Insulin and Igf-1 Elicit Robust Transcriptional Regulation to Modulate Autophagy in Astrocytes

Author(s)

Geffken, S. J., Moon, S., Smith, C. O., Tang, S., Lee, H. H., Lewis, K., Wong, C. W., Huang, Y., Huang, Q., Zhao, Y.-T., & Cai, W.

Title

Insulin and Igf-1 Elicit Robust Transcriptional Regulation to Modulate Autophagy in Astrocytes

Date

2022

Publisher

Elsevier BV

Subject

Insuling
IGF-1
Astrocytes
Transcription
Autophagy
Proteostasis

Language

English

Abstract

Objective

Insulin is a principal metabolic hormone. It regulates a plethora of metabolic pathways in peripheral tissues. The highly homologous insulin-like growth factor 1 (IGF-1), on the other hand, is important for development and growth. Recent studies have shown that insulin and IGF-1 signaling plays fundamental roles in the brain. Loss of insulin or IGF-1 receptors in astrocytes leads to altered glucose handling, mitochondrial metabolism, neurovascular coupling, and behavioral abnormalities in mice. Here, we aim to investigate molecular mechanisms by which insulin and IGF-1 signaling regulates astrocyte functions.

Methods

IR-flox and IRKO primary astrocytes were treated with 100 nM insulin or IGF-1 for 6 h, and their transcriptomes were analyzed. Astrocytes with either IR deletion, IGF1R deletion or both were used to examine receptor-dependent transcriptional regulations using qPCR. Additional immunoblotting and confocal imaging studies were performed to functionally validate pathways involved in protein homeostasis.

Results

Using next-generation RNA sequencing, we show that insulin significantly regulates the expression of over 1,200 genes involved in multiple functional processes in primary astrocytes. Insulin-like growth factor 1 (IGF-1) triggers a similar robust transcriptional regulation in astrocytes. Thus, over 50% of the differentially expressed genes are regulated by both ligands. As expected, these commonly regulated genes are highly enriched in pathways involved in lipid and cholesterol biosynthesis. Additionally, insulin and IGF-1 induce the expression of genes involved in ribosomal biogenesis, while suppressing the expression of genes involved in autophagy, indicating a common role of insulin and IGF-1 on protein homeostasis in astrocytes. Insulin-dependent suppression of autophagy genes, including p62 , Ulk1/2 , and several Atg genes, is blunted only when both IR and IGF1R are deleted.

Conclusions

In summary, insulin and IGF-1 potently suppress autophagy in astrocytes through transcriptional regulation. Both IR and IGF1R can elicit ligand-dependent transcriptional suppression of autophagy. These results demonstrate an important role of astrocytic insulin/IGF-1 signaling on proteostasis. Impairment of this regulation in insulin resistance and diabetes may contribute to neurological complications related to diabetes.

Source

Molecular Metabolism Volume 66, December 2022, page 101647

Rights

Copyright © 2022 The Authors

Format

PDF

Type

Text

Bibliographic Citation

Geffken, S. J., Moon, S., Smith, C. O., Tang, S., Lee, H. H., Lewis, K., Wong, C. W., Huang, Y., Huang, Q., Zhao, Y.-T., & Cai, W. (2022). Insulin and IGF-1 elicit robust transcriptional regulation to modulate autophagy in astrocytes. In Molecular Metabolism (Vol. 66, p. 101647). Elsevier BV. https://doi.org/10.1016/j.molmet.2022.101647

Files

1-s2.0-S2212877822002162-main.pdf

Citation

Geffken, S. J., Moon, S., Smith, C. O., Tang, S., Lee, H. H., Lewis, K., Wong, C. W., Huang, Y., Huang, Q., Zhao, Y.-T., & Cai, W., Insulin and Igf-1 Elicit Robust Transcriptional Regulation to Modulate Autophagy in Astrocytes. Molecular Metabolism Volume 66, December 2022, page 101647, New York Tech Institutional Repository, accessed April 28, 2024, https://repository.nyitlibrary.org/items/show/3774

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