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主要组织相容性复合体I类和白细胞介素2基因转导的黑色素瘤细胞联合疫苗接种可协同治愈术后已形成的肺转移瘤。

Combined vaccination with major histocompatibility class I and interleukin 2 gene-transduced melanoma cells synergizes the cure of postsurgical established lung metastases.

作者信息

Porgador A, Tzehoval E, Vadai E, Feldman M, Eisenbach L

机构信息

Department of Cell Biology, Weizmann Institute of Science, Rehovot, Israel.

出版信息

Cancer Res. 1995 Nov 1;55(21):4941-9.

PMID:7585534
Abstract

We have analyzed and compared in detail the malignant phenotypes of, the immune mechanisms induced by, and the immunotherapeutic potentials of B16-F10.9 melanoma cells manipulated by gene transfer to express syngeneic H-2Kb molecules or to secrete the cytokines interleukin 2 (IL-2) or IL-6. Local tumor growth in the footpad of transduced cells is mainly retarded by expression of H-2Kb and IL-2 genes and less by expression of IL-6. Mice given injections intrafootpad of tumorigenic doses of transduced clones manifested significantly reduced postsurgical spontaneous metastasis. After i.v. inoculation, mice given injections of F10.9-Kb expressors did not develop experimental lung metastases; mice given injections of F10.9-IL-6 secretors developed reduced metastatic loads; whereas mice given injections of F10.9-IL-2 secretors developed high loads of lung metastases. On the basis of injections into nude mice, in vivo depletions of CD4+, CD8+, and NK1.1+ cells, and in vitro CTL and natural killer (NK) assays, we show that all F10.9-modified cells induce CD8+ tumor-specific CTL activity and that F10.9-IL-2 secretors also induce nonspecific NK/lymphokine-activated killer cell activity. Vaccinations with F10.9-modified cells were capable of significantly reducing metastatic spread from small established F10.9 footpad tumors. However, in mice carrying preestablished lung metastases, a highly therapeutic effect was achieved only when H-2Kb expressors and IL-2 secretors were combined in vaccination, whereas individual vaccines or other combinations had marginal effects. This higher efficiency of the combined vaccine is due to the combined effect of efficient CTL induction and NK/lymphokine-activated killer cell activity as concluded from depletion of CD8+ and NK1.1 cells during immunotherapy. Thus, the cure of established metastasis can be achieved by the synergistic effects of vaccination with class I and IL-2-transduced tumor cells.

摘要

我们已经详细分析和比较了通过基因转移来表达同基因H-2Kb分子或分泌细胞因子白细胞介素2(IL-2)或IL-6的B16-F10.9黑色素瘤细胞的恶性表型、诱导的免疫机制以及免疫治疗潜力。转导细胞在足垫中的局部肿瘤生长主要因H-2Kb和IL-2基因的表达而受到抑制,因IL-6的表达而受到的抑制较小。给小鼠足垫注射致瘤剂量的转导克隆后,术后自发转移明显减少。静脉接种后,注射F10.9-Kb表达细胞的小鼠未发生实验性肺转移;注射F10.9-IL-6分泌细胞的小鼠转移负荷降低;而注射F10.9-IL-2分泌细胞的小鼠发生了高负荷的肺转移。基于对裸鼠的注射、体内CD4 +、CD8 +和NK1.1 +细胞的清除以及体外细胞毒性T淋巴细胞(CTL)和自然杀伤(NK)测定,我们表明所有F10.9修饰的细胞均诱导CD8 +肿瘤特异性CTL活性,并且F10.9-IL-2分泌细胞还诱导非特异性NK/淋巴因子激活的杀伤细胞活性。用F10.9修饰的细胞进行疫苗接种能够显著减少已形成的小F10.9足垫肿瘤的转移扩散。然而,在携带预先建立的肺转移的小鼠中,只有当H-2Kb表达细胞和IL-2分泌细胞联合用于疫苗接种时才能获得高度治疗效果,而单独的疫苗或其他组合的效果甚微。联合疫苗的这种更高效率归因于免疫治疗期间CD8 +和NK1.1细胞清除所推断的有效CTL诱导和NK/淋巴因子激活的杀伤细胞活性的联合作用。因此,通过用I类和IL-2转导的肿瘤细胞进行疫苗接种的协同作用可以实现对已建立转移的治愈。

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