The development of highly potent and selective small molecule correctors of Z α1-antitrypsin misfolding.

John Liddle,Andrew C. Pearce,Christopher C. Arico-Muendel,Svetlana L. Belyanskaya,Andrew Brewster,Murray J.B. Brown,Chun-wa Chung,Alexis Denis,Nerina Dodic,Anthony Dossang,Peter Eddershaw,Diana Klimaszewska,Imran Haq,Duncan S. Holmes,Alistair M. Jagger,Toral Jakhria,Emilie Jigorel,Ken Lind,Jeffrey A. Messer,Margaret Neu,Allison Olszewski,Riccardo Ronzoni,James E. Rowedder,Martin Rüdiger,Steve Skinner,Kathrine J. Smith,Lionel Trottet,Iain Uings,Zhengrong Zhu,James A. Irving,David A. Lomas

The development of highly potent and selective small molecule correctors of Z α1-antitrypsin misfolding.

2021

Abstract α1-antitrypsin deficiency is characterised by the misfolding and intracellular polymerisation of mutant α1-antitrypsin protein within the endoplasmic reticulum (ER) of hepatocytes. Small molecules that bind and stabilise Z α1-antitrypsin were identified via a DNA-encoded library screen. A subsequent structure based optimisation led to a series of highly potent, selective and cellular active α1-antitrypsin correctors.

Keywords:

Small molecule
Intracellular
Mutant
α1 antitrypsin
structure based
Biophysics
Chemistry
Endoplasmic reticulum

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