Abstract
BackgroundLINE-1s (L1, Long Interspersed Element-1) are the most abundant autonomous non-LTR retrotransposons in the human genome and replicate by reverse transcription of an RNA intermediate. Full-length L1 encodes two open reading frames (ORF1, ORF2) and ORF2 has reverse transcriptase activity.ResultsHere we expressed human L1 RT in E. coli and the purified protein displayed the same RT activity as that of ORF2p expressed in insect cells. We tested the effect of different reverse transcriptase inhibitors on L1 RT and found that all four tested nucleoside inhibitors efficiently inhibited L1 RT activity competitively. The Ki values of NRTIs were calculated (AZTTP, 16.4 ± 4.21 nM; d4TTP, 0.73 ± 0.22 nM; ddCTP, 0.72 ± 0.16 nM; 3TCTP, 12.9 ± 2.07 nM). L1 RT was less sensitive to non-nucleoside reverse transcriptase inhibitors, among these nevirapine had no effect, even at concentrations up to 500 μM. We also examined the effect of RT inhibitors on L1 retrotransposition efficiency in vivo using a cell-based retrotransposition assay. Similarly, all analog inhibitors decreased L1 retrotransposition frequency with different potencies whereas nevirapine had little or no effect on L1 retrotransposition. For comparison, we also tested the same inhibitors to highly purified RT of an LTR-retrotransposon (Ty1) and found it was less sensitive to NRTIs than L1 RT and has the same inhibition profile as L1 RT to NNRTIs.ConclusionsThese data indicate that bacterially expressed L1 RT is an active reverse transcriptase sensitive to nucleoside RT inhibitors but not to non-nucleoside inhibitors.
Highlights
LINE-1s (L1, Long Interspersed Element-1) are the most abundant autonomous non-LTR retrotransposons in the human genome and replicate by reverse transcription of an RNA intermediate
A full-length L1 element is about 6 kb in length and contains a 5’ untranslated region (UTR), two non-overlapping open reading frames (ORF1 and ORF2), followed by a short 3’ UTR that ends in a poly adenosine tail [7,8,9,10,11,12]
Several lines of evidence suggest that L1 transposes via a mechanism known as target primed reverse transcription (TPRT) [25], in which reverse transcription of L1 RNA is the crucial step
Summary
LINE-1s (L1, Long Interspersed Element-1) are the most abundant autonomous non-LTR retrotransposons in the human genome and replicate by reverse transcription of an RNA intermediate. Full-length L1 encodes two open reading frames (ORF1, ORF2) and ORF2 has reverse transcriptase activity. The product of ORF1 encodes a 40 kDa protein (ORF1p) with nucleic acid binding and chaperone activities [13,14,15,16]. ORF2 encodes a ~150 kDa multifunctional protein (ORF2p) with endonuclease (EN) [17], reverse transcriptase (RT) activities [18,19,20] and a cysteine-rich domain of unknown function [21]. Full-length human ORF2 protein expressed in baculovirus-infected insect cells has strong RNA-dependent and DNA-dependent DNA polymerase activities [19,20,25]. Active L1 RT or ORF2p had not been successfully expressed in prokaryotic hosts such as E. coli
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