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RNA polymerase I stability couples cellular growth to metal availability

Abstract:

Zinc is an essential cofactor of all major eukaryotic RNA polymerases. How the activity of these enzymes is coordinated or regulated according to cellular zinc levels is largely unknown. Here we show that the stability of RNA polymerase I (RNAPI) is tightly coupled to zinc availability invivo. In zinc deficiency, RNAPI is specifically degraded by proteolysis in the vacuole ina pathway dependent on the exportin Xpo1p anddeubiquitination of the RNAPI large subunit Rpa190p by Ubp2p and Ubp4p. RNAPII is unaffected, which allows for the expression of genes required in zinc deficiency. RNAPI export to the vacuole is required for survival during zinc starvation, suggesting that degradation of zinc-binding subunits might provide a last resort zinc reservoir. These results reveal a hierarchy of cellular transcriptional activities during zinc starvation and show that degradation of the most active cellular transcriptional machinery couples cellular growth and proliferation to zinc availability. © 2013 Elsevier Inc.

Año de publicación:

2013

Keywords:

    Fuente:

    googlegoogle
    scopusscopus

    Tipo de documento:

    Article

    Estado:

    Acceso abierto

    Áreas de conocimiento:

    • Biología molecular
    • Biología

    Áreas temáticas:

    • Microorganismos, hongos y algas
    • Bioquímica
    • Fisiología y materias afines

    Contribuidores:

    Fernando A. Gonzales-ZubiateFernando A. Gonzales-Zubiate
    Lee Y.J.Lee Y.J.
    Vashisht A.A.Vashisht A.A.
    Grzechnik A.Grzechnik A.
    Lee C.Y.Lee C.Y.
    Chanfreau G.F.Chanfreau G.F.
    Lee A.Lee A.
    Wohlschlegel J.Wohlschlegel J.