2007
DOI: 10.1128/jvi.02511-06
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Preferential Selection of Human T-Cell Leukemia Virus Type 1 Provirus Lacking the 5′ Long Terminal Repeat during Oncogenesis

Abstract: In adult T-cell leukemia (ATL) cells, a defective human T-cell leukemia virus type 1 (HTLV-1) provirus lacking the 5 long terminal repeat (LTR), designated type 2 defective provirus, is frequently observed. To investigate the mechanism underlying the generation of the defective provirus, we sequenced HTLV-1 provirus integration sites from cases of ATL. In HTLV-1 proviruses retaining both LTRs, 6-bp repeat sequences were adjacent to the 5 and 3 LTRs. In 8 of 12 cases with type 2 defective provirus, 6-bp repeats… Show more

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Cited by 107 publications
(131 citation statements)
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“…Although some failure during the PCR process could be responsible for a remote possible mistaken interpretation of results; however another real explanation is that defective proviruses would be generated during the infection process to oral keratinocytes. In order to support the last explanation, previous studies report the existence of defective HTLV-1 provirus in lymphocytic infections not only in ATL (9,20,11,15) but also in HAM/TSP patients (29,30,16,14). In this sense our results would be the first to document the existence of defective HTLV-1 provirus in infected oral keratinocytes.…”
Section: Immunophenotyping Of Oral Epithelium Cells Culturedsupporting
confidence: 64%
See 1 more Smart Citation
“…Although some failure during the PCR process could be responsible for a remote possible mistaken interpretation of results; however another real explanation is that defective proviruses would be generated during the infection process to oral keratinocytes. In order to support the last explanation, previous studies report the existence of defective HTLV-1 provirus in lymphocytic infections not only in ATL (9,20,11,15) but also in HAM/TSP patients (29,30,16,14). In this sense our results would be the first to document the existence of defective HTLV-1 provirus in infected oral keratinocytes.…”
Section: Immunophenotyping Of Oral Epithelium Cells Culturedsupporting
confidence: 64%
“…Although not direct evidence have obtained, the presence of defective provirus not only in lymphocytes but in oral keratinocytes, strongly suggest the possibility that low levels of viremia and/or low efficiency in the contact cell-to-cell could possibly favor post integration process that increase the frequency of defective provirus (15); however this statement in oral mucosa keratinocytes needs to be tested. …”
Section: Proviral Region Length (Bp)mentioning
confidence: 99%
“…During later stages of infection, several arguments support a very low expression of Tax in ATL cells because of deletion or hypermethylation of the 5 0 LTR and even in some cases to the appearance of stop codons in the Tax coding sequence. [33][34][35] By contrast, the HBZ RNA is well expressed in ATL cells. 36,37 From these observations, it has been proposed that Tax by inhibiting hTERT favors an unstable genomic state at early steps of transformation, whereas at late stages HBZ would drive with JunD a high expression of hTERT and consequently a high telomerase activity.…”
Section: Discussionmentioning
confidence: 95%
“…Celle-ci est codée par le brin antisens du provirus HTLV-1 à partir de la région 3'LTR. Les ARN et protéines HBZ sont constitutivement exprimés tout au long du processus d'oncogenèse, probablement parce que les régions 3'LTR sont moins sensibles à la méthylation et/ou aux anomalies géné-tiques [60]. HBZ est importante dans la maintenance du phénotype tumoral des cellules infectées par HTLV-1 et ce même en l'absence de Tax [61][62][63].…”
Section: Mutations Ponctuelles Et Anomalies éPigénétiquesunclassified