factors preventing the use of SCs in humans are moral, ethical, religious and legal aspects related to the source and method of obtaining cells, as well as possible immunocompromised complications due to incompatibility of donor cells with the recipient of the main histocompatibility complex antigens. The safest is the use of autologous SCs (the patient’s own cells), as it does not require the use of immunosuppressive protocols. Due to the relative safety and ease of production, the most common are multipotent mesenchymal stem cells (MSCs), namely MSCs of the bone marrow (BM). Numerous preclinical studies in experimental animals with modeled II, as well as clinical trials conducted over the past 15 years, have shown the safety and feasibility of transplantation of autologous MSCs in patients with severe neurological deficits after II. Two different approaches to the use of MSCs are discussed: neuroprotection in the acute phase and neurorestoration in the chronic phase II. Proposals are currently being developed for phase II/III clinical trials in acute and chronic stroke using BM MSCs, the results of which will form the basis for certified standardized II treatment protocols.
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自体细胞用于缺血性脑血管意外患者功能缺损的修复
中风是一个全球性的医疗和社会经济问题,对替代疗法的需求很大,其中最主要的是干细胞(SC)疗法。缺血性中风的发病过程(II)通过形成中央梗死区(“缺血核心”)和缺血性“半影”区,触发神经元坏死和凋亡死亡的机制;损伤的严重程度和可逆性直接取决于缺血的持续时间。在发病过程的同时,发生内源性神经发生——神经源性干细胞和祖细胞(NSC/NPC)的增殖及其向缺血灶的迁移;然而,大多数NSCs和新形成的神经元发生凋亡,并且没有发生丧失功能的恢复。目前正在努力寻找控制神经发生的方法,特别是通过移植外源性干细胞。阻止SC在人类中使用的主要因素是与获得细胞的来源和方法有关的道德、伦理、宗教和法律方面,以及由于供体细胞与主要组织相容性复合物抗原受体不相容而可能出现的免疫功能低下并发症。最安全的是使用自体SC(患者自身的细胞),因为它不需要使用免疫抑制方案。由于相对安全和易于生产,最常见的是多能间充质干细胞(MSC),即骨髓的MSC。在具有模型II的实验动物中进行的大量临床前研究,以及在过去15年中进行的临床试验,已经表明在II后严重神经缺陷的患者中移植自体MSCs的安全性和可行性。讨论了使用MSCs的两种不同方法:急性期的神经保护和慢性II期的神经修复。目前正在制定使用骨髓间充质干细胞进行急性和慢性中风II/III期临床试验的建议,其结果将构成经认证的标准化II治疗方案的基础。
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