Shrewd Consulting LLC, Impel Pharmaceuticals, Seattle, WA, USA.
, 3770 Poppy lane, Fallbrook, CA, 92028, USA.
Pharmaceut Med. 2023 Nov;37(6):451-461. doi: 10.1007/s40290-023-00495-7. Epub 2023 Aug 3.
Pharmacokinetics (PK) includes how a drug is absorbed, distributed, metabolized and eliminated. The compartment providing this information is usually the plasma. This is as close to the tissue of interest that we can get, although biopsies may be obtained to give "tissue levels" of drugs. Ultimately, the goal of PK is to understand how long the drug is actually engaged with the target in the tissue of interest after a dose has been administered. Most drugs at some point in their development will have been administered intravenously (IV), which acts as the standard for 100% bioavailability. By comparing various routes of administration to IV, the percentage of drug delivered to the plasma, on a dose-normalized basis, can be calculated and is referred to as the "absolute bioavailability". As pharmacology has advanced and more drugs have become available, many older products have been reformulated to be given by routes other than those originally intended (often oral). As the drawbacks of oral (or IV) administration have become better appreciated, non-oral, non-IV formulations and methods of administration have become more popular. Nasal administration is one route that has historically been overlooked as an alternative to oral administration-particularly for products needing rapid and non-invasive access to the target tissue-mostly via the blood stream. But attention is now focused on nasal administration for direct access to the brain, as that has the potential to bypass the blood-brain-barrier (BBB), which not even IV administration can always achieve. Assessing PK for these drugs targeting the brain may require serial sampling of the cerebrospinal fluid (CSF), making PK assessments of CNS drugs more invasive and complex, but still possible in future product development. However, we are now seeing more drugs reformulated for nasal delivery to gain faster systemic levels than oral administration (especially in patients with known or suspected gastrointestinal dysmotility), while avoiding the use of needles. For example, in recent years several different formulations and delivery methods for an old drug, dihydroergotamine (DHE), have been developed and these show very different characteristics, suggesting that delivery to different parts of the nose may have very different PK profiles. This review summarizes the systemic PK of different nasal DHE options that have been, or are being, developed and suggests that delivery of drugs to the upper nasal space (UNS) may represent an optimal target. Further research is required to ascertain if this route could also be utilized for direct administration to the CNS (as an attractive alternative to intrathecal delivery) via the olfactory or trigeminal nerves-but already preclinical data (and some human data) suggest this is entirely possible.
药代动力学(PK)包括药物的吸收、分布、代谢和消除方式。提供这些信息的隔室通常是血浆。虽然可以获得活检以提供药物的“组织水平”,但这是我们能接近目标组织的程度。最终,PK 的目标是了解在给予剂量后,药物与目标组织中的靶标实际结合的时间长度。在药物开发的某个阶段,大多数药物都曾通过静脉内(IV)给药,这是 100%生物利用度的标准。通过比较各种给药途径与 IV 给药,以剂量归一化的方式计算递送至血浆的药物百分比,并将其称为“绝对生物利用度”。随着药理学的进步和更多药物的出现,许多旧产品已被重新配方为通过最初预期以外的途径(通常为口服)给药。随着口服(或 IV)给药的缺点得到更好的认识,非口服、非 IV 制剂和给药方法变得更加流行。鼻腔给药是一种历史上被忽视的口服替代途径-特别是对于需要快速且非侵入性进入目标组织的产品-主要通过血流。但是,现在人们开始关注鼻腔给药以直接进入大脑,因为它有可能绕过血脑屏障(BBB),即使是 IV 给药也不一定能实现。评估这些针对大脑的药物的 PK 可能需要对脑脊液(CSF)进行连续采样,这使得中枢神经系统药物的 PK 评估更加具有侵入性和复杂性,但在未来的产品开发中仍然是可行的。然而,我们现在看到更多的药物被重新配方为鼻腔给药,以获得比口服给药更快的全身水平(特别是在已知或疑似胃肠道动力障碍的患者中),同时避免使用针头。例如,近年来,已经开发了几种不同的旧药物二氢麦角胺(DHE)的制剂和给药方法,这些方法显示出非常不同的特征,这表明药物输送到鼻腔的不同部位可能具有非常不同的 PK 特征。这篇综述总结了已经开发或正在开发的不同鼻腔 DHE 选择的全身 PK,并表明将药物输送到上鼻腔空间(UNS)可能是一个理想的目标。需要进一步的研究来确定该途径是否也可用于通过嗅觉或三叉神经直接向中枢神经系统(作为鞘内给药的有吸引力的替代方案)给药-但已经有临床前数据(和一些人体数据)表明这是完全可能的。
