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辐射诱导的脑损伤:神经再生的易解决问题

Radiation-induced brain injury: low-hanging fruit for neuroregeneration.

作者信息

Burns Terry C, Awad Ahmed J, Li Matthew D, Grant Gerald A

机构信息

Department of Neurosurgery and Institute for Stem Cell Biology and Regenerative Medicine, Stanford University, Stanford, California;

Department of Neurosurgery, Icahn School of Medicine at Mount Sinai, New York, New York;

出版信息

Neurosurg Focus. 2016 May;40(5):E3. doi: 10.3171/2016.2.FOCUS161.

Abstract

Brain radiation is a fundamental tool in neurooncology to improve local tumor control, but it leads to profound and progressive impairments in cognitive function. Increased attention to quality of life in neurooncology has accelerated efforts to understand and ameliorate radiation-induced cognitive sequelae. Such progress has coincided with a new understanding of the role of CNS progenitor cell populations in normal cognition and in their potential utility for the treatment of neurological diseases. The irradiated brain exhibits a host of biochemical and cellular derangements, including loss of endogenous neurogenesis, demyelination, and ablation of endogenous oligodendrocyte progenitor cells. These changes, in combination with a state of chronic neuroinflammation, underlie impairments in memory, attention, executive function, and acquisition of motor and language skills. Animal models of radiation-induced brain injury have demonstrated a robust capacity of both neural stem cells and oligodendrocyte progenitor cells to restore cognitive function after brain irradiation, likely through a combination of cell replacement and trophic effects. Oligodendrocyte progenitor cells exhibit a remarkable capacity to migrate, integrate, and functionally remyelinate damaged white matter tracts in a variety of preclinical models. The authors here critically address the opportunities and challenges in translating regenerative cell therapies from rodents to humans. Although valiant attempts to translate neuroprotective therapies in recent decades have almost uniformly failed, the authors make the case that harnessing human radiation-induced brain injury as a scientific tool represents a unique opportunity to both successfully translate a neuroregenerative therapy and to acquire tools to facilitate future restorative therapies for human traumatic and degenerative diseases of the central nervous system.

摘要

脑部放疗是神经肿瘤学中改善局部肿瘤控制的一项基本手段,但它会导致认知功能出现严重且渐进性的损害。神经肿瘤学中对生活质量的日益关注加速了人们对放疗引起的认知后遗症的理解和改善。这一进展与对中枢神经系统祖细胞群体在正常认知中的作用及其在治疗神经疾病方面潜在效用的新认识相契合。接受放疗的大脑会出现一系列生化和细胞紊乱,包括内源性神经发生丧失、脱髓鞘以及内源性少突胶质细胞祖细胞的消融。这些变化与慢性神经炎症状态共同导致记忆、注意力、执行功能以及运动和语言技能习得方面的损害。放疗诱导的脑损伤动物模型已证明,神经干细胞和少突胶质细胞祖细胞都具有强大的能力,能够在脑部放疗后恢复认知功能,这可能是通过细胞替代和营养作用的结合实现的。在各种临床前模型中,少突胶质细胞祖细胞表现出显著的迁移、整合以及对受损白质束进行功能性髓鞘再生的能力。本文作者批判性地探讨了将再生细胞疗法从啮齿动物转化应用于人类所面临的机遇和挑战。尽管近几十年来将神经保护疗法转化应用的英勇尝试几乎都以失败告终,但作者认为,将人类放疗诱导的脑损伤作为一种科学工具,代表着一个独特的机遇,既能成功转化一种神经再生疗法,又能获得有助于未来治疗人类中枢神经系统创伤性和退行性疾病的恢复性疗法的工具。

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