Abstract

The molecular mechanisms underlying the neuronal signaling changes in alcohol addiction and withdrawal are complex and multifaceted. The cortico-striatal circuit is highly implicated in these processes, and the striatum plays a significant role not only in the early stages of addiction, but in the developed-addictive state as well, including withdrawal symptoms. Transcriptional analysis is a useful method for determining changes in gene expression, however, the results do not always accurately correlate with protein levels. In this study, we employ label-free proteomic analysis to determine changes in protein expression within the striatum during chronic ethanol use and early withdrawal. The striatum, composed primarily of medium spiny GABAergic neurons, glutamatergic and dopaminergic nerve terminals and astrocytes, is relatively homogeneous for proteomic analysis. We were able to analyze more than 5000 proteins from both the dorsal (caudate and putamen) and ventral (nucleus accumbens) striatum and identified significant changes following chronic intermittent ethanol exposure and acute (8 h) withdrawal compared to ethanol naïve and ethanol exposure groups respectively. Our results showed significant changes in proteins involved in glutamate and opioid peptide signaling, and also uncovered novel pathways including mitochondrial function and lipid/cholesterol metabolism, as revealed by changes in electron transport chain proteins and RXR activation pathways. These results will be useful in the development of novel treatments for alcohol withdrawal and thereby aid in recovery from alcohol use disorder.

Highlights

  • The cortico-striatal circuit is highly implicated in both substance addiction and withdrawal

  • In this report we undertook a label-free proteomic approach to identify novel proteins associated with chronic ethanol exposure and more importantly, withdrawal from that condition

  • It is of paramount importance that we elucidate novel proteins and their associated molecular pathways in order to adequately utilize pharmacological treatment strategies to help individuals suffering from this disease

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Summary

Introduction

The cortico-striatal circuit is highly implicated in both substance addiction and withdrawal. We performed a total protein analysis using label-free proteomics on the entire striatum of C57BL/6J mice undergoing chronic intermittent ethanol (CIE) exposure or acute withdrawal. This quantitative method of measuring protein levels provides a comprehensive and accurate depiction of real-time molecular events without relying on substrate labeling procedures. By comparing this systematic analysis of protein expression to previous transcriptional studies, the underlying mechanisms behind dysfunctional signaling in multiple regions of the striatum during various phases of addiction and withdrawal may be more accurately determined

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