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H-2K与H-2D抗原的差异表达可区分高转移克隆和低转移克隆,这与肿瘤细胞的免疫原性特性相关。

The differential expression of H-2K versus H-2D antigens, distinguishing high-metastatic from low-metastatic clones, is correlated with the immunogenic properties of the tumor cells.

作者信息

Eisenbach L, Hollander N, Greenfeld L, Yakor H, Segal S, Feldman M

出版信息

Int J Cancer. 1984 Oct 15;34(4):567-73. doi: 10.1002/ijc.2910340421.

Abstract

Two clones of the 3LL Lewis lung carcinoma, a low-metastatic clone A9 and a high-metastatic clone D122, were studied for MHC expression and immunogenic properties. Using monoclonal antibodies, we demonstrated that the A9 clone expresses both the H-2Kb and the H-2Db, whereas the D122 expresses only the H-2Db, and lacks the expression of the H-2Kb encoded molecules. Cells of the low-metastatic clone A9 grew progressively in syngeneic (C57BL/6J) or in F1 mice, but were rejected in allogeneic recipients. The high-metastatic D122 grew progressively in all mouse strains tested, yet metastases were formed only in syngeneic recipients. When H-2 recombinant mice were used, the A9 again manifested a significantly greater immunogenic potency than the metastatic D122, which grew in all 4 recombinants tested. Metastases, however, were formed in B10HTG and to a lesser extent in B10A(4R), thus indicating that metastasis formation is restricted by both C57BL background and H-2Db sub region. We subsequently tested whether the higher immunogenicity of the H-2Kb-positive A9 cells is expressed also in syngeneic mice, to examine whether this could account for its low metastatic phenotype. We found that immunization by A9 cells significantly inhibited the growth of a subsequent A9 graft and even of D122, yet D122 did not retard the growth of secondary D122 or A9 cells. The increased immunogenic effect was expressed also in the generation of syngeneic cytotoxic lymphocytes by A9 but not by D122 cells. We suggest that expression of H-2K molecules on the 3LL clones, immunogenicity and the metastatic phenotype are causally related in this system.

摘要

对3LL Lewis肺癌的两个克隆株进行了研究,一个是低转移克隆株A9,另一个是高转移克隆株D122,研究内容包括主要组织相容性复合体(MHC)表达和免疫原性特性。使用单克隆抗体,我们证明A9克隆株同时表达H-2Kb和H-2Db,而D122仅表达H-2Db,且缺乏H-2Kb编码分子的表达。低转移克隆株A9的细胞在同基因(C57BL/6J)或F1小鼠中逐渐生长,但在异基因受体中被排斥。高转移的D122在所有测试的小鼠品系中都逐渐生长,但仅在同基因受体中形成转移瘤。当使用H-2重组小鼠时,A9再次表现出比转移的D122显著更高的免疫原性效力,D122在所有4种测试的重组小鼠中都能生长。然而,转移瘤在B10HTG中形成,在B10A(4R)中形成的程度较小,这表明转移瘤的形成受到C57BL背景和H-2Db亚区域的限制。随后,我们测试了H-2Kb阳性的A9细胞的较高免疫原性在同基因小鼠中是否也有表现,以检查这是否可以解释其低转移表型。我们发现,用A9细胞免疫可显著抑制后续A9移植瘤甚至D122移植瘤的生长,但D122不会抑制二次接种的D122或A9细胞的生长。A9细胞在产生同基因细胞毒性淋巴细胞方面也表现出增强的免疫原性作用,而D122细胞则没有。我们认为,在这个系统中,3LL克隆株上H-2K分子的表达、免疫原性和转移表型之间存在因果关系。

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