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脑向血中转运荧光素的体外研究。

Brain-to-blood transport of fluorescein in vitro.

机构信息

Carl-Ludwig-Institute of Physiology, Medical Faculty, Leipzig University, Liebigstr. 27, 04103, Leipzig, Germany.

出版信息

Sci Rep. 2024 Oct 26;14(1):25572. doi: 10.1038/s41598-024-77040-2.

Abstract

Investigating blood-brain barrier (BBB) dysfunction has become a pre-clinical and clinical research focus as it accompanies many neurological disorders. Nevertheless, knowledge of how diagnostic BBB tracers cross the endothelium from blood-to-brain or vice versa often remains incomplete. In particular, brain-to-blood transport (efflux) may reduce tracer extravasation of intravascularly (i.v.) applied tracers. Conversely, impaired efflux could mimic phenotypic extravasation. Both processes would affect conclusions on BBB properties primarily attributed to blood-to-brain leakage. Here, we specifically investigated efflux of fluorescent BBB tracers, focusing on the most common non-toxic marker, sodium fluorescein, which is applicable in patients. We used acute neocortical slices from mice and applied fluorescein, sulforhodamine-B, rhodamine-123, FITC dextran to the artificial cerebrospinal fluid. Anionic low molecular weight (MW) fluorescein and sulforhodamine-B, but not ~ 10-fold larger FITC-dextran and cationic low MW rhodamine-123, showed efflux into the lumen of blood vessels. Our data suggest that fluorescein efflux depends on organic anion transporter polypeptides (Oatp) rather than P-glycoprotein. Furthermore, sodium-potassium ATPase inhibition and incomplete oxygen-glucose deprivation (OGD, 20% O) reduced fluorescein efflux, while complete OGD (0% O) abolished efflux. We provide evidence for active efflux of fluorescein in vitro. Impaired efflux of fluorescein could thus contribute to the frequently observed BBB dysfunction in neuropathologies in addition to blood-to-brain leakage.

摘要

研究血脑屏障(BBB)功能障碍已成为临床前和临床研究的重点,因为它伴随着许多神经疾病。然而,关于诊断性 BBB 示踪剂如何从血液穿过内皮进入大脑或反之亦然的知识往往并不完整。特别是,脑向血液的转运(外排)可能会减少血管内(iv)应用示踪剂的示踪剂外渗。相反,外排受损可能会模拟表型外渗。这两个过程都会影响对主要归因于血脑漏的 BBB 特性的结论。在这里,我们特别研究了荧光 BBB 示踪剂的外排,重点研究了最常见的无毒标记物,即可应用于患者的荧光素钠。我们使用来自小鼠的急性新皮层切片,并将荧光素、磺基罗丹明 B、罗丹明 123 和 FITC 葡聚糖应用于人工脑脊液。带负电荷的低分子量(MW)荧光素和磺基罗丹明 B,但不是大约 10 倍大的 FITC-葡聚糖和带正电荷的低 MW 罗丹明 123,显示出向血管腔的外排。我们的数据表明,荧光素的外排取决于有机阴离子转运蛋白多肽(Oatp)而不是 P-糖蛋白。此外,钠钾 ATP 酶抑制和不完全氧葡萄糖剥夺(OGD,20% O)减少了荧光素的外排,而完全 OGD(0% O)则消除了外排。我们提供了体外荧光素主动外排的证据。因此,除了血脑漏之外,荧光素外排受损可能会导致神经病理学中经常观察到的 BBB 功能障碍。

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