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Article
Nature 445, 501-505 (1 February 2007) | doi:10.1038/nature05467; Received 17 October 2006; Accepted 21 November 2006; Published online 20 December 2006
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Termination of asymmetric cell division and differentiation of stomata
Lynn Jo Pillitteri1, Daniel B. Sloan1, Naomi L. Bogenschutz1 & Keiko U. Torii1,2,3
- Department of Biology and,
- Institute for Stem Cell and Regenerative Medicine, University of Washington, Seattle, Washington 98195, USA
- CREST, Japan Science and Technology Agency, Saitama, 332-0012, Japan
Correspondence to: Correspondence and requests for materials should be addressed to K.U.T. (Email: ktorii@u.washington.edu).
Abstract
Stomata consist of a pair of guard cells that mediate gas and water-vapour exchange between plants and the atmosphere. Stomatal precursor cells—meristemoids—possess a transient stem-cell-like property and undergo several rounds of asymmetric divisions before further differentiation. Here we report that the Arabidopsis thaliana basic helix–loop–helix (bHLH) protein MUTE is a key switch for meristemoid fate transition. In the absence of MUTE, meristemoids abort after excessive asymmetric divisions and fail to differentiate stomata. Constitutive overexpression of MUTE directs the entire epidermis to adopt guard cell identity. MUTE has two paralogues: FAMA, a regulator of guard cell morphogenesis, and SPEECHLESS (SPCH). We show that SPCH directs the first asymmetric division that initiates stomatal lineage. Together, SPCH, MUTE and FAMA bHLH proteins control stomatal development at three consecutive steps: initiation, meristemoid differentiation and guard cell morphogenesis. Our findings highlight the roles of closely related bHLHs in cell type differentiation in plants and animals.
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RESEARCH
Transcription factor control of asymmetric cell divisions that establish the stomatal lineageNature Letters to Editor (01 Feb 2007)
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