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First published online September 21, 2007; 10.1105/tpc.107.054528

The Plant Cell 19:2736-2748 (2007)
© 2007 American Society of Plant Biologists

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The GIGANTEA-Regulated MicroRNA172 Mediates Photoperiodic Flowering Independent of CONSTANS in Arabidopsis[W],[OA]

Jae-Hoon Junga, Yeon-Hee Seoa, Pil Joon Seoa, Jose Luis Reyesb, Ju Yuna, Nam-Hai Chuab and Chung-Mo Parka,1

a Molecular Signaling Laboratory, Department of Chemistry, Seoul National University, Seoul 151-742, Korea
b Laboratory of Plant Molecular Biology, The Rockefeller University, New York, New York 10021-3699

1 Address correspondence to cmpark{at}snu.ac.kr.

Regulated RNA metabolism appears to be a critical component of molecular mechanisms directing flowering initiation in plants. A group of RNA binding proteins exerts their roles through the autonomous flowering pathway. Posttranscriptional mechanisms regulated by microRNAs (miRNAs) also play a key role in flowering-time control. Here, we demonstrate that the GIGANTEA (GI)-regulated miR172 defines a unique genetic pathway that regulates photoperiodic flowering by inducing FLOWERING LOCUS T (FT) independent of CONSTANS (CO). A late-flowering mutant in which a miR172 target gene, TARGET OF EAT1, is constitutively activated by the nearby insertion of the cauliflower mosaic virus 35S enhancer normally responded to vernalization and gibberellic acid treatments. By contrast, its response to daylength changes was severely disrupted. In the mutant, FT was significantly repressed, but other flowering genes were unaffected. Notably, miR172 abundance is regulated by photoperiod via GI-mediated miRNA processing. Accordingly, miR172-overproducing plants exhibit early flowering under both long days and short days, even in the absence of functional CO, indicating that miR172 promotes photoperiodic flowering through a CO-independent genetic pathway. Therefore, it appears that GI-mediated photoperiodic flowering is governed by the coordinated interaction of two distinct genetic pathways: one mediated via CO and the other mediated via miR172 and its targets.




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