The new kids on the block: RNA‐binding proteins regulate autophagy in disease

Author:

Dushnitzky Shai1,Ishtayeh Hasan1,Ashkenazi Avraham12ORCID

Affiliation:

1. The Department of Cell and Developmental Biology, Faculty of Medical & Health Sciences Tel Aviv University Israel

2. Sagol School of Neuroscience Tel Aviv University Israel

Abstract

Mammalian autophagy is a highly regulated and conserved cellular homeostatic process. Its existence allows the degradation of self‐components to mediate cell survival in different stress conditions. Autophagy is involved in the regulation of cellular metabolic needs, protecting the cell or tissue from starvation through the degradation and recycling of cytoplasmic materials and organelles to basic molecular building blocks. It also plays a critical role in eliminating damaged or harmful proteins, organelles, and intracellular pathogens. Thus, a deterioration of the process may result in pathological conditions, such as aging‐associated disorders and cancer. Understanding the crucial role of autophagy in maintaining the normal physiological function of cells, tissue, or organs has led to copious and expansive research regarding the regulation of this process. So far, most of the research has revolved around transcriptional and post‐translational regulation. Here, we discuss the regulation of autophagy‐related (ATG) mRNA transcripts by RNA‐binding proteins (RBPs). This analysis focuses on how RBPs modulate autophagy in disease. A deeper understanding of the involvement of RBPs in autophagy can facilitate further research and treatment of a variety of human diseases.

Funder

Azrieli Foundation

Publisher

Wiley

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