A protein hydroxylase couples epithelial membrane biology to nucleolar ribosome biogenesis

Author:

Hendrix Eline,Andrijes Regina,Boora Uncaar,Kaur Arashpreet,Bundred James R,Officer-Jones Leah,Pennie Rachel,Powley Ian R,Zayer Adam,Heilig Raphael,Westrip Christian A E,Fletcher Sally C,Eaton Charlotte D,Kennedy Tristan J,Piasecka Sonia,Fischer Roman,Smerdon Stephen J,Le Quesne John,Coleman Mathew LORCID

Abstract

AbstractJumonji-C (JmjC) ribosomal protein hydroxylases are an ancient class of oxygen- and Fe(II)-dependent oxygenases that spawned the wider JmjC family and Histone Lysine Demethylases (KDMs) in eukaryotes. Myc-induced Antigen (MINA) has been implicated in ribosome biogenesis and was assigned as a nucleolar-localized JmjC histidyl hydroxylase of the large ribosomal subunit protein RPL27A, consistent with reports that it supports cell growth and viability in a variety of tumor cell types. Reported roles in diverse aspects of disease biology may be consistent with additional MINA functions, although the molecular mechanisms involved remain unclear. Here, we describe an extra-nucleolar interaction of MINA with the Hinge domain of the membrane-associated guanylate kinase, MPP6. We show that MINA promotes the expression and membrane localization of MPP6 and that the MINA-MPP6 pathway is required for epithelial tight junction integrity and barrier function. The function of MINA in this novel pathway is suppressed by ribosomal RNA transcription and the nucleolar MINA interactome. In this way, MINA couples epithelial membrane biology to nucleolar ribosome biogenesis. Our work sheds light on how quiescent cells lose adhesion as they switch to proliferative states associated with increased ribosome biogenesis.

Publisher

Cold Spring Harbor Laboratory

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