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Differential repression of alternative transcripts: A screen for miRNA targets
被引:53
作者:
Legendre, Matthieu
[1
]
Ritchie, William
[1
]
Lopez, Fabrice
[1
]
Gautheret, Daniel
[1
]
机构:
[1] Univ Mediterranee, INSERM, ERM 206, Marseille, France
关键词:
D O I:
10.1371/journal.pcbi.0020043
中图分类号:
Q5 [生物化学];
学科分类号:
071010 ;
081704 ;
摘要:
Alternative polyadenylation sites produce transcript isoforms with 39 untranslated regions ( UTRs) of different lengths. If a microRNA ( miRNA) target is present in the UTR, then only those target- containing isoforms should be sensitive to control by a cognate miRNA. We carried out a systematic examination of 39 UTRs containing multiple poly( A) sites and putative miRNA targets. Based on expressed sequence tag ( EST) counts and EST library information, we observed that levels of isoforms containing targets for miR-1 or miR- 124, two miRNAs causing downregulation of transcript levels, were reduced in tissues expressing the corresponding miRNA. This analysis was repeated for all conserved 7- mers in 39 UTRs, resulting in a selection of 312 motifs. We show that this set is significantly enriched in known miRNA targets and mRNA- destabilizing elements, which validates our initial hypothesis. We scanned the human genome for possible cognate miRNAs and identified phylogenetically conserved precursors matching our motifs. This analysis can help identify target- miRNA couples that went undetected in previous screens, but it may also reveal targets for other types of regulatory factors.
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页码:333 / 342
页数:10
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