Published April 7, 2021 | Version v1
Publication Metadata-only

Self-acetylation at the active site of phosphoenolpyruvate carboxykinase (PCK1) controls enzyme activity

Latorre Muro, Pedro
Baeza, Josue
Hurtado Guerrero, Ramón
Hicks, Thomas
Delso, Ignacio
Hernández Ruiz, Cristina
Velázquez Campoy, Adrián
Lawton, Alexis J.
Angulo Álvarez, Jesús
Denu, John M.
Carrodeguas, José Alberto
Other:
Universidad de Sevilla. Departamento de Química orgánica

Description

Acetylation is known to regulate the activity of cytosolic phosphoenolpyruvate carboxykinase (PCK1), a key enzyme in gluconeogenesis, by promoting the reverse reaction of the enzyme (converting phosphoenolpyruvate to oxaloacetate). It is also known that the histone acetyltransferase p300 can induce PCK1 acetylation in cells, but whether that is a direct or indirect function was not known. Here we initially set out to determine whether p300 can acetylate directly PCK1 in vitro. We report that p300 weakly acetylates PCK1, but surprisingly, using several techniques including protein crystallization, mass spectrometry, isothermal titration calorimetry, saturationtransfer difference nuclear magnetic resonance and molecular docking, we found that PCK1 is also able to acetylate itself using acetyl-CoA independently of p300. This reaction yielded an acetylated recombinant PCK1 with a 3-fold decrease in kcat without changes in Km for all substrates. Acetylation stoichiometry was determined for 14 residues, including residues lining the active site. Structural and kinetic analyses determined that site-directed acetylation of K244, located inside the active site, altered this site and rendered the enzyme inactive. In addition, we found that acetyl-CoA binding to the active site is specific and metal dependent. Our findings provide direct evidence for acetyl-CoA binding and chemical reaction with the active site of PCK1 and suggest a newly discovered regulatory mechanism of PCK1 during metabolic stress.

Abstract

Ministerio de Economía, Industria y Competitividad AGL2015-66177

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Universidad de Zaragoza UZ-2015-BIO-01

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Ministerio de Ciencia, Innovación y Universidades CTQ2013-44367-C2-2-P, BFU2016-75633-P, BFU2016-78232-P, PID2019-109395GB-100

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Gobierno de Aragón E34-R17, LMP58-18, E45-17R

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European Union BioStruct-X N283570, BIOSTRUCTX-5186

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Biotechnology and biological Sciences Research Council BB/P010660/1

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National Institutes of Health GM065386

Additional details

Identifiers Origin repository
Created:
December 4, 2022
Modified:
November 28, 2023