首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Expression of alternatively spliced human T-lymphotropic virus type I pX mRNA in infected cell lines and in primary uncultured cells from patients with adult T-cell leukemia/lymphoma and healthy carriers.
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Expression of alternatively spliced human T-lymphotropic virus type I pX mRNA in infected cell lines and in primary uncultured cells from patients with adult T-cell leukemia/lymphoma and healthy carriers.

机译:成年T细胞白血病/淋巴瘤患者和健康携带者的受感染细胞系和原代未培养细胞中交替剪接的I型人T淋巴病毒I pX mRNA的表达。

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摘要

Although human T-cell lymphotropic virus type I (HTLV-I) is the etiologic agent of adult T-cell leukemia/lymphoma (ATL), the role of viral gene expression in the progression to and maintenance of the leukemic state in vivo is unclear because of the inability of most previous studies to readily detect HTLV-I RNA in infected individuals. By using the reverse transcriptase-polymerase chain reaction, we detected spliced messages for the HTLV-I pX regulatory genes in primary uncultured cells from ATL patients and healthy asymptomatic carriers. In addition to the expected doubly spliced pX message, three alternatively spliced mRNAs were demonstrated (pX delta 17, pX-p21rex, and pX-orfII mRNAs, where orf = open reading frame). The same splice sites were shown in the messages from uncultured ATL cells and from the HTLV-I-producing C10/MJ cell line. Alternatively spliced pX mRNAs have the potential to code for known and putative pX gene products. Among the transcripts is a monocistronic mRNA likely to code for p21rex (pX-p21rex mRNA). Since alternative splicing of HTLV-I pX mRNA can be found in primary uncultured cells, it is likely to have a functional significance in vivo. This suggests possible roles for HTLV-I gene expression in the progression to and maintenance of ATL, as well as in the phase preceding it.
机译:尽管I型人T细胞淋巴病毒(HTLV-1)是成人T细胞白血病/淋巴瘤(ATL)的病原体,但病毒基因表达在体内向白血病状态发展和维持中的作用尚不清楚由于大多数先前的研究无法在受感染的个体中轻松检测HTLV-1 RNA。通过使用逆转录酶-聚合酶链反应,我们在来自ATL患者和健康无症状携带者的原代未培养细胞中检测到HTLV-1 pX调控基因的剪接信息。除了预期的双重剪接的pX信息外,还显示了三个交替剪接的mRNA(pX delta 17,pX-p21rex和pX-orfII mRNA,其中orf =开放阅读框)。在未培养的ATL细胞和产生HTLV-1的C10 / MJ细胞系的消息中显示了相同的剪接位点。或者,剪接的pX mRNA具有编码已知和假定的pX基因产物的潜力。转录物中有一个单顺反子mRNA,可能编码p21rex(pX-p21rex mRNA)。由于可以在未培养的原代细胞中发现HTLV-1 pX mRNA的可变剪接,因此它可能在体内具有功能性意义。这表明HTLV-1基因表达在ATL的发展和维持中以及在其之前的阶段中的可能作用。

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