A human tissue screen identifies a regulator of ER secretion as a brain-size determinant

A human tissue screen identifies a regulator of ER secretion as a brain-size determinant

Abstract

Loss-of-function (LOF) screens provide a powerful approach to identify regulators in biological processes. Pioneered in laboratory animals, LOF screens of human genes are currently restricted to two-dimensional cell cultures, which hinders the testing of gene functions requiring tissue context. Here, we present CRISPR–lineage tracing at cellular resolution in heterogeneous tissue (CRISPR-LICHT), which enables parallel LOF studies in human cerebral organoid tissue. We used CRISPR-LICHT to test 173 microcephaly candidate genes, revealing 25 to be involved in known and uncharacterized microcephaly-associated pathways. We characterized IER3IP1, which regulates the endoplasmic reticulum (ER) function and extracellular matrix protein secretion crucial for tissue integrity, the dysregulation of which results in microcephaly. Our human tissue screening technology identifies microcephaly genes and mechanisms involved in brain-size control.

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Authors
  • Esk, Christopher
  • Lindenhofer, Dominic
  • Haendeler, Simon
  • Wester, Roelof A.
  • Pflug, Florian G
  • Schroeder, Benoit
  • Bagley, Joshua A.
  • Elling, Ulrich
  • Zuber, Johannes
  • von Haeseler, Arndt
  • Knoblich, Jürgen A.
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Shortfacts
Category
Journal Paper
Divisions
Bioinformatics and Computational Biology
Journal or Publication Title
Science
ISSN
0036-8075
Publisher
American Association for the Advancement of Science
Place of Publication
Washington, DC
Page Range
pp. 935-941
Number
6519
Volume
370
Date
20 November 2020
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