Anaerobic Transcription by OxyR: A Novel Paradigm for Nitrosative Stress

Overview

Journal Antioxid Redox Signal

Specialty Endocrinology

Date 2019 Nov 7

PMID 31691575

Citations 5

Authors

Divya Seth

Alfred Hausladen

Jonathan S Stamler

Affiliations

Soon will be listed here.

Abstract

S-nitrosylation, the post-translational modification by nitric oxide (NO) to form S-nitrosothiols (SNOs), regulates diverse aspects of cellular function, and aberrant S-nitrosylation (nitrosative stress) is implicated in disease, from neurodegeneration to cancer. Essential roles for S-nitrosylation have been demonstrated in microbes, plants, and animals; notably, bacteria have often served as model systems for elucidation of general principles. Recent conceptual advances include the idea of a molecular code through which proteins sense and differentiate S-nitrosothiol (SNO) from alternative oxidative modifications, providing the basis for specificity in SNO signaling. In , S-nitrosylation relies on an enzymatic cascade that regulates, and is regulated by, the transcription factor OxyR under anaerobic conditions. S-nitrosylated OxyR activates an anaerobic regulon of >100 genes that encode for enzymes that both mediate S-nitrosylation and protect against nitrosative stress. Mitochondria originated from endosymbiotic bacteria and generate NO under hypoxic conditions, analogous to conditions in . Nitrosative stress in mitochondria has been implicated in Alzheimer's and Parkinson's disease, among others. Many proteins that are S-nitrosylated in mitochondria are also S-nitrosylated in . Insights into enzymatic regulation of S-nitrosylation in may inform the identification of disease-relevant regulatory machinery in mammalian systems. Using as a model system, in-depth analysis of the anaerobic response controlled by OxyR may lead to the identification of enzymatic mechanisms regulating S-nitrosylation in particular, and hypoxic signaling more generally, providing novel insights into analogous mechanisms in mammalian cells and within dysfunctional mitochondria that characterize neurodegenerative diseases.

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