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内吞含抗原的IgG脂质体的树突状细胞可引发有效的抗肿瘤免疫。

Dendritic cells that endocytosed antigen-containing IgG-liposomes elicit effective antitumor immunity.

作者信息

Kawamura Kazuko, Kadowaki Norimitsu, Suzuki Ryo, Udagawa Satoshi, Kasaoka Satoshi, Utoguchi Naoki, Kitawaki Toshio, Sugimoto Nakaba, Okada Naoki, Maruyama Kazuo, Uchiyama Takashi

机构信息

Department of Hematology and Oncology, Graduate School of Medicine, Kyoto University, Kyoto, Japan.

出版信息

J Immunother. 2006 Mar-Apr;29(2):165-74. doi: 10.1097/01.cji.0000190169.61416.f5.

DOI:10.1097/01.cji.0000190169.61416.f5
PMID:16531817
Abstract

Liposomes represent a promising vehicle to deliver exogenous antigens to dendritic cells (DCs) for tumor immunotherapy. Targeting exogenous antigens to Fcgamma receptors on DCs has been shown to result in efficient presentation of antigen-derived peptides on major histocompatibility complex (MHC) class I and class II molecules. In this study, it was investigated whether DCs that endocytosed physicochemically optimized antigen-containing liposomes conjugated with IgG efficiently present antigens on MHC class I and class II molecules, and consequently induce strong antitumor immune responses. IgG-conjugated liposomes that were 200 nm in diameter without attaching polyethylene glycol were most efficiently endocytosed by DCs. Human monocyte-derived DCs that endocytosed tetanus toxoid (TT)-containing IgG liposomes via CD32 stimulated CD4(+) T cells more strongly than DCs pulsed with TT-containing bare liposomes or with soluble TT. Immunization of mice with DCs that endocytosed ovalbumin (OVA)-containing IgG liposomes but not OVA-containing bare liposomes or soluble OVA completely prevented the growth of OVA-expressing lymphoma cells. Importantly, administration of DCs that endocytosed OVA-containing IgG liposomes to the mice with established OVA-expressing tumors strongly suppressed tumor growth. This study demonstrates an IgG liposome with physicochemical properties suitable for delivering antigens to DCs and paves the way to the application of IgG liposomes for tumor immunotherapy using DCs.

摘要

脂质体是一种很有前景的载体,可将外源性抗原递送至树突状细胞(DC)用于肿瘤免疫治疗。已证明将外源性抗原靶向DC上的Fcγ受体可导致抗原衍生肽在主要组织相容性复合体(MHC)I类和II类分子上有效呈递。在本研究中,研究了内吞与IgG缀合的理化性质优化的含抗原脂质体的DC是否能在MHC I类和II类分子上有效呈递抗原,从而诱导强烈的抗肿瘤免疫反应。直径为200 nm且未连接聚乙二醇的IgG缀合脂质体最易被DC内吞。通过CD32内吞含破伤风类毒素(TT)的IgG脂质体的人单核细胞衍生DC比用含TT的裸脂质体或可溶性TT脉冲处理的DC更强烈地刺激CD4(+) T细胞。用内吞含卵清蛋白(OVA)的IgG脂质体而非含OVA的裸脂质体或可溶性OVA的DC免疫小鼠可完全阻止表达OVA的淋巴瘤细胞的生长。重要的是,将内吞含OVA的IgG脂质体的DC给予已建立表达OVA肿瘤的小鼠可强烈抑制肿瘤生长。本研究证明了一种具有适合将抗原递送至DC的理化性质的IgG脂质体,并为使用DC的IgG脂质体在肿瘤免疫治疗中的应用铺平了道路。

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