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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Cytokine-mediated blood brain barrier disruption as a conduit for cancer/chemotherapy-associated neurotoxicity and cognitive dysfunction
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Cytokine-mediated blood brain barrier disruption as a conduit for cancer/chemotherapy-associated neurotoxicity and cognitive dysfunction

机译:细胞因子介导的血脑屏障破坏作为癌症/化学疗法相关神经毒性和认知功能障碍的管道

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摘要

Neurotoxicity is a common side effect of chemotherapy treatment, with unclear molecular mechanisms. Clinical studies suggest that the most frequent neurotoxic adverse events affect memory and learning, attention, concentration, processing speeds and executive function. Emerging preclinical research points toward direct cellular toxicity and induction of neuroinflammation as key drivers of neurotoxicity and subsequent cognitive impairment. Emerging data now show detectable levels of some chemotherapeutic agents within the CNS, indicating potential disruption of blood brain barrier integrity or transport mechanisms. Blood brain barrier disruption is a key aspect of many neurocognitive disorders, particularly those characterized by a proinflammatory state. Importantly, many proinflammatory mediators able to modulate the blood brain barrier are generated by tissues and organs that are targets for chemotherapy-associated toxicities. This review therefore aims to explore the hypothesis that peripherally derived inflammatory cytokines disrupt blood brain barrier permeability, thereby increasing direct access of chemotherapeutic agents into the CNS to facilitate neuroinflammation and central neurotoxicity.
机译:神经毒性是化学疗法治疗的常见副作用,其分子机制尚不清楚。临床研究表明,最常见的神经毒性不良事件会影响记忆和学习,注意力,注意力,加工速度和执行功能。新兴的临床前研究指向直接细胞毒性和神经炎症的诱导,将其作为神经毒性和随后的认知障碍的主要驱动力。现在,新出现的数据显示,中枢神经系统中某些化学治疗剂的水平可检测,表明血脑屏障完整性或转运机制可能受到破坏。血脑屏障破坏是许多神经认知障碍的关键方面,尤其是那些以促炎状态为特征的障碍。重要的是,许多能够调节血脑屏障的促炎性介质是由组织和器官产生的,而组织和器官是化学疗法相关毒性的靶标。因此,本综述旨在探讨以下假设:外周来源的炎性细胞因子破坏血脑屏障通透性,从而增加化学治疗剂直接进入中枢神经系统的通路,从而促进神经炎症和中枢神经毒性。

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