Interplay between Nrf2 and αB-crystallin in the lens and heart of zebrafish under proteostatic stress.

Front Mol Biosci

From the Department of Molecular Physiology and Biophysics, Vanderbilt University, Nashville, TN, United States.

Published: July 2023

AI Article Synopsis

  • A stress response activated by Nrf2 helps protect cells from reactive oxygen species, which can cause diseases like cataracts and heart problems.
  • Researchers used zebrafish to study how Nrf2 and small heat shock proteins interact; they found that losing Nrf2 function significantly increases a specific heat shock protein in the heart.
  • In the lens, the combination of losing Nrf2 and a small heat shock protein leads to increased cholesterol production, which helps counteract negative effects, while the absence of Nrf2 worsens heart swelling in zebrafish lacking that heat shock protein.

Article Abstract

A coordinated oxidative stress response, partly triggered by the transcription factor Nrf2, protects cells from the continual production of reactive oxygen species. Left unbuffered, reactive oxygen species can lead to protein aggregation that has been implicated in a spectrum of diseases such as cataract of the ocular lens and myopathy of the heart. While proteostasis is maintained by diverse families of heat shock proteins, the interplay between the oxidative and proteostatic stress responses in the lens and heart has not been investigated. Capitalizing on multiple zebrafish lines that have compromised function of Nrf2 and/or the two zebrafish small heat shock proteins αBa- and αBb-crystallin, we uncovered a transcriptional relationship that leads to a substantial increase in αBb-crystallin transcripts in the heart in response to compromised function of Nrf2. In the lens, the concomitant loss of function of Nrf2 and αBa-crystallin leads to upregulation of the cholesterol biosynthesis pathway, thus mitigating the phenotypic consequences of the αBa-crystallin knockout. By contrast, abrogation of Nrf2 function accentuates the penetrance of a heart edema phenotype characteristic of embryos of αB-crystallin knockout lines. Multiple molecular pathways, such as genes involved in extracellular interactions and implicated in cardiomyopathy, are revealed from transcriptome profiling, thus identifying novel targets for further investigation. Together, our transcriptome/phenotypic analysis establishes an intersection between oxidative stress and chaperone responses in the lens and heart.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10422029PMC
http://dx.doi.org/10.3389/fmolb.2023.1185704DOI Listing

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