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建立乳腺癌脑转移模型的方法会影响靶向治疗纳米颗粒的脑摄取和疗效。

Method of establishing breast cancer brain metastases affects brain uptake and efficacy of targeted, therapeutic nanoparticles.

作者信息

Wyatt Emily A, Davis Mark E

机构信息

Chemical Engineering California Institute of Technology Pasadena CA.

出版信息

Bioeng Transl Med. 2018 Nov 5;4(1):30-37. doi: 10.1002/btm2.10108. eCollection 2019 Jan.

Abstract

HER2-targeted therapies effectively control systemic disease, but their efficacy against brain metastases is hindered by their low penetration of the blood-brain and blood-tumor barriers (BBB and BTB). We investigate brain uptake and antitumor efficacy of transferrin receptor (TfR)-targeted, therapeutic nanoparticles designed to transcytose the BBB/BTB in three murine models. Two known models involving intracranial (IC) or intracardiac (ICD) injection of human breast cancer cells were employed, as was a third model developed here involving intravenous (IV) injection of the cells to form whole-body tumors that eventually metastasize to the brain. We show the method of establishing brain metastases significantly affects therapeutic BBB/BTB penetration. Free drug accumulates and delays growth in IC- and ICD-formed brain tumors, while non-targeted nanoparticles show uptake and inhibition only in IC-established metastases. TfR-targeted nanoparticles accumulate and significantly delay growth in all three models, suggesting the IV model maintains a more intact BBB/BTB than the other models.

摘要

HER2靶向疗法能有效控制全身疾病,但其对脑转移瘤的疗效因血脑屏障和血肿瘤屏障(BBB和BTB)的低渗透率而受到阻碍。我们在三种小鼠模型中研究了转铁蛋白受体(TfR)靶向的治疗性纳米颗粒的脑摄取和抗肿瘤疗效,这些纳米颗粒旨在通过跨细胞作用穿过BBB/BTB。我们采用了两种已知的模型,即颅内(IC)或心内(ICD)注射人乳腺癌细胞,还采用了在此开发的第三种模型,即静脉内(IV)注射细胞以形成最终转移至脑部的全身肿瘤。我们发现,建立脑转移瘤的方法会显著影响治疗性药物对BBB/BTB的渗透。游离药物在IC和ICD形成的脑肿瘤中积累并延缓生长,而非靶向纳米颗粒仅在IC建立的转移瘤中显示摄取和抑制作用。TfR靶向纳米颗粒在所有三种模型中均有积累并显著延缓生长,这表明IV模型比其他模型保持了更完整的BBB/BTB。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7134/6336738/926b3f921429/BTM2-4-30-g001.jpg

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