MAP65-3 Microtubule-Associated Protein Is Essential for Nematode-Induced Giant Cell Ontogenesis inArabidopsis

Author:

Caillaud Marie-Cécile123,Lecomte Philippe123,Jammes Fabien123,Quentin Michaël123,Pagnotta Sophie4,Andrio Emilie123,de Almeida Engler Janice123,Marfaing Nicolas123,Gounon Pierre4,Abad Pierre123,Favery Bruno123

Affiliation:

1. Institut National de la Recherche Agronomique, Unité Mixte de Recherche 1301 Interactions Biotiques et Santé Végétale, F-06903 Sophia Antipolis, France

2. Centre National de la Recherche Agronomique, Unité Mixte de Recherche 6243 Interactions Biotiques et Santé Végétale, F-06903 Sophia Antipolis, France

3. Université de Nice-Sophia Antipolis, Unité Mixte de Recherche Interactions Biotiques et Santé Végétale, F-06903 Sophia Antipolis, France

4. Université de Nice-Sophia Antipolis, Centre Commun de Microscopie Appliquée, F-06108 Nice, France

Abstract

AbstractThe infection of plants by obligate parasitic nematodes constitutes an interesting model for investigating plant cytoskeleton functions. Root knot nematodes have evolved the ability to manipulate host functions to their own advantage by redifferentiating root cells into multinucleate and hypertrophied feeding cells. These giant cells result from repeated rounds of karyokinesis without cell division. Detailed functional analyses demonstrated that Arabidopsis thaliana  Microtubule-Associated Protein65-3 (MAP65-3) was essential for giant cell ontogenesis and that cytokinesis was initiated but not completed in giant cells. In developing giant cells, MAP65-3 was associated with a novel kind of cell plate—the giant cell mini cell plate—that separates daughter nuclei. In the absence of functional MAP65-3, giant cells developed but failed to fully differentiate and were eventually destroyed. These defects in giant cells impaired the maturation of nematode larvae. Thus, MAP65-3 is essential for giant cell development during root knot nematode infection. Subcellular localization of MAP65-3 and analysis of microtubule organization in the dyc283 T-DNA map65-3 mutant demonstrated that MAP65-3 played a critical role in organizing the mitotic microtubule array during both early and late mitosis in all plant organs. Here, we propose a model for the role of MAP65-3 in giant cell ontogenesis.

Publisher

Oxford University Press (OUP)

Subject

Cell Biology,Plant Science

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