Effect of Poly(ethylene glycol) Configuration on Microbubble Pharmacokinetics

IF 5.5 2区医学 Q2 MATERIALS SCIENCE, BIOMATERIALS

ACS Biomaterials Science & Engineering Pub Date : 2024-04-11 DOI:10.1021/acsbiomaterials.3c01764

J. Angel Navarro-Becerra*, Jair I. Castillo and Mark A. Borden,

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引用次数: 0

Abstract

Microbubbles (MBs) hold substantial promise for medical imaging and therapy; nonetheless, knowledge gaps persist between composition, structure, and in vivo performance, especially with respect to pharmacokinetics. Of particular interest is the role of the poly(ethylene glycol) (PEG) layer, which is thought to shield the MB against opsonization and rapid clearance but is also known to cause an antibody response upon multiple injections. The goal of this study was, therefore, to elucidate the role of the PEG layer in circulation persistence of MBs in the naïve animal (prior to an adaptive immune response). Here, we directly observe the number and size of individual MBs obtained from blood samples, unifying size and concentration into the microbubble volume dose (MVD) parameter. This approach enables direct evaluation of the pharmacokinetics of intact MBs, comprising both the lipid shell and gaseous core, rather than separately assessing the lipid or gas components. We examined the in vivo circulation persistence of 3 μm diameter phospholipid-coated MBs with three different mPEG₂₀₀₀ content: 2 mol % (mushroom), 5 mol % (intermediate), and 10 mol % (brush). MB size and concentration in the blood were evaluated by a hemocytometer analysis over 30 min following intravenous injections of 20 and 40 μL/kg MVD in Sprague–Dawley rats. Interestingly, pharmacokinetic analysis demonstrated that increasing PEG concentration on the MB surface resulted in faster clearance. This was evidenced by a 1.6-fold reduction in half-life and area under the curve (AUC) (p < 0.05) in the central compartment. Conversely, the AUC in the peripheral compartment increased with PEG density, suggesting enhanced MB trapping by the mononuclear phagocyte system. This was supported by an in vitro assay, which showed a significant rise in complement C3a activation with a higher PEG content. In conclusion, a minimal PEG concentration on the MB shell (mushroom configuration) was found to prolong circulation and mitigate immunogenicity.

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聚乙二醇配置对微泡药物动力学的影响

微气泡（MBs）在医学成像和治疗方面大有可为；然而，在成分、结构和体内性能（尤其是药代动力学方面）之间仍然存在知识差距。聚乙二醇（PEG）层的作用尤其引人关注，它被认为可以保护气泡不被吸附和快速清除，但也被认为在多次注射后会引起抗体反应。因此，本研究的目的是阐明 PEG 层在天真动物（适应性免疫反应之前）的甲基溴循环持久性中的作用。在这里，我们直接观察从血液样本中获得的单个 MB 的数量和大小，将大小和浓度统一为微泡体积剂量（MVD）参数。这种方法能够直接评估完整微泡的药代动力学，包括脂质外壳和气体核心，而不是单独评估脂质或气体成分。我们研究了三种不同 mPEG2000 含量的 3 μm 直径磷脂涂层 MB 的体内循环持久性：2摩尔%（蘑菇型）、5摩尔%（中间型）和10摩尔%（刷型）。对 Sprague-Dawley 大鼠静脉注射 20 和 40 μL/kg MVD 后的 30 分钟内，通过血球计数器分析评估了血液中 MB 的大小和浓度。有趣的是，药代动力学分析表明，甲基溴表面的 PEG 浓度越高，清除速度越快。这表现在中心区的半衰期和曲线下面积（AUC）缩短了 1.6 倍（p < 0.05）。相反，外周区的 AUC 随 PEG 密度的增加而增加，这表明单核吞噬细胞系统对甲基溴的捕获能力增强。体外试验也证明了这一点，该试验显示，PEG 含量越高，补体 C3a 的激活率就越高。总之，研究发现，甲基溴外壳（蘑菇构型）上的 PEG 浓度越低，循环时间越长，免疫原性越小。

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来源期刊

ACS Biomaterials Science & Engineering Materials Science-Biomaterials

CiteScore

10.30

自引率

3.40%

发文量

413

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