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Letters to Nature
Nature 432, 235-240 (11 November 2004) | doi:10.1038/nature03120; Received 14 June 2004; Accepted 19 October 2004; Published online 7 November 2004
The Microprocessor complex mediates the genesis of microRNAs
Richard I. Gregory1,2, Kai-ping Yan1,2, Govindasamy Amuthan1, Thimmaiah Chendrimada1, Behzad Doratotaj1, Neil Cooch1 & Ramin Shiekhattar1
- The Wistar Institute, 3601 Spruce Street, Philadelphia, Pennsylvania 19104, USA
- These authors contributed equally to this work
Correspondence to: Ramin Shiekhattar1 Email: shiekhattar@wistar.upenn.edu
Abstract
MicroRNAs (miRNAs) are a growing family of small non-protein-coding regulatory genes that regulate the expression of homologous target-gene transcripts. They have been implicated in the control of cell death and proliferation in flies1, 2, haematopoietic lineage differentiation in mammals3, neuronal patterning in nematodes4 and leaf and flower development in plants5, 6, 7, 8. miRNAs are processed by the RNA-mediated interference machinery. Drosha is an RNase III enzyme that was recently implicated in miRNA processing. Here we show that human Drosha is a component of two multi-protein complexes. The larger complex contains multiple classes of RNA-associated proteins including RNA helicases, proteins that bind double-stranded RNA, novel heterogeneous nuclear ribonucleoproteins and the Ewing's sarcoma family of proteins. The smaller complex is composed of Drosha and the double-stranded-RNA-binding protein, DGCR8, the product of a gene deleted in DiGeorge syndrome. In vivo knock-down and in vitro reconstitution studies revealed that both components of this smaller complex, termed Microprocessor, are necessary and sufficient in mediating the genesis of miRNAs from the primary miRNA transcript.
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