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<i>Trans</i> -Acting Transcriptional Activation of the Long Terminal Repeat of Human T Lymphotropic Viruses in Infected Cells
777
Citations
51
References
1984
Year
Viral ReplicationViral Polymerase MechanismGeneticsImmunologyLtr SequencesHuman RetrovirusVirus GeneViral GeneticsVirologyT Cell ImmunityHtlv InfectionCell BiologyTranscriptional ActivationInfected CellsLong Terminal RepeatPathogenesisAdult T-cell Leukemia-lymphomaMedicineViral Immunity
Retroviral transcription initiates from LTR sequences flanking the provirus, and two HTLV subtypes are linked to distinct disease phenotypes. The article investigates whether LTR sequences of different HTLV subtypes differ in transcriptional activity across differentiated cell types. Trans‑acting factors in HTLV‑infected cells stimulate LTR‑driven gene expression in a subtype‑specific manner, underscoring the diverse biological effects of HTLV infection.
The transcription initiation signals for retroviruses lie within the long terminal repeat (LTR) sequences that flank the integrated provirus. Two subtypes of human T lymphotropic virus (HTLV) are associated with different disease phenotypes. In this article it is shown that marked differences exist in the ability of LTR sequences of these subtypes to function as transcriptional elements in differentiated cell types. It is also shown that trans-acting regulatory factors present in HTLV-infected cells stimulate gene expression directed by these LTR sequences in a type-specific manner. These results have implications for understanding the diverse biological effects of HTLV infection.
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