优化乳腺癌脑转移的药物递送：一种肿瘤靶向的新方法。

Optimizing Drug Delivery to the Brain for Breast Metastasis: A Novel Method for Tumor Targeting.

作者信息

Krishnamurthy Satish, Oh Justin Y, Gautham Shruti, Li Jie, Shen Yimin

机构信息

Neurological Surgery, State University of New York Upstate Medical University, Syracuse, USA.

Radiology, Wayne State University, Detroit, USA.

出版信息

Cureus. 2024 Nov 13;16(11):e73598. doi: 10.7759/cureus.73598. eCollection 2024 Nov.

DOI:10.7759/cureus.73598

PMID:39677180

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11645177/

Abstract

INTRODUCTION

Brain metastases are difficult to treat due to the blood-brain barrier limiting the delivery of therapeutic agents to the brain effectively. Intraventricular drug delivery has not been well studied for intra-axial pathologies. However, our prior work demonstrated that intraventricular drug delivery in a hyperosmolar vehicle showed preferential accumulation of drug within breast cancer tissue compared to surrounding brain parenchyma. The focus of this study was to explore the molecular parameters of intraventricular drug administration that may optimize drug delivery to intra-axial brain metastases. Our hypothesis was that a low molecular weight drug with a high osmolarity solution would increase drug delivery to tumor tissue.

METHODS

We used an intracerebral breast cancer tumor model in adult female nude rats divided into six experimental groups. We examined three iron-labeled dextran molecules (3 kD, 5 kD, and 10 kD) in 337 mOsm/L solution and three different osmolarities of delivery solution (307, 353, and 368 mOsm/L) with 10 kD dextran. 7T magnetic resonance imaging (MRI) was used to analyze dextran distribution at different time points. All animals were sacrificed after two hours, and the quantity of dextran particles was determined by histopathology.

RESULTS

Breast cancer tumor cells were successfully implanted in all rats. The MRI quantification of dextran concentration was well corroborated by histopathology. Varying the molecular size of dextran resulted in the smallest molecule reaching peak levels in tumor tissue earlier than the larger molecules, but the larger molecules remained concentrated in tumor tissue for a longer time. Varying the osmolarity of the delivery solution resulted in the preferential accumulation of 10 kD dextran in tumor tissue except for when dextran was delivered in 368 mOsm/L solution where no preferential distribution was seen.

CONCLUSION

Hyperosmolar intraventricular delivery of chemotherapeutic drugs could be effective in preferentially delivering drugs to abnormal tumor tissues.

摘要

引言

由于血脑屏障限制治疗药物有效递送至脑内，脑转移瘤难以治疗。脑室内给药治疗脑实质内病变的研究尚不充分。然而，我们之前的研究表明，与周围脑实质相比，在高渗载体中进行脑室内给药时，药物在乳腺癌组织内有优先蓄积。本研究的重点是探索脑室内给药的分子参数，这些参数可能会优化药物向脑实质内脑转移瘤的递送。我们的假设是，低分子量药物与高渗溶液联合使用会增加药物向肿瘤组织的递送。

方法

我们在成年雌性裸鼠中建立了脑内乳腺癌肿瘤模型，并将其分为六个实验组。我们研究了三种铁标记的葡聚糖分子（3 kD、5 kD和10 kD）在337 mOsm/L溶液中的情况，以及三种不同渗透压的给药溶液（307、353和368 mOsm/L）与10 kD葡聚糖联合使用的情况。使用7T磁共振成像（MRI）分析不同时间点葡聚糖的分布。两小时后处死所有动物，通过组织病理学确定葡聚糖颗粒的数量。

结果

所有大鼠均成功植入乳腺癌肿瘤细胞。组织病理学很好地证实了MRI对葡聚糖浓度的定量分析。改变葡聚糖的分子大小导致最小的分子比大分子更早达到肿瘤组织中的峰值水平，但大分子在肿瘤组织中保持浓缩的时间更长。改变给药溶液的渗透压导致10 kD葡聚糖在肿瘤组织中优先蓄积，但当葡聚糖在368 mOsm/L溶液中给药时未观察到优先分布。