The Deep Phenotype of Lamin A/C Cardiomyopathy

Title: 
The Deep Phenotype of Lamin A/C Cardiomyopathy
Recruitment Status: 
Status Last Updated: 
October 16, 2019
Clinical Phenotype(s): 
Gene(s): 
Study Purpose: 

This study seeks to discover clinically useful tests to improve the diagnosis of a rare and serious heart muscle disease caused by mutations in a gene called 'Lamin'.

Patients born with lamin gene mutations have apparently healthy hearts initially, they begin experiencing symptoms in their twenties or thirties, and by age 45 the majority have undergone a heart transplant, experienced a major cardiac complication, or have died. Sudden heart rhythm abnormalities are a major cause of sudden death so earlier diagnosis can save lives by enabling timely treatment or implantation of specialised pacemakers (defibrillators). In clinical practice, diagnosis of lamin heart disease currently relies on the genetic test. Very little is known about the detailed imaging features of the hearts of patients with lamin heart disease although advanced echocardiography and cardiac MRI now offer the opportunity to study the health of the heart without the need for radiation.

Phase: 
Study Description: 

Research participants will undergo resting 12-lead ECG, 24-hour ambulatory ECG, baseline echocardiography, exercise echocardiography, cardiac MRI scan.

Blood samples will be collected in all participants from both centers for immediate laboratory testing.

Blood and urine samples will be collected in all participants and used for metabolomic, proteomic and lipidomic profiling and for targeted metabolite and enzyme analysis.

Blood samples will be collected in all participants for future gene code analysis (DNA / RNA).

Study Type: 
Official Title: 
The Deep Phenotype of Lamin A/C Cardiomyopathy - A Proof-of-principle Relax-omic Pipeline
Study Start Date: 
March 7, 2019
Study Completion Date: 
February 1, 2025
Primary Objective(s): 
  1. Positive and negative predictive value of imaging-omics test for diagnosing LMNA-related heart muscle disease. [ Time Frame: 3-4 years ]
Secondary Objective(s): 

None

Eligibility: 

Ages Eligible for Study: 16 Years and older   (Child, Adult, Older Adult)

Sexes Eligible for Study: All

Accepts Healthy Volunteers: Yes

Sampling Method: Non-Probability Sample

Inclusion Criteria: 
  • LMNA+ cases with pathogenic LMNA mutations for LMNA+ and heart myocardial samples from the explanted hearts of LMNA+ patients who are scheduled to undergo clinically indicated heart transplantation at the Papworth Hospital NHS Trust.
  • DCMWT cases: patients with heart muscle failure but with wild-type lamin gene. Heart myocardial samples from the explanted hearts of DCMWT patients who are scheduled to undergo clinically indicated heart transplantation at the Papworth Hospital NHS Trust.
  • HV (controls): matched to cases.
Exclusion Criteria: 
  • Needle-phobia that would preclude blood-letting
  • Participants unwilling to consent
  • Patients that have a conventional contraindication for cardiac magnetic resonance imaging (MRI).
  • Patients that have had a blood transfusion within the last month and patients having haemodialysis will be excluded.
Study Site(s)/Location(s): 

United Kingdom

University Hospital Birmingham (UHB) - Birmingham, United Kingdom

Barts Heart Center, St Bartholomew's Hospital NHS Trust - London, United Kingdom 

Royal Brompton Hospital NHS Trust (RBHT) - Royal Free Hospital NHS Trust (RFH) - London, United Kingdom

University College London Hospital NHS Trust (UCLH) - London, United Kingdom

Papworth Hopsital NHS Trust - Papworth Everard, United Kingdom

Sponsors & Collaborators: 

University College, London

NIHR Rare Diseases Translational Research Collaboration

Barts Cardiovascular registry

Principal Investigator(s): 

Dr Rick Steeds, Consultant Cardiologist

Dr Saidi Mohiddin, Consultant Cardiologist

Dr Sanjay Prasad, Consultant Cardiologist

Dr Gabriella Captur, Consultant Cardiologist

Dr Simon J Woldman, Consultant Cardiologist

Dr Stephen Pettit, Consultant Cardiologist

For more information, please contact the Study Coordinator: 

Contact:  

Email: 

Phone: 

ClinicalTrials.gov ID: 
 NCT03860454