Literature DB >> 8367298

p21X mRNA is expressed as a singly spliced pX transcript from defective provirus genomes having a partial deletion of the pol-env region in human T-cell leukemia virus type 1-infected cells.

S Orita1, H Kobayashi, Y Aono, A Saiga, M Maeda, H Igarashi.   

Abstract

In addition to the three typical transcripts such as genomic/gag-pol mRNA, env mRNA and tax/rex mRNA, we previously found the singly spliced pX mRNA, termed p21X mRNA, responsible for producing the p21X protein in human T-cell leukemia virus type 1 (HTLV-1)-infected cells. Our finding of the p21X mRNA being constitutively expressed in the fresh peripheral blood mononuclear cells (PBMCs) from patients with ATL has suggested that the expression mechanism is quite different from that of the others. In this paper, the expression mechanism of p21X mRNA was investigated by analyzing the organization of the proviral genomes present in the representative HTLV-1-infected cell lines which are positive or negative for the expression of p21X mRNA. Southern and PCR analyses show that most of the analyzed cell lines contain both one complete and one defective genome each. However, one cell line without the p21X mRNA expression, C91/PL, contains only the complete genome, suggesting that the complete HTLV-1 has no ability to express p21X mRNA in spite of having the ability to produce the infectious virus. The defective genomes of the p21X mRNA positive cell lines, MT-2 and H582, have a large deletion of the entire pol and parts of the gag and env regions including the common domain of the second exon of the doubly spliced tax/rex mRNA, while another defective genome of the p21X mRNA negative cell line, MT-1, has a deletion within the gag-pol gene. We show that these defective genomes have the ability to express their distinct, defective genomic mRNA, suggesting they are active. The defective genomic mRNAs in MT-2 and H582 cells retain the first splice donor and the second splice acceptor sites, suggesting the possibility of synthesizing p21X mRNA by splicing singly with these sites. These findings assume that defective HTLV-1 genomes deleting the second exon region acquire the ability to express p21X mRNA but no ability to express tax/rex mRNA. Such a deletion may explain the difference between the expression mechanisms in the p21X mRNA transcript and those in the other viral transcripts.

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Year:  1993        PMID: 8367298      PMCID: PMC309895          DOI: 10.1093/nar/21.16.3799

Source DB:  PubMed          Journal:  Nucleic Acids Res        ISSN: 0305-1048            Impact factor:   16.971


  42 in total

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Journal:  Nature       Date:  1981-12-24       Impact factor: 49.962

3.  Transformation of human leukocytes by cocultivation with an adult T cell leukemia virus producer cell line.

Authors:  N Yamamoto; M Okada; Y Koyanagi; M Kannagi; Y Hinuma
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4.  Isolation and transmission of human retrovirus (human t-cell leukemia virus).

Authors:  M Popovic; P S Sarin; M Robert-Gurroff; V S Kalyanaraman; D Mann; J Minowada; R C Gallo
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5.  Bovine leukemia virus RNA sequences involved in dimerization and specific gag protein binding: close relation to the packaging sites of avian, murine, and human retroviruses.

Authors:  I Katoh; T Yasunaga; Y Yoshinaka
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6.  Establishment of human cytotoxic T cell lines specific for human adult T cell leukemia virus-bearing cells.

Authors:  M Kannagi; K Sugamura; H Sato; K Okochi; H Uchino; Y Hinuma
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7.  Trans-acting transcriptional activation of the long terminal repeat of human T lymphotropic viruses in infected cells.

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8.  Encapsidation sequences for spleen necrosis virus, an avian retrovirus, are between the 5' long terminal repeat and the start of the gag gene.

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9.  Human adult T-cell leukemia virus: complete nucleotide sequence of the provirus genome integrated in leukemia cell DNA.

Authors:  M Seiki; S Hattori; Y Hirayama; M Yoshida
Journal:  Proc Natl Acad Sci U S A       Date:  1983-06       Impact factor: 11.205

10.  Human T-cell leukemia-lymphoma virus (HTLV): cloning of an integrated defective provirus and flanking cellular sequences.

Authors:  V Manzari; F Wong-Staal; G Franchini; S Colombini; E P Gelmann; S Oroszlan; S Staal; R C Gallo
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Authors:  J Rovnak; J W Casey
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2.  cis-Acting inhibitory elements within the pol-env region of human T-cell leukemia virus type 1 possibly involved in viral persistence.

Authors:  A Saiga; S Orita; N Minoura-Tada; M Maeda; Y Aono; M Asakawa; K Nakahara; R Kubota; M Osame; H Igarashi
Journal:  J Virol       Date:  1997-06       Impact factor: 5.103

3.  Cytoplasmic forms of human T-cell leukemia virus type 1 Tax induce NF-kappaB activation.

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4.  Human T-cell leukemia virus type II nucleotide sequences between env and the last exon of tax/rex are not required for viral replication or cellular transformation.

Authors:  P L Green; T M Ross; I S Chen; S Pettiford
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5.  The cutaneous T cell lymphoma, mycosis fungoides, is a human T cell lymphotropic virus-associated disease. A study of 50 patients.

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6.  HTLV-1 Rex: the courier of viral messages making use of the host vehicle.

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Review 7.  HTLV-1 Rex Tunes the Cellular Environment Favorable for Viral Replication.

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8.  Elucidation of the Mechanism of Host NMD Suppression by HTLV-1 Rex: Dissection of Rex to Identify the NMD Inhibitory Domain.

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  8 in total

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