Autosomal recessive Noonan syndrome associated with biallelic LZTR1 variants

Johnston, Jennifer J.; Smagt, Jasper J. van der; Rosenfeld, Jill A.; Pagnamenta, Alistair T.; Alswaid, Abdulrahman; Baker, Eva H.; Blair, Edward; Borck, Guntram; Brinkmann, Julia; Craigen, William J.; Dũng, Vũ Chí; Emrick, Lisa; Everman, David B.; Gassen, Koen van; Gülsüner, Süleyman; Harr, Margaret; Jain, Mahim; Kuechler, Alma; Leppig, Kathleen A.; McDonald‐McGinn, Donna M.; Can, Ngoc Thi Bich; Peleg, Amir; Roeder, Elizabeth; Rogers, R. Curtis; Sagi‐Dain, Lena; Sapp, Julie C.; Schäffer, Alejandro A.; Schanze, Denny; Stewart, Helen; Taylor, Jenny C.; Verbeek, Nienke E.; Walkiewicz, Magdalena; Zackai, Elaine H.; Zweier, Christiane; Zenker, Martin; Lee, Brendan; Biesecker, Leslie G.

doi:10.1038/gim.2017.249

Cited by 170 publications

(214 citation statements)

References 23 publications

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“…Exome sequencing in search of disease‐causing variants revealed a pair of compound heterozygous LZTR1 variants (NM_006767.4:c.1605C > A [p.Tyr535Ter] [rs753347937] and NM_006767.4:c.2387T > C [p.Ile796Thr] [rs141672122]) that have never been associated with a disorder before but here co‐segregated with phenotype. According to the American College of Medical Genetics and Genomics consensus criteria (Richards et al, ), the former nonsense variant was evaluated as “pathogenic” and the latter as “likely pathogenic.” In line with the literature, our patients harbored a combination of one null and one putatively hypomorphic variant, further supporting the proposed loss‐of‐function mechanism of the disease (Johnston et al, ).…”

Section: Resultssupporting

confidence: 90%

“…Eighty percent of the patients carry dominant mutations in either the PTPN11 , KRAS , SOS1 , SOS2 , RAF1 , NRAS , BRAF , or RIT1 , all of which are members of the RAS/MAPK signaling cascade (Aoki, Niihori, Inoue, & Matsubara, ). Recently, recessive variants in the LZTR1 ( leucine‐zipper‐like transcription regulator 1 ) gene (OMIM #600574) were identified from genetic analyses of NS patients who had tested negative for known RAS/MAPK gene mutations (Johnston et al, ; Nakaguma, Jorge, & Arnhold, ; Umeki et al, ). LZTR1 is now emerging as a novel causative gene of NS pathophysiology.…”

Section: Introductionmentioning

confidence: 99%

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Noonan syndrome‐associated biallelic LZTR1 mutations cause cardiac hypertrophy and vascular malformations in zebrafish

Nakagama

Takeda

Ogawa

et al. 2019

Molec Gen & Gen Med

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Background Variants in the LZTR1 (leucine‐zipper‐like transcription regulator 1) gene (OMIM #600574) have been reported in recessive Noonan syndrome patients. In vivo evidence from animal models to support its causative role is lacking. Methods By CRISPR‐Cas9 genome editing, we generated lztr1‐mutated zebrafish (Danio rerio). Analyses of histopathology and downstream signaling were performed to investigate the pathogenesis of cardiac and extracardiac abnormalities in Noonan syndrome. Results A frameshift deletion allele was created in the zebrafish lztr1. Crosses of heterozygotes obtained homozygous lztr1 null mutants that modeled LZTR1 loss‐of‐function. Histological analyses of the model revealed ventricular hypertrophy, the deleterious signature of Noonan syndrome‐associated cardiomyopathy. Further, assessment for extracardiac abnormalities documented multiple vascular malformations, resembling human vascular pathology caused by RAS/MAPK activation. Due to spatiotemporal regulation of LZTR1, its downstream function was not fully elucidated from western blots of adult tissue. Conclusion Our novel zebrafish model phenocopied human recessive Noonan syndrome and supported the loss‐of‐function mechanism of disease‐causing LZTR1 variants. The discovery of vascular malformations in mutants calls for the clinical follow‐up of patients to monitor for its emergence. The model will serve as a novel platform for investigating the pathophysiology linking RAS/MAPK signaling to cardiac and vascular pathology.

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Section: Resultssupporting

confidence: 90%

Section: Introductionmentioning

confidence: 99%

Noonan syndrome‐associated biallelic LZTR1 mutations cause cardiac hypertrophy and vascular malformations in zebrafish

Nakagama

Takeda

Ogawa

et al. 2019

Molec Gen & Gen Med

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“…CBL, NRAS, and LZTR1 pathogenic variants were also detected in this study. In particular, germline LZTR1 pathogenic variants have been shown to be associated with NS in recent studies, which can follow either recessive or dominant inheritance patterns . In our study, two novel compound heterogeneous variants in the LZTR1 gene were identified in one patient with a typical NS phenotype, while neither her mother nor her father were clinically affected.…”

Section: Discussionmentioning

confidence: 50%

“…Noonan syndrome [NS (MIM 163950)] is an autosomal dominant/recessive disorder characterized by short stature, craniofacial dysmorphism, cardiac abnormalities, short and/or webbed neck, and cryptorchidism in male patients. Pathogenic variants in the genes encoding proteins implicated in the RAS‐MAPK signaling pathway are responsible for Noonan syndrome, leading to pathway dysregulation . Fifteen genes have been reported to be involved in NS to date: PTPN11, SOS1, RAF1, BRAF, HRAS, KRAS, NRAS, SHOC2, MAP2K1, MAP2K2, CBL, RIT1, RASA2, A2ML1 , and LZTR1 …”

Section: Introductionmentioning

confidence: 99%

Molecular and phenotypic spectrum of Noonan syndrome in Chinese patients

Yao

Tan

et al. 2019

Clinical Genetics

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Noonan syndrome (NS) is a common autosomal dominant/recessive disorder. No large‐scale study has been conducted on NS in China, which is the most populous country in the world. Next‐generation sequencing (NGS) was used to identify pathogenic variants in patients that exhibited NS‐related phenotypes. We assessed the facial features and clinical manifestations of patients with pathogenic or likely pathogenic variants in the RAS‐MAPK signaling pathway. Gene‐related Chinese NS facial features were described using artificial intelligence (AI).NGS identified pathogenic variants in 103 Chinese patients in eight NS‐related genes: PTPN11 (48.5%), SOS1 (12.6%), SHOC2 (11.7%), KRAS (9.71%), RAF1 (7.77%), RIT1 (6.8%), CBL (0.97%), NRAS (0.97%), and LZTR1 (0.97%). Gene‐related facial representations showed that each gene was associated with different facial details. Eight novel pathogenic variants were detected and clinical features because of specific genetic variants were reported, including hearing loss, cancer risk due to a PTPN11 pathogenic variant, and ubiquitous abnormal intracranial structure due to SHOC2 pathogenic variants. NGS facilitates the diagnosis of NS, especially for patients with mild/moderate and atypical symptoms. Our study describes the genotypic and phenotypic spectra of NS in China, providing new insights into distinctive clinical features due to specific pathogenic variants.

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“…Additional extracardiac features include neurodevelopmental disabilities, cryptorchidism, delayed puberty, lymphedema, bleeding disorders, and a slightly increased predisposition to hematologic and solid cancers (Roberts, Allanson, Tartaglia, & Gelb, ). Transmission was established to be autosomal dominant, although an autosomal recessive form has recently been identified (Johnston et al, ). The phenotype is variable, but penetrance is believed to be complete.…”

Section: Noonan Syndrome and The Rasopathiesmentioning

confidence: 99%

Congenital heart defects in Noonan syndrome: Diagnosis, management, and treatment

Linglart

Gelb

2020

American J of Med Genetics Pt C

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Noonan syndrome is a pleomorphic genetic disorder, in which a high percentage of affected individuals have cardiovascular involvement, most prevalently various forms of congenital heart disease (i.e., pulmonary valve stenosis, septal defects, left‐sided lesions, and complex forms with multiple anomalies). Care includes attentiveness to several comorbidities, some directly impacting cardiac management (bleeding diatheses and lymphatic anomalies). More than 50% of patients with Noonan syndrome harbor PTPN11 pathogenic variation, which results in hyperactivation of RAS/mitogen‐activated protein kinase signaling. Several other disease genes with similar biological effects have been uncovered for NS and phenotypically related disorders, collectively called the RASopathies. Molecular diagnosis with gene resequencing panels is now widely available, but phenotype variability and in some cases, subtlety, continues to make identification of Noonan syndrome difficult. Until genetic testing becomes universal for patients with congenital heart disease, alertness to Noonan syndrome's broad clinical presentations remains crucial. Genotype–phenotype associations for Noonan syndrome enable better prognostication for affected patients when a molecular diagnosis is established. We still lack Noonan syndrome‐specific treatment; however, newly developed anticancer RAS pathway inhibitors could fill that gap if safety and efficacy can be established for indications such as pulmonary valve stenosis.

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Autosomal recessive Noonan syndrome associated with biallelic LZTR1 variants

Cited by 170 publications

References 23 publications

Noonan syndrome‐associated biallelic LZTR1 mutations cause cardiac hypertrophy and vascular malformations in zebrafish

Noonan syndrome‐associated biallelic LZTR1 mutations cause cardiac hypertrophy and vascular malformations in zebrafish

Molecular and phenotypic spectrum of Noonan syndrome in Chinese patients

Congenital heart defects in Noonan syndrome: Diagnosis, management, and treatment

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