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The expression of mutant epidermal keratin cDNAs transfected in simple epithelial and squamous cell carcinoma lines.

机译:在简单的上皮和鳞状细胞癌系中转染的突变型表皮角蛋白cDNA的表达。

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We have deleted cDNA sequences encoding portions of the carboxy-terminal end of a human type I epidermal keratin K14, and examined the molecular consequences of forcing the expression of these mutants in simple epithelial and squamous cell carcinoma lines. To follow the expression of our mutant products in transfected cells, we have tagged the 3' end of the K14 coding sequence with a sequence encoding an antigenic domain of the neuropeptide substance P. Using DNA transfection and immunohistochemistry (with an antibody against substance P), we have identified a collection of mutants that have a wide range of morphological effects on the endogenous keratin filament networks of transfected cells. Mutants that are missing most of the nonhelical carboxy-terminal domain of K14 incorporate into the endogenous keratin filaments without any visible perturbations on the network. In contrast, mutants that are missing as few as 10 of the 310 amino acids of the central alpha-helical domain of the polypeptide cause gross alterations in the keratin network. In some cases, the entire cytoskeletal network of keratins was disrupted, leaving no evidence of 8-nm filaments. These results reveal the existence of a dynamic exchange between newly synthesized subunits and preexisting keratin filaments.
机译:我们已经删除了编码人类I型表皮角蛋白K14羧基末端部分的cDNA序列,并研究了强迫这些突变体在简单的上皮和鳞状细胞癌系中表达的分子后果。为了跟踪突变产物在转染细胞中的表达,我们用编码神经肽物质P抗原结构域的序列标记了K14编码序列的3'端。使用DNA转染和免疫组化(使用针对P物质的抗体) ,我们确定了一组突变体,这些突变体对转染细胞的内源性角蛋白丝网络具有广泛的形态学影响。缺少K14的大多数非螺旋羧基末端结构域的突变体可以并入内源性角蛋白丝中,而在网络上没有任何可见的干扰。相反,缺少该多肽的中央α-螺旋结构域的310个氨基酸中仅有10个氨基酸的突变体会导致角蛋白网络的总体改变。在某些情况下,整个角蛋白的细胞骨架网络都被破坏了,没有证据表明存在8 nm的细丝。这些结果揭示了新合成的亚基和先前存在的角蛋白丝之间存在动态交换。

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