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Risler JK, et al.  (2012) Host co-factors of the retrovirus-like transposon Ty1. Mob DNA 3(1):12

Abstract: ABSTRACT: BACKGROUND: Long-terminal repeat (LTR) retrotransposons have complex modes of mobility involving reverse transcription of their RNA genomes in cytoplasmic virus-like particles (VLPs) and integration of the cDNA copies into the host genome. The limited coding capacity of retrotransposons necessitates an extensive reliance on host co-factors; however, it has been challenging to identify co-factors that are required for endogenous retrotransposon mobility because retrotransposition is such a rare event. RESULTS: To circumvent the low frequency of Ty1 LTR-retrotransposon mobility in Saccharomyces cerevisiae, we used modified synthetic genetic array (SGA) analysis to isolate host mutations that reduce retrotransposition. Query strains that harbor a chromosomal Ty1his3AI reporter element and either the rtt101[del] or med1[del] mutation, both of which confer a hypertransposition phenotype, were mated to 4,847 haploid ORF deletion strains. Retrotransposition was measured in the double mutant progeny, and a set of 275 ORF deletions that suppress the hypertransposition phenotypes of both rtt101[del] and med1[del] were identified. The corresponding set of 275 retrotransposition host factors (RHFs) includes 45 previously identified Ty1 or Ty3 co-factors. More than half of the RHF genes have statistically robust human homologs (E <1 x 10-10). The level of unintegrated Ty1 cDNA in 181 rhf[del] single mutants was altered <2-fold, suggesting that the corresponding co-factors stimulate retrotransposition at a step after cDNA synthesis. However, deletion of 43 RHF genes, including specific ribosomal protein and ribosome biogenesis genes and RNA degradation, modification and transport genes resulted in low Ty1 cDNA levels. The level of Ty1 Gag but not RNA was reduced in ribosome biogenesis mutants bud21[del], hcr1[del], loc1[del] and puf6[del]. CONCLUSION: Ty1 retrotransposition is dependent on multiple co-factors acting at different steps in the replication cycle. Human orthologs of these RHFs are potential, or in a few cases, presumptive HIV-1 co-factors in human cells. RHF genes whose absence results in decreased Ty1 cDNA include characterized RNA metabolism and modification genes, consistent with their having roles in early steps in retrotransposition such as expression, nuclear export, translation, localization or packaging of Ty1 RNA. Our results suggest that Bud21, Hcr1, Loc1 and Puf6 promote efficient synthesis or stability of Ty1 Gag.FAU - Risler, Jenni.

Status: Epub ahead of print Type: Journal Article PubMed ID: 22856544

Topics addressed in this paper

Number of different genes curated to this paper: 52

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Topics Topics not linked to Genes Genes linked to topics (#1 - 10 )
BUD21 BUD22 DBR1 DHH1 HCR1 HOS2 LOC1 MED1 MET13 MRP17
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Topics Genes linked to topics (#11 - 20 )
MRPL39 MRPL49 MRPL7 MRPL8 MRPS28 MRT4 NAM7 NMD2 PAT1 PUF6
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Topics Genes linked to topics (#21 - 30 )
RKM4 RPL16B RPL19A RPL27A RPL31A RPL33B RPL34A RPL37A RPL43A RPL7A
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Topics Genes linked to topics (#31 - 40 )
RPP1A RPS11A RPS19A RPS19B RPS25A RPS27B RPS30A RSA3 RTT101 SET3
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Topics Genes linked to topics (#41 - 50 )
SNF5 SNF6 SPT3 SPT8 SQS1 SWI3 TEC1 UPF3 UTP30 XRN1
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Topics Genes linked to topics (#51 - 52 )
YGR054W ZUO1
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