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An adenovirus 2-coded tumor antigen located on the endoplasmic reticulum and nuclear envelope is required for growth of transformed cells in Ca2+-deficient media.

机译:位于Ca2 +缺乏培养基中的转化细胞的生长需要位于内质网和核被膜上的腺病毒2编码的肿瘤抗原。

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摘要

Rat embryo cell lines containing the adenovirus 2 E1a region together with normal or mutant forms of the N-terminal half of the E1b region (HindIII G fragment) were generated by using a dominant selection marker, neo. Biochemically transformed cells containing a nonmutated HindIII G fragment proliferated more rapidly in Ca2+-deficient media, whereas cells containing a specific deletion within the E1b-encoded, 175-amino-acid (175R) (19-kilodalton) T-antigen gene and nontransformed cells grew at a slower rate. Furthermore, transformed cells that did not express the 175R T antigen and untransformed cells could not replicate their DNA efficiently in low-Ca2+ medium. Our results suggest that Ca2+ ions may provide an important stimulus for cell proliferation in adenovirus-transformed cells through a mechanism that involves the functions of the 175R T antigen.
机译:通过使用显性选择标记neo生成包含腺病毒2 E1a区以及E1b区N末端一半(HindIII G片段)的正常或突变形式的大鼠胚胎细胞系。生化转化的含有未突变的HindIII G片段的细胞在缺乏Ca2 +的培养基中增殖更快,而含有E1b编码的175个氨基酸(175R)(19-千屈顿)T抗原基因中特定缺失的细胞和未转化的细胞增长速度较慢。此外,不表达175R T抗原的转化细胞和未转化的细胞无法在低Ca2 +培养基中有效地复制其DNA。我们的结果表明,Ca2 +离子可能通过涉及175R T抗原功能的机制为腺病毒转化细胞中的细胞增殖提供重要的刺激。

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