Origin of the human L1 elements: Proposed progenitor genes deduced from a consensus DNA sequence

Scott, Alan F.; Schmeckpeper, Barbara J.; Abdelrazik, Mona; Comey, Catherine T.; O’Hara, Bruce F.; Rossiter, Judith Pratt; Cooley, Tim; Heath, P. J.; Smith, Kirby D.; Margolet, Louise

doi:10.1016/0888-7543(87)90003-6

Cited by 304 publications

(221 citation statements)

References 67 publications

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“…Only a very small fraction of these repetitive sequences are still able to actively transpose. Full length L1 elements are about 6kb long and encode the proteins necessary for autonomous retrotransposition (Scott et al 1987). Alu elements are much smaller, 300-350bp long, and lack any protein-coding capacity.…”

Section: Introductionmentioning

confidence: 99%

De novo Alu element insertions targeted to a sequence common to the BRCA1 and BRCA2 genes

et al. 2005

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Linkage analysis suggests that mutations in the BRCA1 and BRCA2 genes are responsible for cancer predisposition in more than 80% of the families with high incidence of breast/ovarian cancer. However, pathogenic mutations in the BRCA1/2 genes are generally identified in much less than half of the families investigated in a diagnostic setting with the currently used PCR-based screening protocols. Here we report the identification of two different de novo Alu element insertions within the BRCA1/2 coding sequences in three out of the 50 families in which we found a cancer predisposing mutation, suggesting that this type of mutation is much more common than suggested by their occurrence in mutation databases. The Alu insertion in the BRCA2 gene resulted in the removal of the targeted exon from the corresponding mRNA molecule. Unexpectedly the Target Site Duplications generated by both Alu element insertions contained a specific 9 bp long segment, which might eventually serve as a recognition site for the transposition machinery. Finally, in contrast to the disease causing Alu insertions reported to date, the transposon identified in the BRCA1 gene does not belong to a "young" AluY but to an AluS subfamily, indicating that some of these "old" Alu elements, which are supposed to be non-functional fossil relics, are still able to retrotranspose in vivo.

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Section: Introductionmentioning

confidence: 99%

De novo Alu element insertions targeted to a sequence common to the BRCA1 and BRCA2 genes

et al. 2005

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“…L1 contains two open reading frames (ORF1 and ORF2) that are translated from a single bicistronic transcript (Scott et al, 1987), though various splice products diversify the potential mechanisms of translation (Perepelitsa-Belancio and Deininger 2003;Belancio et al, 2006). Both proteins are necessary for L1 retrotransposition.…”

Section: Introductionmentioning

confidence: 99%

LINE-1 ORF1 protein enhances Alu SINE retrotransposition

Wallace

Wagstaff

Deininger

et al. 2008

Gene

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Retroelements have contributed over one third of the human genome mass. The currently active LINE-1 (L1) codes for two proteins (ORF1p and ORF2p), both strictly required for retrotransposition. In contrast, the non-coding parasitic SINE (Alu) only appears to need the L1 ORF2p for its own amplification. This requirement was previously determined using a tissue culture assay system in human cells (HeLa). Because HeLa are likely to express functional L1 proteins, it is possible that low levels of endogenous ORF1p are necessary for the observed tagged Alu mobilization. By individually expressing ORF1 and ORF2 proteins from both human (L1 RP and LRE3) and rodent (L1 A102 and L1 spa ) L1 sources, we demonstrate that increasing amounts of ORF1 expressing vector enhances tagged Alu mobilization in HeLa cells. In addition, using chicken fibroblast cells as an alternate cell culture source, we confirmed that ORF1p is not strictly required for Alu mobilization in our assay. Supporting our observations in HeLa cells, we find that tagged Alu retrotransposition is improved by supplementation of ORF1p in the cultured chicken cells. We postulate that L1 ORF1p plays either a direct or indirect role in enhancing the interaction between the Alu RNA and the required factors needed for its retrotransposition.

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“…Although most L1s are immobile, it is estimated that the average human genome contains approximately 60-100 retrotransposition-competent L1s (RC-L1s) and their mobility can cause human disease (Sassaman et al, 1997, Brouha et al, 2003, Hulme et al, 2006, Kazazian et al, 1988. RC-L1s are composed of a 5' UTR that harbors an internal promoter, two non-overlapping open reading frames (ORF1 and ORF2), and a 3' UTR that ends in a poly (A) tail (Swergold, 1990, Scott et al, 1987, Dombroski et al, 1991, Minakami et al, 1992. The ORF2 encoded protein (ORF2p) contains both endonuclease and reverse transcriptase activities, which are required for retrotransposition , Feng et al, 1996.…”

Section: Introductionmentioning

confidence: 99%

Selective inhibition of Alu retrotransposition by APOBEC3G

Hulme

Bogerd

Cullen

et al. 2007

Gene

142

159

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The non-LTR retrotransposon LINE-1 (L1) comprises ~17% of the human genome, and the L1-encoded proteins can function in trans to mediate the retrotransposition of non-autonomous retrotransposons (i.e., Alu and probably SVA elements) and cellular mRNAs to generate processed pseudogenes. Here, we have examined the effect of APOBEC3G and APOBEC3F, cytidine deaminases that inhibit Vif-deficient HIV-1 replication, on Alu retrotransposition and other L1-mediated retrotransposition processes. We demonstrate that APOBEC3G selectively inhibits Alu retrotransposition in an ORF1p-independent manner. An active cytidine deaminase site is not required for inhibition of Alu retrotransposition and the resultant integration events lack G to A or C to T hypermutation. These data demonstrate a differential restriction of L1 and Alu retrotransposition by APOBEC3G, and suggest that the Alu ribonucleoprotein complex may be targeted by APOBEC3G.

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Origin of the human L1 elements: Proposed progenitor genes deduced from a consensus DNA sequence

Cited by 304 publications

References 67 publications

De novo Alu element insertions targeted to a sequence common to the BRCA1 and BRCA2 genes

De novo Alu element insertions targeted to a sequence common to the BRCA1 and BRCA2 genes

LINE-1 ORF1 protein enhances Alu SINE retrotransposition

Selective inhibition of Alu retrotransposition by APOBEC3G

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