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Evaluation of region selective bilirubin-induced brain damage as a basis for a pharmacological treatment

机译:评价区域选择性胆红素诱发的脑损伤作为药物治疗的基础

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摘要

The neurologic manifestations of neonatal hyperbilirubinemia in the central nervous system (CNS) exhibit high variations in the severity and appearance of motor, auditory and cognitive symptoms, which is suggestive of a still unexplained selective topography of bilirubin-induced damage. By applying the organotypic brain culture (OBC: preserving in vitro the cellular complexity, connection and architecture of the in vivo brain) technique to study hyperbilirubinemia, we mapped the regional target of bilirubin-induced damage, demonstrated a multifactorial toxic action of bilirubin, and used this information to evaluate the efficacy of drugs applicable to newborns to protect the brain. OBCs from 8-day-old rat pups showed a 2–13 fold higher sensitivity to bilirubin damage than 2-day-old preparations. The hippocampus, inferior colliculus and cerebral cortex were the only brain regions affected, presenting a mixed inflammatory-oxidative mechanism. Glutamate excitotoxicity was appreciable in only the hippocampus and inferior colliculus. Single drug treatment (indomethacin, curcumin, MgCl2) significantly improved cell viability in all regions, while the combined (cocktail) administration of the three drugs almost completely prevented damage in the most affected area (hippocampus). Our data may supports an innovative (complementary to phototherapy) approach for directly protecting the newborn brain from bilirubin neurotoxicity.
机译:新生儿中枢神经系统(CNS)的高胆红素血症的神经系统表现在运动,听觉和认知症状的严重程度和外观方面存在很大差异,这表明尚无法解释的选择性胆红素诱发的损伤的地形。通过应用器官型脑培养(OBC:在体外保存细胞的复杂性,体内大脑的连接和结构)技术来研究高胆红素血症,我们绘制了胆红素诱导的损伤的区域靶标,证明了胆红素的多因素毒性作用,并且利用这些信息来评估适用于新生儿以保护大脑的药物的功效。 8天大的幼崽的OBC对胆红素损伤的敏感性比2天大的制剂高2-13倍。海马,下丘脑和大脑皮层是受影响的唯一大脑区域,呈现出混合的炎症-氧化机制。谷氨酸兴奋性毒性仅在海马和下丘脑中可见。单一药物治疗(吲哚美辛,姜黄素,MgCl2)显着改善了所有区域的细胞活力,而三种鸡尾酒的联合(鸡尾酒)给药几乎完全防止了最受影响区域(海马)的损伤。我们的数据可能支持直接保护新生儿大脑免受胆红素神经毒性的创新方法(与光疗互补)。

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