Aortopathies in mouse models of Pompe, Fabry and Mucopolysaccharidosis IIIB lysosomal storage diseases

Maria Paola Belfiore; Francesca Iacobellis; Emma Acampora; Martina Caiazza; Marta Rubino; Emanuele Monda; Maria Rosaria Magaldi; Antonietta Tarallo; Marcella Sasso; Valeria De Pasquale; Roberto Grassi; Salvatore Cappabianca; Paolo Calabrò; Simona Fecarotta; Salvatore Esposito; Giovanni Esposito; Antonio Pisani; Luigi Michele Pavone; Giancarlo Parenti; Giuseppe Limongelli

doi:10.1371/journal.pone.0233050

Aortopathies in mouse models of Pompe, Fabry and Mucopolysaccharidosis IIIB lysosomal storage diseases

PLoS One. 2020 May 19;15(5):e0233050. doi: 10.1371/journal.pone.0233050. eCollection 2020.

Authors

Maria Paola Belfiore¹, Francesca Iacobellis¹, Emma Acampora², Martina Caiazza³, Marta Rubino³, Emanuele Monda³, Maria Rosaria Magaldi³, Antonietta Tarallo², Marcella Sasso², Valeria De Pasquale⁴, Roberto Grassi¹, Salvatore Cappabianca¹, Paolo Calabrò³, Simona Fecarotta², Salvatore Esposito⁵, Giovanni Esposito², Antonio Pisani², Luigi Michele Pavone⁴, Giancarlo Parenti², Giuseppe Limongelli^{3

6}

Affiliations

¹ Department of Radiology, University of Campania "L. Vanvitelli", Naples, Italy.
² Department of Translational Medical Sciences, Federico II University, Naples, Italy.
³ Department of Translational Medical Sciences, University of Campania "Luigi Vanvitelli", Naples, Italy.
⁴ Department of Molecular Medicine and Medical Biotechnology, Federico II University, Naples, Italy.
⁵ Unit of Pathological Anatomy, Aversa Hospital, Caserta, Italy.
⁶ Institute of Cardiovascular Sciences, University College of London and St. Bartholomew's Hospital, London, United Kingdom.

Abstract

Introduction: Lysosomal storage diseases (LSDs) are rare inherited metabolic diseases characterized by an abnormal accumulation of various toxic materials in the cells as a result of enzyme deficiencies leading to tissue and organ damage. Among clinical manifestations, cardiac diseases are particularly important in Pompe glycogen storage diseases (PD), in glycosphingolipidosis Fabry disease (FD), and mucopolysaccharidoses (MPS). Here, we evaluated the occurrence of aortopathy in knock out (KO) mouse models of three different LSDs, including PD, FD, and MPS IIIB.

Methods: We measured the aortic diameters in 15 KO male mice, 5 for each LSD: 5 GLA-/- mice for FD, 5 NAGLU-/- mice for MPS IIIB, 5 GAA-/- mice for PD, and 15 wild type (WT) mice: 5 for each strain. In order to compare the aortic parameters between KO and WT mice deriving from the same colonies, different diameters were echocardiographically measured: aortic annulus, aortic sinus, sino-tubular junction, ascending aorta, aortic arch and descending aorta. Storage material content and aortic defects of the KO mice were also analyzed by histology, when available.

Results: Compared to their correspondent WT mice: GAA-/- mice showed greater diameters of ascending aorta (1.61mm vs. 1.11mm, p-value = 0.01) and descending aorta (1.17mm vs 1.02mm, p-value 0.04); GLA-/- mice showed greater diameters of aortic annulus (1.35mm vs. 1.22mm, p-value = 0.01), sinus of Valsalva (1.6mm vs. 1.38mm, p-value<0.01), ascending aorta (1.57mm vs. 1.34mm, p-value<0.01), aortic arch (1.36mm vs. 1.22mm, p-value = 0.03) and descending aorta (1.29mm vs. 1.11mm, p-value<0.01); NAGLU-/- mice showed greater diameters of sinus of Valsalva (1.46mm vs. 1.31mm, p-value = 0.05), ascending aorta (1.42mm vs. 1.29mm, p-value<0.01), aortic arch (1.34mm vs. 1.28mm, p-value<0.01) and descending aorta (1.18mm vs. 1.1mm, p-value 0.01).

Conclusions: We evaluated for the first time the aortic diameters in 3 LSD mouse models and identified different aortopathy patterns, in concordance with recent human findings. Our results are relevant in view of using KO mouse models for efficiently testing the efficacy of new therapies on distinct cardiovascular aspects of LSDs.

MeSH terms

Acetylglucosaminidase / genetics*
Animals
Aortic Diseases / diagnostic imaging
Aortic Diseases / etiology*
Disease Models, Animal
Echocardiography
Fabry Disease / complications
Fabry Disease / genetics
Glycogen Storage Disease Type II / complications
Glycogen Storage Disease Type II / genetics
Lysosomal Storage Diseases / complications*
Lysosomal Storage Diseases / genetics
Male
Mice
Mice, Knockout
Mucopolysaccharidosis III / complications
Mucopolysaccharidosis III / genetics
alpha-Galactosidase / genetics*
alpha-Glucosidases / genetics*

Substances

alpha-Glucosidases
alpha-Galactosidase
alpha-N-acetyl-D-glucosaminidase
Acetylglucosaminidase

Grants and funding

The author(s) received no specific funding for this work.