Isogenic Human Cell Lines for Drug Discovery: Regulation of Target Gene Expression by Engineered Zinc-Finger Protein Transcription Factors

Author:

Liu Pei-Qi,Tan Siyuan,Mendel Matthew C.1,Murrills Richard J.,Bhat Bheem M.2,Schlag Brian3,Samuel Rachelle,Matteo Jeanne J.2,de la Rosa Ragan,Howes Katherine,Reik Andreas,Case Casey C.1,Bex Frederick J.2,Young Kathleen3,Gregory Philip D.1

Affiliation:

1. Sangamo BioSciences, Inc., Richmond, CA

2. Women’s Health & Bone, Wyeth Research, Collegeville, PA

3. Neurosciences, Wyeth Research, Princeton, NJ

Abstract

Isogenic cell lines differing only in the expression of the protein of interest provide the ideal platform for cell-based screening. However, related natural lines differentially expressing the therapeutic target of choice are rare. Here the authors report a strategy for drug screening employing isogenic human cell lines in which the expression of the target protein is regulated by a gene-specific engineered zinc-finger protein (ZFP) transcription factor (TF). To demonstrate this approach, a ZFP TF activator of the human parathyroid hormone receptor 1 (PTHR1) gene was identified and introduced into HEK293 cells (negative for PTHR1). Following induction of ZFP TF expression, this cell line produced functional PTHR1 protein, resulting in a robust and ligand-specific cyclic adenosine monophosphate (cAMP) response. Reciprocally, the natural expression of PTHR1 observed in SAOS2 cells was dramatically reduced by the introduction of the appropriate PTHR1-specific ZFP TF repressor. Moreover, this ZFP-driven PTHR1 repression selectively eliminated the functional cAMP response invoked by known ligands of PTHR1. These data establish ZFP TF–generated isogenic lines as a general approach for the identification of therapeutic agents specific for the target gene of interest.

Publisher

Elsevier BV

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