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A single regulator NrtR controls bacterial NAD+ homeostasis via its acetylation.


ABSTRACT: Nicotinamide adenine dinucleotide (NAD+) is an indispensable cofactor in all domains of life, and its homeostasis must be regulated tightly. Here we report that a Nudix-related transcriptional factor, designated MsNrtR (MSMEG_3198), controls the de novo pathway of NAD+biosynthesis in M. smegmatis, a non-tuberculosis Mycobacterium. The integrated evidence in vitro and in vivo confirms that MsNrtR is an auto-repressor, which negatively controls the de novo NAD+biosynthetic pathway. Binding of MsNrtR cognate DNA is finely mapped, and can be disrupted by an ADP-ribose intermediate. Unexpectedly, we discover that the acetylation of MsNrtR at Lysine 134 participates in the homeostasis of intra-cellular NAD+ level in M. smegmatis. Furthermore, we demonstrate that NrtR acetylation proceeds via the non-enzymatic acetyl-phosphate (AcP) route rather than by the enzymatic Pat/CobB pathway. In addition, the acetylation also occurs on the paralogs of NrtR in the Gram-positive bacterium Streptococcus and the Gram-negative bacterium Vibrio, suggesting that these proteins have a common mechanism of post-translational modification in the context of NAD+ homeostasis. Together, these findings provide a first paradigm for the recruitment of acetylated NrtR to regulate bacterial central NAD+ metabolism.

SUBMITTER: Gao R 

PROVIDER: S-EPMC6800001 | biostudies-literature | 2019 Oct

REPOSITORIES: biostudies-literature

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A single regulator NrtR controls bacterial NAD<sup>+</sup> homeostasis via its acetylation.

Gao Rongsui R   Wei Wenhui W   Hassan Bachar H BH   Li Jun J   Deng Jiaoyu J   Feng Youjun Y  

eLife 20191009


Nicotinamide adenine dinucleotide (NAD<sup>+</sup>) is an indispensable cofactor in all domains of life, and its homeostasis must be regulated tightly. Here we report that a Nudix-related transcriptional factor, designated MsNrtR (MSMEG_3198), controls the <i>de novo</i> pathway of NAD<sup>+</sup>biosynthesis in <i>M. smegmatis</i>, a non-tuberculosis <i>Mycobacterium</i>. The integrated evidence <i>in vitro</i> and <i>in vivo</i> confirms that MsNrtR is an auto-repressor, which negatively contr  ...[more]

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