Diagnostic Criteria and Disease Staging for Desmoplakin Cardiomyopathy

  1. Eric Smith
  2. Alessio Gasperetti
  3. Richard T Carrick
  4. Alexandros Protonotarios
  5. Petros Syrris
  6. Barbara Bauce
  7. Kalliopi Pilichou
  8. Brittney Murray
  9. Crystal Tichnell
  10. Cristina Basso
  11. Paul Anders Sletten Olsen
  12. Chiara Cappelletto
  13. Victoria N. Parikh
  14. Liang Chen
  15. Stacey Peters
  16. Antonella Mancinelli
  17. Anna Maria Iorio
  18. Roberta Scotto
  19. Julia Cadrin-Tourigny
  20. Nisha A. Gilotra
  21. Manuela Iseppi
  22. Giovanni Peretto
  23. Marco Schiavone
  24. Mark Abela
  25. Daniela Vargas
  26. Cinzia Crescenzi
  27. Leonardo Calò
  28. James Ware
  29. Lia Crotti
  30. Michele Ciabatti
  31. Michela Casella
  32. Alexandra Apostu
  33. Ruxandra Jurcut
  34. Claudia Raineri
  35. Filippo Angelini
  36. Carlos Fernández-Sellers
  37. Esther Zorio
  38. Sing-Chien Yap
  39. Moniek G Cox
  40. Arman Salavati
  41. Anneline te Riele
  42. Arthur Wilde
  43. Ahmad S. Amin
  44. Peter van Tintelen
  45. Ardan M. Saguner
  46. Firat Duru
  47. Dominic Abrams
  48. Marina Cerrone
  49. Maddalena Graziosi
  50. Elena Biagini
  51. Juan Ramon Gimeno
  52. Estelle Gandjbakhch
  53. Neal Lakdawala
  54. Maurizio Pieroni
  55. Marco Merlo
  56. Gianfranco Sinagra
  57. Kristina Haugaa
  58. Elena Arbelo
  59. Perry M. Elliott
  60. Matthew Taylor
  61. Luisa Mestroni
  62. Hugh Calkins
  63. Cynthia A. James
  64. Adam S. Helms
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Abstract

Background

Desmoplakin (DSP) cardiomyopathy, caused by variants in the gene DSP , is a unique subtype of cardiomyopathy distinct from typical dilated or arrhythmogenic right ventricular cardiomyopathies. Specific diagnostic and disease staging criteria have yet to be developed for DSP cardiomyopathy.

Objective

Utilizing a large cohort of DSP cardiomyopathy patients and their genotype-positive family members, this study aims to develop diagnostic and disease staging criteria for DSP cardiomyopathy.

Methods

Patients from the DSP -ERADOS Network with complete rhythm monitoring, electrocardiogram and cardiac magnetic resonance imaging were enrolled. Diagnostic criteria were assessed in initially-presenting patients (probands) and their genotype-positive family members. Early disease criteria (with preserved left ventricular ejection fraction, LVEF) were integrated into standard LVEF-based classifications. Diagnostic and staging criteria were assessed by time-event analyses (major ventricular arrhythmia and heart failure events).

Results

A total of 605 patients with complete diagnostic testing were included (mean age 40 yr, 60% female, 40% probands). The most prevalent disease features in probands were premature ventricular contractions (PVCs) >500/24hr (66%), nonsustained ventricular tachycardia (NSVT, 29%), LV late gadolinium enhancement (LGE, 53%), and reduced LVEF (44%). The presence of any one of these features was 97% sensitive for diagnosis (along with a DSP pathogenic variant) and were therefore considered as diagnostic criteria. Using these criteria, 77% of genotype-positive family members were considered clinically affected. Isolated right ventricular (RV) involvement occurred in only 0.7%. The absence of diagnostic criteria identified a low-risk group (composite event rate 0.8%/year, p<0.001). Integration of these criteria into LVEF-based classification improved identification of composite arrhythmia/heart failure events (early: diagnostic criteria with LVEF >50%, HR 2.7, p=0.04; intermediate: LVEF 41-49%, HR 3.7, p=0.009; advanced: LVEF <40% HR 10.3, p<0.001). LGE was mostly subepicardial (87%). Circumferential (ring-like) LGE was more frequent in intermediate or advanced vs early disease (66% vs 48%, p<0.001).

Conclusion

This study identifies genotype-specific diagnostic and disease staging criteria for DSP cardiomyopathy that improve identification of risk for both heart failure and sustained ventricular arrhythmias. This work highlights how gene-specific criteria may be used to refine diagnosis and staging for cardiomyopathy subtypes – a critical step as gene-targeted treatments move toward clinical trials.

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  1. Version published to 10.1101/2025.06.16.25329734v1 on medRxiv