Polyphosphate and tyrosine phosphorylation in the N-terminal domain of the human mitochondrial Lon protease disrupts its functions

Author:

Kunová Nina,Ondrovičová Gabriela,Bauer Jacob A.,Krajčovičová Veronika,Pinkas Matyáš,Stojkovičová Barbora,Havalová Henrieta,Lukáčová Veronika,Kohútová Lenka,Košťan Július,Martináková Lucia,Baráth Peter,Nováček Jiří,Zoll Sebastian,Kereϊche Sami,Kutejová Eva,Pevala Vladimír

Abstract

AbstractPhosphorylation plays a crucial role in the regulation of many fundamental cellular processes. Phosphorylation levels are increased in many cancer cells where they may promote changes in mitochondrial homeostasis. Proteomic studies on various types of cancer identified 17 phosphorylation sites within the human ATP-dependent protease Lon, which degrades misfolded, unassembled and oxidatively damaged proteins in mitochondria. Most of these sites were found in Lon’s N-terminal (NTD) and ATPase domains, though little is known about the effects on their function. By combining the biochemical and cryo-electron microscopy studies, we show the effect of Tyr186 and Tyr394 phosphorylations in Lon’s NTD, which greatly reduce all Lon activities without affecting its ability to bind substrates or perturbing its tertiary structure. A substantial reduction in Lon’s activities is also observed in the presence of polyphosphate, whose amount significantly increases in cancer cells. Our study thus provides an insight into the possible fine-tuning of Lon activities in human diseases, which highlights Lon’s importance in maintaining proteostasis in mitochondria.

Funder

Grantová Agentura České Republiky

Interreg

European Regional Development Fund, European Union

European Regional Development Fund

Agentúra na Podporu Výskumu a Vývoja

Vedecká Grantová Agentúra MŠVVaŠ SR a SAV

Publisher

Springer Science and Business Media LLC

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