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Each Cellular Compartment Has a Characteristic Protein Reactive Cysteine Ratio Determining Its Sensitivity to Oxidation. | LitMetric

AI Article Synopsis

  • - Signaling and detoxification of Reactive Oxygen Species (ROS) are crucial for understanding various diseases, yet there's limited knowledge about how ROS impact different cell components.
  • - This study highlights the significance of cysteine (Cys) thiol groups in proteins for redox defense and signaling, revealing that each subcellular area has a unique concentration of these thiol groups.
  • - The research found that the nucleolus has the highest amount of thiol concentrations linked to ROS sensitivity, while protein thiol groups per protein are more abundant in the nucleoplasm, particularly in specific structures related to RNA processing.

Article Abstract

Signaling and detoxification of Reactive Oxygen Species (ROS) are important patho-physiologcal processes. Despite this, we lack comprehensive information on individual cells and cellular structures and functions affected by ROS, which is essential to build quantitative models of the effects of ROS. The thiol groups from cysteines (Cys) in proteins play a major role in redox defense, signaling, and protein function. In this study, we show that the proteins in each subcellular compartment contain a characteristic Cys amount. Using a fluorescent assay for -SH in thiolate form and amino groups in proteins, we show that the thiolate content correlates with ROS sensitivity and signaling properties of each compartment. The highest absolute thiolate concentration was found in the nucleolus, followed by the nucleoplasm and cytoplasm whereas protein thiolate groups per protein showed an inverse pattern. In the nucleoplasm, protein reactive thiols concentrated in SC35 speckles, SMN, and the IBODY that accumulated oxidized RNA. Our findings have important functional consequences, and explain differential sensitivity to ROS.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10295259PMC
http://dx.doi.org/10.3390/antiox12061274DOI Listing

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