To infect its host plant maize, the fungal parasite Ustilago maydis uses a complex of seven proteins. Numerous findings reveal an essential role of the complex in causing disease and suggest a widespread occurence in fungal plant pathogens.
Each year, fungal plant pathogens such as rusts, rice blast and mildews destroy huge amounts of cereal crops that could feed millions of people. Many of these fungi are biotrophic pathogens: Instead of killing their host plants, they manipulate host cells to assure that these sustain fungal growth. Among these pathogens, the corn smut fungus Ustilago maydis has emerged as a model for basic research on biotrophic fungi.
During the infection, U. maydis releases an entire cocktail of so-called effectors which function either in the interaction zone between fungus and host or are delivered to plant cells. Effector proteins suppress plant immunity, alter plant biosynthesis pathways and re-initiate cell division in leaf tissue, leading to prominent tumor-like structures from which the fungus spreads its spores. At present, the mechanism how effectors of plant-pathogenic fungi end up in plant cells remains a mystery.
Over many years, researchers around Regine Kahmann at the Max Planck Institute for Terrestrial Microbiology have worked on elucidating the molecular function of effectors. In the present study they have identified five fungal effectors plus two transmembrane proteins, which form a stable protein complex. If only one of these seven proteins is missing, the infection process stops entirely. Such a strong contribution to virulence is highly unusual for effectors which individually usually have only a modest contribution to virulence. Mutants lacking complex members fail to downregulate host immunity, suggesting an involvement of the complex in effector delivery. Localization experiments in part conducted with collaboration partners in the US and at the Philipps-Universität in Marburg revealed that complex proteins reside in structures extending from the fungus into host cells.