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Cloning and charaterization of a human ribosomal protein gene with enhanced expression in fetal and neoplastic cells

机译:人核糖体蛋白基因在胎儿和肿瘤细胞中表达增强的克隆和鉴定

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Hepatocellular carcinoma is strongly associated with hepatitis B virus carrier patients who usually have HBV sequences integrated in the chromosomal DNA of liver cells. To assess the possible effects of HBV regulatory sequences (e.g., the enhancer) on expression of neighboring host genes we have screened for cellular genes that are both overexpressed and adjacent to integrated HBV sequences in hepatocellular carcinoma cells . The cloned cDNA for one such gene encodes a protein similar to the E. coli L-3 ribosomal protein which is thought to play a role in mRNA binding to the ribosome. The protein encoded by the cDNA localizes to the nucleolus and is also found in ribosomes; possibly it is the mammalian homologue of L-3 (MRL3). The expression of MRL3 is higher in colon carcinoma and lymphoma cell lines than in normal liver , placenta and diploid fibroblasts, and is also higher in fetal than in adult liver. Therefore, MRL3 overexpression seems to be a property of rapidly dividing cells and is not directly linked to oncogenesis.
机译:肝细胞癌与乙型肝炎病毒携带者患者密切相关,这些患者通常具有整合在肝细胞染色体DNA中的HBV序列。为了评估HBV调控序列(例如增强子)对邻近宿主基因表达的可能影响,我们筛选了肝细胞癌细胞中过度表达且与整合的HBV序列相邻的细胞基因。一个这样的基因的克隆的cDNA编码一种类似于大肠杆菌L-3核糖体蛋白的蛋白,该蛋白被认为在与核糖体结合的mRNA中起作用。由cDNA编码的蛋白质位于核仁,也存在于核糖体中。可能是L-3(MRL3)的哺乳动物同源物。 MRL3在结肠癌和淋巴瘤细胞系中的表达高于正常肝,胎盘和二倍体成纤维细胞,在胎儿中也比在成人肝脏中更高。因此,MRL3的过表达似乎是细胞快速分裂的特性,并且与肿瘤发生没有直接联系。

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