2003
DOI: 10.1046/j.1432-1033.2003.03921.x
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HIV‐1 integrase can process a 3′‐end crosslinked substrate

Abstract: Integrase of the human immunodeficiency virus type-1 (HIV-1) recognizes specific sequences located in the U3 and U5 regions at the ends of viral DNA. We synthesized DNA duplexes mimicking the U5 region and containing either 2¢-aminonucleosides or non-nucleoside 1,3-propanediol insertions at the third and terminal positions and studied their interactions with HIV-1 integrase. Both modifications introduced a local structural distortion in the DNA double helix. Replacement of the terminal nucleosides by correspon… Show more

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Cited by 9 publications
(8 citation statements)
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References 27 publications
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“…All these modifications at position 3 destabilized the DNA double helix (supplemental Table S1). This destabilization may stimulate 3Ј-end processing, consistent with previous data demonstrating an increase in 3Ј-processing activity because of destabilization of the 3rd bp (26,35,36).…”
Section: Initial Processing Ratesupporting
confidence: 91%
See 1 more Smart Citation
“…All these modifications at position 3 destabilized the DNA double helix (supplemental Table S1). This destabilization may stimulate 3Ј-end processing, consistent with previous data demonstrating an increase in 3Ј-processing activity because of destabilization of the 3rd bp (26,35,36).…”
Section: Initial Processing Ratesupporting
confidence: 91%
“…Destabilization of the A/T Pair at Position 3 Is Necessary for 3Ј-End Processing-Modification of the thymidine at position 3 in the unprocessed strand, by P insertion or 2Ј-modified nucleosides (U N and U M ), increased 3Ј-end processing rate (Table 3) probably because of local destabilization of the A/T base pair, as suggested previously (36). The processing stimulation following the thymidine replacement likely points to an absence of specific contact between IN and this base.…”
Section: Discussionsupporting
confidence: 63%
“…to adopt a structure intermediate between B-DNA and A-DNA (Figure 4a and c and Figure 5). The highly conserved C14pA15 step in the upper strand is known for its involvement in the viral DNA integration (62,63). The distortions that affect this step could be the foundation upon which the LTR-end of viral DNA is specifically recognized and cleaved by IN.…”
Section: Discussionmentioning
confidence: 99%
“…3A). The retardation of the latter could be caused either by DNAprotein cross-linking or by cross-linking within DNA [17][18][19][20]. Further experiments on purified plasmid and genomic DNA revealed that EDC induced interchain crosslinking within the double-stranded DNA ( fig.…”
mentioning
confidence: 99%