| کد مقاله | کد نشریه | سال انتشار | مقاله انگلیسی | نسخه تمام متن |
|---|---|---|---|---|
| 2035643 | 1072201 | 2013 | 15 صفحه PDF | دانلود رایگان |
• Isolated highly active LINE-1 ribonucleoprotein particle complexes from human cells
• 37 identified interactors comprise known and novel factors, notably UPF1 and PCNA
• L1 RNP is linked by a both protein-protein (PCNA) and protein-RNA (UPF1) interactions
• PCNA binds to ORF2p via a PIP box and is critical for retrotransposition
SummaryLINE-1s are active human DNA parasites that are agents of genome dynamics in evolution and disease. These streamlined elements require host factors to complete their life cycles, whereas hosts have developed mechanisms to combat retrotransposition’s mutagenic effects. As such, endogenous L1 expression levels are extremely low, creating a roadblock for detailed interactomic analyses. Here, we describe a system to express and purify highly active L1 RNP complexes from human suspension cell culture and characterize the copurified proteome, identifying 37 high-confidence candidate interactors. These data sets include known interactors PABPC1 and MOV10 and, with in-cell imaging studies, suggest existence of at least three types of compositionally and functionally distinct L1 RNPs. Among the findings, UPF1, a key nonsense-mediated decay factor, and PCNA, the polymerase-delta-associated sliding DNA clamp, were identified and validated. PCNA interacts with ORF2p via a PIP box motif; mechanistic studies suggest that this occurs during or immediately after target-primed reverse transcription.
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Journal: - Volume 155, Issue 5, 21 November 2013, Pages 1034–1048