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[利用自组装载体将药物递送至靶器官的疫苗研发]

[Development of Vaccines with Self-assembled Carriers That Deliver Drugs to Target Organs].

作者信息

Kurosaki Tomoaki

机构信息

Department of Hospital Pharmacy, Nagasaki University Hospital.

出版信息

Yakugaku Zasshi. 2020;140(3):363-368. doi: 10.1248/yakushi.19-00174.

DOI:10.1248/yakushi.19-00174
PMID:32115553
Abstract

I have developed novel ternary complexes of various vaccines with cationic materials and anionic polymers. Plasmid DNA (pDNA) encoding firefly luciferase was used as a model drug to form adequate ternary complexes. Cationic binary complexes were constructed using pDNA and polyethylenimine, and these binary complexes were coated with various anionic polymers to form ternary complexes. These ternary complexes significantly improved cytotoxicity and aggregation with erythrocytes in comparison to the binary complexes. On the other hand, most of those ternary complexes showed little in vitro transgene efficiency because of their anionic surface charge. γ-Polyglutamic acid (γ-PGA)-ternary complexes, however, demonstrated high in vitro transgene efficiency. After the intravenous administration of γ-PGA-ternary complexes to mice, extremely high gene expression was detected in the marginal zone of the spleen, which is rich in antigen-presenting cells. This spleen-specific phenomenon of γ-PGA-ternary complexes appeared to be suited to DNA vaccines against cancer. I therefore examined the preventive effect of γ-PGA-ternary complexes containing pUb-M, a pDNA encoding melanoma surface antigen, against melanoma-bearing mice. Vaccinations of γ-PGA-ternary complexes into mice significantly suppressed the tumor growth of B16-F10 melanoma cells subcutaneously injected into the mice. In the same manner, vaccinations of γ-PGA-ternary complexes containing ovalbumin (OVA) completely suppressed the growth of E.G7-OVA cells expressing OVA. These results strongly suggest that γ-PGA-ternary complexes are useful in the manufacture of specific tumor vaccines.

摘要

我已研发出多种疫苗与阳离子材料和阴离子聚合物形成的新型三元复合物。编码萤火虫荧光素酶的质粒DNA(pDNA)被用作模型药物以形成合适的三元复合物。使用pDNA和聚乙烯亚胺构建阳离子二元复合物,然后用各种阴离子聚合物包裹这些二元复合物以形成三元复合物。与二元复合物相比,这些三元复合物显著改善了细胞毒性以及与红细胞的聚集。另一方面,由于其阴离子表面电荷,大多数这些三元复合物的体外转基因效率较低。然而,γ-聚谷氨酸(γ-PGA)-三元复合物表现出较高的体外转基因效率。将γ-PGA-三元复合物静脉注射到小鼠体内后,在富含抗原呈递细胞的脾脏边缘区检测到极高的基因表达。γ-PGA-三元复合物的这种脾脏特异性现象似乎适用于抗癌DNA疫苗。因此,我研究了含有pUb-M(一种编码黑色素瘤表面抗原的pDNA)的γ-PGA-三元复合物对荷黑色素瘤小鼠的预防效果。将γ-PGA-三元复合物接种到小鼠体内可显著抑制皮下注射到小鼠体内的B16-F10黑色素瘤细胞的肿瘤生长。同样地,接种含有卵清蛋白(OVA)的γ-PGA-三元复合物可完全抑制表达OVA的E.G7-OVA细胞的生长。这些结果有力地表明,γ-PGA-三元复合物可用于制备特异性肿瘤疫苗。

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