Matrisome and Immune Pathways Contribute to Extreme Vascular Outcomes in Williams-Beuren Syndrome

Delong Liu; Charles J Billington Jr; Neelam Raja; Zoe C Wong; Mark D Levin; Wulfgang Resch; Camille Alba; Daniel N Hupalo; Elisa Biamino; Maria Francesca Bedeschi; Maria Cristina Digilio; Gabriella Maria Squeo; Roberta Villa; Pheobe C R Parrish; Russell H Knutsen; Sharon Osgood; Joy A Freeman; Clifton L Dalgard; Giuseppe Merla; Barbara R Pober; Carolyn B Mervis; Amy E Roberts; Colleen A Morris; Lucy R Osborne; Beth A Kozel

doi:10.1161/JAHA.123.031377

Matrisome and Immune Pathways Contribute to Extreme Vascular Outcomes in Williams-Beuren Syndrome

J Am Heart Assoc. 2024 Feb 6;13(3):e031377. doi: 10.1161/JAHA.123.031377. Epub 2024 Jan 31.

Authors

Delong Liu¹, Charles J Billington Jr^{1

2}, Neelam Raja¹, Zoe C Wong¹, Mark D Levin¹, Wulfgang Resch³, Camille Alba⁴, Daniel N Hupalo⁴, Elisa Biamino⁵, Maria Francesca Bedeschi⁶, Maria Cristina Digilio⁷, Gabriella Maria Squeo⁸, Roberta Villa⁶, Pheobe C R Parrish^{1

9}, Russell H Knutsen¹, Sharon Osgood¹, Joy A Freeman¹, Clifton L Dalgard¹⁰, Giuseppe Merla^{8

11}, Barbara R Pober¹², Carolyn B Mervis¹³, Amy E Roberts¹⁴, Colleen A Morris¹⁵, Lucy R Osborne¹⁶, Beth A Kozel¹

Affiliations

¹ National Heart, Lung, and Blood Institute National Institutes of Health Bethesda MD.
² Department of Pediatrics University of Minnesota Minneapolis MN.
³ The High Performance Computing Facility Center for Information Technology, National Institutes of Health Bethesda MD.
⁴ Henry M Jackson Foundation for the Advancement of Military Medicine Bethesda MD.
⁵ Department of Pediatrics University of Turin Italy.
⁶ Fondazione IRCCS Ca Granda Ospedale Maggiore Policlinico Medical Genetic Unit Milan Italy.
⁷ Medical Genetics Department Bambino Gesù Children's Hospital, IRCCS Rome Italy.
⁸ Laboratory of Regulatory and Functional Genomics Fondazione IRCCS Casa Sollievo della Sofferenza San Giovanni Rotondo (Foggia) Italy.
⁹ Department of Genome Sciences University of Washington Seattle WA.
¹⁰ Department of Anatomy, Physiology and Genetics, School of Medicine the Uniformed Services University of the Health Sciences Bethesda MD.
¹¹ Department of Molecular Medicine and Medical Biotechnology University of Naples Federico II Naples Italy.
¹² Section of Genetics, Department of Pediatrics Massachusetts General Hospital Boston MA.
¹³ Department of Psychological and Brain Sciences University of Louisville Louisville KY.
¹⁴ Department of Cardiology and Division of Genetics and Genomics, Department of Pediatrics Boston Children's Hospital Boston MA.
¹⁵ Department of Pediatrics Kirk Kerkorian School of Medicine at UNLV Las Vegas NV.
¹⁶ Departments of Medicine and Molecular Genetics University of Toronto Canada.

Abstract

Background: Supravalvar aortic stenosis (SVAS) is a characteristic feature of Williams-Beuren syndrome (WBS). Its severity varies: ~20% of people with Williams-Beuren syndrome have SVAS requiring surgical intervention, whereas ~35% have no appreciable SVAS. The remaining individuals have SVAS of intermediate severity. Little is known about genetic modifiers that contribute to this variability.

Methods and results: We performed genome sequencing on 473 individuals with Williams-Beuren syndrome and developed strategies for modifier discovery in this rare disease population. Approaches include extreme phenotyping and nonsynonymous variant prioritization, followed by gene set enrichment and pathway-level association tests. We next used GTEx v8 and proteomic data sets to verify expression of candidate modifiers in relevant tissues. Finally, we evaluated overlap between the genes/pathways identified here and those ascertained through larger aortic disease/trait genome-wide association studies. We show that SVAS severity in Williams-Beuren syndrome is associated with increased frequency of common and rarer variants in matrisome and immune pathways. Two implicated matrisome genes (ACAN and LTBP4) were uniquely expressed in the aorta. Many genes in the identified pathways were previously reported in genome-wide association studies for aneurysm, bicuspid aortic valve, or aortic size.

Conclusions: Smaller sample sizes in rare disease studies necessitate new approaches to detect modifiers. Our strategies identified variation in matrisome and immune pathways that are associated with SVAS severity. These findings suggest that, like other aortopathies, SVAS may be influenced by the balance of synthesis and degradation of matrisome proteins. Leveraging multiomic data and results from larger aorta-focused genome-wide association studies may accelerate modifier discovery for rare aortopathies like SVAS.

Keywords: Williams–Beuren syndrome; adaptive/innate immune system; elastin (ELN); extreme phenotype; pathway analysis; supravalvar aortic stenosis.

MeSH terms

Aortic Stenosis, Supravalvular* / genetics
Aortic Stenosis, Supravalvular* / metabolism
Aortic Stenosis, Supravalvular* / surgery
Genome-Wide Association Study
Humans
Proteomics
Rare Diseases
Williams Syndrome* / genetics

Grants and funding

R01 NS035102/NS/NINDS NIH HHS/United States