用硝基化合物OKN-007暂时打开血脑屏障。

IF 2 Q3 RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING
American journal of nuclear medicine and molecular imaging Pub Date : 2021-10-15 eCollection Date: 2021-01-01
Rheal A Towner, Debra Saunders, Megan Lerner, Robert Silasi Mansat, Tian Yuan, Dylan Barber, Janet Faakye, Adam Nyul-Toth, Anna Csiszar, Beverley Greenwood-Van Meerveld, Nataliya Smith
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引用次数: 0

摘要

血脑屏障(BBB)通常是几种药物无法渗透的,这阻碍了各种脑相关疾病的治疗。有几种打开血脑屏障的方法,包括颈动脉内输注高渗透浓度的阿拉伯糖、甘露醇、油酸或亚油酸或烷基甘油,静脉输注慢动蛋白B2,给药霍乱弧菌ZO毒素片段,用siRNA或新型拟肽药物靶向紧密连接的特定成分(如claudin-5),或使用微泡超声。我们建议使用一种低分子量(MW)的硝基化合物OKN-007,它可以暂时打开血脑屏障1-2小时。以钆(Gd)为基础的化合物评估的分子量范围从546 (Gd- dtpa)到465 kDa (β-半乳糖苷酶-Gd- dota)。我们还纳入了基于白蛋白的CA(白蛋白- gd - dtpa -生物素)进行评估,以及针对结合Gd-DOTA的神经元特异性生物标志物(抗ephb2 -Gd-DOTA)的抗体(Ab)。对于抗ephb2(山羊Ab)-Gd-DOTA的评估,我们使用了与马萝卜过氧化物酶(HRP)结合的抗山羊Ab来确认抗ephb2 -Gd-DOTA探针的存在。此外,将Cy5标记的抗ephb2抗体与抗ephb2 - gd - dota探针共同施用,并在体外进行评估。这项研究表明,OKN-007可能能够暂时打开血脑屏障,以增加各种化合物的递送,其分子量从~550到~470 kDa不等。该化合物是临床试验中治疗胶质母细胞瘤(GBM)的新药。人类使用的转化能力,以增加非血脑屏障渗透药物的递送是非常高的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Temporary opening of the blood-brain barrier with the nitrone compound OKN-007.

Temporary opening of the blood-brain barrier with the nitrone compound OKN-007.

Temporary opening of the blood-brain barrier with the nitrone compound OKN-007.

The blood-brain barrier (BBB) is usually impermeable to several drugs, which hampers treatment of various brain-related diseases/disorders. There have been several approaches to open the BBB, including intracarotid infusion of hyperosmotic concentrations of arabinose, mannitol, oleic or linoleic acids, or alkylglycerols, intravenous infusion of bradykinin B2, administration of a fragment of the ZO toxin from vibrio cholera, targeting specific components of the tight junctions (e.g. claudin-5) with siRNA or novel peptidomimetic drugs, or the use of ultrasound with microbubbles. We propose the use of a low molecular weight (MW), nitrone-type compound, OKN-007, which can temporarily open up the BBB for 1-2 hours. Gadolinium (Gd)-based compounds assessed ranged in MW from 546 (Gd-DTPA) to 465 kDa (β-galactosidase-Gd-DOTA). We also included an albumin-based CA (albumin-Gd-DTPA-biotin) for assessment, as well as an antibody (Ab) against a neuron-specific biomarker conjugated to Gd-DOTA (anti-EphB2-Gd-DOTA). For the anti-EphB2 (goat Ab)-Gd-DOTA assessment, we utilized an anti-goat Ab conjugated with horse radish peroxidase (HRP) for confirmation of the presence of the anti-EphB2-Gd-DOTA probe. In addition, a Cy5 labeled anti-EphB2 Ab was co-administered with the anti-EphB2-Gd-DOTA probe, and assessed ex vivo. This study demonstrates that OKN-007 may be able to temporarily open up the BBB to augment the delivery of various compounds ranging in MW from as small as ~550 to as large as ~470 kDa. This compound is an investigational new drug for glioblastoma (GBM) therapy in clinical trials. The translational capability for human use to augment the delivery of non-BBB-permeable drugs is extremely high.

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来源期刊
American journal of nuclear medicine and molecular imaging
American journal of nuclear medicine and molecular imaging RADIOLOGY, NUCLEAR MEDICINE & MEDICAL IMAGING-
自引率
4.00%
发文量
4
期刊介绍: The scope of AJNMMI encompasses all areas of molecular imaging, including but not limited to: positron emission tomography (PET), single-photon emission computed tomography (SPECT), molecular magnetic resonance imaging, magnetic resonance spectroscopy, optical bioluminescence, optical fluorescence, targeted ultrasound, photoacoustic imaging, etc. AJNMMI welcomes original and review articles on both clinical investigation and preclinical research. Occasionally, special topic issues, short communications, editorials, and invited perspectives will also be published. Manuscripts, including figures and tables, must be original and not under consideration by another journal.
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