A New Zebrafish Model for Pseudoxanthoma Elasticum

Overview

Journal Front Cell Dev Biol

Specialty Cell Biology

Date 2021 Mar 26

PMID 33768091

Citations 3

Authors

David Czimer

Klaudia Porok

Daniel Csete

Zsolt Gyure

Viktoria Lavro

Krisztina Fulop

Zelin Chen

Hella Gyergyak

Gabor E Tusnady

Shawn M Burgess

Attila Mocsai

Andras Varadi

Mate Varga

Affiliations

Soon will be listed here.

Abstract

Calcification of various tissues is a significant health issue associated with aging, cancer and autoimmune diseases. There are both environmental and genetic factors behind this phenomenon and understanding them is essential for the development of efficient therapeutic approaches. Pseudoxanthoma elasticum (PXE) is a rare genetic disease, a prototype for calcification disorders, resulting from the dysfunction of ABCC6, a transport protein found in the membranes of cells. It is identified by excess calcification in a variety of tissues (e.g., eyes, skin, arteries) and currently it has no cure, known treatments target the symptoms only. Preclinical studies of PXE have been successful in mice, proving the usefulness of animal models for the study of the disease. Here, we present a new zebrafish () model for PXE. By resolving some ambiguous assemblies in the zebrafish genome, we show that there are two functional and one non-functional paralogs for in zebrafish (, and , respectively). We created single and double mutants for the functional paralogs and characterized their calcification defects with a combination of techniques. Zebrafish deficient in show defects in their vertebral calcification and also display ectopic calcification foci in their soft tissues. Our results also suggest that the impairment of does not affect this biological process.

Citing Articles

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