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肿瘤细胞致瘤性和转移性的改变与磷酸钙介导的DNA转染过程有关。

Alteration of the tumorigenic and metastatic properties of neoplastic cells is associated with the process of calcium phosphate-mediated DNA transfection.

作者信息

Kerbel R S, Waghorne C, Man M S, Elliott B, Breitman M L

出版信息

Proc Natl Acad Sci U S A. 1987 Mar;84(5):1263-7. doi: 10.1073/pnas.84.5.1263.

Abstract

During the course of studies designed to assess the effect of human Ha-ras gene expression on the malignant behavior of transfected mouse tumor cells we noted that the process of Ca3(PO4)2-mediated DNA transfection was itself associated with profound alterations in tumorigenic or metastatic behavior. The cell line used as a recipient for these studies was a tumorigenic nonmetastatic CBA/J mouse mammary adenocarcinoma line called SP1. When cotransfected with plasmids containing the neo gene (pSV2neo) and the activated Ha-ras gene (pT24-c3), cells from the pooled (5-10 colonies) G418-resistant colonies gave rise to spontaneous lung metastases in 85% of mice after subcutaneous inoculation. However, we noted that 17% of control mice inoculated with G418-resistant pSV2neo-transfected SP1 cells also had lung metastases and that this number approached 100% as the inoculum comprised a greater pool size (50-100 colonies). When cell lines established from isolated pSV2neo-transfected colonies were examined, 3/16 were found to be metastatic. We also found that 3/16 clones grew slowly, or not at all, in CBA/J mice, whereas they grew readily in athymic (nude) mice. The increase in immunogenicity of two out of three of these latter clones was accompanied by expression of the class I H-2Dk major histocompatibility complex antigen that was not detectable in the parental SP1 cells. At least some of these results would appear to be due to exposure to Ca3(PO4)2 alone, as we found that it resulted in 5/20 (25%) clones manifesting metastatic properties. Our results suggest that heritable changes in malignant behavior of transfected tumor cells can be observed at high frequency subsequent to the process of Ca3(PO4)2-mediated DNA transfection, and these changes may be brought about in part by inherited disturbances in expression of recipient cell genes.

摘要

在旨在评估人Ha-ras基因表达对转染的小鼠肿瘤细胞恶性行为影响的研究过程中,我们注意到Ca3(PO4)2介导的DNA转染过程本身与致瘤或转移行为的深刻改变有关。用作这些研究受体的细胞系是一种致瘤性非转移性CBA/J小鼠乳腺腺癌细胞系,称为SP1。当与含有新霉素基因(pSV2neo)和活化的Ha-ras基因(pT24-c3)的质粒共转染时,来自合并的(5-10个克隆)G418抗性克隆的细胞在皮下接种后,85%的小鼠出现自发性肺转移。然而,我们注意到,接种G418抗性pSV2neo转染的SP1细胞的对照小鼠中有17%也有肺转移,并且随着接种物包含更大的克隆池大小(50-100个克隆),这个数字接近100%。当检查从分离的pSV2neo转染克隆建立的细胞系时,发现16个中有3个具有转移性。我们还发现,16个克隆中有3个在CBA/J小鼠中生长缓慢或根本不生长,而它们在无胸腺(裸)小鼠中生长良好。这三个克隆中有两个免疫原性的增加伴随着I类H-2Dk主要组织相容性复合体抗原的表达,而在亲本SP1细胞中未检测到该抗原。至少其中一些结果似乎是由于单独暴露于Ca3(PO4)2,因为我们发现它导致20个克隆中有5个(25%)表现出转移特性。我们的结果表明,在Ca3(PO4)2介导的DNA转染过程之后,可以高频观察到转染肿瘤细胞恶性行为的可遗传变化,并且这些变化可能部分是由受体细胞基因表达的遗传性干扰引起 的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c974/304407/9d85686bad38/pnas00270-0146-a.jpg

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