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动脉内与静脉内过继细胞疗法在小鼠肿瘤模型中的比较。

Intra-arterial Versus Intravenous Adoptive Cell Therapy in a Mouse Tumor Model.

机构信息

Departments of Surgical Oncology.

Immunology, Roswell Park Cancer Institute, Buffalo, NY.

出版信息

J Immunother. 2018 Sep;41(7):313-318. doi: 10.1097/CJI.0000000000000235.

Abstract

Adoptive cell transfer therapy for cancer has existed for decades and is experiencing a resurgence in popularity that has been facilitated by improved methods of production, techniques for genetic modification, and host preconditioning. The trafficking of adoptively transferred lymphocytes and infiltration into the tumor microenvironment is sine qua non for successful tumor eradication; however, the paradox of extremely poor trafficking of lymphocytes into the tumor microenvironment raises the issue of how best to deliver these cells to optimize entry into tumor tissue. We examined the route of administration as a potential modifier of both trafficking and antitumor efficacy. Femoral artery cannulation and tail vein injection for the intra-arterial (IA) and IV delivery, respectively, were utilized in the B16-OVA/OT-I mouse model system. Both IV and IA infusions showed decreased tumor growth and prolonged survival. However, although significantly increased T-cell tumor infiltration was observed in IA mice, tumor growth and survival were not improved as compared with IV mice. These studies suggest that IA administration produces increased early lymphocyte trafficking, but a discernable survival benefit was not seen in the murine model examined.

摘要

过继性细胞转移疗法治疗癌症已经存在了几十年,并且由于生产方法的改进、遗传修饰技术和宿主预处理,其再次受到欢迎。被过继转移的淋巴细胞的运输和浸润到肿瘤微环境是成功消除肿瘤的必要条件;然而,淋巴细胞进入肿瘤微环境的极差运输的悖论提出了如何最好地递送这些细胞以优化进入肿瘤组织的问题。我们研究了给药途径作为改变运输和抗肿瘤疗效的潜在因素。股动脉插管和尾静脉注射分别用于动脉内(IA)和静脉内(IV)给药,在 B16-OVA/OT-I 小鼠模型系统中进行了研究。IV 和 IA 输注均显示肿瘤生长减少和生存时间延长。然而,尽管在 IA 小鼠中观察到 T 细胞肿瘤浸润显著增加,但与 IV 小鼠相比,肿瘤生长和生存并未得到改善。这些研究表明,IA 给药可增加早期淋巴细胞的运输,但在检查的小鼠模型中并未观察到明显的生存获益。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/15ab/6092084/edcf72135b02/cji-41-313-g001.jpg

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