Early-Onset Marfan Syndrome: A Case Series

Ardhanari, Mohanageetha; Barbouth, Deborah; Swaminathan, Sethuraman

doi:10.1055/s-0038-1675338

Cited by 7 publications

(11 citation statements)

References 22 publications

(25 reference statements)

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“…Although MVR in early infancy is often challenging, recent improvements in surgical techniques and devices have improved its surgical performance. 18) Children with MFS generally exhibit average intellectual and gross motor development. 23) In our patient, neurological development was consistent with that reported in a previous report.…”

Section: Discussionmentioning

confidence: 99%

“…We found a total of 20 cases that have been reported in 16 studies (Table ). 3,[7][8][9][10][11][12][13][14][15][16][17][18][19][20][21] Various surgical procedures such as mitral valvuloplasty (31%), MVR (26%), mitral annu- loplasty (11%), tricuspid annuloplasty (9%), tricuspid valvuloplasty (9%), tricuspid valve replacement (6%), valvesparing aortic root replacement (3%), Bentall procedure (3%), and repair of mitral chordae tendineae rupture (3%) were performed in these cases. In these cases, 11 (55%) patients were female, and the average age at surgery was 20 months (range, 1 month to 7 years).…”

Section: Case Reportmentioning

confidence: 99%

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Successful Mitral Valve Replacement in an Infant with Neonatal Marfan Syndrome due to a Novel Missense Mutation of the <i>FBN1</i> Gene

et al. 2022

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Marfan syndrome is an autosomal dominant genetic disorder of the fibrous connective tissue caused by pathogenic mutations in the fibrillin-1 gene. Neonatal Marfan syndrome is a rare type of Marfan syndrome that is genotypically and phenotypically different from classical Marfan syndrome and has a poor prognosis. Most patients with neonatal Marfan syndrome die during infancy due to severe and rapidly progressive cardiovascular disorders. Here, we present a case of an 11-year-old girl with neonatal Marfan syndrome due to a novel missense mutation in exon 27 of the fibrillin-1 gene. Her condition was critical due to progressive mitral and tricuspid regurgitation. Mitral valve replacement, performed at the age of 6 months, improved her critical condition. Our case suggests that early mitral valve replacement may lead to better outcomes in patients with neonatal Marfan syndrome.

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Section: Discussionmentioning

confidence: 99%

Section: Case Reportmentioning

confidence: 99%

Successful Mitral Valve Replacement in an Infant with Neonatal Marfan Syndrome due to a Novel Missense Mutation of the <i>FBN1</i> Gene

et al. 2022

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“…8 Indeed, by Hennekam's criteria, our patient had EOMFS rather than neonatal MFS, and his FBN1 point mutation (c.6313_5G > A; extended splice site) is in intron 51 rather than in the region purportedly associated with higher risk for neonatal MFS. 6,8,10 Dural ectasia is reported in 63 to 92% of MFS patients, and unlike other features of classic MFS in adulthood, it is present in 40% of pediatric patients. 5,11 It can lead to cerebrospinal fluid leaks and thereby to spontaneous intracranial hypotension (SIH): subdural fluid collections, most of which are SDHy, are present in 50% of SIH patients (regardless of MFS).…”

Section: Literature Review and Discussionmentioning

confidence: 99%

“…Mutations of FBN1 in the region between exons 24 and 32 belong to the few generally accepted genotypephenotype correlations of MFS and are associated with neonatal MFS. [8][9][10] Although all reported mutations associated with neonatal MFS are found in that region, mutations associated with EOMFS or classic MFS can be found there as well, rendering it impossible to predict whether a given mutation in exons 24 to 32 will be associated with classic MFS, EOMFS, or neonatal MFS. 8 Indeed, by Hennekam's criteria, our patient had EOMFS rather than neonatal MFS, and his FBN1 point mutation (c.6313_5G > A; extended splice site) is in intron 51 rather than in the region purportedly associated with higher risk for neonatal MFS.…”

Section: Literature Review and Discussionmentioning

confidence: 99%

Subdural Hygroma in an Infant with Marfan's Syndrome

et al. 2021

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Based on a patient encounter in which genetically confirmed Marfan's syndrome (MFS) underlay a spontaneously resolving subdural hygroma (SDHy) diagnosed in infancy, we review the literature of MFS clinically manifest in early life (early-onset MFS [EOMFS]) and of differential diagnoses of SDHy and subdural hemorrhage (SDHe) at this age. We found that rare instances of SDHy in the infant are associated with EOMFS. The most likely triggers are minimal trauma in daily life or spontaneous intracranial hypotension. The differential diagnosis of etiologies of SDHy include abusive and nonabusive head trauma, followed by perinatal events and infections. Incidental SDHy and benign enlargement of the subarachnoid spaces must further be kept in mind. SDHy exceptionally also may accompany orphan diseases. Thus, in the infant, EOMFS should be considered as a cause of SDHe and/or SDHy. Even in the absence of congestive heart failure, the combination of respiratory distress syndrome, muscular hypotonia, and joint hyperflexibility signals EOMFS. If EOMFS is suspected, monitoring is indicated for development of SDHe and SDHy with or without macrocephaly. Close follow-up is mandatory.

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“…Aortic root dilatation is also commonly present in children with nMFS but does not account for the most significant morbidity and mortality in this age group. Most children with nMFS die within the 1 st year of life of cardiac failure (20), although the number of survivors into teenage years is increasing thanks to improvement in care (23,24).…”

Section: Cardiomyopathy In Neonatal and Infantile Marfan Syndromementioning

confidence: 99%

Cardiomyopathy in Genetic Aortic Diseases

Muiño-Mosquera

Backer

2021

Front. Pediatr.

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Genetic aortic diseases are a group of illnesses characterized by aortic aneurysms or dissection in the presence of an underlying genetic defect. They are part of the broader spectrum of heritable thoracic aortic disease, which also includes those cases of aortic aneurysm or dissection with a positive family history but in whom no genetic cause is identified. Aortic disease in these conditions is a major cause of mortality, justifying clinical and scientific emphasis on the aorta. Aortic valve disease and atrioventricular valve abnormalities are known as important additional manifestations that require careful follow-up and management. The archetype of genetic aortic disease is Marfan syndrome, caused by pathogenic variants in the Fibrillin-1 gene. Given the presence of fibrillin-1 microfibers in the myocardium, myocardial dysfunction and associated arrhythmia are conceivable and have been shown to contribute to morbidity and mortality in patients with Marfan syndrome. In this review, we will discuss data on myocardial disease from human studies as well as insights obtained from the study of mouse models of Marfan syndrome. We will elaborate on the various phenotypic presentations in childhood and in adults and on the topic of arrhythmia. We will also briefly discuss the limited data available on other genetic forms of aortic disease.

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Early-Onset Marfan Syndrome: A Case Series

Cited by 7 publications

References 22 publications

Successful Mitral Valve Replacement in an Infant with Neonatal Marfan Syndrome due to a Novel Missense Mutation of the <i>FBN1</i> Gene

Successful Mitral Valve Replacement in an Infant with Neonatal Marfan Syndrome due to a Novel Missense Mutation of the <i>FBN1</i> Gene

Subdural Hygroma in an Infant with Marfan's Syndrome

Cardiomyopathy in Genetic Aortic Diseases

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