未成熟中枢神经系统中炎症的“易感性窗口”的特征是血脑屏障渗漏以及炎症趋化因子的局部表达。
The "window of susceptibility" for inflammation in the immature central nervous system is characterized by a leaky blood-brain barrier and the local expression of inflammatory chemokines.
作者信息
Schoderboeck Lucia, Adzemovic Milena, Nicolussi Eva-Maria, Crupinschi Claudia, Hochmeister Sonja, Fischer Marie-Therese, Lassmann Hans, Bradl Monika
机构信息
Medical University Vienna, Center for Brain Research, Department of Neuroimmunology, Spitalgasse 4, A-1090 Wien, Austria.
出版信息
Neurobiol Dis. 2009 Sep;35(3):368-75. doi: 10.1016/j.nbd.2009.05.026. Epub 2009 Jun 9.
Abstract
Early in postnatal development, the immature central nervous system (CNS) is more susceptible to inflammation than its adult counterpart. We show here that this "window of susceptibility" is characterized by the presence of leaky vessels in the CNS, and by a global chemokine expression profile which is clearly distinct from the one observed in the adult CNS and has three important characteristics. First, it contains chemokines with known roles in the differentiation and maturation of glia and neurons. Secondly, these chemokines have been described before in inflammatory lesions of the CNS, where they are important for the recruitment of monocytes and T cells. Lastly, the chemokine profile is shaped by pathological changes like oligodendrocyte stress and attempts of myelin repair. Changes in the chemokine expression profile along with a leaky blood-brain barrier pave the ground for an accelerated development of CNS inflammation.
摘要
在出生后发育早期,未成熟的中枢神经系统(CNS)比成年中枢神经系统更容易受到炎症影响。我们在此表明,这种“易感性窗口”的特征是中枢神经系统中存在渗漏血管,以及整体趋化因子表达谱,该谱明显不同于在成年中枢神经系统中观察到的谱,且具有三个重要特征。首先,它包含在神经胶质细胞和神经元的分化与成熟中具有已知作用的趋化因子。其次,这些趋化因子之前已在中枢神经系统的炎性病变中被描述过,在那里它们对单核细胞和T细胞的募集很重要。最后,趋化因子谱由少突胶质细胞应激和髓鞘修复尝试等病理变化塑造。趋化因子表达谱的变化以及血脑屏障渗漏为中枢神经系统炎症的加速发展奠定了基础。
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