A Multi-institutional Experience in Vascular Ehlers-Danlos Syndrome Diagnosis

Overview

Journal J Vasc Surg

Publisher Elsevier

Specialties Cardiology & Vascular Diseases
General Surgery

Date 2019 Jul 30

PMID 31353273

Citations 11

Authors

Sherene Shalhub

Peter H Byers

Kelli L Hicks

Dawn M Coleman

Frank M Davis

Giovanni De Caridi

K Nicole Weaver

Erin M Miller

Marc L Schermerhorn

Katie Shean

Gustavo Oderich

Mauricio Ribeiro

Cole Nishikawa

Kristofer Charlton-Ouw

Christian-Alexander Behrendt

E Sebastian Debus

Yskert von Kodolitsch

Devin Zarkowsky

Richard J Powell

Melanie Pepin

Dianna M Milewicz

Ellen S Regalado

Peter F Lawrence

Karen Woo

Affiliations

Soon will be listed here.

Abstract

Objective: Vascular Ehlers-Danlos syndrome (vEDS) is a rare disorder and 1 of 13 types of EDS. The syndrome results in aortic and arterial aneurysms and dissections at a young age. Diagnosis is confirmed with molecular testing via skin biopsy or genetic testing for COL3A1 pathogenic variants. We describe a multi-institutional experience in the diagnosis of vEDS from 2000 to 2015.

Methods: This is a multi-institutional cross-sectional retrospective study of individuals with vEDS. The institutions were recruited through the Vascular Low Frequency Disease Consortium. Individuals were identified using the International Classification of Diseases-9 and 10-CM codes for EDS (756.83 and Q79.6). A review of records was then performed to select individuals with vEDS. Data abstraction included demographics, family history, clinical features, major and minor diagnostic criteria, and molecular testing results. Individuals were classified into two cohorts and then compared: those with pathogenic COL3A1 variants and those diagnosed by clinical criteria alone without molecular confirmation.

Results: Eleven institutions identified 173 individuals (35.3% male, 56.6% Caucasian) with vEDS. Of those, 11 (9.8%) had nonpathogenic alterations in COL3A1 and were excluded from the analysis. Among the remaining individuals, 86 (47.7% male, 68% Caucasian, 48.8% positive family history) had pathogenic COL3A1 variants and 76 (19.7% male, 19.7% Caucasian, 43.4% positive family history) were diagnosed by clinical criteria alone without molecular confirmation. Compared with the cohort with pathogenic COL3A1 variants, the clinical diagnosis only cohort had a higher number of females (80.3% vs 52.3%; P < .001), mitral valve prolapse (10.5% vs 1.2%; P = .009), and joint hypermobility (68.4% vs 40.7%; P < .001). Additionally, they had a lower frequency of easy bruising (23.7% vs 64%; P < .001), thin translucent skin (17.1% vs 48.8%; P < .001), intestinal perforation (3.9% vs 16.3%; P = .01), spontaneous pneumothorax/hemothorax (3.9% vs 14%, P.03), and arterial rupture (9.2% vs 17.4%; P = .13). There were no differences in mortality or age of mortality between the two cohorts.

Conclusions: This study highlights the importance of confirming vEDS diagnosis by testing for pathogenic COL3A1 variants rather than relying on clinical diagnostic criteria alone given the high degree of overlap with other forms genetically triggered arteriopathies. Because not all COL3A1 variants are pathogenic, the interpretation of the genetic testing results by an individual trained in variant assessment is essential to confirm the diagnosis. An accurate diagnosis is critical and has serious implications for lifelong screening and treatment strategies for the affected individual and family members.

Citing Articles

Integrative Multi-Omics Approach in Vascular Ehlers-Danlos Syndrome: Further Insights into the Disease Mechanisms by Proteomic Analysis of Patient Dermal Fibroblasts.

Chiarelli N, Cinquina V, Zoppi N, Bertini V, Maddaluno M, De Leonibus C Biomedicines. 2025; 12(12.

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Temporal Pattern Analysis of Ultrasound Surveillance Data in Vascular Connective Tissue Disorders.

Walter C, Leinweber M, Mlekusch I, Assadian A, Hofmann A Diagnostics (Basel). 2024; 14(16).

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Clinical Approach to Genetic Cerebral Arteriopathy in the Adult Patient With Ischemic Stroke.

Haddad E, Kumar P, Shearn-Nance G, Kharal G, Dhawan A Neurol Genet. 2024; 10(5):e200182.

PMID: 39176127 PMC: 11341007. DOI: 10.1212/NXG.0000000000200182.

Open repair of abdominal aortic aneurysms in patients with vascular Ehlers-Danlos syndrome.

Dittman J, Saldana-Ruiz N, Newhall K, Byers P, Starnes B, Shalhub S J Vasc Surg Cases Innov Tech. 2023; 9(2):101194.

PMID: 37251601 PMC: 10220481. DOI: 10.1016/j.jvscit.2023.101194.

Diagnosis and management of vascular Ehlers-Danlos syndrome: Experience of the UK national diagnostic service, Sheffield.

Bowen J, Hernandez M, Johnson D, Green C, Kammin T, Baker D Eur J Hum Genet. 2023; 31(7):749-760.

PMID: 36977837 PMC: 10326011. DOI: 10.1038/s41431-023-01343-7.

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