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干细胞与粒细胞集落刺激因子治疗创伤性脑损伤中的神经炎症:衰老作为一个合并症因素

Stem cells and G-CSF for treating neuroinflammation in traumatic brain injury: aging as a comorbidity factor.

作者信息

Dela Peña I, Sanberg P R, Acosta S, Tajiri N, Lin S Z, Borlongan C V

机构信息

Center of Excellence for Aging and Brain Repair Department of Neurosurgery and Brain Repair University of South Florida Morsani College of Medicine Tampa, FL, USA -

出版信息

J Neurosurg Sci. 2014 Sep;58(3):145-9. Epub 2014 May 20.

Abstract

Traumatic brain injury (TBI), often called the signature wound of Iraq and Afghanistan wars, is characterized by a progressive histopathology and long-lasting behavioral deficits. Treatment options for TBI are limited and patients are usually relegated to rehabilitation therapy and a handful of experimental treatments. Stem cell-based therapies offer alternative treatment regimens for TBI, and have been intended to target the delayed therapeutic window post-TBI, in order to promote "neuroregeneration," in lieu of "neuroprotection" which can be accomplished during acute TBI phase. However, these interventions may require adjunctive pharmacological treatments especially when aging is considered as a comorbidity factor for post-TBI health outcomes. Here, we put forward the concept that a combination therapy of human umbilical cord blood cell (hUCB) and granulocyte-colony stimulating factor (G-CSF) attenuates neuroinflammation in TBI, in view of the safety and efficacy profiles of hUCB and G-CSF, their respective mechanisms of action, and efficacy of hUCB+G-CSF combination therapy in TBI animal models. Further investigations on the neuroinflammatory pathway as a key pathological hallmark in acute and chronic TBI and also as a major therapeutic target of hUCB+G-CSF are warranted in order to optimize the translation of this combination therapy in the clinic.

摘要

创伤性脑损伤(TBI),常被称为伊拉克和阿富汗战争的标志性创伤,其特征在于进行性组织病理学变化和长期的行为缺陷。TBI的治疗选择有限,患者通常只能接受康复治疗和少数几种实验性治疗。基于干细胞的疗法为TBI提供了替代治疗方案,旨在针对TBI后的延迟治疗窗口,以促进“神经再生”,而非在急性TBI阶段所能实现的“神经保护”。然而,这些干预措施可能需要辅助药物治疗,尤其是当衰老被视为TBI后健康结果的合并症因素时。在此,鉴于人脐带血细胞(hUCB)和粒细胞集落刺激因子(G-CSF)的安全性和有效性概况、它们各自的作用机制以及hUCB+G-CSF联合疗法在TBI动物模型中的疗效,我们提出hUCB和G-CSF联合疗法可减轻TBI中的神经炎症这一概念。鉴于神经炎症途径是急性和慢性TBI的关键病理标志,也是hUCB+G-CSF的主要治疗靶点,有必要对其进行进一步研究,以优化这种联合疗法在临床上的转化应用。

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