Rational evolution for altering the ligand preference of estrogen receptor alpha-Reference-Cited by-同舟云学术

Rational evolution for altering the ligand preference of estrogen receptor alpha

Published:2024-03-21 Issue:4 Volume:33 Page:
ISSN:0961-8368
Container-title:Protein Science
language:en
Short-container-title:Protein Science

Author:

Eerlings Roy¹²³^ORCID,Gupta Purvi⁴,Lee Xiao Yin¹,Nguyen Tien⁴,El Kharraz Sarah¹,Handle Florian¹,Smeets Elien¹,Moris Lisa¹⁵,Devlies Wout¹⁵,Vandewinkel Bram⁶,Thiry Irina⁶,Ta Duy Tien⁶,Gorkovskiy Anton²³,Voordeckers Karin²³^ORCID,Henckaerts Els⁶,Pinheiro Vitor B.⁷,Claessens Frank¹,Verstrepen Kevin J.²³,Voet Arnout⁴^ORCID,Helsen Christine¹^ORCID

Affiliation:

1. Molecular Endocrinology Laboratory, Department of Cellular and Molecular Medicine KU Leuven Leuven Belgium

2. Laboratory of Systems Biology VIB‐KU Leuven Center for Microbiology Leuven Belgium

3. Laboratory for Genetics and Genomics, Center of Microbial and Plant Genetics, Department M2S KU Leuven Heverlee Belgium

4. Laboratory of Biomolecular Modelling and Design, Department of Chemistry KU Leuven Heverlee Belgium

5. Department of Urology University Hospitals Leuven Leuven Belgium

6. Laboratory of Viral Cell Biology and Therapeutics, Department of Cellular and Molecular Medicine, Department of Microbiology, Immunology and Transplantation KU Leuven Leuven Belgium

7. KU Leuven, Department of Pharmaceutical and Pharmacological Sciences Rega Institute for Medical Research Leuven Belgium

Abstract

AbstractEstrogen receptor α is commonly used in synthetic biology to control the activity of genome editing tools. The activating ligands, estrogens, however, interfere with various cellular processes, thereby limiting the applicability of this receptor. Altering its ligand preference to chemicals of choice solves this hurdle but requires adaptation of unspecified ligand‐interacting residues. Here, we provide a solution by combining rational protein design with multi‐site‐directed mutagenesis and directed evolution of stably integrated variants in Saccharomyces cerevisiae. This method yielded an estrogen receptor variant, named TERRA, that lost its estrogen responsiveness and became activated by tamoxifen, an anti‐estrogenic drug used for breast cancer treatment. This tamoxifen preference of TERRA was maintained in mammalian cells and mice, even when fused to Cre recombinase, expanding the mammalian synthetic biology toolbox. Not only is our platform transferable to engineer ligand preference of any steroid receptor, it can also profile drug‐resistance landscapes for steroid receptor‐targeted therapies.

Funder

KU Leuven

Publisher

Wiley

Link

https://onlinelibrary.wiley.com/doi/pdf/10.1002/pro.4940

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