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血红素结合蛋白在脑出血后的神经保护作用。

Neuroprotective role of haptoglobin after intracerebral hemorrhage.

机构信息

Stroke Program, Department of Neurology, University of Texas Health Science Center, Medical School at Houston, Houston, Texas 77030, USA.

出版信息

J Neurosci. 2009 Dec 16;29(50):15819-27. doi: 10.1523/JNEUROSCI.3776-09.2009.

Abstract

After intracerebral hemorrhage (ICH), the brain parenchyma is exposed to blood containing red blood cells (RBCs) and consequently to its lysis products. Iron-rich hemoglobin (Hb) is the most abundant protein in RBCs. When released into the brain parenchyma during hemolysis, Hb becomes a central mediator of cytotoxicity. Our study indicates that haptoglobin (Hp), an acute-phase response protein primarily synthesized in the liver and known to bind and neutralize Hb in the bloodstream, is also expressed in brain in which it plays an important role in defending neurons from damage induced by hemolytic products after ICH. We demonstrate that the Hb-induced hypohaptoglobinemia aggravates ICH-induced brain damage while pharmacologic intervention with sulforaphane to induce brain Hp is linked to a reduction in brain damage. In agreement with these findings, Hp deficiency worsens whereas Hp overexpression alleviates ICH-mediated brain injury. We also identified that oligodendroglia are the primary source of brain-derived Hp among brain cells and that oligodendroglia-released Hp plays protective roles against Hb-mediated toxicity to neurons and oligodendrocytes. We conclude that Hp, particularly the brain-derived Hp, plays cytoprotective roles and represents a potential therapeutic target for ICH treatment.

摘要

脑出血(ICH)后,脑实质暴露于含有红细胞(RBC)的血液中,进而暴露于其溶解产物中。富含铁的血红蛋白(Hb)是 RBC 中最丰富的蛋白质。当 Hb 在溶血过程中释放到脑实质中时,它成为细胞毒性的中心介质。我们的研究表明,触珠蛋白(Hp)是一种急性期反应蛋白,主要在肝脏中合成,已知在血液中结合和中和 Hb,它在脑内也发挥重要作用,可保护神经元免受 ICH 后溶血产物引起的损伤。我们证明,Hb 诱导的低触珠蛋白血症加重了 ICH 引起的脑损伤,而用萝卜硫素进行药物干预以诱导脑 Hp 与脑损伤减少有关。与这些发现一致,Hp 缺乏症使 ICH 介导的脑损伤恶化,而 Hp 过表达则减轻了脑损伤。我们还确定,少突胶质细胞是脑内细胞中脑源性 Hp 的主要来源,并且少突胶质细胞释放的 Hp 对神经元和少突胶质细胞的 Hb 介导的毒性具有保护作用。我们得出结论,Hp,特别是脑源性 Hp,发挥细胞保护作用,是 ICH 治疗的潜在治疗靶点。

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