首页> 外文期刊>Virology >Identification of a 17-nucleotide splicing enhancer in HPV-16 L1 that counteracts the effect of multiple hnRNP A1-binding splicing silencers.
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Identification of a 17-nucleotide splicing enhancer in HPV-16 L1 that counteracts the effect of multiple hnRNP A1-binding splicing silencers.

机译:在HPV-16 L1中鉴定出一种17核苷酸的拼接增强子,该增强子可抵消多个hnRNP A1结合的拼接沉默子的作用。

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Human papillomavirus type 16 (HPV-16) infections can in rare cases persist and cause lesions that may progress to cervical cancer. Cells in the lesions are not permissive for virus production, nor are cervical cancer cells. The intracellular environment is such that it prevents production of the highly immunogenic, viral structural proteins L1 and L2. One may speculate that inhibition of L1 and L2 expression is a prerequisite for persistence and cancer progression. We have therefore investigated how expression of HPV-16 L1 is regulated. We found that the only splice site in the HPV-16 late region, which is used to produce L1 mRNAs, is under control of a splicing enhancer located in the 17 nucleotides immediately downstream of the splice site. However, the function of this enhancer in cervical cancer cells is largely overshadowed by multiple splicing silencers in the late region which bind to hnRNP A1. High levels of hnRNP A1 therefore inhibit HPV-16 L1 expression. Immunohistological analysis of cervical epithelia revealed that hnRNP A1 is expressed primarily in the lower layers of the epithelium. hnRNP A1 is undetectable in terminally differentiated cells that can express HPV-16 late genes, which supports the conclusion that high levels of hnRNP A1 inhibit HPV-16 L1 expression.
机译:人类乳头瘤病毒16型(HPV-16)感染在极少数情况下会持续存在并导致可能发展为宫颈癌的病变。病变中的细胞不允许产生病毒,子宫颈癌细胞也不允许。细胞内环境使得其阻止产生高度免疫原性的病毒结构蛋白L1和L2。有人可能认为抑制L1和L2表达是持久性和癌症发展的先决条件。因此,我们研究了如何调节HPV-16 L1的表达。我们发现,HPV-16晚期区域中用于产生L1 mRNA的唯一剪接位点处于剪接增强子的控制之下,该剪接增强子位于剪接位点下游的17个核苷酸中。但是,这种增强子在宫颈癌细胞中的功能在后期被多个剪接的沉默子所覆盖,而这些沉默子与hnRNP A1结合。因此,高水平的hnRNP A1会抑制HPV-16 L1的表达。宫颈上皮的免疫组织学分析显示,hnR​​NP A1主要在上皮的下层表达。在可以表达HPV-16晚期基因的终末分化细胞中无法检测到hnRNP A1,这支持高水平的hnRNP A1抑制HPV-16 L1表达的结论。

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