| Literature DB >> 29739839 |
Alessia Armezzani1, Ursula Abad1, Olivier Ali1,2, Amélie Andres Robin1, Laetitia Vachez1, Antoine Larrieu1, Ewa J Mellerowicz3, Ludivine Taconnat4,5, Virginie Battu1, Thomas Stanislas1, Mengying Liu1, Teva Vernoux1, Jan Traas6, Massimiliano Sassi1.
Abstract
The shoot apical meristem of higher plants continuously generates new tissues and organs through complex changes in growth rates and directions of its individual cells. Cell growth, which is driven by turgor pressure, largely depends on the cell walls, which allow cell expansion through synthesis and structural changes. A previous study revealed a major contribution of wall isotropy in organ emergence, through the disorganization of cortical microtubules. We show here that this disorganization is coupled with the transcriptional control of genes involved in wall remodelling. Some of these genes are induced when microtubules are disorganized and cells shift to isotropic growth. Mechanical modelling shows that this coupling has the potential to compensate for reduced cell expansion rates induced by the shift to isotropic growth. Reciprocally, cell wall loosening induced by different treatments or altered cell wall composition promotes a disruption of microtubule alignment. Our data thus indicate the existence of a regulatory module activated during organ outgrowth, linking microtubule arrangements to cell wall remodelling.Entities:
Keywords: Auxin; Cell wall; Microtubules; Morphogenesis; Shoot apical meristem
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Year: 2018 PMID: 29739839 DOI: 10.1242/dev.162255
Source DB: PubMed Journal: Development ISSN: 0950-1991 Impact factor: 6.868