Interplay of EXO70 and MLO proteins modulates trichome cell wall composition and powdery mildew susceptibility

生物 外囊肿 细胞生物学 毛状体 白粉病 突变体 细胞壁 胞吐 分泌物 生物化学 植物 基因
作者
Jan W. Huebbers,George A. Caldarescu,Zdeňka Kubátová,Peter Sabol,Sophie Levecque,Harald Kühn,Ivan Kulich,Anja Reinstädler,Kim Büttgen,Alba Manga‐Robles,Hugo Mélida,Markus Pauly,Ralph Panstruga,Viktor Žárský
标识
DOI:10.1101/2022.12.30.521597
摘要

Abstract EXO70 proteins are essential constituents of the octameric exocyst complex implicated in vesicle tethering during exocytosis, while MLO proteins are plant-specific calcium channels of which some isoforms play a key role during fungal powdery mildew pathogenesis. We here detected by a variety of histochemical staining procedures an unexpected phenotypic overlap of A. thaliana exo70H4 and mlo2 mlo6 mlo12 triple mutant plants regarding the biogenesis of leaf trichome secondary cell walls. Biochemical and Fourier transform infrared spectroscopic analyses of isolated trichomes corroborated deficiencies in the composition of trichome cell walls in exo70H4 and mlo2 mlo6 mlo12 mutants. Transgenic lines expressing fluorophore- tagged EXO70H4 and MLO variants exhibited extensive co-localization of these proteins at the trichome plasma membrane and cell wall. Furthermore, mCherry- EXO70H4 mislocalized in trichomes of the mlo triple mutant and, vice versa , MLO6- GFP exhibited aberrant subcellular localization in trichomes of the exo70H4 mutant. Transgenic expression of GFP-marked PMR4 callose synthase, a previously identified cargo of EXO70H4 dependent exocytosis, revealed reduced cell wall delivery of GFP- PMR4 in mlo triple mutant plants. In vivo protein-protein interaction assays uncovered isoform-preferential physical interaction between EXO70 and MLO proteins. Finally, exo70H4 and mlo mutants, when combined, showed synergistically enhanced resistance to powdery mildew attack. Taken together, our data point to an isoform- specific interplay of EXO70 and MLO proteins in the modulation of trichome cell wall biogenesis and powdery mildew susceptibility, possibly by (co-)regulating focal secretion of cell wall-related cargo.
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