4.5 Review

Role of misfolding in rare enzymatic deficits and use of pharmacological chaperones as therapeutic approach

Journal

FRONTIERS IN BIOSCIENCE-LANDMARK
Volume 26, Issue 12, Pages 1627-1642

Publisher

IMR PRESS
DOI: 10.52586/5056

Keywords

Misfolding; Parmacological chaperones; Gaucher disease; Phenylketonuria; Primary hyperoxaluria

Funding

  1. Oxalosis and Hyperoxaluria Foundation [OHF2017]

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Cells have evolved sophisticated molecular control systems to maximize the efficiency of the folding process, but any subtle alteration of the environment or protein can lead to misfolding. Pharmacological chaperones (PCs) are a promising approach for treating conformational disorders by stabilizing functional folding to increase enzyme activity.
Cells have evolved sophisticated molecular control systems to maximize the efficiency of the folding process. However, any subtle alteration of the environment or the protein can lead to misfolding or affect the conformational plasticity of the native states. It has been widely demonstrated that misfolding and/or conformational instability are the underlying mechanisms of several rare disorders caused by enzymatic deficits. In fact, disease-causing mutations often lead to the substitution of amino acids that are crucial for the achievement of a folded conformation, or play a role on the equilibrium between native-state conformers. One of the promising approaches to treat conformational disorders is the use of pharmacological chaperones (PCs), small molecules that specifically bind a target protein and stabilize a functional fold, thus increasing the amount of functionally active enzyme. Molecules acting as PCs are usually coenzymes, substrate analogues behaving as competitive inhibitors, or allosteric modulators. In this review, the general features of PCs are described, along with three examples of diseases (Gaucher disease, Phenylketonuria, and Primary Hyperoxaluria) in which this approach is currently under study at preclinical and/or clinical level.

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