Np9 Protein of Human Endogenous Retrovirus K Interacts with Ligand of Numb Protein X

Armbruester, Vivienne; Sauter, Marlies; Roemer, Klaus; Best, Barbara; Hahn, Steffen; Nty, Achille; Schmid, Andreas; Philipp, Stephan E.; Müeller, Anja; Mueller‐Lantzsch, Nikolaus

doi:10.1128/jvi.78.19.10310-10319.2004

Cited by 83 publications

(125 citation statements)

References 36 publications

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“…This result provides support for the idea that cORF rather than full-length env protein is responsible for cell transformation. Recently, a novel gene, np9, resulting from use of a unique HERV-K type 1-specific splice donor site, was confirmed to be expressed in various tumor tissues and transformed cell lines but not in normal, nontransformed cells, suggesting that the protein may function in tumorigenesis (Armbruester et al, 2002). It remains to be seen whether the variants that we have identified here will possess tumorigenic properties similar to the np9 variant just reported.…”

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confidence: 82%

Quantitation of HERV-K env gene expression and splicing in human breast cancer

et al. 2003

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Human endogenous retroviruses (HERVs) comprise up to 8% of the human genome. In previous studies, we demonstrated that type 1 HERV-K envelope (env) transcripts are expressed in most human breast cancers, but not in normal breast tissues. In the current study, we report that type 2 HERV-K env transcripts are also present in human breast cancers. By real-time RT-PCR, the expression of HERV-K env transcripts was 5-10-fold higher in breast cancer cell lines treated with estradiol and progesterone than in cells without treatment, and expression was significantly higher in most breast cancer tissues than in normal breast tissues. Furthermore, both types of HERV-K env transcripts were capable of being spliced into subgenomic env transcripts and various splice donor and acceptor sites were detected in breast cancers. The selective expression and distribution of multiple HERV-K endogenous retroviral element splice variants in breast cancer, but not in normal controls, suggests that they are novel breast tumor markers.

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confidence: 82%

Quantitation of HERV-K env gene expression and splicing in human breast cancer

et al. 2003

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“…Armbruester et al (24) found np9 transcripts in most transformed human cell lines by using an RT-PCR method. Interestingly, nearly all healthy and malignant tissues from humans express full-length HERV-K type 1 mRNAs, but no np9 transcripts are generated in normal human tissues.…”

Section: Proviral Organization and Transcripts Of Herv-kmentioning

confidence: 99%

“…Recently, a HERV-K type 1-specific transcript coding for a 9-kDa protein, designated Np9, has been identified (24). This transcript represents a kind of type 1 substitute for the Rec sequence of type 2 proviruses.…”

Section: Proviral Organization and Transcripts Of Herv-kmentioning

confidence: 99%

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Retroelements and the human genome: New perspectives on an old relation

Bannert

Kurth

2004

Proc. Natl. Acad. Sci. U.S.A.

460

426

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Retroelements constitute a large portion of our genomes. One class of these elements, the human endogenous retroviruses (HERVs), is comprised of remnants of ancient exogenous retroviruses that have gained access to the germ line. After integration, most proviruses have been the subject of numerous amplifications and have suffered extensive deletions and mutations. Nevertheless, HERV-derived transcripts and proteins have been detected in healthy and diseased human tissues, and HERV-K, the youngest, most conserved family, is able to form virus-like particles. Although it is generally accepted that the integration of retroelements can cause significant harm by disrupting or disregulating essential genes, the role of HERV expression in the etiology of malignancies and autoimmune and neurologic diseases remains controversial. In recent years, striking evidence has accumulated indicating that some proviral sequences and HERV proteins might even serve the needs of the host and are therefore under positive selection. The remarkable progress in the analysis of host genomes has brought to light the significant impact of HERVs and other retroelements on genetic variation, genome evolution, and gene regulation.A lmost half of the mammalian genome is derived from ancient transposable elements. The two general types, (DNA)-transposons and retroelements, often regarded as ''selfish DNA parasites or junk DNA,'' encompass Ϸ2.8% and 42.2% of the human genome, respectively (1, 2). This striking finding is one of the many insights from recent large-scale sequencing projects that have provided the most valuable information in this field since the initial discovery of mobile elements in 1956 by Barbara McClintock (3, 4). Whereas DNA-transposons amplify without an RNA intermediate, retroelements rely on an RNA transcript that is retrotranscribed by a reverse transcriptase before integration in the genome. Here, we briefly review the characteristics of retroelements, their present classification, and the available evidence for their biological significance and function in normal and pathological processes. The focus is on human endogenous retroviruses (HERVs), the remnants of ancient germ-cell infections. Although most of the HERV proviruses have undergone extensive deletions and mutations, some have retained ORFs coding for functional proteins. A few families, including the HERV-K (HML-2) group, have been shown to form viral particles (5, 6), and an apparently intact provirus has recently been discovered in a small fraction of the human population, indicating a very recent acquisition (5-7). Classification of RetroelementsRetroelements constitute 90% of the Ϸ3 million transposable elements present in the human genome (1). They are split into two large groups, the non-LTR and LTR elements (Fig. 1). Two of the non-LTR members are present in extremely high copy numbers in the mammalian germ line: the short interspersed elements (SINE) with the prominent Alu and MIR repeats and the long-terminal interspersed elements (LINE) containing the...

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“…In fact, Np9 and Rec have been shown to be highly expressed in transformed tissues (Np9), to cause carcinoma in situ in mice (Rec), and to be associ-ated with the Notch pathway and pathways affecting c-myc expression (Np9 and both, respectively) (13,15,16,(62)(63)(64)(65). Our laboratory has noted high expression levels of both proteins during HIV-1-associated lymphoma (unpublished observations).…”

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confidence: 99%

Regulation of the Human Endogenous Retrovirus K (HML-2) Transcriptome by the HIV-1 Tat Protein

Gonzalez-Hernandez

Cavalcoli

Sartor

et al. 2014

J Virol

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Approximately 8% of the human genome is made up of endogenous retroviral sequences. As the HIV-1 Tat protein activates the overall expression of the human endogenous retrovirus type K (HERV-K) (HML-2), we used next-generation sequencing to determine which of the 91 currently annotated HERV-K (HML-2) proviruses are regulated by Tat. Transcriptome sequencing of total RNA isolated from Tat-and vehicle-treated peripheral blood lymphocytes from a healthy donor showed that Tat significantly activates expression of 26 unique HERV-K (HML-2) proviruses, silences 12, and does not significantly alter the expression of the remaining proviruses. Quantitative reverse transcription-PCR validation of the sequencing data was performed on Tattreated PBLs of seven donors using provirus-specific primers and corroborated the results with a substantial degree of quantitative similarity. IMPORTANCEThe expression of HERV-K (HML-2) is tightly regulated but becomes markedly increased following infection with HIV-1, in part due to the HIV-1 Tat protein.The findings reported here demonstrate the complexity of the genome-wide regulation of HERV-K (HML-2) expression by Tat. This work also demonstrates that although HERV-K (HML-2) proviruses in the human genome are highly similar in terms of DNA sequence, modulation of the expression of specific proviruses in a given biological situation can be ascertained using next-generation sequencing and bioinformatics analysis.

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Np9 Protein of Human Endogenous Retrovirus K Interacts with Ligand of Numb Protein X

Cited by 83 publications

References 36 publications

Quantitation of HERV-K env gene expression and splicing in human breast cancer

Quantitation of HERV-K env gene expression and splicing in human breast cancer

Retroelements and the human genome: New perspectives on an old relation

Regulation of the Human Endogenous Retrovirus K (HML-2) Transcriptome by the HIV-1 Tat Protein

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