Abstract
Mitral valve prolapse (MVP) is a commonly occurring heart condition defined by enlargement and superior displacement of the mitral valve leaflet(s) during systole. Although commonly seen as a standalone disorder, MVP has also been described in case reports and small studies of patients with various genetic syndromes. In this review, we analyzed the prevalence of MVP within syndromes where an association to MVP has previously been reported. We further discussed the shared biological pathways that cause MVP in these syndromes, as well as how MVP in turn causes a diverse array of cardiac and noncardiac complications. We found 105 studies that identified patients with mitral valve anomalies within 18 different genetic, developmental, and connective tissue diseases. We show that some disorders previously believed to have an increased prevalence of MVP, including osteogenesis imperfecta, fragile X syndrome, Down syndrome, and Pseudoxanthoma elasticum, have few to no studies that use up‐to‐date diagnostic criteria for the disease and therefore may be overestimating the prevalence of MVP within the syndrome. Additionally, we highlight that in contrast to early studies describing MVP as a benign entity, the clinical course experienced by patients can be heterogeneous and may cause significant cardiovascular morbidity and mortality. Currently only surgical correction of MVP is curative, but it is reserved for severe cases in which irreversible complications of MVP may already be established; therefore, a review of clinical guidelines to allow for earlier surgical intervention may be warranted to lower cardiovascular risk in patients with MVP.
Keywords: Ehlers‐Danlos syndrome, heart failure, Loeys‐Dietz syndrome, Marfan, MASS phenotype, mitral regurgitation, mitral valve prolapse
Subject Categories: Arrhythmias, Genetics, Animal Models of Human Disease, Valvular Heart Disease, Cardiovascular Surgery
Nonstandard Abbreviations and Acronyms
- ADPKD
autosomal dominant polycystic kidney disease
- BDCS
Boronne Dermato‐Cardio‐Skeletal syndrome
- DZIP1
DAZ interacting protein 1
- ECM
extracellular matrix
- EDS
Ehlers‐Danlos syndrome
- IE
infective endocarditis
- LDS
Loeys‐Dietz syndrome
- MASS
mitral, aorta, skeleton, and skin
- OI
osteogenesis imperfecta
- SCD
sudden cardiac death
- SH3PXD2B
SH3 and PX domains 2B
- TGF‐β
transforming growth factor‐beta
Mitral valve prolapse is a common heart condition that is estimated to affect 2% to 3% of individuals.1 The defining finding in mitral valve prolapse (MVP) is myxomatous degeneration of the mitral valve leaflets,2 which eventually leads to structural incompetence and superior displacement of one or both mitral leaflets into the left atrium (LA) during systole.3 Though it is recognized as a highly prevalent heart condition, the question of whether it is benign has been hotly disputed over the years.1, 4, 5, 6 After initially being described as a risk factor for several diseases including heart failure, atrial fibrillation, stroke, mitral regurgitation, and others,4, 7 an analysis of the Framingham Heart Study offspring cohort in 1999 disputed these findings, arguing that many of these associations were made in hospital‐based cohorts, and therefore patients were sicker and more likely to have comorbid disease.1 Subsequently, a community study of asymptomatic patients with mitral valve prolapse disputed these findings, and reported that the clinical course was much more heterogeneous than described in the Framingham study.8
Despite the controversy, it is now well recognized that mitral valve prolapse poses a significant disease burden and is a major contributor to cardiovascular morbidity and mortality. Based on the prevalence estimates at 2% to 3%, it is hypothesized that >7.8 million people in the United States, and >176 million people worldwide, are living with MVP.3 Another study published in 2020 estimates that prevalence worldwide of degenerative mitral valve disease, defined as myxomatous degeneration of the mitral valve leading to hemodynamically moderate or severe mitral regurgitation, is 18.1 million people (95% uncertainty interval [UI], 17.6 million to 18.6 million) and that the mortality rate from degenerative mitral valve disease in 2017 was 35 700 people (95% UI, 30 500–42 500).9 The discrepancy in prevalent cases between these 2 studies is likely attributable to a more stringent definition of degenerative mitral valve disease, which excludes patients with myxomatous degeneration who have mild or absent regurgitation. Further, it is unclear from the published data whether the mortality associated with degenerative mitral valve disease is a direct result of the valvular dysfunction itself, or as a result of recognized nonvalvular complications of mitral valve disease. Greater than 90 000 mitral valve surgeries occur each year making it the fastest growing cardiovascular intervention in the United States.10 Further, no Food and Drug Administration approved medical treatments exist for MVP, meaning surgical or percutaneous correction is the only treatment available to patients.
The purpose of this review was to summarize and analyze the current understanding of comorbid conditions with MVP. MVP has been identified as a component of many genetic syndromes,11 and genome‐wide association studies have identified primary loci thought to be important for MVP pathogenesis. Further, both cardiac and non‐cardiac diseases have been associated with MVP. An important consideration is that most, if not all, of the publications cited in this manuscript use Barlow disease and MVP interchangeably. There is an important distinction between these 2 types of mitral valve disease. Barlow disease is characterized by pronounced annuluar dilatation, bileaflet prolapse and/or billowing, hooding, and the presence of thick, spongy leaflets because of excessive myxomatous tissue proliferation with or without calcification. The terminology of Barlow does not apply to all cases of MVP, especially in terms of single leaflet prolapse. As these distinctions are generally not well documented in the literature, we will use the more encompassing term of MVP. The following review will focus on analyzing the shared pathophysiology between MVP and other diseases, and the unique pathways that exist in MVP.
Clinical Characteristics of MVP
A diagnosis of MVP is not reliably made using clinical symptoms. In fact, patients with MVP appear to exhibit symptoms that have been previously attributed to MVP (dyspnea, chest pain, and electrocardiographic abnormalities) at an equivalent rate to patients without any identifiable prolapse.1 Even patients with quite severe regurgitation as a result of prolapse may be asymptomatic.8 As such, symptoms should not be used to diagnose MVP, although the presence of symptoms warrant further investigation. Physical exam findings that are associated with MVP include a lower body mass index and a mid‐systolic "click" heard best at the apex on cardiac auscultation.12, 13 A late systolic or holosystolic murmur may be appreciated as well, and suggests the presence of mitral regurgitation.14 Thoracic, or bony abnormalities, as well as other extra‐cardiac findings may suggest the presence of MVP as part of a syndrome.15 Physical exam findings should also not be used to diagnose MVP, as the presence of any of these findings are not sensitive or specific enough to accurately make a diagnosis.12 Echocardiography is the gold standard for diagnosis, as it provides a high‐resolution and dynamic view of the three‐dimensional mitral valve, can quantify leaflet involvement, and is able to detect and quantify characteristics of more severe disease, such as annulus dilation, flail leaflet because of chordal rupture, and severity of regurgitation.4 Cardiac magnetic resonance imaging may also have a place in the MVP workup, as it is exquisitely sensitive and specific, and is able to uniquely detect and quantify fibrosis in patients with MVP by measuring late gadolinium enhancement.16 Electrocardiography or 24‐hour Holter monitoring may also provide utility in the workup of MVP, as both atrial and ventricular arrhythmias may arise in these patients. Patients who experience an increased burden of premature ectopic beats (such as premature ventricular contractions [PVCs]) are at an increased risk of developing more severe, even life‐threatening arrhythmias.17, 18 Many studies have reported a high PVC burden in patients with MVP. In a recent review of patients with MVP who experienced sudden cardiac death, 92% experienced PVCs on Holter monitoring,19 and in another electrophysiologic study, PVCs were identified as a trigger for more complex, life threatening arrhythmias in patients with MVP.20 As such, there is an opportunity to risk stratify patients with MVP using Holter monitoring, to identify subsets of patients who are at an increased risk for sudden cardiac death.
Primary MVP
MVP has been found to follow 2 inheritance patterns: X‐linked and, more commonly, autosomal dominant, but age and sex penetrance combined with phenotypic heterogeneity have made the genetics largely elusive.21, 22, 23 In recent years there has been significant progress in finding genes associated with nonsyndromic autosomal dominant MVP. It was suggested very early on that variations in a collagen gene were to blame since MVP is a common comorbidity of connective tissue disorders, including Marfan Syndrome, and pathological evidence points to an extracellular matrix (ECM) defect.24 However, this idea was discredited in 1989 and no evidence has been found to support it.25, 26 Pedigree linkage studies first demonstrated the immense genetic heterogeneity associated with MVP, identifying 3 loci linked to non‐syndromic autosomal dominant MVP.27, 28, 29
Further investigation into the locus on chromosome 11 associated with MVP led to the discovery of the first gene known to cause nonsyndromic autosomal dominant MVP in humans, DCHS1 (dachsous cadherin‐related 1), which codes for a protein within the cadherin family expressed in fibroblasts.30 Mice with decreased levels of DCHS1 have enlarged mitral leaflets and a missense mutation within DCHS1 segregates with MVP in a large family pedigree.30 However, how decreased DCHS1 expression affects mitral valve development to cause MVP remains unknown.
Significant progress was made in 2015 with the first population‐based genome wide association study of nonsyndromic autosomal dominant MVP.31 This meta‐analysis of 2 GWAS (Genome‐wide association study) for MVP discovered 6 new loci and 2 functional candidate genes, Tensin 1 (TNS1) and LIM and cysteine rich domains protein 1 (LMCD1).31 TNS1 knockout mice have abnormal mitral valves, including thicker posterior mitral leaflets and signs of myxomatous degeneration.31 LMCD1 acts as a co‐regulator of transcription and has been exhibited as a repressor of GATA6 (GATA binding protein 6) a transcriptional regulator important for cardiac development.32 In fact, both TNS1 and LMCD1 are involved in cellular proliferation and migration during valvular development, and it is thought that mutations in these genes cause MVP by affecting embryonic valvulogenesis.31 To date, no additional studies connecting these 2 genes to nonsyndromic autosomal dominant MVP have been done.
Recently, a cilia gene, DZIP1, which encodes DAZ interacting zinc finger protein 1, was identified as a causal gene for nonsyndromic autosomal dominant MVP in humans. A deleterious missense mutation in DZIP1 segregates with MVP in a large family pedigree. Mice with a similar missense mutation knocked in to their DZIP1 locus develop functional MVP with evidence of defects in ciliogenesis during development.33 Population burden tests using previously performed GWAS data sets revealed a bias towards primary cilia genes as contributing to disease phenotype.32. Together, these findings implicate MVP as originating from development defects as well as the disease being considered a ciliopathy. However, because of its genetic and clinical heterogeneity, additional studies need to be done to determine how many cases of MVP are a result of impaired ciliogenesis.
Syndromic MVP
Marfan Syndrome
Marfan syndrome is a rare autosomal dominant connective tissue disorder that affects that affects 1 in 5000 patients.34 Manifestations of Marfan syndrome are diverse, and tend to affect the ocular, musculoskeletal, and cardiovascular systems.35, 36 As a result of its pleiotropic presentation, the diagnosis of Marfan syndrome is made using a clinical assessment known as the Ghent criteria, a specific test which scores the likelihood that a patient has Marfan syndrome over other, similar connective tissue disorders.37 Advances in molecular and genetic testing have further allowed for confirmation of patients who are suspected of having Marfan syndrome and who score positive on the Ghent criteria.38, 39 As a result, extensive clinical analysis of the phenotypic presentation of genetically confirmed patients with Marfan syndrome exists in the literature. Cardiovascular complications represent the main cause of death in Marfan syndrome, with the majority of fatal events occurring because of aortic pathology including aneurisms, and dissections.40 In addition, large numbers of patients diagnosed with Marfan have coexistent MVP; our analysis found a median prevalence of 56.7% (range, 21.9%–100%, Figure S1).41, 42, 43, 44, 45, 46, 47, 48, 49, 50, 51, 52, 53, 54, 55, 56, 57, 58, 59, 60, 61, 62, 63, 64, 65, 66, 67 Indeed, the presence of MVP is considered a minor feature of Marfan syndrome within the most recent Ghent criteria, and is included within the scoring criteria.37
Fibrillin‐1 (FBN1) mutations have been implicated as the major disease‐causing variants within patients with Marfan Syndrome, although other mutations within fibrillin‐2 have been shown to cause Marfan Syndrome.68 Fibrillins are a high molecular weight ECM protein that possesses both structural and nonstructural functions. Structurally, fibrillins are a component of microfibrils, which are complexes of multiple ECM proteins including elastin, that provide mechanical and elastic support to the connective tissues.69 Nonstructurally, fibrillins have been shown to play a role in the regulation of cell signaling, and possess structural similarity to LTBPs (latent transforming growth factor beta binding proteins).68 LTBPs bind transforming growth factor‐beta (TGF‐β) and regulate its ability to interact with its receptors, thereby decreasing TGF‐β signaling when present. Fibrillin mutations decrease the ability for the fibrillin protein to act as an LTBP, and decrease sequestration of the large, latent TGF‐β complex, thereby exposing TGF‐β more easily to cell surface receptors.70 This leads to increased TGF‐β‒mediated cell signaling, through canonical and noncanonical TGF‐β signaling pathways, the proliferation of valve interstitial cells, and activation of these cells to secrete ECM proteins.71, 72 TGF‐β signaling has been shown to be a critical driver of MVP within Marfan syndrome, and inhibition of TGF‐β signaling using antibodies is able to stop the progression of MVP in mice.71 More recently, inflammatory cells have been implicated as drivers of MVP progression in Marfan syndrome, though to what extent the immune system is involved in disease initiation remains unanswered.73
Mitral Aorta Skeleton and Skin Phenotype
The mitral, aorta, skeleton, and skin (MASS) phenotype is a marfanoid syndrome that consists of phenotypes involving MASS, but that doesn't meet the Ghent criteria for Marfan syndrome. As would be expected, MVP is seen at a high prevalence in patients with MASS phenotype. Our analysis shows a median prevalence of 74.3% of MVP in patients diagnosed with the MASS phenotype (Figure S1).44, 74, 75 The genetic basis of MASS phenotype is currently unknown, although some patients who presented with MASS had identifiable FBN1 mutations, leading some researchers to believe that this condition is a milder form of Marfan syndrome.44 As such, it is likely that aberrant TGF‐β signaling drives the progression of MVP in patients with MASS, though this has not been investigated.
Loeys‐Dietz Syndrome
Loeys‐Dietz syndrome (LDS) is a rare autosomal recessive connective tissue disorder caused by aberrant TGF‐β signaling. It is most often caused by mutations in the TGF‐β receptor 1 and 2 genes, though mutations in mothers against decapentaplegic homolog 3(SMAD3), as well as TGFB2, and TGFB3 have also been reported to cause LDS.76, 77 Mild forms of the disease may resemble Marfan syndrome, whilst very severe disease can result in death in childhood as a result of aggressive arterial aneurisms.78 As in Marfan syndrome, MVP is enriched in patients with LDS, although to a lesser extent than is seen in Marfan. Our analysis found a median prevalence of 25% in studies that assessed prevalence of MVP in LDS (Figure S1).41, 53, 76 It seems counterintuitive that a more aggressive marfanoid syndrome would cause a lower prevalence of MVP. Why fewer patients with LDS get prolapse is not well understood.
As with Marfan syndrome, excessive TGF‐β signaling has been implicated as the stimulus for the development of MVP in both Marfan and LDS.76 In LDS, it has been observed that although mutations in the TGF‐β receptor would in theory decrease downstream signaling, a paradoxical increase in SMAD2 phosphorylation is observed in these patients, along with an increase in connective tissue growth factor, a TGF‐β responsive, SMAD‐dependent growth factor, suggesting that mutations result in an increase in signaling.76 This suggests that perhaps TGF‐β is signaling through a different receptor, though it is not known what other receptors may be hyperactivated in this disease state. Furthermore, these recent data seem to dispute other studies that have found that TGF‐β receptor mutations cause a decrease in not only the production of mature receptor, but also a decrease in activation, turnover, and downstream signaling.79 Multiple theories have been proposed to try and rectify the discrepancy, including a loss of canonical TGF‐β‒dependent negative feedback leading to excessive noncanonical TGF‐β signaling, and cell‐dependent effects of loss of TGF‐β.80 Nonetheless, more rigorous interrogation of how canonical TGF‐β pathway disruption leads to MVP are required.
Ehlers‐Danlos Syndrome
Ehlers‐Danlos syndrome (EDS) refers to a heterogeneous group of connective tissue disorders that share some common clinical phenotypes, including joint hypermobility, tissue fragility, and skin hyperextensibility.81 Currently, 13 subtypes of EDS have been identified. Most subtypes of EDS are diagnosed using genetic testing, however, hypermobile EDS, the most common EDS subtype, has no identified genetic cause.81 Hypermobile EDS is therefore diagnosed using clinical criteria, which may obfuscate more mild cases and prevent a definitive diagnosis.81 Although initial discoveries implicated mutations in fibrillar collagen as the cause, subsequent studies on patients with EDS have identified many genes that cause different subtypes of EDS, and are important for collagen biosynthesis and processing, proteoglycan synthesis, and innate immunity. Thus, EDS, though often taught to be a disorder of impaired collagen production to medical students, is significantly more diverse and mechanistically much more complicated.
In addition to many musculoskeletal, autonomic, neurologic, gastrointestinal, and psychiatric manifestations that are seen in patients with EDS, cardiac and vascular manifestations may also be seen. Cardiovascular manifestations are common with subtypes of EDS, in particular vascular EDS, a hallmark of which is brittle vasculature, putting patients at risk of arterial rupture.82 Furthermore, a report identified a cardiac valvular subtype of EDS, in which a series of patients with a collagen type 1 alpha 2 chain mutation were diagnosed with EDS or other similar connective tissue disorders, all of whom had cardiac valvular involvement.83 Cardiac involvement in most other subtypes of EDS is thought to be uncommon, but has been reported in previous literature.84, 85, 86, 87, 88 MVP is mildly enriched in patients with EDS compared with the general population; in studies included in this review, the median prevalence of MVP was 6.2% (range, 2.6%–66.7%) in patients with a diagnosis of EDS with no further classification of subtype (Figure S1).84, 85, 86, 87, 88
The pathophysiology of MVP in patients with EDS is currently not well understood. Most of the genes that are known to cause EDS are associated with the biosynthesis, processing, and turnover of ECM components such as collagen which are important for connective tissue stiffness and strength. It could be hypothesized that less abundant, or less organized collagen causes decreased stiffness and increased flexibility of the connective tissue which results in an increased amount of biomechanical tension within the valve in response to the high pressures exerted on the valve during systolic contraction of the LV. This increase in biomechanical tension may stimulate biomechanical signaling within the valve, activating valve interstitial cells to increase production of glycosaminoglycans and other ECM proteins within the valve; indeed increasing biomechanical forces on valve interstitial cells has been shown to increase the synthesis of ECM proteins.89 Analytical studies of the mitral valve architecture in patients with EDS would be illuminating to better understand how mutations in collagen genes affect valve structure and function.
Ebstein Anomaly
Ebstein anomaly is a developmental heart defect characterized by inferior displacement of the proximal attachments of the tricuspid valve leaflets from the atrioventricular valve ring, resulting in an “atrialized” portion of the right ventricle.90, 91 Ebstein anomaly occurs in ≈1 in 14 000 live births, and has been associated with other cardiovascular defects, including MVP.90, 91, 92, 93, 94, 95, 96, 97 In studies included in this review, we found the median prevalence of MVP was 11.4% in patients who were born with Ebstein anomaly (Figure S1).90, 92, 93, 94, 95, 96, 97, 98 The precise mechanism of MVP development in Ebstein anomaly is not known, but that is unsurprising since the precise cause of Ebstein anomaly is also not known. Lithium, a mood stabilizer used to treat bipolar disorder, was originally thought to be a major causative factor in Ebstein anomaly, and was thought to affect cardiovascular development during the first trimester, although more recent studies dispute this finding.99, 100 In addition, family studies have shown several genes that are associated with Ebstein anomaly.101, 102, 103 The future will hopefully shed light on the precise mechanism of development of Ebstein anomaly.
Familial Myxomatous Valvular Degeneration
Familial myxomatous valvular degeneration, also called familial cardiac valvular dystrophy, is a heterogeneously defined group of disorders characterized by myxomatous degeneration in multiple heart valves.104, 105 The median prevalence of MVP in patients with familial myxomatous valvular degeneration is 38.1% in studies that our analysis identified (Figure S1).104, 105 Mutations in the Xq28 gene encoding filamin A has been found to cause familial myxomatous valvular degeneration.104, 105 In animal studies, knockout of Filamin A was demonstrated to cause enlargement of the mitral valve in the fetal period that progressed to MVP by 2 months of age.106 Further, filamin A mutations were found to disrupt the interactions between filamin A and PTPN12, a tyrosine phosphatase that is a key regulator of cell‐ECM crosstalk, in a yeast 2‐hybrid screen.107 Loss of this interaction appears to disrupt integrin‐mediated adhesion and endothelial cell migration in the developing mitral valve, leading to a structurally weak mitral valve. Further, mechanical stress on the mitral valve has been shown to affect the affinity of filamin A to its binding partners, though no study has specifically looked at the filamin A‐PTPN12 interaction in the context of mechanical stress.108 One recent study also highlights a potential interaction between components of the serotonergic signaling cascade. This may be relevant in light of carcinoid mitral valves, which stem from hyperstimulation of serotonin system on valve endothelial cells.106 Taken together, filamin A disrupts cell behaviors during heart development, and provides a developmental substrate for hemodynamically induced myxomatous degeneration of the mitral valve.
Fragile X Syndrome
Fragile X syndrome is the leading inherited form of intellectual disability. It is a trinucleotide repeat disorder caused by an increase in CGG repeats in the fragile X mental retardation protein translational regulator 1 (FMR1) gene to >200, at which point FMR1 becomes silenced. This gene is critically important for gene transcription, particularly for formation of neuronal synapses; as such, inactivation leads to a decrease in neural connectivity and neuroplasticity, which leads to intellectual disability. In addition to intellectual disability, fragile X is associated with other developmental defects, including (wide set ears, macroorchidism, and cardiac anomalies, including MVP). In our analysis, a median of 37.8% of patients who had fragile X syndrome were found to have coexistent MVP (Figure S1).109, 110, 111, 112, 113, 114 An important caveat to this analysis should be made—nearly all studies that assess the prevalence of MVP within fragile X syndrome patients were conducted before the revision of clinical guidelines for the diagnosis of MVP, and as such, prevalence is likely overestimated. However, the biological pathway responsible for MVP as a result of FMR1 gene silencing has yet to be identified.
Juvenile Polyposis Syndrome
MVP has been reported in juvenile polyposis syndrome. A family study of 4 patients with juvenile polyposis syndrome found that half also had MVP, demonstrating an enrichment for this phenotype, though larger scale analysis of patients with juvenile polyposis syndrome needs to be done to assess the true prevalence of MVP.115 Mutations in SMAD4, a co‐SMAD that complexes with phosphorylated SMAD2 as part of the TGF‐β signaling pathway, has been identified as the cause of juvenile polyposis syndrome, aortopathy, and mitral valve features in these patients. This once again demonstrates the importance of TGF‐β signaling in the mitral valve.115
Osteogenesis Imperfecta
Osteogenesis imperfecta (OI) is a connective tissue disorder characterized by abnormally brittle bones and an increased risk of fractures that is apparent in early infancy or even prenatally.116 There are 4 subtypes of OI that differ in level of severity; type 1, the most common, is typically a milder form of disease, type 2 is frequently lethal at birth, and types 3, and 4 are of varying severity.117 Most subtypes of OI are caused by mutations in the procollagen subunits, that cause abnormal truncation of 1 of the 3 subunits, which leads to abnormal triple helix formation, and subsequent intracellular or extracellular degradation before it can be incorporated into the collagen fibers.117 As with many connective tissue disorders, MVP has been reported at increased frequency in OI patients. However, our analysis identified only a mildly increased prevalence; a median of 5.4% of patients with OI had MVP in 4 studies (Figure S1).118, 119, 120, 121 It has been theorized that MVP is not seen at an increased frequency in patients with OI; MVP was over‐diagnosed through the use of M‐mode echocardiography before guideline revisions came into effect in the early 2000s, and studies before that had proposed that the prevalence of MVP in the general population was similar to that seen in patients with OI.119 As a result, no studies have looked into how MVP occurs in OI.
Mucopolysaccharidosis
Mucopolysaccharidosis is a family of disorders that occur because of mutations in lysosomal enzymes that degrade glycosaminoglycans.122 There are 11 different enzyme deficiencies that give rise to 7 different identifiable subtypes of mucopolysaccharidosis. Deficiencies of these enzymes leads to accumulation of glycosaminoglycan substrates, which results in end organ dysfunction that can be more mild or more severe depending on the amount of residual enzyme activity.123 Cardiovascular manifestations are common in mucopolysaccharidosis, and include thickening of the interventricular septum, asymmetric septal hypertrophy, and valvular issues, including MVP.122 Our analysis of 3 studies that were comprised of patients with all 6 different types of mucopolysaccharidosis found that the median prevalence of MVP was 11.5% (Figure S1).122, 124, 125 Importantly, all studies analyzed found that mucopolysaccharidosis type III, also called Sanfilippo syndrome, was associated with a lower risk of MVP compared with other types of mucopolysaccharidosis.122, 124, 125 It is thought that decreased metabolism of glycosaminoglycans leads to an accumulation of dermatan sulfate in the cardiac valvular tissue, causing valve thickening which, over time, can cause further enlargement, mechanical incompetence, and the development of cardiac valve pathology.122
Pseudoxanthoma Elasticum
Pseudoxanthoma elasticum is a heritable connective tissue disorder characterized by calcification of elastin fibers of the skin, arteries, and retina that eventually causes loss of skin elasticity, arterial insufficiency, and macular degeneration.126 Patients with Pseudoxanthoma elasticum have characteristic yellowing, grouped papules, and plaques present on the skin of flexural areas of the body.127 Cardiovascular complications are common in Pseudoxanthoma elasticum, and typically are related to premature atherosclerotic calcification, and loss of elasticity of the arteries.127 In addition, MVP has been reported. Our analysis found that a median of 43.4% of patients with Pseudoxanthoma elasticum had MVP, though the 2 studies that assessed prevalence had significantly divergent findings, and were conducted before the adaptation of new diagnostic guidelines for MVP (Figure S1).127, 128 The precise mechanism linking Pseudoxanthoma elasticum to MVP is not known; theories have suggested that abnormal degeneration of collagen, destruction of elastin, or myocardial ischemia and subsequent chordal rupture could all be the shared pathway between the 2 disorders.127, 128
Stickler Syndrome
Stickler syndrome is an autosomal dominant disorder of collagen connective tissue that results in ocular, skeletal, otologic and joint abnormalities.129 Mutations in the genes that encode type II and type XI collagen have been identified as causative for Stickler syndrome.129 To our knowledge, 2 studies assessed MVP prevalence in patients with Stickler syndrome.129, 130 The first study, conducted in 1986, found a nearly 50% prevalence of MVP in affected patients, while the second study, which used more current echocardiographic diagnostic criteria, found 0 of 78 patients analyzed had MVP.129, 130 As such, it is suggested that Stickler syndrome is not in fact associated with an increase in MVP prevalence.
Down Syndrome
Down syndrome, also called trisomy 21, is a chromosomal abnormality that results from meiotic non‐disjunction of chromosome 21, Robertsonian translocation of a large part of chromosome 21, or a somatic nondisjunction event early in embryologic life that causes 3 copies of chromosome 21 to be present in the majority of cells. Cardiovascular manifestations are common in Down syndrome and include MVP, which has a median prevalence of 31.4% in the 7 studies analyzed for this review (Figure S1).131, 132, 133, 134, 135, 136, 137, 138 The precise cause of MVP in Down syndrome is unclear. However, it is known that patients with Down syndrome have joint and ligament laxity, and it has been further shown that there is a decrease in collagen density and abnormal protein structure in the tendons of patients with Down syndrome.135 Furthermore, the 21st chromosome has genes that encode 2 of the subunits of collagen VI that both map to the downs obligate region of chromosome 21, and are expressed in human fetal heart tissue.139 Taken together, abnormalities in connective tissue synthesis as a result of chromosomal abnormalities appear to cause MVP in Down syndrome, but a precise mechanism has not yet been clearly delineated.
Larsen‐Like Syndrome
MVP is one of the several heart malformations that occur as a result of mutations in beta‐1,3‐glucuronyltransferase 3, which cause a subtype of Larsen‐like syndrome. Mutations cause decreased production of glucuronosyltransferase‐1, a Golgi apparatus enzyme responsible for the initial step in the synthesis of glycosaminoglycan side chains for the proteoglycans dermatan sulfate, heparin sulfate, and chondroitin sulfate. This results in a partial deficiency of these 3 proteoglycans, disrupting the ECM, and causing the MVP phenotype in affected patients. In a family enriched for this gene mutation, 4 of 5 children that were homozygous for the mutation had MVP, in addition to various other heart, craniofacial, and skeletal abnormalities.140 Further study of Larsen‐like syndrome are needed however, as only 1 paper which analyzed 5 patients has actually assessed cardiovascular traits in Larsen‐like syndrome.
Syndrome With Sinus Node Dysfunction, Arrhythmias, Left Ventricular NonCompaction
A series of recent studies reported several families that suffered from a mutation in a cardiac ion channel that, in addition to having electrophysiologic abnormalities, had structural heart abnormalities, and MVP.141, 142, 143 Mutations in hyperpolarization activated cyclic nucleotide‐gated potassium channel 4, cause dysfunction of hyperpolarization‐activated cyclic nucleotide channel 4, an important contributor to the pacemaker current of sinoatrial node cells.143 Patients with this mutation exhibit sinus bradycardia, as well as left ventricular noncompaction, a cardiomyopathy characterized by noncompacted left ventricular myocardial layer with many trabeculations and deep intertrabecular recesses.141 MVP was also identified in 3 of 15 patients described in a recent study of this gene mutation.142 It is unclear why patients with an ion channelopathy develop MVP or abnormalities in the ventricular myocardium.141 A few theories have emerged: in the first, loss of hyperpolarization activated cyclic nucleotide‐gated potassium channel 4, which is involved in early heart in addition to its role in the developed sinoatrial node, causes atypical signaling in pathways important for ventricular wall maturation and compaction, with resultant hypertrabeculated myocardial tissue and prolapse.143 In the second, hyperpolarization activated cyclic nucleotide‐gated potassium channel 4 itself acts as a signaling molecule, and decreased expression of hyperpolarization activated cyclic nucleotide‐gated potassium channel 4 in the cardiac progenitor cells that eventually form the LV directly causes improper compaction. In the third, left ventricular noncompaction is an acquired compensatory feature that results to improve stroke volume and cardiac output in the patient with bradycardia.142 None of the authors speculate specifically about how MVP develops in these patients; perhaps abnormal trabeculation of the LV allows for retrograde movement of the mitral valve during systole attributable to abnormal mechanics through the chordae tendineae, or atypical development around the mitral valve annulus causes disjunction, and abnormal valve prolapse.
Borrone Dermato‐Cardio‐Skeletal Syndrome
Borrone Dermato‐Cardio‐Skeletal syndrome (BDCS syndrome) is characterized by skin, skeletal, and cardiac abnormalities, including MVP, which is seen in an average (median) of 62.5% of patients analyzed across 6 studies (Figure S1).144, 145, 146, 147, 148, 149 A recent linkage analysis of a consanguineous family with a child diagnosed with BDCS syndrome found homozygous mutations in 2 different genes, BDCS1 and BDCS3. These genes encode the protein SH3PXD2B (SH3 and PX domains 2B). Mutation results in a truncated protein, and complete loss of SH3PXD2B in affected patient fibroblasts. SH3PXD2B is an adapter protein required for formation of podosomes, which are actin‐rich membrane protrusions involved in cellular adhesion, migration, and ECM remodeling. SH3PXD2B is highly expressed in the heart during development, and may cause MVP through diminished recruitment of matrix metalloproteases and impaired ECM remodeling during valve development, ultimately leading to a structurally incompetent mitral valve.145 SH3PXD2B missense and frameshift mutations are also responsible for ≈50% of patients with another similar autosomal recessive condition called Frank‐Ter‐Haar syndrome147; in fact, as a result of recent studies, the BDCS and Frank‐Ter‐Haar syndrome are now thought to represent the same disease entity,145 with pleiotropic effects being responsible for the phenotypic differences between the 2 conditions.
Williams‐Beuren Syndrome
Williams‐Beuren syndrome (sometimes referred to as Williams syndrome) is a rare autosomal dominant disease that is characterized by cardiovascular connective tissue, and central nervous system abnormalities, as well as mild mental retardation and extroverted personality.150 MVP is reported to be among the most common cardiovascular abnormalities in this condition, with a median prevalence of 22.3% across 10 studies (Figure S1).151, 152, 153, 154, 155, 156, 157, 158, 159, 160 The causal mutation is a recurrent 7q11.23 contiguous gene deletion, which contains the elastin gene within the deleted region.161 This results in abnormal vascular stiffness in the major elastic arteries of the body, causing progressive arterial stenosis most commonly in the aorta and pulmonary trunk.150 The precise mechanism linking Williams‐Beuren syndrome to MVP is not known, though it can be theorized that abnormal connective tissue structure, and decreased elastic properties of the mitral valve because of elastin deficiency contribute to myxomatous degeneration and the development of prolapse. Furthermore, defects in the structure of elastin are seen in Marfan syndrome, as fibrillin is a component of elastic microfibrils. Mutated fibrillin is known to affect sequestration of latent TGF‐β, increasing signaling through that pathway, and causing excessive myxomatous matrix production. Therefore, it may be possible that a driving force behind myxomatous valve degeneration in Williams‐Beuren syndrome is an increase in TGF‐β signaling.
Autosomal Dominant Polycystic Kidney Disease
Autosomal dominant polycystic kidney disease (ADPKD) is one of the most commonly observed hereditary conditions, and is estimated to affect almost 1 in 400 to 1000 people.162 The disease is characterized by the age‐related development and enlargement of renal cysts, stemming from the tubular epithelium. Extrarenal involvement of multiple other tissues has been shown in patients with ADPKD, including liver, spleen, pancreas, blood vessels, and the heart.163 MVP is enriched in patients with ADPKD compared with the general population; in the 8 studies analyzed for the current review, we found the mean prevalence of MVP was 21.4% in patients with ADPKD (Figure S1).164, 165, 166, 167, 168, 169, 170, 171
Two genes, PKD1 and PKD2, have been implicated in the vast majority of ADPKD cases.172, 173, 174 These genes encode for integral membrane proteins called polycystins 1 and 2, which are found in the plasma membranes and primary cilia of renal tubular epithelial cells, as well as in hepatic bile ductules, and pancreatic ducts.175 Defects in these genes impair their ability to localize to primary cilia, and are thought to affect mechanosensing of the primary cilia, and structural organization of the epithelial cells, which leads to the formation of cysts, which enlarge over time.176 Genes involved in primary ciliogenesis are also associated with MVP outside of syndromes as well. In 2019, the cilia gene, DZIP1 was identified as a causative gene in idiopathicnonsyndromic MVP.33 It is therefore hypothesized that defects in the organization, assembly, and maintenance of primary cilia underlie the mitral valve involvement in ADPKD.
Cardiac Associations of MVP
Mitral Regurgitation
A study estimated that MVP related complications occur in patients at a rate of ≈1.0 per 100 patient years, or about 1%. The most common complication observed in patients were prosthetic mitral valve implantation or mitral valve repair attributable to severe mitral regurgitation, which occurred in 3.5% of the population over the course of the entire study. Further, baseline presence of a holosystolic murmur, thought to indicate more severe mitral regurgitation, was strongly associated with fatal and nonfatal complications.177
Mitral regurgitation is a natural consequence of MVP.178, 179 It is thought that regurgitation develops in patients with MVP through 2 distinct, albeit related pathways—in the first pathway, changes in valve geometry that occur as a result of the myxomatous degeneration process underlying MVP cause separation of the anterior and posterior mitral leaflets, which decreases valve coaptation and allows for retrograde blood flow through the mitral valve during systole.180, 181, 182, 183 Regurgitation that develops in this way gradually worsens as the valve geometry changes and valve coaptation decreases.184 Eventually, a cyclical pattern develops (Figure), where worsening regurgitation causes an increase in volume overload, which further increases the annulus diameter and further worsens the amount of regurgitation.184 The annual rate of progression of the regurgitant volume in patients was estimated to be ≈5.9 mL/year.184 In the second pathway, mechanical stressors on the chordae tendineae leads to degeneration and rupture,185, 186, 187 which causes a flail leaflet that is untethered to the papillary muscle (Figure). This causes a much more rapid progression of mitral regurgitation; the annual increase in regurgitant volume in this group was 18.4 mL/year, >3 times higher compared with patients without flail leaflet.184 Mitral regurgitation can also develop in the setting of ischemia, and occurs as a result of diminished contractility of the LV, with subsequent papillary muscle displacement, which, as a result of tethering to the valve leaflets, diminishes valve coaptation and increases regurgitation.188
Figure 1. Flowchart showing the inter‐relatedness of pathophysiology of syndromic vs nonsyndromic mitral valve prolapse.
B3GAT3 indicates beta‐1,3‐glucuronyltransferase 3; DCHS1, dachsous cadherin‐related 1; DZIP, DAZ interacting protein 1; EF, ejection fraction; FLNA, filamin A; FMR1, fragile X mental retardation protein 1; HCN4, hyperpolarization activated cyclic nucleotide‐gated potassium channel 4; IFT88, intraflagellar transport 88; LMCD1, LIM and cysteine rich domains protein 1; LV, left ventricle; LVNC, left ventricular noncompaction; PKD, polycystic kidney disease; SH3PXD2B; SH3 and PX domains 2B; SMAD3, mothers against decapentaplegic homolog 3; SMAD4, mothers against decapentaplegic homolog 4; TGFBR2, TGF‐beta receptor 2; TGF‐β, transforming growth factor beta; and TNS1, tensin 1.
The estimated prevalence of regurgitation in patients with MVP has been discussed in several populations, both community‐based,1, 15, 189, 190 and hospital‐based cohorts.8, 191 In a series of publications on the Framingham Heart Study, there was a greater degree of mitral regurgitation in patients with MVP compared with controls without prolapse, but the amount of regurgitation seen was, on average, mild.5 Further, the rate of severe regurgitation, defined as having an area of the regurgitant jet >40% of the area of the LA, was 7% when compared cross‐sectionally at baseline.1 It is worth noting, however that the primary goal of this study was to examine the prevalence of MVP in the community, and the examination of comorbidities performed was on small numbers of MVP positive patients and was done in a cross‐sectional manner. Subsequent longitudinal analysis on the Framingham cohort has demonstrated that the rate of patients with MVP at baseline progressing to severe mitral regurgitation (MR) requiring surgery is 25% over a follow‐up period of 3 to 16 years.182
In a second study comprised of 833 asymptomatic patients with MVP defined by echocardiography at baseline, the presence of comorbidities was analyzed longitudinally. In this cohort, 7.6% were determined to have an MVP‐related event, defined as death, heart failure related to MVP, endocarditis, or mitral surgery in 10 years of follow‐up. Further, severity of mitral regurgitation at baseline was the strongest risk factor for cardiovascular morbidity.8 In the Strong Heart Study, patients with MVP had a significantly higher prevalence of both mild mitral regurgitation (28.1% versus 18.9%) and moderate‐to‐severe mitral regurgitation (8.8% versus 2.1%) compared with patients without MVP. Whilst the above studies make it clear that MVP is not as benign of a disease as was originally thought, more work needs to be done to understand why some patients have a more severe disease course, while others do not.
MVP is the most common cause of severe mitral regurgitation requiring surgery.192, 193, 194 By one estimate, ≈0.2% to 3.5% of patients with prolapse will require surgery for their condition at some point in their lifetime, depending on their demographics.195 Mitral valve surgery, carries significant risks,196 but is highly effective at preventing mortality in patients with severe regurgitation.197 Moreover, less invasive percutaneous catheter‐based procedures have been developed, are available for patients who are not ideal candidates for surgery, and have been shown to improve quality of life, reduce rehospitalizations, and promote favorable ventricular remodeling, although they were not shown to improve survival at 1 year.198
Atrial Fibrillation
Rates of atrial fibrillation (AF) appear to be low in patients with MVP without significant amounts of regurgitation.1 However, as the degree of mitral regurgitation increases, so does the prevalence of AF,199, 200, 201, 202, 203, 204, 205, 206 suggesting that the AF incidence seen in patients with MVP occurs as a secondary result of the increasing regurgitation.204 Estimates of the prevalence of AF in patients with severe regurgitation have ranged from 20% to 55%202, 205, 207 depending on the type of cohort analyzed (eg, symptomatic, asymptomatic, surgical, etc). Most recently, a multicentered prospective study of 2425 patients with severe regurgitation because of flail leaflets found that ≈30% had coexistent AF.200 Though MVP is not the only etiology of a flail leaflet, as we have previously discussed it is the most common etiology.185, 186 Further, in a smaller scale study conducted by the same group in 2002, the results demonstrated that the incidence of AF in patients with regurgitation who were medically managed was similar whether a patient had regurgitation because of simple MVP or a flail leaflet.206 Taken together, the presence of regurgitation of increasing severity appears to drive the development of AF, and the prevalence of AF in patients with severe regurgitation is high.
Despite its prevalence a paucity of data is present to support a mechanistic link of regurgitation to AF. However, previous studies have compiled a rough understanding of how this might occur based on observations in other diseases that affect the hemodynamics of the mitral valve. Mechanistically, regurgitation of blood through the mitral valve returns blood to the LA, which increases the amount of blood the LA has to accommodate, causing pressure and volume overload.199 Reflecting this, clinical studies have previously shown that LA volume can predict the development of AF in patients with severe MR.208 The mechanical stress seen in LA volume overload appears to alter cell‐cell coupling of atrial cardiomyocytes, cause tissue fibrosis, and affect the conduction velocity of the atrial tissue, causing currents to travel at differing velocities through conduction pathways in the atria.209, 210, 211 This in turn increases the propensity for reentrant circuits to develop, thus, providing the substrate for AF (Figure).
The interplay between surgical treatment, AF, and regurgitation attributable to MVP has been controversial over the years. It has been well established that patients who have AF at the time of MR surgery have worse outcomes compared with patients without AF.200, 201, 206, 212, 213 However, surgery has previously been associated with an increase in the incidence of AF,213, 214 though more recent data argue that medical management produces worse outcomes than surgical intervention irrespective of whether a patient is in sinus rhythm, has paroxysmal AF, or persistent AF.200 In addition, one study that found that even though there was an increase in the incidence of AF in patients who were treated surgically compared with conservative treatment, the risk of death from cardiac causes was lower, and the incidence of congestive heart failure was also lower.213 Others have further argued that concomitant ablation has the ability to decrease the incidence of AF in patients who are undergoing mitral valve surgery.212 Though current American Heart Association/American College of Cardiology guidelines recommend waiting to perform MR surgery until a patient has new onset AF, these recent studies demonstrating that this waiting approach will lead to worse outcomes has increased calls to amend the guidelines to intervene earlier.199, 200, 202
Ventricular Arrhythmias and Sudden Cardiac Death
The estimated annual risk of sudden cardiac death in patients with MVP ranges from 0.2% to 1.9% depending on the patient characteristics of the study.215, 216 Despite this heterogeneity, what is clear is that MVP appears to be a significant player in the development of sudden cardiac death (SCD) in certain patients. A report in 2001 found that isolated MVP was the suspected cause of SCD in 12% of all cases of SCD in the study population, making it the third leading cause of SCD behind arrhythmogenic right ventricular cardiomyopathy (14%), and premature atherosclerosis (21%).217 Subsequent analysis of 650 young (<40) patients with SCD performed by the same group found MVP to be implicated in 7% of young patients with SCD. It is important to note that this population has a systematic government‐implemented electrocardiography screening protocol that is used to prevent exercise‐associated SCD attributable to cardiomyopathies and ion channelopathies,218 thus the incidence of SCD attributable to MVP in this population is likely high compared with other populations; studies on other populations implicate MVP in ≈1.7% of SCD cases.219
Although we have long appreciated the association between MVP with significant regurgitation and the development of ventricular arrhythmias,216, 220 it is becoming evident that regurgitation does not have to be present or severe to increase the risk for SCD. Several recent studies have identified a subset of patients with MVP that have little to no regurgitation, but have a significantly elevated incidence of ventricular arrhythmias, including sudden death.221, 222, 223 The patients described in these reports display a remarkably similar phenotype; young, female, bileaflet MVP without significant regurgitation, a mid‐systolic click on cardiac auscultation, presence of mitral annulus disjunction, signs of cardiac fibrosis observed on cardiac magnetic resonance imaging, a high burden of premature ventricular contractions, and increased rates of nonsustained and sustained ventricular tachycardia, ventricular fibrillation, and cardiac arrest.215
A proposed mechanism for this “arrhythmogenic mitral valve prolapse syndrome” has begun to emerge.215 The baseline finding is mitral annulus disjunction, which is an echocardiographic and morphologic finding characterized by increased distance between the atrial mitral valve attachment and the left ventricular attachment.215, 224, 225 This abnormality allows for increased mechanical stress on the annulus and leads to irregular curling motion of the mitral valve annulus during systole, in turn increasing the mitral valve annulus diameter during systole.224 Myxomatous degeneration, in combination with these abnormal stressors on the annulus, leads to increases in mechanical stress on the inferobasal myocardial wall, as well as on the papillary muscles through the chordae tendineae.225 These stressors increase fibrogenesis in the myocardium,16 providing the substrate for ventricular arrhythmogenesis through the well documented effects on cardiomyocyte electrical conduction in the context of fibrosis.226 At the same time, an increase in the observance in PVCs are seen in patients with MVP.227, 228 Electrophysiologic mapping in these patients has demonstrated that these originate most frequently in the papillary muscles, as well as the fascicles, and the left ventricular outflow tract.20, 228, 229, 230 Purkinje tissue in these zones appears to be the trigger for ventricular ectopic beats,231 and has been theorized to result from either mechanical stretch of the cells as a result of direct mechanical forces from the mitral leaflet on the myocardium, or because of aberrant electrical activity in damaged cells as a result of abnormal calcium handling and the evocation of delayed afterdepolarizations.222 Together, these provide the substrate (fibrosis and altered electrical conductivity of the myocardium), and trigger (PVCs) for reentrant circuits to develop, causing malignant ventricular arrhythmias.
Treatment for malignant ventricular arrhythmias in patients with MVP follows the standard of care for all patients who experience life threatening ventricular arrhythmias. Ablation procedures have been used successfully to treat ventricular arrhythmias in patients with MVP, but recurrent ventricular arrhythmias can re‐emerge in patients treated with this technology.230 Internal cardioverter defibrillator implantation is often used in these patients for additional prophylaxis, and has been shown to successfully manage subsequent ventricular arrhythmias in some, but not all patients.228 However, these therapies only work in patients who survive out‐of‐hospital cardiac arrest, of which only 8.4% of patients do, on average.232 More work needs to be done to better understand why some patients with hemodynamically benign MVP are at high risk for ventricular arrhythmias and SCD.
Infective Endocarditis
It is estimated that patients with MVP have a 3‐ to 8‐fold increased risk of developing infective endocarditis (IE), although the estimated annual risk is still quite low, at 0.02%.233 Nonetheless, endocarditis is a pernicious complication of MVP when it does occur. Mortality rates in patients with infective endocarditis are between 10% and 30%, even in spite of advances in diagnosis and surgical/antibiotic treatment.234, 235 Proposed risk factors for endocarditis in patients with MVP are the presence of mitral regurgitation as suggested by a systolic murmur, increased age, male sex, and leaflet thickening/redundancy.233
According to studies documenting the etiology of IE in MVP, dental procedures are the most common cause,233, 236, 237 although in a recent study of patients with IE who had underlying MVP, an identifiable portal of entry was only seen in 37% of cases.235 An oral source of the infection is further supported when we consider the organisms implicated in IE. Viridans group Streptococci (which are known to colonize the oral mucosa238), in addition to other normal flora of the oral microbiota, accounted for >85% of IE cases in a recent study of patients with MVP.235 This is in line with previous studies that implicate Viridans group Streptococci as the major cause of infective endocarditis in patients with MVP.239, 240 Based on these findings, it can be hypothesized that in many of the cases of IE without a portal of entry, traumatic inoculation of bacteria during chewing, or brushing may be the stimulus that is responsible for the increased rate, although this has not been tested. Dental procedures or oral trauma allow for oral microbes to enter the bloodstream, causing a transient bacteremia, and providing a trigger for patients to develop endocarditis. Other causes of bacteremia, including gastrointestinal and genitourinary procedures, surgery, indwelling catheters, and intravenous drug use, are further implicated as trigger agents for the development of endocarditis, though to a lesser extent than dental work in patients with MVP.235
This leads to an important question: Why then do patients with MVP develop endocarditis at increased rates compared with patients without valve abnormalities? Studies have theorized changes in ECM components as a result of myxomatous degeneration, though this still remains unproven.240 Other studies have further implicated turbulent flow through the mitral valve,233 and microthrombi formation on the mitral valve leaflets as promoters of microbial adhesion to the surface of the mitral valve, which is accomplished through complex interactions between microbial surface components recognizing adhesive matrix molecules, (Such as adhesins, dextrans, fructans, and other microbial surface components), and ECM ligands including fibronectin, collagen, laminin, fibrinogen, vitronectin, thrombospondin, elastin, and bone sialoprotein.241, 242 In turn, virulent organisms are capable of activating platelets,241 and binding coagulation cascade proteins,242 facilitating growth of the vegetation, which in turn facilitates the adhesion of additional bacteria, forming a cyclical growth pattern that results in enlargement of the vegetation.242 Another option is that in MVP, the endothelium may become compromised or broken and thereby provide a niche for bacteria to colonize. Bacterial‐mediated destruction of the mitral valve, chordal rupture, septic emboli, hemodynamic instability, organ failure, and death can then result.
Though endocarditis is seen at increased rates in patients with MVP, and despite calls to use prophylaxis in all patients with MVP who have evidence of regurgitation,233 MVP is currently defined as an intermediate risk cardiac condition for endocarditis, and as such, antibiotic prophylaxis for this condition is not recommended.69 Historically, this has been a controversial issue.239 Assuming 2% to 3% of the population are living with MVP, this would mean putting millions of patients on antibiotic prophylaxis, which would be a significant economic burden and, an enormous cost to the healthcare system, and a burden for patients, in addition to the problematic effects such a strategy would have on emerging antibiotic resistance. Nonetheless, since the changes in guidelines in 2007, the prevalence of endocarditis attributable to streptococcal species has been rising.243 Studies have identified subgroups that would benefit more from prophylaxis; restricting antibiotic prophylaxis to patients with a systolic murmur, for example, is estimated to provide cover to ≈90% of patients likely to develop infective endocarditis.237 Further, recent studies have suggested that restricting antibiotic prophylaxis to patients with MVP undergoing dental procedures could be of benefit, given that the vast majority of bacteria causing IE in patients with MVP originate from the mouth.235 Nonetheless, current guidelines find insufficient evidence that antibiotic prophylaxis would be effective in preventing infective endocarditis in MVP.244
Heart Failure
Heart failure occurs when the heart is unable to pump sufficient blood to meet the physiologic demands of the rest of the body. In the literature, heart failure is defined heterogeneously, and can be established as a diagnosis in multiple different ways based on the presence of symptoms, as well as based on objective measurements of heart function observed through cardiac imaging.245, 246 MVP without regurgitation was conventionally not considered to directly cause heart failure.247 Instead, MVP was thought to cause heart failure through worsening mitral regurgitation, which causes hyperdynamic LV function, volume overload, and eventual decompensation.248 However, this viewpoint is changing in light of recent data which implicate MVP in the development of left ventricular fibrosis even when mild to no regurgitation is present.249, 250 In a study that compared patients with MVP and regurgitation to matched patients with regurgitation but no prolapse, a third of patients with MVP had established cardiac fibrosis compared with just 3% of patients with isolated regurgitation.251 Furthermore, even in patients with clinically mild regurgitation, presence of MVP was significantly associated with increased LV dimensions and remodeling independent of the amount of regurgitation.252 Perhaps most significantly, 1 in 5 patients who receives corrective surgery to treat MVP will develop an acute decline in their LV dysfunction, even though echocardiographic parameters before their surgery are normal.253 These findings taken together suggest that, while there are no doubt changes in volume handling as a result of regurgitation play a role in the progression of heart failure, isolated mechanical effects as a direct result of a prolapsing leaflet is also likely contributory.
When mitral regurgitation becomes heart failure is also heterogeneously defined in the literature. For the purposes of discussion here, and based on our interpretation of the guidelines, the development of heart failure in a patient with mitral regurgitation would hinge on the development of the clinical symptoms of heart failure (eg, dyspnea, exercise intolerance), which is denoted “Severe symptomatic mitral regurgitation” by the 2014 American Heart Association/American College of Cardiology guidelines on the management of patients with valvular heart disease executive summary.254 Indeed, many studies that describe the outcomes of patients with severe mitral regurgitation describe the severity of symptoms using the New York Heart Association functional criteria for heart failure.255, 256, 257 This of course makes it difficult to delineate the 2 disorders from one another.
Because heart failure is defined in many ways, and as a result of the inter‐relatedness of heart failure and mitral regurgitation, it is difficult to estimate the risk of developing heart failure in patients with MVP; nonetheless studies have tried to do so. In the Olmstead study of 833 patients with asymptomatic MVP, 5.7% developed heart failure that was determined to be a result of their disease. In the same study, however, 66 patients had mitral valve surgery, which may demonstrate additional patients who initially developed symptoms of heart failure, but who met criteria for surgery.8 In another cohort of patients with mitral regurgitation that that met criteria for valve surgery, a third of patients went on to develop heart failure within 10 years, but in the same cohort, 370 out of 576 patients, or nearly 2 in 3 patients, had a diagnosis of heart failure before their surgery,213 presumably because of the presence of symptoms of heart failure. In an editorial in 2018, Gillam et al further highlighted the problems with using presence of symptoms as a tool for diagnosis of symptomatic mitral regurgitation/heart failure. They argue that it can be difficult to differentiate the patient with severe regurgitation who is “at risk” for heart failure (meaning in New York Heart Association class 1, but without symptoms) from someone who meets criteria for a diagnosis of heart failure because patients with mild exercise intolerance will subconsciously curtail the amount of physical activity they engage in.258 In a nationwide hospital‐based registry study, Andell et al found that 39.3% of patients with a diagnosis of mitral regurgitation had a coexistent diagnosis of heart failure, yet they also point out that this is a 2‐way street; primary MR reduces effective stroke volume and causes heart failure, but mitral regurgitation can also result from annular dilation secondary to left ventricular dilation in heart failure or ischemic heart disease.207 For the purposes of this review, we focused primarily on the mechanisms through which primary regurgitation can cause worsening left and right heart function, and eventually cause heart failure.
Patients can present with symptoms of heart failure (eg, dyspnea, exercise intolerance) as a result of MVP through several different pathophysiologic mechanisms. First, as MVP worsens, higher amounts of biomechanical tension are applied to the LV through the chordae tendineae.259 In addition, mitral annulus disjunction contributes to increased biomechanical forces experienced by the basal LV.224 These locations of increased tension correlate with regions of left ventricular fibrosis, and suggest that increasing tension applied to the myocardium as a result of prolapse is causing left ventricular fibrosis.225, 228 Fibrosis in turn increases the stiffness of the myocardium, and impairs contractility, which ultimately causes worsening systolic and diastolic heart function until the symptoms of heart failure develop.260 LV fibrogenesis caused by increases in chordal tugging forces as a result of a prolapsing valve are independent of mitral regurgitation, which further demonstrates the role of biomechanical tension as an initiator in driving pathogenesis.251 In addition, a recent study that performed hybrid cardiac magnetic resonance imaging and positron emission tomography scanning of patients with MVP found that regions of myocardial fibrosis exhibited increased fluorodeoxyglucose uptake, demonstrating a hypermetabolic state of the fibrous zones, and suggesting that there is subclinical myocardial inflammation occurring in response to increased mechanical tension.261 How tension causes regionalized fibrosis and the role of myocardial inflammation in this process is not well understood and will be the subject of much interesting work in the future.
Second, MVP can also cause left ventricular dysfunction, and systolic heart failure.262, 263, 264 Although patients with severe regurgitation, may have a completely “normal” ejection fraction, this doesn't reflect the true underlying hemodynamic alterations that are occurring. To do a quick calculation, in severe regurgitation (defined in the Framingham Heart Study as regurgitant jet area >40% of the volume of the LA1), assuming a normal left atrial volume index of ≈41 mL/m2 for a male patient, ≈16 mL of blood would be regurgitated with each beat of the ventricle. Assuming a normal ventricular stroke volume index of 65 mL/m2, ≈25% of the blood ejected from the heart each beat is flowing from LV to LA. This implies that only 75% of the blood ejected with each beat makes it to systemic circulation, and therefore, the cardiac output has to increase 33% to pump enough blood in the forward direction to meet the body's metabolic demands. The initial response by the LV is a compensatory increase in left ventricular end‐diastolic volume and force of contraction supported by the frank starling mechanism,265 but chronically, this volume overload causes increased LV wall stress, LV hypertrophy, fibrosis, increases in LV afterload, and a gradually worsening systolic function.264, 265 The best evidence that ventricular systolic dysfunction exists in patients with severe mitral regurgitation is the acute decline in ejection fraction that occurs in patients just after mitral valve surgery.201, 266, 267, 268 Even further, patients with impaired preoperative ejection fraction had a much more drastic reduction in ejection fraction with their operation, and patients with a more significant reduction in ejection fraction carried a worse prognosis.266 In a prospective study of asymptomatic patients with severe mitral regurgitation, immediate surgical correction was compared with a conventional treatment strategy that waited to perform surgery until they developed symptoms (exertional dyspnea), or they experienced a declination in ejection fraction (<60), an increase in LV end systolic diameter (>45 mm), AF, or pulmonary hypertension (pulmonary arterial pressure >50 mm Hg). In follow‐up, conventional management resulted in an estimated actuarial 7‐year cardiac mortality rate of 5%, compared with 0% with immediate surgery.197 As such, the 2017 American Heart Association/American College of Cardiology focused update on the management of valvular heart disease guidelines state that surgical intervention in a patient with a normal ejection fractionF (>60%) who has increasing LV size or worsening ejection fractionF is reasonable, since an ejection fractionF <60% indicates these patients are already in LV dysfunction.
Third, as regurgitation through the mitral valve worsens, increasing amounts of blood are expelled into the LA instead of through the aorta, causing left atrial pressure and volume overload.269 This results in left atrial enlargement, and may cause AF, as has been discussed in our section on AF.208 At the same time, worsening regurgitation has been associated with increases in pulmonary arterial pressures,184, 270 likely as a result of pulmonary congestion because of the regurgitant blood and left atrial volume overload.271 Even in asymptomatic patients with severe regurgitation, 34% had elevated pulmonary systolic pressures during exercise, suggesting that these patients may have subclinical pulmonary congestion that has not yet progressed to symptomatic pulmonary hypertension.271 In another study of patients with left ventricular dysfunction (defined by an EF <50%), severity of mitral regurgitation was found to independently predict pulmonary arterial pressure.272 These findings suggest that regurgitation drives the onset of pulmonary hypertension independent of left ventricular dysfunction. Worsening pulmonary hypertension, in turn, increases right ventricular afterload, and causes right ventricular remodeling and hypertrophy, but this is ultimately insufficient to overcome the increase in pulmonary afterload, and right‐sided heart failure develops.273 Severity of pulmonary hypertension in patients with mitral regurgitation is associated with worse outcomes. In a study of 1318 patients with severe mitral regurgitation attributable to myxomatous degeneration, an elevated right ventricular systolic pressure (>35 mm Hg) was seen in 77% of patients who died, and there was a positive trend that showed the higher your baseline right ventricular systolic pressure, the higher your mortality risk.274 Despite the risks of pulmonary hypertension on adverse outcomes in MR patients, current American Heart Association/American College of Cardiology guidelines recommend avoiding surgical intervention on patients with regurgitation until the development of pulmonary hypertension, when their right ventricular systolic pressures reach 50 mm Hg.254 As such, current guidelines may wait too long to intervene in patients with mildly elevated right ventricular systolic pressures, and delay care that may be associated with a more favorable outcome.274
Finally, regurgitation can develop abruptly as a result of papillary muscle, or chordal rupture. As was previously discussed, changes in valve geometry and myxomatous enlargement of the leaflets causes an increase in mechanical stress on the chordae tendineae, which eventually may rupture.185, 186 Mitral regurgitation develops abruptly and without appropriate compensation by the LA. This leads to acute left atrial volume overload, and causes pulmonary edema and symptoms of respiratory distress.275 Mechanistic studies in dogs have nicely demonstrated these effects, showing that when mitral regurgitation was acutely induced through chordal severance, massive increases in LA volumes and pressures are seen, as well as a significant rise in left ventricular end diastolic pressure, a marker of preload.276 Further, this study found a decrease in the LV systolic pressure with acute regurgitation, consistent with a decrease in effective afterload on the LV, as well as forward cardiac output to the systemic circulation. In support of this, administration of isoproterenol (a beta‐adrenergic agonist that may decrease peripheral resistance through its effects on β2 receptors) as well as nitroprusside (an antihypertensive that decreases peripheral resistance through production of nitric oxide) decreased left ventricular end‐diastolic pressure, findings that demonstrate administration of these drugs increases forward flow, decreases left ventricular preload, in turn decreasing effective regurgitant orifice size and regurgitant fraction, and reducing LA volume overload.276 Early surgery is recommended in patients with mitral regurgitation because of flail leaflets, and is associated with a good outcome.277, 278, 279
“NonCardiac” Associations
The association between MVP and stroke has long been debated. Early case reports and case‐control studies that found an association between MVP and stroke in young patients are criticized for using older, less stringent MVP specifications which led to an overdiagnosis and consequently an over association.280, 281, 282, 283, 284 These MVP disease criteria were redefined in the late 1980s, and a prominent case‐control study was then published in 1999 that contradicted the previous reports of an association between MVP and stroke in young patients.285 However, one group disagrees with the power of case‐control studies and in 2003 conducted a community‐based study, which they say takes away bias in picking cases and controls, increases sample number, and allows for long‐term follow‐up. This paper reported that individuals over the age of 50 years with MVP have increased risk of stroke possibly because of AF and increased valvular surgery.280 The controversy around the association between MVP and stroke will remain until there is knowledge of the pathophysiology that connects the 2.
Left atrial myxomas are noncancerous tumors found in the LA of the heart.286 They have been loosely associated with MVP, with a handful of case reports documenting them as comorbidities.287, 288, 289, 290, 291 However, no case‐control studies have been conducted to determine the association between left atrial myxomas and MVP.
The association between cardiovascular disease and erectile dysfunction has been established for a number of years.292, 293 The link between the 2 is thought to be systemic inflammation, a symptom that has been known to cause MVP.294, 295 Despite this, little is known about the association between erectile dysfunction and MVP specifically. The first study to determine that this association exists was published just last year in 2019. Using data from the Taiwan National Health Insurance Research Database, these researchers found that people currently suffering from erectile dysfunction were more likely to have previously been diagnosed with MVP than controls.296 While the exact mechanisms that cause MVP are still being resolved, these researchers hypothesize that the link between MVP and erectile dysfunction may come from shared features such as oxidative stress and endothelial dysfunction that affects blood flow.296
Many studies have found that MVP is significantly associated with lower body mass index as compared with controls.297, 298, 299, 300 However, the underlying link between these 2 physical characteristics remains unknown. It is interesting to point out the patients with anorexia nervosa have been shown to develop MVP and then recover while receiving therapy and treatment.301 It has been suggested that this occurs because of the "ventriculo‐valvular disproportion," meaning that patients with anorexia nervosa lose cardiac muscle but not valve tissue and these disproportionally large valves are more likely to prolapse.302, 303 Whether or not this phenomenon is true for people with just lower body mass indexes is to be determined.
The Future: Nonsurgical Therapy for MVP
Mitral valve surgery or percutaneous intervention is the only currently available treatment for MVP, and because of the invasive nature and significant risks associated with these procedures, it is reserved for patients with severe disease.244 Although surgery is effective at preventing many of the complications of MVP,193, 197, 213, 274, 277, 278, 279 it is not always curative. Long‐term follow‐up of patients with mitral valve repair found that re‐repair of the valve or recurrent nontrivial mitral regurgitation may develop in 4% to 35% of patients,304, 305, 306, 307, 308 demonstrating that although valve repair does provide a benefit to the patient, it doesn't necessarily stop the underlying pathophysiology.
A growing interest in the field is the development of nonsurgical pharmacologic treatments to MVP. MVP is observed in 70% of small breed dogs,309, 310, 311 with macroscopic and microscopic pathological findings consistent with primary MVP in humans.312, 313, 314 Drugs commonly prescribed to affected dogs include angiotensin‐converting enzyme inhibitors,315 diuretics,316 vasodilators,317 β‐adrenergic receptor blockers (β‐blockers),318, 319 and inotropes.320, 321, 322 Angiotensin‐converting enzyme inhibitors promote a reduction in cardiac after‐load by decreasing arterial pressure, thus, reducing mitral regurgitation.315, 323 Loop diuretics, such as furosemide and torsemide, promote natriuresis, reducing cardiac preload by decreasing total blood volume.316 In addition, torsemide produces vasodilation; enhances cardiac function, and abrogates aldosterone‐induced cardiac remodeling.324, 325, 326, 327, 328, 329, 330, 331 Vasodilators, such as nitroglycerin and angiotensin‐converting enzyme inhibitors, decrease cardiac preload and afterload, leading to a reduction in systemic vascular resistance. Medical management with vasodilators lends to a reduction in mitral regurgitation in patients with severe mitral valve disease.332 β‐blockers promote negative inotropic and chronotropic effects, decreasing cardiac demand, and oxygen demand.318, 319 While β‐blockers have not been proven to reduce mitral regurgitation in the setting of human or canine MVP, a reduction in the incidence of heart palpitations and arrhythmias is observed.333 Additionally, β‐blockers are purported to prevent deleterious cardiac remodeling by preventing adrenergic over‐activation.334 Lastly, positive inotropic agents, such as the cardiac glycoside digoxin, are used to enhance cardiac contractility and to treat AF in canines with severe MVP.320, 335 In addition to digoxin, the calcium sensitizer and phosphodiesterase 3 inhibitor pimobendan is used in canines because of its positive inotropic and dilatory effects.336 In the EPIC (Evaluation of Pimobendan in dogs with Cardiomegaly caused by preclinical mitral valve disease) trial, dogs treated with pimobendan experienced 15 more months of symptom‐free life than did dogs treated with placebo.321, 322 Despite the plethora of medications used to provide moderate symptomatic relief in canines, there are no drugs available that target disease initiating pathways associated with deleterious myxomatous degeneration.
Dysregulation of the TGF‐β1 (transforming growth factor beta 1) pathway contributes to the pathogenic myxomatous valvular remodeling seen in MVP, making TGF‐β receptor 1 an attractive anti‐target.337, 338, 339, 340 Furthermore, activation of the TGF‐β1 signaling pathway in MVP induces valvular interstitial cell differentiation into contractile myofibroblasts, contributing to ECM remodeling.339 A study by Ng et al demonstrated that TGF‐β antagonism in vivo rescued the valve phenotype in a mouse model of Marfan syndrome,341 suggesting aberrant TGF‐β signaling contributes to cell proliferation and survival in MVP.342 Losartan, an angiotensin receptor type II blocker, reduces TGF‐β levels and may represent an avenue to modulate the pathological progression of MVP.343, 344, 345, 346 Similar to angiotensin‐converting enzyme inhibitors, losartan decreases cardiac afterload, leading to a reduction in left ventricular end‐systolic wall stress and mitral regurgitation.347 Finally, following the discovery of increased inflammatory cells within myxomatous valves, as well as data that show that deficiency of circulating monocytes inhibits progression of MVP, immunomodulating drugs may be of interest, although these carry significant side‐effect profiles.73, 348 Future directions should include the use of unbiased genetic screening approaches to identify novel druggable targets in the setting of MVP, as well as targeted therapeutics that can decrease systemic administration of agents while increasing drug concentrations within the mitral valve. Safe and effective therapies, if identified, could slow the rate of myxomatous degeneration, potentially delaying the need for surgery and improving outcomes.
Conclusions
Our review of the literature found that while MVP is enriched in several genetic and syndromic disorders, many disease associations that have previously been reported either do not have enough data available to assess the true prevalence of disease, or were reported before the adaptation of new clinical diagnostic guidelines for MVP that took the saddle shape of the mitral valve annulus into account. As such, diseases such as osteogenesis imperfecta, fragile X syndrome, Down syndrome, and Pseudoxanthoma elasticum, which have all been previously associated with MVP, may be over‐reporting the prevalence of MVP. Finally, MVP may be a phenotype present in other genetic syndromes not discussed within this paper, but that have not been well documented in the literature. Additional studies, which use up‐to‐date diagnostic criteria for MVP, will be important to assess whether MVP is truly associated with these conditions.
Our review further demonstrates the shared pathways through which MVP can develop in a heterogeneous group of conditions. First, the vast majority of mutations that have been identified that cause syndromic and nonsyndromic MVP cause alterations in valve geometry through either increases in ECM production, impaired ECM remodeling, or altered cell migration and valve morphogenesis. Second, the new, novel role for primary cilia as a master regulator of valve morphogenesis and major cause of MVP has shed new light on how disruptions in early cardiac valve development may “prime” patients to develop worsening MVP by altering their valve architecture early on in their lifetime. Finally, the role of TGF‐β dependent cell signaling highlights the importance of cell signaling, proliferation, and activation in driving MVP pathophysiology. Taken together, we propose a model in which changes in valve geometry, and subsequent alterations in valvular dynamics during the cardiac cycle, create a feed forward cycle that, through altered cell signaling, interstitial cell activation, and ECM production and remodeling, drives myxomatous degeneration and the development of MVP. A prolapsing valve then drives the further development of cardiovascular disorders through changes in biomechanics and hemodynamics (Figure).
Over the past 20 years, our understanding of MVP has evolved considerably. Precise definition of the disorder has allowed for large, population level studies to occur which have shown that even though MVP is a common and often benign entity, the lifetime cardiovascular risk of patients with MVP is both substantial and diverse. Through the hard work of many clinical and basic science researchers, genetic causes of MVP have been identified, and animal models of MVP have been developed which allow in‐depth investigation of the molecular drivers of mitral valve enlargement, myxomatous tissue formation, and prolapse.30, 31, 32, 33, 73, 104 With these tools, future investigations can focus on how MVP progresses beyond the valve, to the ventricle, and whether new studies may inform revised clinical guidelines or application of rationale remedial therapies to blunt disease progression or severity.
Sources of Funding
This work was supported by Grant Sponsor National Institutes of Health; Grant Numbers: HL131546 (Norris), GM103444 (Norris), HL149696 (Norris); HL122906 (Norris), T32HL007260 (Beck). Grant Sponsor: American Heart Association; Grant Numbers: 19TPA34850095 (Norris), 20SRG35540029 (Norris), 19TPA34900016 (Norris), 17CSA33590067 (Norris). The work at Medical University of South Carolina was performed in a facility constructed with support from the National Institutes of Health grant number C06 RR018823 from the Extramural Research Facilities Program of the National Center for Research Resources.
Disclosures
None.
Supporting information
Figure S1
(J Am Heart Assoc. 2021;10:e020919. DOI: 10.1161/JAHA.121.020919.)
Supplementary Material for this article is available at https://www.ahajournals.org/doi/suppl/10.1161/JAHA.121.020919
For Sources of Funding and Disclosures, see page 17.
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Supplementary Materials
Figure S1