High-content Synaptic Phenotyping in Human Cellular Models Reveals a Role for BET Proteins in Synapse Assembly

Overview

Journal Elife

Specialty Biology

Date 2023 Apr 21

PMID 37083703

Authors

Martin H Berryer

Gizem Rizki

Anna Nathanson

Jenny A Klein

Darina Trendafilova

Sara G Susco

Daisy Lam

Angelica Messana

Kristina M Holton

Kyle W Karhohs

Beth A Cimini

Kathleen Pfaff

Anne E Carpenter

Lee L Rubin

Lindy E Barrett

Affiliations

Soon will be listed here.

Abstract

Resolving fundamental molecular and functional processes underlying human synaptic development is crucial for understanding normal brain function as well as dysfunction in disease. Based upon increasing evidence of species-divergent features of brain cell types, coupled with emerging studies of complex human disease genetics, we developed the first automated and quantitative high-content synaptic phenotyping platform using human neurons and astrocytes. To establish the robustness of our platform, we screened the effects of 376 small molecules on presynaptic density, neurite outgrowth, and cell viability, validating six small molecules that specifically enhanced human presynaptic density in vitro. Astrocytes were essential for mediating the effects of all six small molecules, underscoring the relevance of non-cell-autonomous factors in synapse assembly and their importance in synaptic screening applications. Bromodomain and extraterminal (BET) inhibitors emerged as the most prominent hit class and global transcriptional analyses using multiple BET inhibitors confirmed upregulation of synaptic gene expression. Through these analyses, we demonstrate the robustness of our automated screening platform for identifying potent synaptic modulators, which can be further leveraged for scaled analyses of human synaptic mechanisms and drug discovery efforts.

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