YqfB protein from Escherichia coli: an atypical amidohydrolase active towards N4-acylcytosine derivatives

Author:

Stanislauskienė RūtaORCID,Laurynėnas Audrius,Rutkienė Rasa,Aučynaitė Agota,Tauraitė Daiva,Meškienė Rita,Urbelienė Nina,Kaupinis Algirdas,Valius MindaugasORCID,Kaliniene Laura,Meškys RolandasORCID

Abstract

AbstractHuman activating signal cointegrator homology (ASCH) domain-containing proteins are widespread and diverse but, at present, the vast majority of those proteins have no function assigned to them. This study demonstrates that the 103-amino acid Escherichia coli protein YqfB, previously identified as hypothetical, is a unique ASCH domain-containing amidohydrolase responsible for the catabolism of N4-acetylcytidine (ac4C). YqfB has several interesting and unique features: i) it is the smallest monomeric amidohydrolase described to date, ii) it is active towards structurally different N4-acylated cytosines/cytidines, and iii) it has a high specificity for these substrates (kcat/Km up to 2.8 × 106 M−1 s−1). Moreover, our results suggest that YqfB contains a unique Thr-Lys-Glu catalytic triad, and Arg acting as an oxyanion hole. The mutant lacking the yqfB gene retains the ability to grow, albeit poorly, on N4-acetylcytosine as a source of uracil, suggesting that an alternative route for the utilization of this compound exists in E. coli. Overall, YqfB ability to hydrolyse various N4-acylated cytosines and cytidines not only sheds light on the long-standing mystery of how ac4C is catabolized in bacteria, but also expands our knowledge of the structural diversity within the active sites of amidohydrolases.

Publisher

Springer Science and Business Media LLC

Subject

Multidisciplinary

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