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Dynamic dual-isotope molecular imaging elucidates principles for optimizing intrathecal drug delivery

机译:动态双同位素分子成像阐明了优化鞘内给药的原理

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摘要

The intrathecal (IT) dosing route offers a seemingly obvious solution for delivering drugs directly to the central nervous system. However, gaps in understanding drug molecule behavior within the anatomically and kinetically unique environment of the mammalian IT space have impeded the establishment of pharmacokinetic principles for optimizing regional drug exposure along the neuraxis. Here, we have utilized high-resolution single-photon emission tomography with X-ray computed tomography to study the behavior of multiple molecular imaging tracers following an IT bolus injection, with supporting histology, autoradiography, block-face tomography, and MRI. Using simultaneous dual-isotope imaging, we demonstrate that the regional CNS tissue exposure of molecules with varying chemical properties is affected by IT space anatomy, cerebrospinal fluid (CSF) dynamics, CSF clearance routes, and the location and volume of the injected bolus. These imaging approaches can be used across species to optimize the safety and efficacy of IT drug therapy for neurological disorders.
机译:鞘内给药途径为将药物直接递送至中枢神经系统提供了看似明显的解决方案。然而,在哺乳动物IT空间的解剖学和动力学独特的环境中理解药物分子行为的差距阻碍了建立药物动力学原理以优化沿神经区域的药物暴露。在这里,我们利用高分辨率单光子发射断层扫描和X射线计算机断层摄影技术来研究IT大剂量注射后的多分子成像示踪剂的行为,并支持组织学,放射自显影,断层断层扫描和MRI。使用同步双同位素成像,我们证明了具有不同化学性质的分子的区域CNS组织暴露受IT空间解剖结构,脑脊液(CSF)动力学,CSF清除途径以及注射推注的位置和体积的影响。这些成像方法可跨物种使用,以优化IT药物治疗神经系统疾病的安全性和有效性。

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