Deciphering Fact from Artifact when Using Reporter Assays to Investigate the Roles of Host Factors on L1 Retrotransposition

Overview

Journal Mob DNA

Publisher Biomed Central

Specialty Genetics

Date 2016 Nov 30

PMID 27895722

Citations 2

Authors

Pamela R Cook

G Travis Tabor

Affiliations

Soon will be listed here.

Abstract

Background: The Long INterspersed Element-1 (L1, LINE-1) is the only autonomous mobile DNA element in humans and has generated as much as half of the genome. Due to increasing clinical interest in the roles of L1 in cancer, embryogenesis and neuronal development, it has become a priority to understand L1-host interactions and identify host factors required for its activity. Apropos to this, we recently reported that L1 retrotransposition in HeLa cells requires phosphorylation of the L1 protein ORF1p at motifs targeted by host cell proline-directed protein kinases (PDPKs), which include the family of mitogen-activated protein kinases (MAPKs). Using two engineered L1 reporter assays, we continued our investigation into the roles of MAPKs in L1 activity.

Results: We found that the MAPK p38δ phosphorylated ORF1p on three of its four PDPK motifs required for L1 activity. In addition, we found that a constitutively active p38δ mutant appeared to promote L1 retrotransposition in HeLa cells. However, despite the consistency of these findings with our earlier work, we identified some technical concerns regarding the experimental methodology. Specifically, we found that exogenous expression of p38δ appeared to affect at least one heterologous promoter in an engineered L1 reporter, as well as generate opposing effects on two different reporters. We also show that two commercially available non-targeting control (NTC) siRNAs elicit drastically different effects on the apparent retrotransposition reported by both L1 assays, which raises concerns about the use of NTCs as normalizing controls.

Conclusions: Engineered L1 reporter assays have been invaluable for determining the functions and critical residues of L1 open reading frames, as well as elucidating many aspects of L1 replication. However, our results suggest that caution is required when interpreting data obtained from L1 reporters used in conjunction with exogenous gene expression or siRNA.

Citing Articles

sRNA/L1 retrotransposition: using siRNAs and miRNAs to expand the applications of the cell culture-based LINE-1 retrotransposition assay.

Tristan-Ramos P, Morell S, Sanchez L, Toledo B, Garcia-Perez J, Heras S Philos Trans R Soc Lond B Biol Sci. 2020; 375(1795):20190346.

PMID: 32075559 PMC: 7061984. DOI: 10.1098/rstb.2019.0346.

Dynamic silencing of somatic L1 retrotransposon insertions reflects the developmental and cellular contexts of their genomic integration.

Kannan M, Li J, Fritz S, Husarek K, Sanford J, Sullivan T Mob DNA. 2017; 8:8.

PMID: 28491150 PMC: 5424313. DOI: 10.1186/s13100-017-0091-2.

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