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Noonan syndrome associated with hypoplastic left heart syndrome

Published online by Cambridge University Press:  22 August 2022

Kendall M. Lawrence Open the ORCID record for Kendall M. Lawrence [Opens in a new window] ,
Danielle S. Burstein ,
Rebecca Ahrens-Nicklas ,
J. William Gaynor  and
Muhammad A. Nuri
Kendall M. Lawrence
Affiliation:
Division of Cardiovascular Surgery, University of Pennsylvania, Philadelphia, PA, USA
Danielle S. Burstein
Affiliation:
Division of Cardiology, Children’s Hospital of Philadelphia, Philadelphia, PA, USA
Rebecca Ahrens-Nicklas
Affiliation:
Division of Human Genetics, Children’s Hospital of Philadelphia, Philadelphia, PA, USA
J. William Gaynor
Affiliation:
Division of Cardiothoracic Surgery, Children’s Hospital of Philadelphia, Philadelphia, PA, USA
Muhammad A. Nuri*
Affiliation:
Division of Cardiothoracic Surgery, Children’s Hospital of Philadelphia, Philadelphia, PA, USA
*
Author for correspondence: Kendall M. Lawrence, MD, 3401 Civic Center Blvd, Division of Cardiac Surgery, Philadelphia, PA 19104, USA. E-mail: [email protected]
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Abstract

Noonan syndrome is an inherited disorder caused by alterations in the RAS-MAPK pathway. There have been several identified genotype–phenotype associations made with respect to congenital cardiac lesions and Noonan syndrome variants, but limited data exist regarding single ventricle disease in this population. Here, we report two patients with PTPN11-related Noonan syndrome and hypoplastic left heart syndrome variants.

Keywords

Noonan syndromehypoplastic left heart syndromelymphatic disorders
Type
Brief Report
Information
Cardiology in the Young , Volume 33 , Issue 4 , April 2023 , pp. 652 - 654
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Copyright
© The Author(s), 2022. Published by Cambridge University Press

Noonan syndrome is an autosomal dominant genetic disorder in which a high percentage of affected individuals have cardiovascular involvement. There are more than 14 described genes in the RAS-MAPK pathway that are associated with Noonan syndrome. Reference Roberts, Allanson, Tartaglia and Gelb1 There have been several genotype–phenotype associations made with respect to CHD associated with Noonan syndrome. Reference Pierpont and Digilio2,Reference Linglart and Gelb3 Here, we present two cases of PTPN11 variant Noonan syndrome with hypoplastic left heart syndrome variants. There has been one previous report of hypoplastic left heart syndrome and Noonan syndrome with the RAF1 mutation but, Reference Schulz, Fröber, Kraus and Schneider4 to our knowledge, a PTPN11 mutation genotype–phenotype association has not previously been described.

Case 1

A term male with prenatally diagnosed unbalanced atrioventricular canal to the right with arch hypoplasia was born to healthy, non-related parents. Postnatal echocardiography confirmed the prenatal diagnosis and additionally demonstrated mild to moderate right ventricular hypertrophy with normal function and severe left ventricle hypoplasia without pulmonary valve stenosis.

The patient underwent a Norwood procedure with a Blalock–Thomas–Taussig shunt at which time chylous fluid was identified in the pericardium. At 5 months of age, he underwent an elective bidirectional superior cavo-pulmonary connection. His post-operative course was complicated by refractory bilateral chylous effusions requiring multiple thoracostomy tube placements, pleurodeses, and thoracic duct embolisations with eventual takedown of the superior cavo-pulmonary connection and conversion to an aortopulmonary shunt. His post-operative course was further complicated by sepsis and eventual death at 13 months.

Autopsy showed a hypoplastic left heart variant with incomplete common atrioventricular canal with severe imbalance toward the right ventricle, and aortic valve hypoplasia. Additionally, there was evidence of dilated lymphatic channels through multiple organ systems on microscopic analysis.

He was diagnosed with Noonan syndrome shortly before he passed away and found to have a heterozygous pathogenic PTPN11 variant (c.1507G>C, p. Gly503Arg) Reference Tartaglia, Kalidas and Shaw5 with a normal microarray. There was no prior family history of Noonan syndrome.

Case 2

This patient was born at 37 weeks to healthy, non-related parents. He was postnatally diagnosed with unbalanced atrioventricular canal defect toward the right ventricle with aortic arch hypoplasia. Echocardiography also demonstrated moderate right atrioventricular regurgitation and stenosis and moderate right ventricle hypertrophy without pulmonary valve pathology.

On day of life 12, he underwent the Norwood procedure with a Blalock-Thomas-Taussig shunt. Postoperatively, he required chest washout for mediastinal haemorrhage. The postoperative course was further complicated by neuroblastoma, respiratory failure, and cardiac arrest secondary to acute shunt occlusion requiring venoarterial ECMO. Due to failure to wean from ECMO, his care was withdrawn and he passed away at 7 weeks old.

His autopsy showed a hypoplastic left heart variant with unbalanced atrioventricular canal defect and neuroblastoma with a dominant retroperitoneal mass as well as diffuse liver and lymph node involvement.

He was diagnosed with Noonan syndrome during his hospitalisation and found to have a heterozygous previously-reported pathogenic PTPN11 variant (c.182A>G, p. Asp61Gly) Reference Tartaglia, Kalidas and Shaw5 with a normal microarray. There was no prior family history of Noonan syndrome.

Discussion

Noonan syndrome is an autosomal dominant disorder with a high percentage of affected individuals having cardiovascular involvement. Many Noonan syndrome-associated PTPN11 pathogenic variants increase signalling through the RAS-MAPK pathway, which can have downstream effects on growth factors that influence cellular proliferation, survival and differentiation (Fig 1). Reference Roberts, Allanson, Tartaglia and Gelb1 These transcriptional effects can present with wide phenotypic variability which can often lead to a delay in diagnosis, as was seen in our first case. Atrioventricular canal defects can occur in up to 8% of patients with Noonan syndrome, and recent studies show an association with PTPN11 variants. Reference Linglart and Gelb3,Reference Digilio, Romana Lepri and Dentici6 Severely unbalanced atrioventricular defects leading to a hypoplastic left heart syndrome variants, however, have only been described one time in the literature in a patient with a RAF1 mutation. Reference Schulz, Fröber, Kraus and Schneider4 A better understanding of genotype–phenotype associations can lead to earlier diagnosis and improved care.

Figure 1. Growth factors bind to a receptor. Through the docking protein GRB2, SOS1, and PTPN11 are recruited which promotes activation of RAS and MAP-K pathway. ERK can enter the nucleus and alter transcription which has downstream effects on cellular proliferation and differentiation. MEK inhibitors, like trametinib, can inhibit this pathway. Gene variants associated with Noonan syndrome are depicted in green.

In patients with Noonan syndrome and hypoplastic left heart syndrome, there are several important periprocedural considerations. At least 10% of Noonan syndrome patients will have lymphovascular disorders including thoracic duct abnormalities which can be unmasked by cardiac surgery and present as refractory chylothoraces or lymphatic pericardial effusions as was seen in patient 1. Reference Linglart and Gelb3 Therefore, patients with Noonan syndrome may not tolerate the transition to Glenn or Fontan physiology which can increase venous congestion and exacerbate lymphatic disorders. Therefore, when anatomy permits, a patient with Noonan syndrome may benefit from biventricular repair or hybrid operative approach. Recently severe lymphovascular disorders have been successfully treated with trametinib, a RAS-MAPK pathway inhibitor, in a patient with the SOS1 variant of Noonan syndrome (Fig 1). Reference Dori, Smith and Pinto7 This may be an important treatment adjunct for patients with Noonan syndrome that must proceed down the single ventricle pathway, but more studies will need to be done to determine its efficacy in patients with the PTPN11 mutation.

Noonan syndrome may also affect the haematologic system with up to 65% of patients with Noonan syndrome having bleeding diatheses, including factor deficiencies and qualitative platelet disorders. Reference Artoni, Selicorni and Passamonti8 Patient 2 exhibited numerous haematologic complications including postoperative bleeding and early shunt thrombosis. Haematologic consultation to identify these coagulation disorders, therefore, is recommended prior to surgical intervention in patients with Noonan syndrome and could potentially improve perioperative outcomes. Haematologic malignancies and solid organ tumours can also occur frequently in Noonan syndrome from dysregulation of the RAS-MAPK pathway. Reference Smpokou, Zand, Rosenbaum and Summar9 For example, 2.9% of patients with neuroblastoma have pathogenic PTPN11 variants, so screening for these and other commonly associated malignancies is an important consideration in the care and prognosis of these patients.

Given these factors that can complicate periprocedural care, prognosis of patients with Noonan syndrome and hypoplastic left heart syndrome is poor. Both patients in this series, as well as the only other patient reported in the literature, Reference Schulz, Fröber, Kraus and Schneider4 suffered early death. Recently RAS-MAPK pathway inhibitors have been used to successfully manage lymphovascular complications and hypertrophic cardiomyopathy-related heart failure. Reference Andelfinger, Marquis and Raboisson10 In the future, other similar targeted therapies may be developed for patients with the PTPN11-related Noonan syndrome. We hope that a better understanding of the genotype–phenotype association between PTPN11 variant Noonan syndrome and hypoplastic left heart syndrome variants may lead to earlier diagnosis, more informed decisions around periprocedural care, and the potential for earlier availability of targeted therapies.

Acknowledgements

None.

Financial support

This research received no specific grant from any funding agency, commercial, or not-for-profit sectors.

Conflicts of interest

The authors have no conflicts to disclose.

Statements and declarations

None. The authors report no competing financial or non-financial interests that are related to the work submitted for publication.

References

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Figure 0

Figure 1. Growth factors bind to a receptor. Through the docking protein GRB2, SOS1, and PTPN11 are recruited which promotes activation of RAS and MAP-K pathway. ERK can enter the nucleus and alter transcription which has downstream effects on cellular proliferation and differentiation. MEK inhibitors, like trametinib, can inhibit this pathway. Gene variants associated with Noonan syndrome are depicted in green.