Bicuspid Aortic Valve: Genetic and Clinical Insights

• Abstract
• Introduction
• Bicuspid Aortic Valve Genetics: Many Links Yet an Unsolved Riddle
• Nonsyndromic Bicuspid Aortic Valve Genetics
• Syndromic Bicuspid Aortic Valve Genetics
• Animal Models
• Bicuspid Aortic Valve Phenotypes: Sievers Classification
• Cascade Screening: What Is the Clinical Utility?
• Conclusion
• References

Abstract

Bicuspid aortic valve (BAV) is the most common valvular congenital heart disease, with a prevalence of 0.5 to 2% in the general population. Patients with BAV are at risk for developing cardiovascular complications, some of which are life-threatening. BAV has a wide spectrum of clinical presentations, ranging from silent malformation to severe and even fatal cardiac events. Despite the significant burden on both the patients and the health systems, data are limited regarding pathophysiology, risk factors, and genetics. Family studies indicate that BAV is highly heritable, with autosomal dominant inheritance, incomplete penetrance, variable expressivity, and male predominance. Owing to its complex genetic model, including high genetic heterogenicity, only a few genes were identified in association with BAV, while the majority of BAV genetics remains obscure. Here, we review the different forms of BAV and the current data regarding its genetics. Given the clear heritably of BAV with the potential high impact on clinical outcome, the clinical value and cost effectiveness of cascade screening are discussed.

Introduction

Bicuspid aortic valve (BAV) is the most common valvular congenital heart disease, with a prevalence of 0.5 to 2% in the general population.[1] BAV was first described more than 500 years ago by Leonardo da Vinci, illustrating the valve anatomy. Since data on BAV clinical significance have been established, a substantial proportion of aortic valve diseases were found to be due to BAV, regardless of a patient's age.[2] Patients with BAV have an increased risk of developing aortic valve diseases such as calcification and stenosis, regurgitation, and infective endocarditis. Aortopathies are also prevalent among BAV patients. These include coarctation of the aorta, aortic aneurysm, and dissection. BAV patients are prone to require aortic valve replacement (AVR) and aortic surgery, procedures that carry substantial risks and costs.[3] Population-based studies have found a 53% risk for AVR and a 25% risk for aortic surgery during 25-year follow-up, and the risk for aortic dissection was eight times higher than in the general population.[4] Moreover, the mean age for valve replacement or surgical intervention for aortic dilation is markedly younger for BAV patients compared with patients with tricuspid aortic valve.[2] [4] BAV was estimated to cause more morbidity and mortality than the combination of all other congenital heart defects, generating a considerable health burden to both patients and the health system.[5]

BAV can be classified as sporadic BAV (sporadic isolated defect), familial nonsyndromic BAV (nsBAV; in clusters within families without associated anomaly), or syndromic BAV (considered familial and associated with other anomalies including cardiovascular defects). The method of choice for diagnosis and follow-up is echocardiography ([Fig. 1]).

BAV clinical presentation varies significantly from a silent disease to severe life-threatening complications, even at a young age. Little is known about most dimensions of BAV, including the identity of the biochemical pathways involved in its pathogenesis. The determinants of the valve morphology and of the wide spectrum of clinical presentations and complications over time are mostly unelucidated.

Genetic data provide a very powerful and unbiased tool for understanding the basic mechanisms culminating in valve dysfunction and disease. Better understanding of the molecular processes of the disease may lead to future development of novel personalized management approaches, ultimately leading to individual risk stratification, sparing unnecessary interventions to low-risk patients, and preventing potentially fatal complications for patients at high risk.

Here, we summarize the current data regarding BAV genetics and discuss its potential clinical implication.

Bicuspid Aortic Valve Genetics: Many Links Yet an Unsolved Riddle

It is well established that BAV has a significant genetic component.[6] [7] Various studies demonstrated familial clustering of BAV.[7] The prevalence of BAV was found to be 10-fold higher among first-degree relatives of an affected individual compared with the general population.[8] In family studies, the heritability index for BAV, representing the degree of phenotypic variance explained by inherited rather than environmental factors, was found to be as high as 89%, suggesting marked involvement of genetic factors on disease development.[7] Among familial BAV, most pedigrees suggest an autosomal-dominant inheritance pattern with incomplete penetrance and male predominance in a 3:1 ratio[8] ([Fig. 2]). According to Mendelian genetics, autosomal-dominant inheritance pattern implies that half of first-degree relatives are expected to carry the disease-causing allele. Accounting for 50% penetrance (i.e., half of the carriers will demonstrate clinical disease), 25% of first-degree relatives are expected to be clinically affected with BAV. However, the actual rate of BAV among first degree relatives in family studies ranges from 6 to 30%. This large range, along with the wide spectrum of structural and clinical phenotypes, is thought to be the result of the complexity of the developmental mechanisms at play in aortic valve development, involving genetic, epigenetic, and environmental factors ([Fig. 3]).

A high prevalence rate of aorthopathies, including aneurysm, dissection, and aortic coarctation, has been demonstrated among BAV patients and their relatives. Both the aortic root and the aortic valve have the same specific embryologic origin: the cardiac neural crest and the second heart field.[9] Thoracic aortic aneurysm (TAA) frequently affects patients with BAV, or their first-degree relatives with a morphologically normal valve. TAA and BAV are thus thought to have a common genetic etiology.[6] This observation adds support to the concept that BAV does not represent a dichotomous phenotype but would rather be integrated in a continuous spectrum of phenotypic expressions.

Nonsyndromic Bicuspid Aortic Valve Genetics

Since 2005, with the identification of NOTCH1 in nsBAV cases, few other genes were found to be associated with nsBAV with varying degrees of supporting evidence ([Table 1]). Each of these genes explains only a small percentage of the overall nsBAV prevalence and involves different molecular pathways that do not necessarily assemble into one common mechanism. In light of its high phenotypic and genotypic heterogeneity, establishing a genetic causality for BAV is challenging. Causality can only be determined when the mutation has a robust effect, the familial segregation and linkage analyses are strong, and when the association is supported by experimental and functional models.[10]

NOTCH pathway: the first and currently single gene considered definitively causal for nsBAV is NOTCH1.[11] NOTCH1 signaling is a highly conserved pathway of signal transduction, leading to transcription of endothelial and vascular smooth muscle cells. Altered NOTCH signaling is a well-known cause of human cardiovascular disease. NOTCH1 genetic variants were demonstrated to be associated with the development of calcific aortic valve stenosis, with or without BAV. Yet, this gene is estimated to be involved in only approximately 5 to 10% of nsBAV cases, leaving the vast majority of the genetic causes of BAV unexplained. Other members of the NOTCH1 pathway ([Fig. 4]) were linked to BAV and to other left-ventricular outflow tract obstruction pathologies, including mastermind-like transcriptional coactivator 1 (MAML1), rho GTPase activating protein 31 (ARHGAP31), jumonji and AT-rich interaction domain containing 2 (JARID2), and SWI/SNF-related matrix-associated actin-dependent regulator of chromatin, subfamily A, member 4 (SMARCA4).[12]

TGF-β Pathway: The SMAD family member 6 (SMAD6) gene encodes a signal transduction protein highly expressed in the embryonic heart and involved in many pathways, including transforming growth factor beta (TGF-β). This pathway plays a key role in vascular matrix remolding and was linked to connective tissue disorders ([Fig. 4]). The association of SMAD6 with BAV was shown by targeted resequencing of individuals with BAV and TAA, contributing to the development of BAV/TAA in 2.5% of the cases.[13] Recently, T-box transcription factor 20 (TBX20) was identified as a possible contributing gene for BAV using copy number variation analysis, explaining 1% of the BAV/TAA cases.[14] This gene was found to be related to SMAD6 in in-vivo studies, and was described in association to other congenital cardiac malformations.[15] Of note, other components of the TGFβ pathway (TGFβ2, TGF-β3, TGF-ßR1, TGF-ßR2, and SMAD3) are involved in syndromic aortopathies where BAV is present in 5 to 30% of the cases.[16] [17]

The GATA family: GATA binding protein genes encode zinc-finger transcription factors that play a role in heart valve differentiation.[18] GATA4 was recently identified as a predisposing gene for BAV in a human genome-wide association study (GWAS) involving 466 BAV cases and 4,660 controls, with odds ratios ranging from 1.4 to 2.4 depending on the variant.[19] Rare variants of the GATA5 gene, highly expressed in the endocardium, were also linked to nsBAV,[20] although these results have not been consolidated in subsequent studies. A GATA6 disruptive variant was found in an nsBAV family,[21] and in vitro studies demonstrated that GATA6 haploinsufficiency interrupts the aortic valve remodeling and extracellular matrix composition.[22] Loss-of-function mutations in the NK2 Homeobox 5 (NKX2.5) gene, which encodes a homeodomain-containing transcription factor that is involved in the aortic valve development, was found in a nsBAV family to disrupt the interaction between NKX2.5 and GATA5, supporting involvement of both genes in the pathology.[23]

The roundabout guidance receptor 4 (ROBO4) gene is involved in endothelial function. Rare variants in the gene were identified by whole exome sequencing in a BAV/TAA family study.[24]

Genetic loci linked to BAV: linkage analyses demonstrated the involvement of human chromosomal regions 18q, 5q, and 13q in BAV alone, and between BAV/TAA and human chromosomal regions 15q25–26,[25] suggesting that unelucidated genetic defects remain to be investigated.

Syndromic Bicuspid Aortic Valve Genetics

BAV can be syndromic, that is, presenting within a constellation of cardiac and noncardiac anomalies ([Table 2]). The highest occurrence of BAV is found in Turner's syndrome. Turner's syndrome results from complete or partial missing of one X chromosome (45X). This leads to a complex developmental disorder, including cardiovascular anomalies. BAV occurs in 15 to 30% of patients and often coexists with coarctation of the aorta.[26] The high prevalence of BAV in Turner's syndrome may be related to high diagnostic rate due to routine cardiac imaging performed in these patients, but may also suggest X-chromosome involvement in BAV formation. This is also supported by the 3:1 male predominance found in BAV, leading to the hypothesis that X chromosome gene hemizygosity (i.e., having one copy only) is involved in BAV development.

Marfan's syndrome (MFS) is a rather common connective tissue disorder manifesting by aortic root dilation among other phenomena. BAV was initially considered more prevalent than in the general population.[27] A recent larger study that included more than 1,400 MFS case, has demonstrated that the prevalence of BAV was 1.8%, equivalent to the population prevalence.[28] However, BAV presentation in MFS was associated with a more severe aortic aneurysm phenotype necessitation repair at an earlier age.[27]

Loeys–Dietz syndromes are a group of connective tissue disorders close to MFS. These syndromic aortopathies are the consequence of abnormal TGF-β signaling, and association with BAV was demonstrated.[17]

As illustrated here, the frequent cooccurrence of BAV and aortic aneurysms in nsBAV and in sporadic BAV, is also the rule in syndromic BAV, supporting the hypothesis that disruption of connective tissue homeostasis is related with BAV.

BAV was also described in Shone complex, a syndrome of multiple left heart obstructive lesions. Like nsBAV, it was also associated with NOTCH1 mutations.[29] BAV is also present in other systemic disorders, such as DiGeorge's syndrome (22q11 deletion), Down's syndrome, and Andersen's syndrome, at very lower frequency. The malformation is also reported in association with other isolated cardiovascular disorders[30] including hypoplastic left heart syndrome, coarctation of the aorta, ventricular septal defects, patent ductus arteriosus, and atrial septal defects.[31]

Animal Models

Animal models may serve as an additional approach for understanding BAV genetics and pathophysiology. There are several mouse and Syrian hamster models for BAV, some of which were developed to support candidate genes found in humans. Of note, similarly to family studies in humans, all animal models have demonstrated incomplete penetrance and, in most cases, presented with other cardiac malformations. In some, male predominance was also observed.[32] The main human and mouse genes involved in BAV are listed in [Table 1].

Notch1 knockout (KO) mice die from cardiac malformation. These mice developed severe aortic valve calcification. Disruption of the Robo signaling pathway (Robo1 and Robo2) in transgenic mice led to BAV development.[33] This pathway was shown to play a role in Notch regulation and was also associated with BAV in humans. The Gata gene family (Gata4, Gata5, and Gata6) was linked to BAV in mice, as well as in humans, leading to BAV with variable penetrance ([Table 1]). Nitric oxide synthase (Nos) produces nitric oxide (NO) that has an important role in cell growth and apoptosis. Mice with induced endothelial NOS-deficiency demonstrated abnormal aortic valve development including BAV.[32] A significantly reduced expression of NOS protein was demonstrated in aortic endothelial cells from BAV patients as compared with normal valve controls.[34] Nkx2–5 KO mice developed BAV among other septal and valvular malformations.[35] This gene is a notable example of a pleiotropic genetic effect (in which one gene leads to more than one phenotype).[35] Notably, a pleiotropic effect is far more often the rule than the exception in many congenital heart disease genes. Tissue-specific KO of activin A receptor type 1 (Acvr1) resulted in aortic valve disorders including BAV, supporting the gene's role in valvular development as seen in TAAD/BAV human cases.[36] However, there is not a full correspondence between the genetic landscapes in mice and in humans. As an example, ROBO4 has been involved in BAV/TAA in humans at heterozygous state with high penetrance, but the effect of complete (homozygous) Robo4 loss of function in mice shows a very low penetrance (15%) with a variety of aortic valve defects.[24]

Bicuspid Aortic Valve Phenotypes: Sievers Classification

Anatomically the bicuspid valve morphology phenotypes are classified according to the cusp's fusion. A “pure” form of BAV consists of two cusps of equal size with no raphe between them and is relativity rare, while the more common configuration of bicuspid valve consists of two unequal cusps, the larger one characterized by a raphe formed between the two fused cusps. A rare form of unicuspidal valve is also found. The BAV morphology type is usually defined by echocardiography and is classified according to Sievers classification as follows: type 0 (no raphe); type 1 (one raphe) with subtypes (1) 1 LR for left–right coronary cusps fusion, (2) 1 RN for right and noncoronary, and (3) 1 NL for noncoronary and left coronary cusps; and type 2 (two raphes). Each morphology type is associated with different pathologies of the valve and the aorta, and may even affect prognosis.[37] It was hypothesized that the different types developed from distinct embryological origins.[38] Our data, as well as previously published data, show, in a large set of pedigrees, that different BAV types are present in a family.[39] [40] To date, no correlation between Sievers type BAV and genetic status was demonstrated. This, once again, highlights the complexity of BAV genetics and phenotypic variability.

Cascade Screening: What Is the Clinical Utility?

High heritability of BAV raises the question of “cascade screening” of relatives of a BAV case. Cascade screening is a method to identify individuals at risk for a genetic condition by the process of systematic screening of first-degree relatives of the index case. The 2014 American Heart Association/American College of Cardiology (AHA/ACC) valvular heart disease guidelines recommend clinical screening of first-degree relatives only if the patient with BAV has an associated aortopathy or a family history of valvular heart disease or aortopathy.[41] There is no clear recommendation, however, for screening in patients with noncomplicated BAV. The European Society of Cardiology and the European Association for Cardio-Thoracic Surgery guidelines for the management of valvular heart disease consider BAV as a risk factor for aortic regurgitation and suggest echocardiographic screening of first-degree relatives.[42] The Canadian Cardiovascular Society indicated screening by echocardiography of first-degree relatives of bicuspid patients, including screening of family members in the pediatric age range.[43] The screening examination by echocardiography itself does not involve any risk for the patient. It can detect BAV or associated pathologies at an early stage and hence prevent complications. This, however, may come at a considerable emotional burden to the families. As described above, 6 to 30% of first-degree relatives are expected to have BAV or related anomaly. It is currently not clear how many of these will clinically benefit from familial screening. Cost analysis studies have demonstrated a significant cost-effectiveness for echocardiography screening.[44] [45] Additional studies are needed to establish the best terms and timing of the optimal screening program.

Conclusion

Even after more than 500 years of its first description by Leonardo da Vinci, BAV still poses a great challenge to clinicians. It presents with a wide clinical and structural phenotypic spectrum, from a silent malformation to a severe complicated disease with significant morbidity and mortality. Biological research to understand BAV and its cause, as in other cardiac malformations, is very active since the discovery of NOTCH1 role in BAV. Complimentary genetic approaches, including association, linkage, and candidate-gene studies, have allowed identification of few other genes, accounting for only a small fraction of the genetic weight in the disease, and our understanding remains very limited. This is probably explained by a complex developmental process. Epigenetic and microenvironmental factors might weight more significantly than expected, unveiling complex inheritance including polygenic involvement. Deciphering genetic models of BAV is now the new challenge, aiming at the objective of optimizing patient's risk stratification and clinical management according to the individual risk.

Conflict of interest

The authors declare no conflict of interest related to this article.

Acknowledgment

Dr. Tessler thanks Ilai Ovadia for his contribution in designing the figures.

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Address for correspondence

Publikationsverlauf

Eingereicht: 22. April 2020

Angenommen: 25. Februar 2021

Artikel online veröffentlicht:
03. Dezember 2021

© 2021. The Author(s). This is an open access article published by Thieme under the terms of the Creative Commons Attribution License, permitting unrestricted use, distribution, and reproduction so long as the original work is properly cited. (https://creativecommons.org/licenses/by/4.0/)

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• References

• 1 Braverman AC. The bicuspid aortic valve and associated aortic disease. In: Otto CM, Bonow RO. eds. Valvular Heart Disease. 4th ed.. Philadelphia, PA: Saunders/Elsevier; 2013: 179-198
  Google Scholar
• 2 Roberts WC, Ko JM. Frequency by decades of unicuspid, bicuspid, and tricuspid aortic valves in adults having isolated aortic valve replacement for aortic stenosis, with or without associated aortic regurgitation. Circulation 2005; 111 (07) 920-925
  CrossrefPubMedGoogle Scholar
• 3 Tzemos N, Therrien J, Yip J. et al. Outcomes in adults with bicuspid aortic valves. JAMA 2008; 300 (11) 1317-1325
  CrossrefPubMedGoogle Scholar
• 4 Michelena HI, Khanna AD, Mahoney D. et al. Incidence of aortic complications in patients with bicuspid aortic valves. JAMA 2011; 306 (10) 1104-1112
  CrossrefPubMedGoogle Scholar
• 5 Ward C. Clinical significance of the bicuspid aortic valve. Heart 2000; 83 (01) 81-85
  CrossrefPubMedGoogle Scholar
• 6 Loscalzo ML, Goh DLM, Loeys B, Kent KC, Spevak PJDH, Dietz HC. Familial thoracic aortic dilation and bicommissural aortic valve: a prospective analysis of natural history and inheritance. Am J Med Genet A 2007; 143A (17) 1960-1967
  CrossrefPubMedGoogle Scholar
• 7 Cripe L, Andelfinger G, Martin LJ, Shooner K, Benson DW. Bicuspid aortic valve is heritable. J Am Coll Cardiol 2004; 44 (01) 138-143
  CrossrefPubMedGoogle Scholar
• 8 Siu SC, Silversides CK. Bicuspid aortic valve disease. J Am Coll Cardiol 2010; 55 (25) 2789-2800
  CrossrefPubMedGoogle Scholar
• 9 Martin PS, Kloesel B, Norris RA, Lindsay M, Milan D, Body SC. Embryonic development of the bicuspid aortic valve. J Cardiovasc Dev Dis 2015; 2 (04) 248-272
  CrossrefPubMedGoogle Scholar
• 10 Marian AJ. Causality in genetics: the gradient of genetic effects and back to Koch's postulates of causality. Circ Res 2014; 114 (02) e18-e21
  CrossrefPubMedGoogle Scholar
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