A Whole Genome-Wide Arrayed CRISPR Screen in Primary Organ Fibroblasts to Identify Regulators of Kidney Fibrosis

Author:

Turner Robert J.1,Golz Stefan2,Wollnik Carina1,Burkhardt Nils2,Sternberger Ina1,Andag Uwe3,Cornils Hauke1

Affiliation:

1. In Vitro Biology, Evotec SE, Hamburg, Germany

2. Lead Discovery, Bayer AG, Wuppertal, Germany

3. Metabolic Disease, Evotec International GmbH, Göttingen, Germany

Abstract

Kidney fibrosis presents a hallmark of chronic kidney disease. With ever-increasing patient numbers and limited treatment options available, novel strategies for therapeutic intervention in kidney disease are warranted. Fibrosis commonly results from a wound healing response to repeated or chronic tissue damage, irrespective of the underlying etiology, and can occur in virtually any solid organ or tissue. In order to identify targets relevant for kidney fibrosis, we aimed to employ CRISPR screening in primary human kidney fibroblasts. We demonstrate that CRISPR technology can be applied in primary kidney fibroblasts and can furthermore be used to conduct arrayed CRISPR screening using a high-content imaging readout in a whole genome-wide manner. Hits coming out of this screen were validated using orthogonal approaches and present starting points for validation of novel targets relevant to kidney disease.

Publisher

Elsevier BV

Subject

Molecular Medicine,Biochemistry,Analytical Chemistry,Biotechnology

Cited by 6 articles. 订阅此论文施引文献 订阅此论文施引文献,注册后可以免费订阅5篇论文的施引文献,订阅后可以查看论文全部施引文献

1. Pooled genetic screens with image‐based profiling;Molecular Systems Biology;2022-11

2. Functional Genomics;Genome Editing in Drug Discovery;2022-03-17

3. Hepatic fibrosis 2022: Unmet needs and a blueprint for the future;Hepatology;2022-01-11

4. In vitro Assays and Imaging Methods for Drug Discovery for Cardiac Fibrosis;Frontiers in Physiology;2021-07-08

5. CRISPRing future medicines;Expert Opinion on Drug Discovery;2021-01-03

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