Variable patterns of retrotransposition in different HeLa strains provide mechanistic insights into SINE RNA mobilization processes

Author:

Moldovan John B1ORCID,Kopera Huira C1,Liu Ying1,Garcia-Canadas Marta2,Catalina Purificacion3,Leone Paola E4,Sanchez Laura2,Kitzman Jacob O15,Kidd Jeffrey M15,Garcia-Perez Jose Luis2,Moran John V16ORCID

Affiliation:

1. Department of Human Genetics, University of Michigan , Ann Arbor, MI 48109, USA

2. Department of Genomic Medicine, GENYO, Centre for Genomics and Oncological Research, Pfizer-University of Granada-Andalusian Regional Government , PTS Granada 18016 , Spain

3. Andalusian Public Health System Biobank , Granada 18016 , Spain

4. Genetics and Genomics Laboratory, SOLCA Hospital , Quito , Ecuador

5. Department of Computational Medicine and Bioinformatics, University of Michigan , Ann Arbor, MI 48109, USA

6. Department of Internal Medicine, University of Michigan , Ann Arbor , MI  48109 , USA

Abstract

Abstract Alu elements are non-autonomous Short INterspersed Elements (SINEs) derived from the 7SL RNA gene that are present at over one million copies in human genomic DNA. Alu mobilizes by a mechanism known as retrotransposition, which requires the Long INterspersed Element-1 (LINE-1) ORF2-encoded protein (ORF2p). Here, we demonstrate that HeLa strains differ in their capacity to support Alu retrotransposition. Human Alu elements retrotranspose efficiently in HeLa-HA and HeLa-CCL2 (Alu-permissive) strains, but not in HeLa-JVM or HeLa-H1 (Alu-nonpermissive) strains. A similar pattern of retrotransposition was observed for other 7SL RNA-derived SINEs and tRNA-derived SINEs. In contrast, mammalian LINE-1s, a zebrafish LINE, a human SINE-VNTR-Alu (SVA) element, and an L1 ORF1-containing mRNA can retrotranspose in all four HeLa strains. Using an in vitro reverse transcriptase-based assay, we show that Alu RNAs associate with ORF2p and are converted into cDNAs in both Alu-permissive and Alu-nonpermissive HeLa strains, suggesting that 7SL- and tRNA-derived SINEs use strategies to ‘hijack′ L1 ORF2p that are distinct from those used by SVA elements and ORF1-containing mRNAs. These data further suggest ORF2p associates with the Alu RNA poly(A) tract in both Alu-permissive and Alu-nonpermissive HeLa strains, but that Alu retrotransposition is blocked after this critical step in Alu-nonpermissive HeLa strains.

Funder

National Institutes of Health

University of Michigan Rogel Cancer Center First and Goal Award

European Research Council

Government of Spain

Andalusian regional Government

Ms. Francisca Serrano

Publisher

Oxford University Press (OUP)

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