Non-syndromic cardiac progeria in a patient with the rare pathogenic p.Asp300Asn variant in the LMNA gene

Aging is associated with a progressive functional decline of multiple organ, including the heart. In the heart, aging commonly manifests with cardiac dysfunction, an impaired chronotropic response, atrial fibrillation, conduction defects, degenerative valvular disease, and coronary atherosclerosis, as well as vascular calcification. The prevalence of these phenotypes, which are typically absent in the young individuals, increases markedly in the elderly. For example, heart failure, with the exception of familial cardiomyopathies, predominantly affects the elderly [1]. Likewise, cardiac conduction defects and arrhythmias are predominantly diseases of the elderly [2]. Similarly, degenerative mitral and aortic valve diseases are also almost exclusive diseases of the elderly, and seldom seen in young individuals except in those patients with a bicuspid aortic valve [3].

The LMNA gene encodes lamin A (and its isoforms C, C2, and Δ10), which is an inner nuclear membrane protein ubiquitously expressed in almost all differentiated cells, including the cardiac cells [4, 5]. Mutations in the LMNA gene cause a diverse array of phenotypes, which are collectively referred to as laminopathies [6]. In the heart, LMNA mutations cause two distinct sets of phenotypes, involving primarily either the myocardium or the coronary arteries, the latter in the context of progeroid syndromes. Most commonly LMNA mutations cause dilated cardiomyopathy (DCM), with variable skeletal muscle involvement [7, 8]. The phenotype is typically associated with early conduction defects and refractory heart failure [7‐11]. Such patients typically do not exhibit premature coronary artery disease (CAD) and myocardial infarction (MI). Less commonly, however, patients with LMNA mutations present with an early onset CAD and premature MI, typically in the context of progeroid syndromes, such as Hutchinson-Gilford Progeria Syndrome (HGPS) and atypical Werner syndrome, which typically involve multiple organs [12, 13].

Phenotypic manifestations of progeroid syndromes is diverse and include impaired growth, alopecia, skin sclerosis, bone abnormalities, subcutaneous fat redistribution, and cardiovascular complications, including atherosclerosis and myocardial infarction, reflective of involvement of multiple cell types and organs [14, 15]. Cardiovascular complications, including advanced atherosclerosis and MI, are the main causes of death in patients with HGPS [16]. We report a young patient who carried a rare missense mutation in the LMNA gene and presented with the phenotype that resembled the progeroid syndromes. However, in contrast to the progeroid syndromes, the phenotype was restricted to the heart and did not involve other organs. The predominant phenotype was premature CAD and MI, but also included degenerative valvular disease, conduction defect, and premature death due to refractory right heart failure.

The patient was a fully developed (height: 165 cm, weight: 110 lbs) Caucasian female who first presented with an acute MI at age 29 years. She did not have a family history of premature CAD and did not have any of the conventional risk factors for MI (dyslipidemia, smoking, diabetes mellitus, and systemic arterial hypertension). She underwent cardiac catheterization and coronary angiography and was found to have advanced CAD. The early onset of CAD in this patient is in contrast to the typical presentation of CAD in the 6th and 7th decades of life in the general population. The presentation is also in discord with that of CAD in patients with HGPS, who typically suffer from CAD and MI in childhood [16]. The patient underwent coronary artery bypass surgery with implantation of the left internal mammary artery to left anterior descending coronary artery and a vein graft to left circumflex coronary artery. The time course of the medical problems and interventions are listed in Table 1 and the list of medication in Additional file 1: Table S1. In brief, during the course of next 10 years, she developed mitral valve regurgitation; requiring surgical repair, chest pain due to obstructive coronary lesions; requiring multiple percutaneous coronary interventions, degenerative mitral and aortic valve diseases; requiring replacement of both valves, and atrial flutter/fibrillation along with conduction defect; requiring catheter ablation and a permanent pacemaker implantation. She developed progressive heart failure, predominantly involving the right ventricle with severe tricuspid regurgitation, and died a year later at the age of 40 years. During the last hospital admission, she was evaluated for heart transplantation. Notable cardiovascular test/procedures findings are summarized in Table 2.

During evaluation for cardiac transplantation other organs were also evaluated. She had no features to suggest a systemic progeroid syndrome and had only a mild pre-renal azotemia and a restrictive physiology on a pulmonary function test. These abnormalities were considered to be secondary to heart failure and not features of progeroid syndromes. Computerized tomography of chest, abdomen, and pelvis were unremarkable, except for abdominal aortic atherosclerosis and evidence of right heart failure (enlarged inferior vena cava and hepatic vein along with a congested liver, and ascites). Her lipid profile was notable for a total cholesterol of 130 mg/dL (desirable level: <200 mg/dL), HDL-C 24 mg/dL (normal range: 40 to 60 mg/dL), LDL-C of 75 mg/dL (optimal level < 100 mg/dL), and triglycerides of 155 mg/dL (normal levels <150 mg/dL). Her other laboratory blood tests were remarkable for an elevated blood homocysteine concentration of 27.2 umol/L (normal range: 4.0 to 10.0 umol/L), anemia of chronic disease (Hg: 9.7 g/dL, normal range: 12.0 -16.0 g/dL), and an elevated B-type natriuretic peptide level of 467 pg/mL (normal range: 0-100 pg/mL), consistent with heart failure. None of the above laboratory values were specific to progeroid syndromes. Considering the constellation of multiple cardiovascular phenotypes, typically observed in the elderly and in the progeroid syndromes, and given the absence of a progeroid phenotype in other organs, the term non-syndromic cardiac progeria was coined to describe the phenotype in the index case.

In view of the well-established role of the LMNA gene in progeroid syndromes, the LMNA gene along with several genes commonly associated with cardiomyopathies, namely, MYH7 (myosin heavy chain 7), MYPBC3 (myosin binding protein C3), TNNT2 (cardiac troponin T), TNNI3 (cardiac troponin I), ACTC1 (cardiac α-actin), and TPM1 (α-tropomyosin) were sequenced using the Big Dye Terminator Cycle Sequencing Ready Reaction Kit on an ABI Genetic Analyzer 3730xl (Applied Biosystems, Foster City, CA), as published [17‐19]. Both sense and anti-sense DNA strands of all exons and the exon-intron boundaries were sequenced. The sequence output was analyzed using Variant Reporter software (Applied Biosystems) and compared the sequence with the corresponding reference GenBank sequence of each gene. A rare LMNA gene p.Asp300Asn missense variant was identified in the proband (Fig. 1). No pathogenic variant in other genes was detected. The proband’s parents and brother either could not be reached or decided not to participate in the genetic studies. The p.Asp300Asn variant was absent in the gnomAD database (http://​gnomad.​broadinstitute.​org/​gene/​ENSG00000160789.). It is predicted to be pathogenic by multiple computational algorithms (Polyphen2 score: 0.995, SIFT score: 0.03, Mutation taster score: 1, CADD_Phred score: 27.6). The mutation affected the coiled coil structure in the rod domain of the LMNA protein, which is involved in binding to lamin A/C dimers and partners.

The p.Asp300Asn was identified a few months after patient’s death about 10 years ago. However, it was not reported because of the uncertainty in unambiguous ascertainment of its causality in a single case, despite its pathogenic nature and biological plausibility. A recent report of detection of the p.Asp300Asn mutation in a Japanese patient who exhibited atypical progeroid/Werner syndrome involving multiple organs [20], provided strong support to the causal role of this mutation in the patient with non-syndromic cardiac progeria. In principle, detection of a rare pathogenic variant in two independent individuals with a similar phenotype provides strong evidence of pathogenicity of the variant in the phenotype of interest [21]. Moreover, a different missense mutation involving the amino acid 300 (p.Asp300Gly) in the LMNA protein has been associated with an autosomal dominant late-onset cardiocutaneous progeria [22]. The skin phenotype associated with the p.Asp300Gly included early hair loss and premature graying, whereas the cardiac involvement was comprised of accelerated atherosclerosis, calcific valve disease, DCM, and MI, the latter leading to premature death at age 44 years [22]. The phenotype in our patient who carried the p.Asp300Asn is unique and distinct from other progeroid syndromes, as it does not involve other organs. It solely restricted to the heart where it affects multiple structures, including coronary arteries, aortic and mitral valves, conduction system, and the right ventricle. Based on the data presented in this report and the existing data on progeroid syndromes caused by the LMNA mutations involving codon 300, we infer that the p.Asp300Asn is responsible for non-syndromic cardiac progeria in the index patient presented in this report.