Iron regulation at the CNS vascular barriers and aging

铁对中枢神经系统血管屏障和衰老的调节

• 批准号: 6994453
• 负责人: RASHID DEANE
• 金额: $ 7.05万
• 依托单位: UNIVERSITY OF ROCHESTER
• 依托单位国家: 美国
• 财政年份: 2004
• 资助国家: 美国
• 起止时间: 2004-12-15 至 2006-11-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6994453
• 关键词: age difference; aging; biological transport; blood brain barrier; chemical kinetics; choroid plexus; gene expression; genetic regulation; genetically modified animals; intermolecular interaction; iron; laboratory rat; membrane transport proteins; neuroregulation; perfusion; protein structure function; radiotracer; transferrin; transferrin receptor

DESCRIPTION (provided by applicant): While iron (Fe) is essential for normal brain function its accumulation in the aging brain is associated with neurodegeneration. The mechanism of accumulation is still unclear. Our recent studies indicated that entry of transferrin (Tf)-bound and free iron into the CNS is determined by (i) initial rapid sequestration by brain capillaries (BBB) and choroid plexus (CP), and (ii) subsequent controlled and slow release from vascular structures into brain interstitial fluid (ISF) and cerebrospinal fluid (CSF). In addition, our pilot data suggest that iron is rapidly cleared from brain into blood across the blood-brain barrier mainly by a Tf-medicated mechanism. Based on these preliminary data, we hypothesize that influx of iron across the blood-brain barrier and CP is a two-step process that requires both Tf receptor (TfR) and DMT1 (divalent metal transporter 1) with DMT1 being a rate limiting step, while efflux of Fe from the CNS is a one-step process that depends on Tf route and requires TfR at the blood-brain barrier. We further hypothesize that imbalance between iron CNS influx and efflux transport mechanisms, due mainly to reduced clearance at the vascular CNS barriers leads to its accumulation in the aging brain. There are two Aims. 1. To determine the role of Tf-mediated and non-Tf route for Fe efflux from CNS and the retention mechanism for Fe in CNS in bold type and DMT1 mutant Belgrade rats at selective ages. 2. To determine the kinetics of Tf and non-Tf mediated Fe influx across blood-brain barrier and CP in wild type and Belgrade rats at selective ages. These Aims will be achieved by using the brain perfusion and clearance techniques and the Belgrade rat (b/b) since it is a physiological knock out for DNT1. The kinetic parameters of Tf and non Tf bound Fe will be determined in b/b/ and control rats to establish the role of DMT1 in the influx and efflux of Fe at the blood-brain barrier and CP. Similar studies in control rats at selected ages will determine age related changes. Relative levels of TfR and DMT1 at blood-brain barrier and CP will be determined by standard molecular techniques to complement the transport studies. This study will help us understand the roles of DMT1 and TfR at the BBB and CP with respect to iron accumulation in the brain, associated neurodegenerative effects, and identify potential targets for future development of brain iron lowering strategies.

描述（由申请人提供）：虽然铁（Fe）是正常脑功能所必需的，但它在衰老的大脑中的积累与神经变性有关。其积累机制尚不清楚。我们最近的研究表明，转铁蛋白（Tf）结合的铁和游离铁进入中枢神经系统是由(i)脑毛细血管（BBB）和脉络膜丛（CP）最初的快速隔离和（ii）随后从血管结构控制和缓慢释放到脑间质液（ISF）和脑脊液（CSF）决定的。此外，我们的试验数据表明，铁主要通过tf药物机制通过血脑屏障从大脑迅速清除到血液中。基于这些初步数据，我们假设铁通过血脑屏障和CP的流入是一个两步过程，需要Tf受体（TfR）和DMT1（二价金属转运蛋白1），其中DMT1是一个限速步骤，而铁从中枢神经系统的流出是一个一步过程，依赖于Tf途径，需要血脑屏障的TfR。我们进一步假设，铁在中枢神经系统内流和外排运输机制之间的不平衡，主要是由于血管中枢神经系统屏障的清除减少导致其在衰老的大脑中积累。有两个目的。目的：探讨粗体型和DMT1突变体贝尔格莱德大鼠在选择年龄时，tf介导和非tf途径在铁从中枢神经系统外排中的作用以及铁在中枢神经系统中的滞留机制。2. 测定野生型和贝尔格莱德大鼠选择年龄时Tf和非Tf介导的Fe在血脑屏障和CP中的内流动力学。这些目标将通过使用脑灌注和清除技术和贝尔格莱德大鼠（b/b）来实现，因为它是DNT1的生理击倒。在b/b/和对照大鼠中测定Tf和非Tf结合铁的动力学参数，以确定DMT1在铁在血脑屏障和CP处的内流和外排中的作用。在选定年龄的对照大鼠中进行类似的研究，以确定年龄相关的变化。血脑屏障和CP处TfR和DMT1的相对水平将通过标准分子技术确定，以补充转运研究。这项研究将帮助我们了解DMT1和TfR在血脑屏障和CP中的作用，以及脑铁积累和相关的神经退行性作用，并确定未来开发脑铁降低策略的潜在靶点。