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低通透率的环糊精 kleptose:外排和管腔表面结合的修饰作用。

Modest Blood-Brain Barrier Permeability of the Cyclodextrin Kleptose: Modification by Efflux and Luminal Surface Binding.

机构信息

Geriatric Research and Clinical Center, Veterans Affairs Puget Sound Health Care System, Seattle, Washington (W.A.B., K.M.H., K.M.B.); Division of Gerontology and Geriatric Medicine, Department of Medicine, University of Washington School of Medicine, Seattle, Washington (W.A.B.); The Engelke Group, Keymar, Maryland (K.E.); and Educational Trainers and Consultants, Melrose, Massachusetts (P.C.)

Geriatric Research and Clinical Center, Veterans Affairs Puget Sound Health Care System, Seattle, Washington (W.A.B., K.M.H., K.M.B.); Division of Gerontology and Geriatric Medicine, Department of Medicine, University of Washington School of Medicine, Seattle, Washington (W.A.B.); The Engelke Group, Keymar, Maryland (K.E.); and Educational Trainers and Consultants, Melrose, Massachusetts (P.C.).

出版信息

J Pharmacol Exp Ther. 2019 Oct;371(1):121-129. doi: 10.1124/jpet.119.260497. Epub 2019 Jul 18.

Abstract

Cyclodextrins (CDs) have a variety of uses from acting as excipients to aiding the ability of lipid soluble drugs to cross the blood-brain barrier (BBB). They are being investigated as an active pharmaceutical ingredient, most recently for the treatment of Niemann-Pick disease, a lysosomal storage disease. Cyclodextrins are helpful in animal models and human subjects/patients afflicted with Neimann-Pick disease, including improving the neurologic component of the disease. The improvement in brain disease by intravenous administration implies that CDs can cross the BBB; however, there are only a few studies that have directly addressed this. In the current studies, multiple-time regression analysis indicated that 2-hydroxypropyl--cyclodextrin [Kleptose (Klep)] radioactively labeled with 14C (C-Klep) crossed the BBB at a slow rate by a nonsaturable mechanism consistent with transcellular diffusion. However, the rate of transport varied greatly by the brain region with no detectable uptake by the spinal cord; additionally, many regions rapidly reached equilibrium between the brain and blood. The presence of a brain-to-blood efflux system was also detected and much of the C-Klep did not completely cross the BBB, but loosely adhered to the luminal surface of brain endothelial cells. Peripheral tissues also took up C-Klep, with the kidney taking up the most, which is consistent with renal clearance. In conclusion, we demonstrated minimal uptake of the -cyclodextrin Kleptose by the brain with accumulation being affected by efflux and reversible luminal binding. SIGNIFICANCE STATEMENT: This cyclodextrin, which produces therapeutic effects on the central nervous system after peripheral administration, penetrates the BBB poorly. Uptake by the brain to a therapeutic level will likely be difficult to achieve without giving high peripheral doses, bypassing the BBB, or otherwise altering penetration into the brain.

摘要

环糊精(CDs)具有多种用途,可作为赋形剂,帮助脂溶性药物穿过血脑屏障(BBB)。它们作为一种活性药物成分正在被研究,最近用于治疗尼曼-皮克病,一种溶酶体贮积病。环糊精在患有尼曼-皮克病的动物模型和人类受试者/患者中是有帮助的,包括改善疾病的神经学成分。静脉给药对脑部疾病的改善意味着 CD 可以穿过 BBB;然而,只有少数研究直接解决了这个问题。在目前的研究中,多次回归分析表明,2-羟丙基--环糊精[Kleptose(Klep)]用 14C 放射性标记[C-Klep]以非饱和机制通过跨细胞扩散以缓慢的速度穿过 BBB。然而,转运速率因脑区而异,脊髓没有可检测到的摄取;此外,许多区域在大脑和血液之间很快达到平衡。还检测到存在脑向血液的外排系统,并且大部分 C-Klep 没有完全穿过 BBB,但松散地附着在脑内皮细胞的腔表面上。外周组织也摄取了 C-Klep,其中肾脏摄取最多,这与肾脏清除率一致。总之,我们证明了 -环糊精 Kleptose 对大脑的摄取很少,积累受到外排和可逆腔结合的影响。意义声明:这种环糊精在周围给药后对中枢神经系统产生治疗作用,但穿透 BBB 的能力很差。如果不给高外周剂量、绕过 BBB 或改变进入大脑的穿透方式,大脑达到治疗水平的摄取将很难实现。

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