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通过重组到脂质体中的病毒相关蛋白引发体外和体内抗1型人类嗜T淋巴细胞病毒的细胞免疫。

Priming for in vitro and in vivo anti-human T lymphotropic virus type 1 cellular immunity by virus-related protein reconstituted into liposome.

作者信息

Noguchi Y, Noguchi T, Sato T, Yokoo Y, Itoh S, Yoshida M, Yoshiki T, Akiyoshi K, Sunamoto J, Nakayama E

机构信息

Department of Oncology, Nagasaki University School of Medicine, Japan.

出版信息

J Immunol. 1991 May 15;146(10):3599-603.

PMID:2026883
Abstract

In vitro and in vivo anti-human T lymphotropic virus type 1 (HTLV-1) cellular immunity was examined by immunizing rats with a truncated hybrid protein (228 amino acids) of gag and env of HTLV-1 produced by Escherichia coli. Animals were immunized with the hybrid protein reconstituted into mannan-derivative-coated liposomes (gag-env-lipo). In vitro sensitization with a HTLV-1-positive cell line, TARS-1, of spleen cells obtained from these animals generated killer cells specific for syngeneic HTLV-1-positive cells. No killer activity was generated when spleen cells were obtained from animals immunized with the hybrid protein alone, the liposome alone, or the hybrid protein reconstituted into conventional liposomes with no polysaccharide coating. Killer cells were CD8+ CTL restricted to MHC class I. Analysis of CD8+ and CD4+ subsets in spleens showed the existence of primed CD8+ T cells in animals immunized with gag-env-lipo. Rats immunized with gag-env-lipo displayed accelerated rejection of TARS-1 but not of two other HTLV-1-negative tumor lines. Injection of carrageenan into animals strongly inhibited generation of killer cells, which indicates the necessity of macrophages for priming of CD8+ T cells with gag-env-lipo. Injection of carrageenan also cancelled in vivo immunity against HTLV-1+ cells induced with gag-env-lipo. These results, taken together, indicate that exogenous protein reconstituted into appropriate liposomes can effectively prime MHC class I restricted CD8+ T cells in vivo with macrophage dependency.

摘要

通过用大肠杆菌产生的人类嗜T淋巴细胞病毒1型(HTLV-1)的gag和env截短杂交蛋白(228个氨基酸)免疫大鼠,检测体外和体内抗HTLV-1细胞免疫。用重构到甘露糖衍生物包被脂质体(gag-env-lipo)中的杂交蛋白免疫动物。用这些动物获得的脾细胞与HTLV-1阳性细胞系TARS-1进行体外致敏,产生了对同基因HTLV-1阳性细胞具有特异性的杀伤细胞。当从仅用杂交蛋白、仅用脂质体或重构到无多糖包被的常规脂质体中的杂交蛋白免疫的动物获得脾细胞时,未产生杀伤活性。杀伤细胞是受MHC I类限制的CD8 + CTL。对脾脏中CD8 +和CD4 +亚群的分析表明,在用gag-env-lipo免疫的动物中存在致敏的CD8 + T细胞。用gag-env-lipo免疫的大鼠对TARS-1的排斥加速,但对另外两个HTLV-1阴性肿瘤细胞系则没有。向动物注射角叉菜胶强烈抑制杀伤细胞的产生,这表明巨噬细胞对于用gag-env-lipo启动CD8 + T细胞是必需的。注射角叉菜胶也消除了用gag-env-lipo诱导的对HTLV-1 +细胞的体内免疫。综上所述,这些结果表明,重构到合适脂质体中的外源蛋白可以在体内有效地启动依赖巨噬细胞的MHC I类限制的CD8 + T细胞。

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引用本文的文献

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HIV-1-specific cell-mediated immune responses induced by DNA vaccination were enhanced by mannan-coated liposomes and inhibited by anti-interferon-gamma antibody.由DNA疫苗诱导的HIV-1特异性细胞介导的免疫反应通过甘露糖包被的脂质体得到增强,并被抗干扰素-γ抗体抑制。
Immunology. 1997 Sep;92(1):111-7. doi: 10.1046/j.1365-2567.1997.00307.x.
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