Your search keyword '"Noonan Syndrome"' showing total 5,768 results

101. The RRAS2 pathogenic variant (c.67G>T; p. Gly23Cys) produces Noonan syndrome with embryonal rhabdomyosarcoma.

Author

Zeng, Lan, Wang, Jin, Zhu, Hui, Huang, Yu, Deng, Yi, Wei, Ping, Nie, Jing, Tang, Bei, Chen, Ai, and Zhu, Shuyao

Subjects

*NOONAN syndrome, *CHROMOSOME analysis, *RHABDOMYOSARCOMA, *LITERATURE reviews, *SHORT stature, *STATURE

Abstract

Background: Noonan syndrome (NS) due to the RRAS2 gene, the pathogenic variant is an extremely rare RASopathies. Our objective was to identify the potential site of RRAS2, combined with the literature review, to find the correlation between clinical phenotype and genotype. De novo missense mutations affect different aspects of the RRAS2 function, leading to hyperactivation of the RAS‐MAPK signaling cascade. Methods: Conventional G‐banding was used to analyze the chromosome karyotype of the patient. Copy number variation sequencing (CNV‐seq) was used to detect the chromosomal gene microstructure of the patient and her parents. The exomes of the patient and her parents were sequenced using trio‐based whole exome sequencing (trio‐WES) technology. The candidate variant was verified by Sanger sequencing. The pathogenicity of the variant was predicted with a variety of bioinformatics tools. Results: Chromosome analysis of the proband revealed 46, XX, and no abnormality was found by CNV‐seq. After sequencing and bioinformatics filtering, the variant of RRAS2(c.67G>T; p. Gly23Cys) was found in the proband, while the mutation was absent in her parents. To the best of our knowledge, our patient was with the typical Noonan syndrome, such as short stature, facial dysmorphism, and developmental delay. Furthermore, our study is the first case of NS with embryonal rhabdomyosarcoma (ERMS) caused by the RRAS2 gene mutation reported in China. Conclusions: Our investigations suggested that the heterozygous missense of RRAS2 may be a potential causal variant in a rare cause of Noonan syndrome, expanding our understanding of the causally relevant mutations for this disorder. [ABSTRACT FROM AUTHOR]

Published

2024

102. RAF1 mutation leading to hypertrophic cardiomyopathy in a Chinese family with a history of sudden cardiac death: A diagnostic insight into Noonan syndrome.

Author

Zheng, Jingjing, Peng, Longyun, Cheng, Ruofei, Li, Zhiyan, Xie, Jianjie, Huang, Erwen, Cheng, Jianding, and Zhao, Qianhao

Subjects

*NOONAN syndrome, *CARDIAC arrest, *HYPERTROPHIC cardiomyopathy, *FAMILY history (Medicine), *FAMILY history (Sociology)

Abstract

Background: Hypertrophic cardiomyopathy (HCM) is predominantly caused by mutations in sarcomeric genes. However, a subset of cases is attributed to genetic disorders unrelated to sarcomeric genes, such as Noonan syndrome (NS) and other RASopathies. In this study, we present a family with a history of sudden cardiac death (SCD) and focus on two adults with syndromic left ventricular hypertrophy (LVH). Methods: Clinical evaluations, including echocardiography, were conducted to assess cardiac manifestations. Whole‐exome sequencing was performed to identify potential genetic variants underlying syndromic LVH in the study participants. Results: Whole‐exome sequencing revealed a missense variant in the RAF1 gene, c.782C>T (p.Pro261Leu). This variant confirmed the diagnosis of NS in the affected individuals. Conclusion: The findings of this study underscore the importance of family history investigation and genetic testing in diagnosing syndromic LVH. By identifying the underlying genetic cause, clinicians can better understand the etiology of RAS‐HCM and its association with SCD in young adults. [ABSTRACT FROM AUTHOR]

Published

2024

103. Restraining of glycoprotein VI- and integrin α2β1-dependent thrombus formation by platelet PECAM1.

Author

Jooss, Natalie J., Diender, Marije G., Fernández, Delia I., Huang, Jingnan, Heubel-Moenen, Floor C. J., van der Veer, Arian, Kuijpers, Marijke J. E., Poulter, Natalie S., Henskens, Yvonne M. C., te Loo, Maroeska, and Heemskerk, Johan W. M.

Abstract

The platelet receptors, glycoprotein VI (GPVI) and integrin α2β1 jointly control collagen-dependent thrombus formation via protein tyrosine kinases. It is unresolved to which extent the ITIM (immunoreceptor tyrosine-based inhibitory motif) receptor PECAM1 and its downstream acting protein tyrosine phosphatase PTPN11 interfere in this process. Here, we hypothesized that integrin α2β1 has a co-regulatory role in the PECAM1- and PTPN11-dependent restraint of thrombus formation. We investigated platelet activation under flow on collagens with a different GPVI dependency and using integrin α2β1 blockage. Blood was obtained from healthy subjects and from patients with Noonan syndrome with a gain-of-function mutation of PTPN11 and variable bleeding phenotype. On collagens with decreasing GPVI activity (types I, III, IV), the surface-dependent inhibition of PECAM1 did not alter thrombus parameters using control blood. Blockage of α2β1 generally reduced thrombus parameters, most effectively on collagen IV. Strikingly, simultaneous inhibition of PECAM1 and α2β1 led to a restoration of thrombus formation, indicating that the suppressing signaling effect of PECAM1 is masked by the platelet-adhesive receptor α2β1. Blood from 4 out of 6 Noonan patients showed subnormal thrombus formation on collagen IV. In these patients, effects of α2β1 blockage were counterbalanced by PECAM1 inhibition to a normal phenotype. In summary, we conclude that the suppression of GPVI-dependent thrombus formation by either PECAM1 or a gain-of-function of PTPN11 can be overruled by α2β1 engagement. [ABSTRACT FROM AUTHOR]

Published

2024

104. A Novel Homozygous Loss-of-Function Variant in SPRED2 Causes Autosomal Recessive Noonan-like Syndrome.

Author

Onore, Maria Elena, Caiazza, Martina, Farina, Antonella, Scarano, Gioacchino, Budillon, Alberto, Borrelli, Rossella Nicoletta, Limongelli, Giuseppe, Nigro, Vincenzo, and Piluso, Giulio

Subjects

*CONGENITAL heart disease, *NOONAN syndrome, *PULMONARY stenosis, *LEFT ventricular hypertrophy, *ATRIAL septal defects

Abstract

Noonan syndrome is an autosomal dominant developmental disorder characterized by peculiar facial dysmorphisms, short stature, congenital heart defects, and hypertrophic cardiomyopathy. In 2001, PTPN11 was identified as the first Noonan syndrome gene and is responsible for the majority of Noonan syndrome cases. Over the years, several other genes involved in Noonan syndrome (KRAS, SOS1, RAF1, MAP2K1, BRAF, NRAS, RIT1, and LZTR1) have been identified, acting at different levels of the RAS-mitogen-activated protein kinase pathway. Recently, SPRED2 was recognized as a novel Noonan syndrome gene with autosomal recessive inheritance, and only four families have been described to date. Here, we report the first Italian case, a one-year-old child with left ventricular hypertrophy, moderate pulmonary valve stenosis, and atrial septal defect, with a clinical suspicion of RASopathy supported by the presence of typical Noonan-like facial features and short stature. Exome sequencing identified a novel homozygous loss-of-function variant in the exon 3 of SPRED2 (NM_181784.3:c.325del; p.Arg109Glufs*7), likely causing nonsense-mediated decay. Our results and the presented clinical data may help us to further understand and dissect the genetic heterogeneity of Noonan syndrome. [ABSTRACT FROM AUTHOR]

Published

2024

105. A bicarotid trunk with associated right retroesophageal subclavian artery in a child with neurofibromatosis type 1 complicated by a left hemispheric stroke.

Author

Guarnizo, Angela, Erripa, José I., and Rugilo, Carlos

Subjects

*SUBCLAVIAN artery, *STROKE, *NEUROFIBROMATOSIS 1, *THORACIC aorta, *CAROTID artery, *NOONAN syndrome

Abstract

Purpose: To describe the association between two aortic arch branch variants and its possible relationship with neurofibromatosis-1. Methods: A 5-year-old female with NF-1 diagnosis presented to the emergency department at 2 months of age with irritability, vomiting and left gaze deviation. Brain MRI showed a left side acute hemispheric stroke and left internal carotid occlusion. Results: CT angiography of the neck showed the right and left common carotid arteries arising from a common vascular trunk coming from the aortic arch and a right retroesophageal subclavian artery. Conclusion: Although the relationship between NF-1 mutation and aortic arch branch abnormalities has not been described, there is a recognized condition known as neurofibromatosis/Noonan syndrome which is an accepted variant of NF-1 with clinical features of both NF-1 and Noonan syndrome caused by dysregulation of the RAS–MAPK pathway. Aortic arch branch variations in patients with NF-1 could be explained by this association. [ABSTRACT FROM AUTHOR]

Published

2023

106. Artificial Intelligence Procedure for the Screening of Genetic Syndromes Based on Voice Characteristics.

Author

Calà, Federico, Frassineti, Lorenzo, Sforza, Elisabetta, Onesimo, Roberta, D'Alatri, Lucia, Manfredi, Claudia, Lanata, Antonio, and Zampino, Giuseppe

Subjects

*GENETIC testing, *ARTIFICIAL intelligence, *SUPPORT vector machines, *NOONAN syndrome, *SYNDROMES, *K-nearest neighbor classification

Abstract

Perceptual and statistical evidence has highlighted voice characteristics of individuals affected by genetic syndromes that differ from those of normophonic subjects. In this paper, we propose a procedure for systematically collecting such pathological voices and developing AI-based automated tools to support differential diagnosis. Guidelines on the most appropriate recording devices, vocal tasks, and acoustical parameters are provided to simplify, speed up, and make the whole procedure homogeneous and reproducible. The proposed procedure was applied to a group of 56 subjects affected by Costello syndrome (CS), Down syndrome (DS), Noonan syndrome (NS), and Smith–Magenis syndrome (SMS). The entire database was divided into three groups: pediatric subjects (PS; individuals < 12 years of age), female adults (FA), and male adults (MA). In line with the literature results, the Kruskal–Wallis test and post hoc analysis with Dunn–Bonferroni test revealed several significant differences in the acoustical features not only between healthy subjects and patients but also between syndromes within the PS, FA, and MA groups. Machine learning provided a k-nearest-neighbor classifier with 86% accuracy for the PS group, a support vector machine (SVM) model with 77% accuracy for the FA group, and an SVM model with 84% accuracy for the MA group. These preliminary results suggest that the proposed method based on acoustical analysis and AI could be useful for an effective, non-invasive automatic characterization of genetic syndromes. In addition, clinicians could benefit in the case of genetic syndromes that are extremely rare or present multiple variants and facial phenotypes. [ABSTRACT FROM AUTHOR]

Published

2023

107. Research on the Pathogenesis of Cognitive and Neurofunctional Impairments in Patients with Noonan Syndrome: The Role of Rat Sarcoma–Mitogen Activated Protein Kinase Signaling Pathway Gene Disturbances.

Author

Braun-Walicka, Natalia, Pluta, Agnieszka, Wolak, Tomasz, Maj, Edyta, Maryniak, Agnieszka, Gos, Monika, Abramowicz, Anna, Landowska, Aleksandra, Obersztyn, Ewa, and Bal, Jerzy

Subjects

*NOONAN syndrome, *FUNCTIONAL magnetic resonance imaging, *PROTEIN kinases, *COGNITION disorders, *LARGE-scale brain networks

Abstract

Noonan syndrome (NS) is one of the most common genetic conditions inherited mostly in an autosomal dominant manner with vast heterogeneity in clinical and genetic features. Patients with NS might have speech disturbances, memory and attention deficits, limitations in daily functioning, and decreased overall intelligence. Here, 34 patients with Noonan syndrome and 23 healthy controls were enrolled in a study involving gray and white matter volume evaluation using voxel-based morphometry (VBM), white matter connectivity measurements using diffusion tensor imaging (DTI), and resting-state functional magnetic resonance imaging (rs-fMRI). Fractional anisotropy (FA) and mean diffusivity (MD) probability distributions were calculated. Cognitive abilities were assessed using the Stanford Binet Intelligence Scales. Reductions in white matter connectivity were detected using DTI in NS patients. The rs-fMRI revealed hyper-connectivity in NS patients between the sensorimotor network and language network and between the sensorimotor network and salience network in comparison to healthy controls. NS patients exhibited decreased verbal and nonverbal IQ compared to healthy controls. The assessment of the microstructural alterations of white matter as well as the resting-state functional connectivity (rsFC) analysis in patients with NS may shed light on the mechanisms responsible for cognitive and neurofunctional impairments. [ABSTRACT FROM AUTHOR]

Published

2023

108. The Cardiofaciocutaneous Syndrome: From Genetics to Prognostic–Therapeutic Implications.

Author

Scorrano, Giovanna, David, Emanuele, Calì, Elisa, Chimenz, Roberto, La Bella, Saverio, Di Ludovico, Armando, Di Rosa, Gabriella, Gitto, Eloisa, Mankad, Kshitij, Nardello, Rosaria, Mangano, Giuseppe Donato, Leoni, Chiara, and Ceravolo, Giorgia

Subjects

*GENETICS, *GENETIC variation, *BRAF genes, *NOONAN syndrome, *CRANIOFACIAL abnormalities

Abstract

Cardiofaciocutaneous (CFC) syndrome is one of the rarest RASopathies characterized by multiple congenital ectodermal, cardiac and craniofacial abnormalities with a mild to severe ocular, gastrointestinal and neurological involvement. It is an autosomal dominant syndrome, with complete penetrance, caused by heterozygous pathogenic variants in the genes BRAF, MAP2K1/MEK1, MAP2K2/MEK2, KRAS or, rarely, YWHAZ, all part of the RAS-MAPK pathway. This pathway is a signal transduction cascade that plays a crucial role in normal cellular processes such as cell growth, proliferation, differentiation, survival, metabolism and migration. CFC syndrome overlaps with Noonan syndrome, Costello syndrome, neurofibromatosis type 1 and Legius syndrome, therefore making the diagnosis challenging. Neurological involvement in CFC is more severe than in other RASopathies. Phenotypic variability in CFC patients is related to the specific gene affected, without a recognized genotype–phenotype correlation for distinct pathogenic variants. Currently, there is no specific treatment for CFC syndrome. Encouraging zebrafish model system studies suggested that, in the future, MEK inhibitors could be a suitable treatment of progressive phenotypes of CFC in children. A multidisciplinary care is necessary for appropriate medical management. [ABSTRACT FROM AUTHOR]

Published

2023

109. A Novel Heterozygous NF1 Variant in a Neurofibromatosis-Noonan Syndrome Patient with Growth Hormone Deficiency: A Case Report.

Author

Si Qin, Yindi Zhang, Fadong Yu, Yinxing Ni, and Jian Zhong

Subjects

*STATURE, *PHYSICAL diagnosis, *GENETIC mutation, *NOONAN syndrome, *MAGNETIC resonance imaging, *HUMAN growth hormone, *MATHEMATICAL variables, *EYEBROWS, *NEUROFIBROMATOSIS 1, *GROWTH disorders, *RARE diseases, *PHENOTYPES

Abstract

Neurofibromatosis-Noonan syndrome (NFNS), a rare autosomal-dominant hereditary disease, is characterized by clinical manifestations of both neurofibromatosis type 1 (NF1) and NS. We present a case of NFNS with short stature caused by a heterozygous nonsense variant of the NF1 gene. A 12-year-old boy was admitted because of short stature, numerous café-au-lait spots, low-set and posteriorly rotated ears, sparse eyebrows, broad forehead, and inverted triangular face. Cranial and spinal magnetic resonance imaging showed abnormal nodular lesions. Molecular analysis revealed a novel heterozygous c.6189 C > G (p.(Tyr2063*)) variant in the NF1 gene. The patient was not prescribed recombinant growth hormone (GH) therapy because exogenous GH may have enlarged the abnormal skeletal lesions. During follow-up, Lisch nodules were found in the ophthalmologic examination. NFNS, a variant form of NF1, is caused by heterozygous mutations in the NF1 gene. The mechanism of GH deficiency caused by NF1 is still unclear. Whether NFNS patients should be treated with exogenous GH remains controversial. [ABSTRACT FROM AUTHOR]

Published

2023

110. An Assessment of the Therapeutic Landscape for the Treatment of Heart Disease in the RASopathies.

Author

Yi, Jae-Sung, Perla, Sravan, and Bennett, Anton M.

Abstract

The RAS/mitogen-activated protein kinase (MAPK) pathway controls a plethora of developmental and post-developmental processes. It is now clear that mutations in the RAS-MAPK pathway cause developmental diseases collectively referred to as the RASopathies. The RASopathies include Noonan syndrome, Noonan syndrome with multiple lentigines, cardiofaciocutaneous syndrome, neurofibromatosis type 1, and Costello syndrome. RASopathy patients exhibit a wide spectrum of congenital heart defects (CHD), such as valvular abnormalities and hypertrophic cardiomyopathy (HCM). Since the cardiovascular defects are the most serious and recurrent cause of mortality in RASopathy patients, it is critical to understand the pathological signaling mechanisms that drive the disease. Therapies for the treatment of HCM and other RASopathy-associated comorbidities have yet to be fully realized. Recent developments have shown promise for the use of repurposed antineoplastic drugs that target the RAS-MAPK pathway for the treatment of RASopathy-associated HCM. However, given the impact of the RAS-MAPK pathway in post-developmental physiology, establishing safety and evaluating risk when treating children will be paramount. As such insight provided by preclinical and clinical information will be critical. This review will highlight the cardiovascular manifestations caused by the RASopathies and will discuss the emerging therapies for treatment. [ABSTRACT FROM AUTHOR]

Published

2023

111. Autism spectrum disorder profiles in RASopathies: A systematic review

Author

Edward Debbaut, Jean Steyaert, and Mouna El Bakkali

Subjects

autism spectrum disorder, cardio‐facio‐cutaneous syndrome, Costello syndrome, developmental phenotype, neurofibromatosis type 1, Noonan syndrome, Genetics, QH426-470

Abstract

Abstract Background RASopathies are associated with an increased risk of autism spectrum disorder (ASD). For neurofibromatosis type 1 (NF1) there is ample evidence for this increased risk, while for other RASopathies this association has been studied less. No specific ASD profile has been delineated so far for RASopathies or a specific RASopathy individually. Methods We conducted a systematic review to investigate whether a specific RASopathy is associated with a specific ASD profile, or if RASopathies altogether have a distinct ASD profile compared to idiopathic ASD (iASD). We searched PubMed, Web of Science, and Open Grey for data about ASD features in RASopathies and potential modifiers. Results We included 41 articles on ASD features in NF1, Noonan syndrome (NS), Costello syndrome (CS), and cardio‐facio‐cutaneous syndrome (CFC). Individuals with NF1, NS, CS, and CFC on average have higher ASD symptomatology than healthy controls and unaffected siblings, though less than people with iASD. There is insufficient evidence for a distinct ASD phenotype in RASopathies compared to iASD or when RASopathies are compared with each other. We identified several potentially modifying factors of ASD symptoms in RASopathies. Conclusions Our systematic review found no convincing evidence for a specific ASD profile in RASopathies compared to iASD, or in a specific RASopathy compared to other RASopathies. However, we identified important limitations in the research literature which may also account for this result. These limitations are discussed and recommendations for future research are formulated.

Published

2024

112. Gonadal dysfunction in a man with Noonan syndrome from the LZTR1 variant: case report and review of literature

Author

Francesca Orsolini, Luisa Pignata, Fulvia Baldinotti, Silvia Romano, Massimo Tonacchera, and Domenico Canale

Subjects

Noonan syndrome, gonadal function, fertility, LZTR1 variant, case report, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Noonan syndrome (NS) is a genetic disorder characterized by multiple congenital defects caused by mutations in the RAS/mitogen-activated protein kinase pathway. Male fertility has been reported to be impaired in NS, but only a few studies have focused on fertility status in NS patients and underlying mechanisms are still incompletely understood. We describe the case of a 35-year-old man who underwent an andrological evaluation due to erectile dysfunction and severe oligospermia. A syndromic facial appearance and reduced testis size were present on clinical examination. Hormonal evaluation showed normal total testosterone level, high FSH level, and low–normal AMH and inhibin B, compatible with primary Sertoli cell dysfunction. Genetic analysis demonstrated the pathogenetic heterozygous variant c.742G>A, p.(Gly248Arg) of the LZTR1 gene (NM_006767.3). This case report provides increased knowledge on primary gonadal dysfunction in men with NS and enriches the clinical spectrum of NS from a rare variant in the novel gene LZTR1.

Published

2024

113. Diagnosis challenges in CHARGE syndrome: A novel variant and clinical description

Author

Samantha Saenz Hinojosa, Carlos Reyes, and Vanessa I. Romero

Subjects

CHARGE syndrome, Genetic testing, Misdiagnosis, CHD7, Noonan syndrome, Science (General), Q1-390, Social sciences (General), H1-99

Abstract

Introduction: In resource-limited settings, patients with uncommon phenotypes often face prolonged diagnostic journeys and potential misdiagnoses. Coloboma, heart defects, atresia choanae, restricted growth and development, genital and ear abnormalities syndrome (CHARGE) syndrome, a congenital condition affecting various body parts such as the heart, ears, eyes, and genitals, exemplifies this challenge. Case presentation: We present the case of a 21-year-old male patient from Ecuador who exhibited hypogonadism, facial deformities, and stunted growth. Due to the scarcity of genetic specialists and limited access to genetic testing in Ecuador, the patient received a misdiagnosis of Noonan syndrome. However, a correct diagnosis of CHARGE syndrome was ultimately reached after eight years, facilitated by genetic sequencing that identified a novel mutation in the Chromodomain helicase DNA binding protein 7 gene. Conclusion: This case highlights the critical role of meticulously assessing patients' symptoms and emphasizes the necessity for enhanced collaboration among physicians and researchers. Such efforts are pivotal in advancing healthcare access and equity for individuals in developing nations.

Published

2024

114. Phenotypic and genotypic spectrum of noonan syndrome: A retrospective analysis of 46 consecutive pediatric patients presented at a regional cardiac center in China

Author

Qinchang Chen, Dian Hong, Yulu Huang, Zhiwei Zhang, and Shushui Wang

Subjects

Noonan syndrome, Genotype, Phenotype, Epidemiology, Science (General), Q1-390, Social sciences (General), H1-99

Abstract

Background: Noonan syndrome (NS) is relatively common but poorly recognized. We aimed to describe the phenotypic and genotypic spectrum of NS in a Chinese cohort. Method: The study retrospectively investigated consecutive pediatric patients who presented at the Guangdong cardiovascular institute between 2018 and 2020 with confirmed known NS-relevant mutations determined by exome sequencing. Dates of genetic testing, Age, sex, institution of genetic testing, mutated gene (related to NS) and its classification, heterozygosity, and parental origin were identified from the sequencing reports. Facial features, cardiac defect and other clinical characteristics were also assessed. Comparisons of categorical variables between groups were examined by Chi-square test or Fisher's exact test when appropriate. Intraclass correlation coefficient (ICC) was performed to evaluate the reliability of evaluation of facial features between different evaluators. Results: The most prevalent mutated genes were PTPN11 (37.0%) and RAF1 (19.6%), and most mutations were pathogenic (67.4%) and de novo (87.0%). Most patients were with NS-relevant facial features (97.4%) and cardiac defects (92.7%), where ventricular hypertrophy, pulmonary valve stenosis, and atrial septal defect were the most prevalent. Patients with mutated RAF1 appeared to be diagnosed at an older age than those with mutated PTPN11, and with higher prevalence of mitral regurgitation, hypertrophic cardiomyopathy, and ventricular hypertrophy, but lower prevalence of pulmonary valve stenosis and pulmonary artery stenosis. Patients presented at an age ≥2 years appeared to be with fewer NS-relevant facial features and cardiac defects than those aged

Published

2024

115. Cross-species analysis of LZTR1 loss-of-function mutants demonstrates dependency to RIT1 orthologs.

Author

Cuevas-Navarro, Antonio, Rodriguez-Muñoz, Laura, Grego-Bessa, Joaquim, Cheng, Alice, Rauen, Katherine A, Urisman, Anatoly, McCormick, Frank, Jimenez, Gerardo, and Castel, Pau

Subjects

Animals, Mice, ras Proteins, Adaptor Proteins, Signal Transducing, Drosophila Proteins, Transcription Factors, Signal Transduction, Cell Proliferation, Ubiquitination, CG3711, D. melanogaster, LZTR1, RASopathy, RIC, RIT1, cancer biology, genetics, genomics, human, mouse, noonan syndrome, 1.1 Normal biological development and functioning, Underpinning research, Generic health relevance, D, melanogaster, Human, Mouse, Biochemistry and Cell Biology

Abstract

RAS GTPases are highly conserved proteins involved in the regulation of mitogenic signaling. We have previously described a novel Cullin 3 RING E3 ubiquitin ligase complex formed by the substrate adaptor protein LZTR1 that binds, ubiquitinates, and promotes proteasomal degradation of the RAS GTPase RIT1. In addition, others have described that this complex is also responsible for the ubiquitination of classical RAS GTPases. Here, we have analyzed the phenotypes of Lztr1 loss-of-function mutants in both fruit flies and mice and have demonstrated a biochemical preference for their RIT1 orthologs. Moreover, we show that Lztr1 is haplosufficient in mice and that embryonic lethality of the homozygous null allele can be rescued by deletion of Rit1. Overall, our results indicate that, in model organisms, RIT1 orthologs are the preferred substrates of LZTR1.

Published

2022

116. Post Marketing Surveillance on Long-term Use With Norditropin® (Short Stature Due to Noonan Syndrome)

Published

2022

117. Charting new frontiers in paediatric cardiomyopathies: lessons from the ESC EORP Cardiomyopathy and Myocarditis Registry in paediatric age.

Author

Sabatino, Jolanda, Budts, Werner, and Salvo, Giovanni Di

Subjects

MYOCARDITIS, CONGENITAL heart disease, PEDIATRICS, NOONAN syndrome, HYPERTROPHIC cardiomyopathy

Abstract

The article discusses the European Paediatric Cardiomyopathy and Myocarditis Registry, which aims to improve understanding and management of childhood-onset cardiomyopathies (CMPs). The registry provides valuable information about the complex nature of CMP and highlights the need for early diagnosis, genetic assessment, and tailored therapeutic approaches. The study also identifies the prevalence of hereditary and genetic disorders in children with CMP and emphasizes the importance of identifying rare disease phenocopies for targeted therapies. However, the study acknowledges limitations in registry studies and the need for further research to overcome obstacles to early diagnosis. Overall, the registry's insights have the potential to improve outcomes and well-being for affected children and their families. [Extracted from the article]

Published

2024

118. A Rare Neurological Presentation of Noonan Syndrome and Its Management—A Case Report.

Author

Mahajan, Shalvi, Narayanan, Vidhya, Narayan, Vinitha, and Depuru, Aparna

Subjects

*NOONAN syndrome, *CONGENITAL heart disease, *CRANIOVERTEBRAL junction, *CONGENITAL disorders, *CEREBROVASCULAR disease

Abstract

Although Noonan syndrome is a relatively common congenital disorder with autosomal dominant inheritance, its association with cerebrovascular anomalies is rare. We report a case of a 20-year-old with Noonan syndrome with cerebrovascular aneurysm, who underwent successful endovascular coiling. Only four cases of cerebrovascular aneurysms in Noonan syndrome have been reported in the literature so far. To the best of our knowledge, this is only the fifth reported case and the first one that has been treated successfully with endovascular coiling. We hereby discuss the management of this case, which had several comorbidities like congenital heart disease and craniovertebral junction anomaly. [ABSTRACT FROM AUTHOR]

Published

2024

119. Noonan Syndrome

Author

Murray, Alison, Sarwark, John F., editor, and Carl, Rebecca L., editor

Published

2023

120. Improvement of synaptic plasticity and cognitive function in RASopathies—a monocentre, randomized, double-blind, parallel-group, placebo-controlled, cross-over clinical trial (SynCoRAS)

Author

Nikolai H. Jung, Silvia Egert-Schwender, Beate Schossow, Victoria Kehl, Ute Wahlländer, Louisa Brich, Viktoria Janke, Christiane Blankenstein, Martin Zenker, and Volker Mall

Subjects

RASopathies, Neurofibromatosis type 1, Noonan syndrome, Transcranial magnetic stimulation, Synaptic plasticity, Attention, Medicine (General), R5-920

Abstract

Abstract Background Cognitive impairment is a common medical issue in rat sarcoma (RAS) pathway disorders, so-called RASopathies, like Neurofibromatosis type 1 (NF1) or Noonan syndrome (NS). It is presumed to be caused by impaired synaptic plasticity. In animal studies, pathway-specific pharmacological interventions with lovastatin (LOV) and lamotrigine (LTG) have been shown to improve synaptic plasticity as well as cognitive function. The aim of this clinical trial is to translate the findings of animal studies to humans and to probe the effect of lovastatin (NS) and lamotrigine (NS and NF1) on synaptic plasticity and cognitive function/alertness in RASopathies. Methods Within this phase IIa, monocentre, randomized, double-blind, parallel-group, placebo-controlled, cross-over clinical trial (syn. SynCoRAS), three approaches (approaches I–III) will be carried out. In patients with NS, the effect of LTG (approach I) and of LOV (approach II) is investigated on synaptic plasticity and alertness. LTG is tested in patients with NF1 (approach III). Trial participants receive a single dose of 300 mg LTG or placebo (I and III) and 200 mg LOV or placebo (II) daily for 4 days with a cross-over after at least 7 days. Synaptic plasticity is investigated using a repetitive high-frequency transcranial magnetic stimulation (TMS) protocol called quadri-pulse theta burst stimulation (qTBS). Attention is examined by using the test of attentional performance (TAP). Twenty-eight patients are randomized in groups NS and NF1 with n = 24 intended to reach the primary endpoint (change in synaptic plasticity). Secondary endpoints are attention (TAP) and differences in short interval cortical inhibition (SICI) between placebo and trial medication (LTG and LOV). Discussion The study is targeting impairments in synaptic plasticity and cognitive impairment, one of the main health problems of patients with RASopathies. Recent first results with LOV in patients with NF1 have shown an improvement in synaptic plasticity and cognition. Within this clinical trial, it is investigated if these findings can be transferred to patients with NS. LTG is most likely a more effective and promising substance improving synaptic plasticity and, consecutively, cognitive function. It is expected that both substances are improving synaptic plasticity as well as alertness. Changes in alertness may be a precondition for improvement of cognition. Trial registration The clinical trial is registered in ClinicalTrials.gov (NCT03504501; https://www.clinicaltrials.gov ; date of registration: 04/11/2018) and in EudraCT (number 2016–005022-10).

Published

2023

121. Proteomic analysis of salivary inflammatory biomarkers of developmental gingival enlargements in patients with West and Noonan syndromes: a preliminary pilot single-center retrospective study.

Author

GUGLIELMI, F., KIRSCHNER, F., STADERINI, E., IAVARONE, F., FIORINO, A., and GALLENZI, P.

Abstract

OBJECTIVE: The aim of the preliminary pilot single-center retrospective cross-sectional study was to analyze and compare the presence of non-secretory salivary inflammatory biomarkers in pediatric patients with West syndrome, Noonan syndrome, and a healthy control group. PATIENTS AND METHODS: A total of 60 saliva samples were collected during dental checkups. The saliva samples collected were analyzed by liquid chromatography. The results were analyzed with a t-test, and the statistical significance was given by a p-value lower than 0.05. RESULTS: We found statistical significance for defensin a1 (p=0.006) and thymosin ß4 (p=0.025) in the Noonan syndrome. In the West syndrome, only the defensin a1 had a statistically significant difference with the other groups (p=0.022). Proteomic analysis revealed an overexpression of peptides related to the innate (thymosin ß4) and acquired (defensin a1, a3) immunity. CONCLUSIONS: W est a nd N oonan's s yndromes showed the overexpression of molecular biomarkers involved in the pathogenesis of chronic periodontitis. The inflammatory status is triggered and amplified by the abnormal overgrowth of gingival tissues, the amplified release of proinflammatory cytokines from the immune cells, and the poor cooperation in maintaining adequate oral hygiene. [ABSTRACT FROM AUTHOR]

Published

2023

122. Noonan syndrome: rhGH treatment and PTPN11 mutation.

Author

Wu, Xian, Wu, Jiali, Yuan, Yi, Yang, Li, and Yu, Lirong

Subjects

*NOONAN syndrome, *HUMAN growth hormone, *SHORT stature, *HEART abnormalities, *BONE metabolism, *SOMATOTROPIN

Abstract

Objective: To analyze the clinical data and genetic characteristics of Noonan syndrome, both the effect and side effects of recombinant human growth hormone (rhGH) treatment. Methods: We collected clinical data from 8 children with Noonan syndrome diagnosed from November 2017 to June 2021. The diagnosis was clarified by exome second‐generation sequencing and parental PCR‐NGS validation and interpretation of the preceding evidence, and growth hormone therapy was administered. Of the cases, four males and four females were seen for slow height growth and the median age at diagnosis was 8 years 7 months (1 year 7 months to 12 years 6 months). Results: Here, 7 children were treated with rhGH. Compared to the pre‐treatment period, the growth rate increased after rhGH treatment [3.7 ± 0.5 cm/year before treatment and 8.0 ± 1.0 cm/year after treatment, p < 0.01], with the maximum growth rate between 3 and 6 months of treatment and decreasing with the duration of treatment thereafter. The growth hormone treatment was discontinued and the orthopedic consultation was ordered with regular follow‐up, which was considered to be related to the PTPN11 mutation. Conclusion: Noonan syndrome is characterized by slow growth, short stature, mental retardation, peculiar facial features, structural heart abnormalities and abnormal bone metabolism. and osteochondroma was found after case 2 rhGH treatment. Genetic examination is mostly caused by PTPN11 mutation. It is recommended to pay attention to bone metabolism abnormalities before growth hormone treatment, especially in children with PTPN11 mutations. We analyze the clinical data and genetic characteristics of Noonan syndrome, both the effect and side effects of recombinant human growth hormone (rhGH) treatment. [ABSTRACT FROM AUTHOR]

Published

2023

123. Neuropsychiatric phenotypes in children with Noonan syndrome.

Author

Naylor, Paige E., Bruno, Jennifer L., Shrestha, Sharon Bade, Friedman, Marcelle, Jo, Booil, Reiss, Allan L., and Green, Tamar

Subjects

*NOONAN syndrome, *SYNDROMES in children, *SENSORY disorders, *AUTISM spectrum disorders, *ATTENTION-deficit hyperactivity disorder, *PHENOTYPES

Abstract

Aim: We investigated neuropsychiatric outcomes in children with Noonan syndrome and addressed limitations in previous research with a focus on prepubertal children, comparison to typically developing children, comprehensive neuropsychiatric evaluation, and controlling for overall cognitive abilities. Method: Forty-five children with Noonan syndrome (mean = 8 years 6 months, SD = 2 years 2 months; 29 females) and 40 typically developing children (mean = 8 years 9 months, SD = 2 years; 22 females) were evaluated with objective, parent-report, and psychiatric interview measures. Results: Children with Noonan syndrome demonstrated elevated symptoms across attention-deficit/hyperactivity disorder (ADHD) (attention, hyperactivity, and inhibition), autism spectrum disorder (ASD) (maintaining social relationships, behavioral rigidity, and sensory sensitivity), and oppositional defiant disorder (ODD) (aggression) symptom clusters relative to typically developing children (all p < 0.05). Group differences in nearly all parent-report measures were significant after accounting for variations in intellectual functioning, suggesting that increased neurodevelopmental symptoms are not simply driven by overall intelligence. Twenty out of 42 children with Noonan syndrome met criteria for ADHD, eight out of 42 for ODD, and 11 out of 43 demonstrated clinically significant symptoms seen in children with ASD. Interpretation: Children with Noonan syndrome are at increased risk for a range of ADHD, ASD, and ODD associated symptoms. A dimensional approach reveals significant ASD symptoms in Noonan syndrome that do not emerge when using the currently accepted categorical diagnostic approach. [ABSTRACT FROM AUTHOR]

Published

2023

124. Rare Congenital Dissecting Thoracic Aortic Aneurysm in a Child with Noonan Syndrome: A Case Report.

Author

Ahmad Maulana, Siti Aishah, Engku Alwi, Sharifah Huda, Hashim, Mohd Shafie, and Abdul Rohim, Rabiatul Adawiyah

Subjects

*DISSECTING aneurysms, *RESPIRATORY diseases, *THORACIC aneurysms, *CHEST X rays, *MEDIASTINUM, *BLOOD vessels, *CARDIAC hypertrophy, *NOONAN syndrome, *SURGICAL complications, *ATRIAL septal defects, *RISK assessment, *ELECTROCARDIOGRAPHY, *COMPUTED tomography, *AORTIC dissection, *RARE diseases, *DISEASE risk factors

Abstract

We present a rare case of congenital thoracic aortic aneurysm (TAA) complicated with dissection in a nine-year-old girl with Noonan syndrome and atrial septal defect. She presented with rapid breathing and upper respiratory tract symptoms. Chest X-ray revealed a huge upper mediastinum with cardiomegaly. Echocardiogram showed possible ascending TAA. Computerized tomography angiogram of the aorta revealed huge aortic root-ascending TAA with small aortic dissection. Despite immediate treatment, the patient passed away due to severe airway compromise. [ABSTRACT FROM AUTHOR]

Published

2023

125. Case report: Noonan syndrome with protein-losing enteropathy.

Author

Yang Ou, Jun-Chao Yuan, Yao Zheng, Jin-Man Zhang, Tian He, Zhi Liang, and Yi-Kun Zhou

Subjects

PROTEIN-losing enteropathy, NOONAN syndrome, CONGENITAL heart disease, SHORT stature, GENETIC mutation

Abstract

Background: Noonan syndrome (NS) is characterized by typical facial features, short stature, congenital heart defects and other comorbidities. Lymphedema and chylous pleural effusions are also common in NS, but protein-losing enteropathy (PLE) is rarely reported. Case presentation: We present the case of a 19-year-old Chinese woman presenting with PLE. Small intestine biopsy showed obvious expansion of lymphatic vessels. The gene mutation results of the patient indicated a c.184T>G missense mutation (p. Tyr62Asp) in the PTPN11 gene (NM_002834.3). Conclusion: NS accompanied by PLE is not common, but hypoproteinemia attributable to PLE may be more common in patients with NS than previously thought. It remains uncertain whether mutation of the PTPN11 gene is related to PLE, indicating that further research is needed. [ABSTRACT FROM AUTHOR]

Published

2023

126. Non-Contrast MR Lymphography and Intranodal Dynamic Contrast MR Lymphangiography in Children with Congenital Heart Disease—Imaging Findings as well as Impact on Patient Management and Outcome.

Author

Bauer, Christoph, Scala, Mario, Sekyra, Pavel, Fellner, Franz, and Tulzer, Gerald

Subjects

*LYMPHANGIOGRAPHY, *CONGENITAL heart disease, *PROTEIN-losing enteropathy, *LYMPHATIC abnormalities, *NOONAN syndrome, *THORACIC duct, *AGENESIS of corpus callosum

Abstract

Lymphatic flow disorders are rare but devastating complications in children with congenital heart disease. T2-weighted magnetic resonance lymphography and intranodal dynamic contrast magnetic resonance lymphangiography are imaging modalities that can depict central lymphatic anatomy and flow pattern. Our objective was to describe the technical aspects and our imaging findings of central lymphatic abnormalities and their impact on patient management and outcomes: We conducted a retrospective review of 26 children with congenital heart disease who presented for lymphatic imaging between 2015 and 2020 at our institution. Eleven had postoperative chylothorax, six had plastic bronchitis, seven had protein-losing enteropathy and three had Noonan syndrome. Our lymphatic imaging demonstrated severely abnormal lymphatic flow in all of the children, but only minor abnormalities in protein-losing enteropathy. No major procedure-related complication occurred. Lymphatic interventions were performed in six patients, thoracic duct decompression in two patients and chylothorax revision in three patients. This led to symptomatic improvements in all of the patients: Lymphatic imaging is safe and essential for the diagnosis of lymphatic flow disorders and therapy planning. Our intranodal lymphangiography depicts an abnormal lymphatic flow pattern from the central lymphatics but failed to demonstrate an abnormal lymphatic flow in protein-losing enteropathy. These imaging techniques are the basis for selective lymphatic interventions, which are promising to treat lymphatic flow disorders. [ABSTRACT FROM AUTHOR]

Published

2023

127. Anterior Uveitis and Coats Disease in a 16-Year-Old Girl with Noonan Syndrome—A Case Report.

Author

Świerczyńska, Marta, Tronina, Agnieszka, Lorenc, Anna, and Filipek, Erita

Subjects

RETINAL disease diagnosis, GENETIC mutation, PHOTOBIOMODULATION therapy, NOONAN syndrome, EYE pain, TELANGIECTASIA, VISUAL acuity, IRIDOCYCLITIS, VISION disorders, PHENOTYPES, CARBOCYCLIC acids, ADOLESCENCE

Abstract

Background: Noonan syndrome (NS) represents a fairly common genetic disorder with a highly variable phenotype. Its features include inherited heart defects, characteristic facial features, short stature, and mild retardation of motor skills. Case presentation: A 16-year-old Caucasian girl with NS reported visual deterioration, photophobia, and pain in the right eye (RE). The initial best-corrected visual acuity (BCVA) was 0.3 in the RE. An examination demonstrated conjunctival and ciliary body hyperemia, keratic precipitates, and flare in the anterior chamber. In addition, post-hemorrhagic floaters, tortuous vessels, and an epiretinal membrane in the RE were present. Diagnosis of unilateral anterior uveitis was made, and this resolved after the use of topical steroids and cycloplegic drops. Due to the presence of retinal telangiectasias and extraocular exudates (consistent with Coats' disease (CD) stage 2A) in the RE, laser therapy was performed. The patient remains under constant follow-up, and after one year, the BCVA in the RE was 0.7. Conclusions: Here, we report the clinical characteristics, genetic findings, and retinal imaging results of a patient with NS. To our knowledge, this is, to date, the first report of an association of NS with a PTPN11 mutation with anterior uveitis and CD. [ABSTRACT FROM AUTHOR]

Published

2023

128. Mastocytosis in a Case of Noonan Syndrome Caused by a De Novo Pathogenic CBL Variant.

Author

Tatsuya Kawaguchi, Tohru Okanishi, Tetsuya Okazaki, Chisako Aoki, Noriko Kasagi, Kaori Adachi, Yuichi Yoshida, Noriko Miyake, Naomichi Matsumoto, and Yoshihiro Maegaki

Subjects

NOONAN syndrome, MAST cell disease, GENETIC disorder diagnosis, CELLULAR signal transduction, BONE marrow

Abstract

Noonan syndrome is an autosomal dominant disease characterized by multi-organ disorders caused by variants of genes involved in the RAS/MAPK signaling pathway. The nine causative genes including PTPN11 and CBL have been identified. Mastocytosis is a disease characterized by mast cell proliferation in skin, bone marrow, and other organs. To date, no previous cases of Noonan syndrome with mastocytosis caused by a pathogenic CBL variant have been reported. A boy was diagnosed with Noonan syndrome at 8 months of age with facial features and minor anomaly of his body. He presented with brown nodules of 5-10 mm on his body since the age of 2 months. The patient was diagnosed with mastocytosis by a biopsy specimen from brown nodules, which showed infiltration of mast cells. Whole-exome sequencing of the parent--patient trio revealed a de novo pathogenic CBL variant. The occurrence of mastocytosis may be a cue for the analysis of the CBL gene in Noonan syndrome. The CBL gene is involved in mastocytosis and various cancers. In the case of the pathogenic variant, long-term follow-up for the risk of cancers related to the CBL variant is necessary. [ABSTRACT FROM AUTHOR]

Published

2023

129. Clinical profile and outcomes of pediatric hypertrophic cardiomyopathy in a South Indian tertiary care cardiac center: a three decade experience.

Author

Mukhtar, Gousia, Sasidharan, Bijulal, Krishnamoorthy, Kavassery Mahadevan, Kurup, Harikrishnan K. N., Gopalakrishnan, Arun, SasiKumar, Deepa, P, Sankara Sarma, Valaparambil, Ajit Kumar, Sivasubramonian, Sivasankaran, and Sivadasanpillai, Harikrishnan

Subjects

HYPERTROPHIC cardiomyopathy, HEART failure, NOONAN syndrome, ATRIAL arrhythmias, VENTRICULAR arrhythmia, CARDIAC arrest, TERTIARY care

Abstract

Introduction: Although much research has been done on adult hypertrophic cardiomyopathy, data on pediatric hypertrophic cardiomyopathy is still limited. Methods and results: The study enrolled all patients with cardiomyopathy who presented to us between 1990 to 2020 and were younger than 18 yrs. During the thirty-year study period, we identified 233 cases of pediatric cardiomyopathy. Sixty-three cases (27%) had hypertrophic cardiomyopathy. Out of the 63 HCM cases, 12% presented in the neonatal period and 37% presented in the first year of life. The median age of presentation was 7 yrs (Range 0.1–18 yrs). Sixteen patients had proven syndromic, metabolic, or genetic disease (25%). LV outflow obstruction was present in 30 patients (47%). Noonan syndrome was present in 9 of the 63 patients (14%). Dyspnea on exertion was the most common mode of presentation. Cardiac MRI was done in 28 patients, out of which 17 had late gadolinium enhancement (LGE). Mid myocardial enhancement was the most common pattern. Four patients had LGE of more than 15%. Over a mean follow-up period of 5.6 years (0.1–30 years), twenty-one were lost to follow-up (33%). Among the patients whose outcome was known, eleven died (26%), and thirty-one (73%) were alive. The 5-year survival rate of HCM patients was 82%, and the 10-year survival rate was 78%. Seven died of sudden cardiac death, three from heart failure, and one from ventricular arrhythmias. Sustained ventricular arrhythmias were seen in three patients and atrial arrhythmias in two. First-degree AV block was seen in 10 patients (15%) and bundle branch blocks (BBB) in five (8%). Eight patients required ICD or transplant (12.7%). Two patients underwent ICD for primary prevention, and one underwent PPI for distal AV conduction disease. Among the various clinical, echocardiographic, and radiological risk factors studied, only consanguinity showed a trend towards higher events of death or ventricular arrhythmias (P-value 0.08). Conclusion: More than one-third of our HCM cohort presented in infancy. LV outflow tract obstruction is common (47%). Mid myocardial enhancement was the most common pattern of late gadolinium enhancement. SCD was the most common cause of death. The outcome in our HCM cohort is good and similar to other population cohorts. Only Consanguinity showed a trend towards higher events of death or ventricular arrhythmias. [ABSTRACT FROM AUTHOR]

Published

2023

130. Abnormalities of pubertal development and gonadal function in Noonan syndrome.

Author

Patti, Giuseppa, Scaglione, Marco, Maiorano, Nadia Gabriella, Rosti, Giulia, Divizia, Maria Teresa, Camia, Tiziana, De Rose, Elena Lucia, Zucconi, Alice, Casalini, Emilio, Napoli, Flavia, Di Iorgi, Natascia, and Maghnie, Mohamad

Subjects

PUBERTY, NOONAN syndrome, GENETIC counseling, LYMPHATIC abnormalities, CONGENITAL heart disease, SHORT stature

Abstract

Background: Noonan syndrome (NS) is a genetic multisystem disorder characterised by variable clinical manifestations including dysmorphic facial features, short stature, congenital heart disease, renal anomalies, lymphatic malformations, chest deformities, cryptorchidism in males. Methods: In this narrative review, we summarized the available data on puberty and gonadal function in NS subjects and the role of the RAS/mitogen-activated protein kinase (MAPK) signalling pathway in fertility. In addition, we have reported our personal experience on pubertal development and vertical transmission in NS. Conclusions: According to the literature and to our experience, NS patients seem to have a delay in puberty onset compared to the physiological timing reported in healthy children. Males with NS seem to be at risk of gonadal dysfunction secondary not only to cryptorchidism but also to other underlying developmental factors including the MAP/MAPK pathway and genetics. Longterm data on a large cohort of males and females with NS are needed to better understand the impact of delayed puberty on adult height, metabolic profile and well-being. The role of genetic counselling and fertility related-issues is crucial. [ABSTRACT FROM AUTHOR]

Published

2023

131. Minor intron retention drives clonal hematopoietic disorders and diverse cancer predisposition

Author

Inoue, Daichi, Polaski, Jacob T, Taylor, Justin, Castel, Pau, Chen, Sisi, Kobayashi, Susumu, Hogg, Simon J, Hayashi, Yasutaka, Pineda, Jose Mario Bello, El Marabti, Ettaib, Erickson, Caroline, Knorr, Katherine, Fukumoto, Miki, Yamazaki, Hiromi, Tanaka, Atsushi, Fukui, Chie, Lu, Sydney X, Durham, Benjamin H, Liu, Bo, Wang, Eric, Mehta, Sanjoy, Zakheim, Daniel, Garippa, Ralph, Penson, Alex, Chew, Guo-Liang, McCormick, Frank, Bradley, Robert K, and Abdel-Wahab, Omar

Subjects

Biological Sciences, Bioinformatics and Computational Biology, Rare Diseases, Genetics, Hematology, Cancer, Stem Cell Research, Aetiology, 2.1 Biological and endogenous factors, Animals, Base Sequence, CRISPR-Cas Systems, Cell Self Renewal, Cell Transformation, Neoplastic, Clone Cells, Female, Genetic Predisposition to Disease, Genome, Human, Hematologic Diseases, Hematopoietic Stem Cells, Humans, Introns, Male, Mice, Knockout, Neoplasms, Noonan Syndrome, Pedigree, RNA, RNA Splicing, Ribonucleoproteins, Spleen, Transcription Factors, Medical and Health Sciences, Developmental Biology, Agricultural biotechnology, Bioinformatics and computational biology

Abstract

Most eukaryotes harbor two distinct pre-mRNA splicing machineries: the major spliceosome, which removes >99% of introns, and the minor spliceosome, which removes rare, evolutionarily conserved introns. Although hypothesized to serve important regulatory functions, physiologic roles of the minor spliceosome are not well understood. For example, the minor spliceosome component ZRSR2 is subject to recurrent, leukemia-associated mutations, yet functional connections among minor introns, hematopoiesis and cancers are unclear. Here, we identify that impaired minor intron excision via ZRSR2 loss enhances hematopoietic stem cell self-renewal. CRISPR screens mimicking nonsense-mediated decay of minor intron-containing mRNA species converged on LZTR1, a regulator of RAS-related GTPases. LZTR1 minor intron retention was also discovered in the RASopathy Noonan syndrome, due to intronic mutations disrupting splicing and diverse solid tumors. These data uncover minor intron recognition as a regulator of hematopoiesis, noncoding mutations within minor introns as potential cancer drivers and links among ZRSR2 mutations, LZTR1 regulation and leukemias.

Published

2021

132. EP18.30: Enlarged yolk sac as a potential new phenotype of RAF1 Noonan syndrome.

Author

Krischer, B., Bahr, A., Ivanovski, I., Kraemer, D., Kapfhammer, E., Hodel, M., and Rauch, A.

Subjects

*MISCARRIAGE, *YOLK sac, *PREGNANCY outcomes, *NOONAN syndrome, *SHORT stature

Abstract

This article discusses a case study involving a patient with an enlarged yolk sac (YS) during pregnancy. While an enlarged YS is typically associated with adverse pregnancy outcomes and aneuploidies, this particular case revealed a maternally inherited variant in the RAF1 gene, leading to Noonan syndrome (NS). NS is a genetically and clinically diverse disorder, and this case suggests that there may be a subgroup of enlarged YS cases with a different etiology. The patient delivered a healthy child without any visible anomalies. [Extracted from the article]

Published

2024

133. A rare mutation in a patient with Noonan syndrome with multiple lentigines

Author

Manuel E. Blanco-Cintrón, MD, Fabiola Pabón-González, BS, and Xavier Sánchez-Flores, MD

Subjects

hyperpigmented skin lesions, lentigines, MAP2K1, MAPK, mitogen-activated protein kinase, Noonan syndrome, Dermatology, RL1-803

Published

2023

134. Rare Congenital Dissecting Thoracic Aortic Aneurysm in a Child with Noonan Syndrome: A Case Report

Author

Siti Aishah Ahmad Maulana

Subjects

atrial septal defect, computed tomography angiography, noonan syndrome, malaysia, Medicine

Abstract

We present a rare case of congenital thoracic aortic aneurysm (TAA) complicated with dissection in a nine-year-old girl with Noonan syndrome and atrial septal defect. She presented with rapid breathing and upper respiratory tract symptoms. Chest X-ray revealed a huge upper mediastinum with cardiomegaly. Echocardiogram showed possible ascending TAA. Computerized tomography angiogram of the aorta revealed huge aortic root-ascending TAA with small aortic dissection. Despite immediate treatment, the patient passed away due to severe airway compromise.

Published

2023

135. Noonan syndrome: rhGH treatment and PTPN11 mutation

Author

Xian Wu, Jiali Wu, Yi Yuan, Li Yang, and Lirong Yu

Subjects

children, Noonan syndrome, PTPN11 mutation, recombinant human growth hormone, Genetics, QH426-470

Abstract

Abstract Objective To analyze the clinical data and genetic characteristics of Noonan syndrome, both the effect and side effects of recombinant human growth hormone (rhGH) treatment. Methods We collected clinical data from 8 children with Noonan syndrome diagnosed from November 2017 to June 2021. The diagnosis was clarified by exome second‐generation sequencing and parental PCR‐NGS validation and interpretation of the preceding evidence, and growth hormone therapy was administered. Of the cases, four males and four females were seen for slow height growth and the median age at diagnosis was 8 years 7 months (1 year 7 months to 12 years 6 months). Results Here, 7 children were treated with rhGH. Compared to the pre‐treatment period, the growth rate increased after rhGH treatment [3.7 ± 0.5 cm/year before treatment and 8.0 ± 1.0 cm/year after treatment, p

Published

2023

136. Lipid profile in Noonan syndrome and related disorders: trend by age, sex and genotype.

Author

Tamburrino, Federica, Mazzanti, Laura, Scarano, Emanuela, Gibertoni, Dino, Sirolli, Maria, Zioutas, Maximiliano, Schiavariello, Concetta, Perri, Annamaria, Mantovani, Alessio, Rossi, Cesare, Tartaglia, Marco, and Pession, Andrea

Subjects

NOONAN syndrome, HIGH density lipoproteins, LIPID metabolism, LIPIDS, APOLIPOPROTEIN B, LIPID synthesis, FEMALES

Abstract

Background: RASopathies are developmental disorders caused by dysregulation of the RAS-MAPK signalling pathway, which contributes to the modulation of multiple extracellular signals, including hormones and growth factors regulating energetic metabolism, including lipid synthesis, storage, and degradation. Subjects and methods: We evaluated the body composition and lipid profiles of a single-centre cohort of 93 patients with a molecularly confirmed diagnosis of RASopathy by assessing height, BMI, and total cholesterol, HDL, triglycerides, apolipoprotein, fasting glucose, and insulin levels, in the context of a cross sectional and longitudinal study. We specifically investigated and compared anthropometric and haematochemistry data between the Noonan syndrome (NS) and Mazzanti syndrome (NS/LAH) groups. Results: At the first evaluation (9.5 ± 6.2 years), reduced growth (-1.80 ± 1.07 DS) was associated with a slightly reduced BMI (-0.34 DS ± 1.15 DS). Lipid profiling documented low total cholesterol levels (< 5th percentile) in 42.2% of the NS group; in particular, in 48.9% of PTPN11 patients and in 28.6% of NS/LAH patients compared to the general population, with a significant difference between males and females. A high proportion of patients had HDL levels lower than the 26th percentile, when compared to the age- and sex-matched general population. Triglycerides showed an increasing trend with age only in NS females. Genotypephenotype correlations were also evident, with particularly reduced total cholesterol in about 50% of patients with PTPN11 mutations with LDL-C and HDL-C tending to decrease during puberty. Similarly, apolipoprotein A1 and apolipoprotein B deficits were documented, with differences in prevalence associated with the genotype for apolipoprotein A1. Fasting glucose levels and HOMA-IR were within the normal range. Conclusion: The present findings document an unfavourable lipid profile in subjects with NS, in particular PTPN11 mutated patients, and NS/LAH. Furtherstudies are required to delineate the dysregulation of lipid metabolism in RASopathies more systematically and confirm the occurrence of previously unappreciated genotype-phenotype correlations involving the metabolic profile of these disorders. [ABSTRACT FROM AUTHOR]

Published

2023

137. Role of SHP2 (PTPN11) in glycoprotein VI-dependent thrombus formation: Improved platelet responsiveness by the allosteric drug SHP099 in Noonan syndrome patients.

Author

Fernández, Delia I., Diender, Marije, Hermida-Nogueira, Lidia, Huang, Jingnan, Veiras, Sonia, Henskens, Yvonne M.C., te Loo, Maroeska W.M., Heemskerk, Johan W.M., Kuijpers, Marijke J.E., and García, Ángel

Subjects

*NOONAN syndrome, *BLOOD coagulation, *BLOOD platelet aggregation, *THROMBOSIS, *BLOOD platelets, *BLOOD platelet disorders

Abstract

The protein tyrosine phosphatase SHP2 (PTPN11) is a negative regulator of glycoprotein VI (GPVI)-induced platelet signal under certain conditions. Clinical trials with derivatives of the allosteric drug SHP099, inhibiting SHP2, are ongoing as potential therapy for solid cancers. Gain-of-function mutations of the PTPN11 gene are observed in part of the patients with the Noonan syndrome, associated with a mild bleeding disorder. Assessment of the effects of SHP2 inhibition in platelets from controls and Noonan syndrome patients. Washed human platelets were incubated with SHP099 and stimulated with collagen-related peptide (CRP) for stirred aggregation and flow cytometric measurements. Whole-blood microfluidics assays using a dosed collagen and tissue factor coating were performed to assess shear-dependent thrombus and fibrin formation. Effects on clot formation were evaluated by thromboelastometry. Pharmacological inhibition of SHP2 did not alter GPVI-dependent platelet aggregation under stirring, but it enhanced integrin αIIbβ3 activation in response to CRP. Using whole-blood microfluidics, SHP099 increased the thrombus buildup on collagen surfaces. In the presence of tissue factor and coagulation, SHP099 increased thrombus size and reduced time to fibrin formation. Blood from PTPN11 -mutated Noonan syndrome patients, with low platelet responsiveness, after ex vivo treatment with SHP099 showed a normalized platelet function. In thromboelastometry, SHP2 inhibition tended to increase tissue factor-induced blood clotting profiles with tranexamic acid, preventing fibrinolysis. Pharmacological inhibition of SHP2 by the allosteric drug SHP099 enhances GPVI-induced platelet activation under shear conditions with a potential to improve platelet functions of Noonan syndrome patients. [Display omitted] • The PTPN11 inhibitor SHP099 was used to study effects in platelets. • SHP099 increased collagen-induced thrombus build-up in whole blood microfluidics. • SHP099 enhanced platelet- and shear-dependent coagulation. • SHP099 restored thrombus formation in Noonan syndrome patients with mutated PTPN11. [ABSTRACT FROM AUTHOR]

Published

2023

138. Genotypic Findings in Noonan and Non-Noonan RASopathies and Patient Eligibility for Growth Hormone Treatment.

Author

Carcavilla, Atilano, Cambra, Ana, Santomé, José L., Seidel, Verónica, Cruz, Jaime, Alonso, Milagros, Pozo, Jesús, Valenzuela, Irene, Guillén-Navarro, Encarna, Santos-Simarro, Fernando, González-Casado, Isabel, Rodríguez, Amparo, Medrano, Constancio, López-Siguero, Juan Pedro, and Ezquieta, Begoña

Subjects

*SOMATOTROPIN, *MOLECULAR diagnosis, *HUMAN growth hormone, *GENOTYPES, *NOONAN syndrome, *PITUITARY dwarfism, *GENETIC testing

Abstract

Molecular study has become an invaluable tool in the field of RASopathies. Treatment with recombinant human growth hormone is approved in Noonan syndrome but not in the other RASopathies. The aim of this study was to learn about the molecular base of a large cohort of patients with RASopathies, with particular emphasis on patients with pathogenic variants in genes other than PTPN11, and its potential impact on rGH treatment indication. We reviewed the clinical diagnosis and molecular findings in 451 patients with a genetically confirmed RASopathy. HRAS alterations were detected in only 2 out of 19 patients referred with a Costello syndrome suspicion, whereas pathogenic variants in RAF1 and SHOC2 were detected in 3 and 2, respectively. In 22 patients referred with a generic suspicion of RASopathy, including cardiofaciocutaneous syndrome, pathogenic alterations in classic Noonan syndrome genes (PTPN11, SOS1, RAF1, LZTR1, and RIT1) were found in 7 patients and pathogenic variants in genes associated with other RASopathies (HRAS, SHOC2, and PPPCB1) in 4. The correct nosological classification of patients with RASopathies is critical to decide whether they are candidates for treatment with rhGH. Our data illustrate the complexity of differential diagnosis in RASopathies, as well as the importance of genetic testing to guide the diagnostic orientation in these patients. [ABSTRACT FROM AUTHOR]

Published

2023

139. The Multifaceted Syndromic Primary Immunodeficiencies in Children.

Author

Ng, Khuen Foong, Goenka, Anu, Manyika, Florence, and Bernatoniene, Jolanta

Subjects

*PRIMARY immunodeficiency diseases, *NOONAN syndrome, *OPPORTUNISTIC infections, *PELVIC inflammatory disease, *GENETIC disorder diagnosis, *MUSCLE dysmorphia

Abstract

Background: Disorders of immunity are poorly recognised in some rare multisystem genetic conditions. We aim to describe syndromic features and immunological defects in children with syndromic primary immunodeficiencies (sPIDs). Methods: This is a retrospective descriptive study of children aged 0–18 years with sPIDs under the care of the paediatric immunology service at the Bristol Royal Hospital for Children, United Kingdom, from January 2006 to September 2021. Results: sPIDs were identified in 36 patients. Genetic diagnoses which are not commonly associated with PIDs and not included in the International Union of Immunological Societies classification were present in 7/36 (19%): Trisomy 22, Arboleda-Tham syndrome, 2p16.3 deletion syndrome, supernumerary ring chromosome 20 syndrome, Myhre syndrome, Noonan syndrome, and trichothiodystrophy/Cockayne syndrome complex. Recurrent and/or severe infections were the most common clinical features (n = 33, 92%). Approximately half had combined immunodeficiency or antibody deficiency. The most common extra-immunological manifestations include dysmorphism (72%), disorders of nervous (78%), musculoskeletal (69%), haematology/lymphatic (58%), and gastrointestinal, hepatic/pancreatic (58%) systems. Conclusions: Patients with sPIDs often have multiorgan involvement and some are non-immunologically mediated. There should be a low threshold to clinically assess and investigate for disorders of immunity in any patients with syndromic features especially when they present with recurrent/severe/opportunistic infections, features of immune dysregulation, autoinflammation or lymphoproliferation. [ABSTRACT FROM AUTHOR]

Published

2023

140. Hypertrophic neuropathy: a possible cause of pain in children with Noonan syndrome and related disorders.

Author

Draaisma, Fieke, Erasmus, Corrie E., Braakman, Hilde M. H., Burgers, Melanie C. J., Leenders, Erika K. S. M., Rinne, Tuula, van Alfen, Nens, and Draaisma, Jos M. T.

Subjects

*NOONAN syndrome, *LEG pain, *SYNDROMES in children, *MAGNETIC resonance imaging, *NEUROPATHY, *ACADEMIC medical centers

Abstract

This study is aimed at describing the findings of high-resolution nerve ultrasound in children with Noonan syndrome (NS) and related disorders experiencing pain in their legs. This retrospective cohort study was conducted in the NS expert center of the Radboud University Medical Center in the Netherlands. Patients were eligible if they were younger than 18 years, clinically and genetically diagnosed with NS or a NS related disorder, and experienced pain in their legs. Anamneses and physical examination were performed in all children. In addition, high-resolution nerve ultrasound was used to assess nerve hypertrophy and, if needed, complemented spinal magnetic resonance imaging was performed. Over a period of 6 months, four children, three with NS and one child with NS with multiple lentigines, who experienced pain of their legs were eligible for inclusion. Muscle weakness was found in two of them. High-resolution nerve ultrasound showed (localized) hypertrophic neuropathy in all patients. One child underwent additional spinal magnetic resonance imaging, which showed profound thickening of the nerve roots and plexus. Conclusion: In the four children included with a NS and related disorders, pain was concomitant with nerve hypertrophy, which suggests an association between these two findings. The use of high-resolution nerve ultrasound and spinal magnetic resonance imaging might result in better understanding of the nature of this pain and the possible association to nerve hypertrophy in patients with NS and related disorders. What is Known: • Children with Noonan syndrome and related disorders may report pain in their legs, which is often interpreted as growing pain. • Some adults with Noonan syndrome and related disorders have hypertrophic neuropathy as a possible cause of neuropathic pain. What is New: • This is the first study using high-resolution nerve ultrasound in children with Noonan syndrome and related disorders experiencing pain in their legs. • Hypertrophic neuropathy was diagnosed as possible cause of pain in four children with Noonan syndrome and related disorders. [ABSTRACT FROM AUTHOR]

Published

2023

141. The most important problems and needs of rasopathy patients with a noonan syndrome spectrum disorder.

Author

Tiemens, Dagmar K., Kleimeier, Lotte, Leenders, Erika, Wingbermühle, Ellen, Roelofs, Renee L., Sibbles, Barbara, Oostwegel, Floor S.M., Vroonland, Eva, van Leeuwen, Conny, Niessen, Hanneke, Sonnega, Paul, Duursma, Anniek, Willemsen, Michel A. A. P., Draaisma, Jos M. T., and Pittens, Carina A.C.M.

Subjects

*NOONAN syndrome, *PATIENTS' attitudes, *MUSCULOSKELETAL system, *COGNITIVE ability, *AGE groups

Abstract

Background: Noonan syndrome spectrum disorders (NSSDs) constitute a group within the Rasopathies, and are one of the largest groups of syndromes with impact on multi-organ involvement known. The extreme variability of the clinical phenotype is, among others, due to the numerous different genes that are involved, and the differences in clinical presentation over the life span. We have studied the needs of patients and their relatives aiming to develop, evaluate and choose focus in research, medical care and policy to better meet their perspectives. Methods: Using the participatory and interactive Dialogue method, 80 patients and relatives mentioned 53 different problems or needs (topics) that were categorized into eight themes. These themes and the topics within each theme, were subsequently prioritized by putting them in order of importance methodologically. Results: The four highest prioritized themes were: (1) Physical problems (non-musculoskeletal related); (2) Social, emotional and behavioral problems; (3) Cognitive functioning and information processing; and (4) Problems related to the musculoskeletal system. Nineteen out of the 53 topics were physical problems. According to the total group of respondents, the top 3 prioritized topics within theme 1 were coagulation problems, heart problems, and feeding problems. Also data stratified by age groups, phenotype (NS and other NSSDs) and gender showed some remarkable results. For instance, feeding problems were prioritized as the most important topic of the highest prioritized theme, according to patients aged 0–12 years. Also feeding problems show a significant difference in its prioritization according to female patients (2) compared to male patients (7). On the other hand, heart problems were not mentioned in the top three prioritized topics in the youngest age groups, although heart problems are generally considered most important for patients with NSSD. Conclusions: With our results we underline the importance of methodologically inventorying the needs of NSSD patients, not only at the group level, but to also focus on specific needs according to e.g. age, phenotype and gender. For instance, it is remarkable that both the current Clinical Guidelines and the Noonan Syndrome diagnostic criteria give little to no attention to feeding problems, though our results indicate that, to the youngest patients, these problems have top priority. A similar situation appears to apply to the clinical management of e.g. coagulation, neuropsychological and musculoskeletal problems (like physiotherapy or occupational therapy) and to a need for (educational) tools to support patients at school or at work. Our study may help to shape targeted (clinical) management, research and policy inside and outside medical (research) institutes and shed light on the complex phenotypes of NSSDs, the families' and patients' perspectives on the everyday consequences of the many different problems, as well as their needs. [ABSTRACT FROM AUTHOR]

Published

2023

142. Oral manifestations of eleven individuals with Noonan syndrome. A case series.

Author

Vavetsi, Konstantina, Panagopoulou, Olga, Fryssira, Ηelen, Bobetsis, Spyridon A., Emmanouil, Dimitris, Madianos, Phoebus N., and Bobetsis, Yiorgos A.

Subjects

ORAL manifestations of general diseases, NOONAN syndrome, GINGIVITIS, CONGENITAL heart disease, GINGIVAL recession, NUCLEIC acid hybridization, SHORT stature

Abstract

Aims: Noonan syndrome (NS) is a clinically and genetically heterogeneous condition characterized by distinctive facial features, short stature, and congenital heart defects. The oral manifestations have not been sufficiently described. In an attempt to enrich our understanding regarding the oral manifestations, the aim of the current study was to present the clinical, radiographic, and microbiological findings of eleven subjects with NS syndrome. Methods and Results: A complete intraoral clinical evaluation, a radiographic analysis using panoramic and cephalometric x‐rays, and a supra‐ and sub‐gingival microbiological profiling of 20 periodontal and cariogenic microbiota using the checkerboard DNA‐DNA hybridization technique were performed in a series of 11 NS individuals. Compared to previous reports very few dental findings were present. Gingivitis and carious lesions were present in all subjects and could be related to poor oral hygiene. High‐arched palate and malocclusions such as crossbite, open‐bite, and deep‐bite were very common findings but without a specific pattern. Two findings that have not been reported before included the different shapes of the condyles and the irregular shape of the sella turcica. Conclusion: Due to the elevated prevalence of gingivitis, caries, and malocclusion, a multidisciplinary approach including dental follow‐ups should be the standard care in NS patients. [ABSTRACT FROM AUTHOR]

Published

2023

143. Molecular and cellular evidence for the impact of a hypertrophic cardiomyopathy-associated RAF1 variant on the structure and function of contractile machinery in bioartificial cardiac tissues.

Author

Nakhaei-Rad, Saeideh, Haghighi, Fereshteh, Bazgir, Farhad, Dahlmann, Julia, Busley, Alexandra Viktoria, Buchholzer, Marcel, Kleemann, Karolin, Schänzer, Anne, Borchardt, Andrea, Hahn, Andreas, Kötter, Sebastian, Schanze, Denny, Anand, Ruchika, Funk, Florian, Kronenbitter, Annette Vera, Scheller, Jürgen, Piekorz, Roland P., Reichert, Andreas S., Volleth, Marianne, and Wolf, Matthew J.

Subjects

*INDUCED pluripotent stem cells, *NOONAN syndrome, *SUDDEN death, *HYPERTROPHIC cardiomyopathy, *GENETIC variation

Abstract

Noonan syndrome (NS), the most common among RASopathies, is caused by germline variants in genes encoding components of the RAS-MAPK pathway. Distinct variants, including the recurrent Ser257Leu substitution in RAF1, are associated with severe hypertrophic cardiomyopathy (HCM). Here, we investigated the elusive mechanistic link between NS-associated RAF1S257L and HCM using three-dimensional cardiac bodies and bioartificial cardiac tissues generated from patient-derived induced pluripotent stem cells (iPSCs) harboring the pathogenic RAF1 c.770 C > T missense change. We characterize the molecular, structural, and functional consequences of aberrant RAF1–associated signaling on the cardiac models. Ultrastructural assessment of the sarcomere revealed a shortening of the I-bands along the Z disc area in both iPSC-derived RAF1S257L cardiomyocytes and myocardial tissue biopsies. The aforementioned changes correlated with the isoform shift of titin from a longer (N2BA) to a shorter isoform (N2B) that also affected the active force generation and contractile tensions. The genotype-phenotype correlation was confirmed using cardiomyocyte progeny of an isogenic gene-corrected RAF1S257L-iPSC line and was mainly reversed by MEK inhibition. Collectively, our findings uncovered a direct link between a RASopathy gene variant and the abnormal sarcomere structure resulting in a cardiac dysfunction that remarkably recapitulates the human disease. Studies on 3D bioartificial cardiac tissues reveal the impacts of hypertrophic cardiomyopathy-associated RAF1 mutations on sarcomere structure, contractile behavior, Ca2+ handling, and intracellular signaling. [ABSTRACT FROM AUTHOR]

Published

2023

144. Improvement of synaptic plasticity and cognitive function in RASopathies—a monocentre, randomized, double-blind, parallel-group, placebo-controlled, cross-over clinical trial (SynCoRAS).

Author

Jung, Nikolai H., Egert-Schwender, Silvia, Schossow, Beate, Kehl, Victoria, Wahlländer, Ute, Brich, Louisa, Janke, Viktoria, Blankenstein, Christiane, Zenker, Martin, and Mall, Volker

Subjects

*NEUROPLASTICITY, *CROSSOVER trials, *COGNITIVE ability, *TRANSCRANIAL magnetic stimulation, *CLINICAL trials, *WAKEFULNESS

Abstract

Background: Cognitive impairment is a common medical issue in rat sarcoma (RAS) pathway disorders, so-called RASopathies, like Neurofibromatosis type 1 (NF1) or Noonan syndrome (NS). It is presumed to be caused by impaired synaptic plasticity. In animal studies, pathway-specific pharmacological interventions with lovastatin (LOV) and lamotrigine (LTG) have been shown to improve synaptic plasticity as well as cognitive function. The aim of this clinical trial is to translate the findings of animal studies to humans and to probe the effect of lovastatin (NS) and lamotrigine (NS and NF1) on synaptic plasticity and cognitive function/alertness in RASopathies. Methods: Within this phase IIa, monocentre, randomized, double-blind, parallel-group, placebo-controlled, cross-over clinical trial (syn. SynCoRAS), three approaches (approaches I–III) will be carried out. In patients with NS, the effect of LTG (approach I) and of LOV (approach II) is investigated on synaptic plasticity and alertness. LTG is tested in patients with NF1 (approach III). Trial participants receive a single dose of 300 mg LTG or placebo (I and III) and 200 mg LOV or placebo (II) daily for 4 days with a cross-over after at least 7 days. Synaptic plasticity is investigated using a repetitive high-frequency transcranial magnetic stimulation (TMS) protocol called quadri-pulse theta burst stimulation (qTBS). Attention is examined by using the test of attentional performance (TAP). Twenty-eight patients are randomized in groups NS and NF1 with n = 24 intended to reach the primary endpoint (change in synaptic plasticity). Secondary endpoints are attention (TAP) and differences in short interval cortical inhibition (SICI) between placebo and trial medication (LTG and LOV). Discussion: The study is targeting impairments in synaptic plasticity and cognitive impairment, one of the main health problems of patients with RASopathies. Recent first results with LOV in patients with NF1 have shown an improvement in synaptic plasticity and cognition. Within this clinical trial, it is investigated if these findings can be transferred to patients with NS. LTG is most likely a more effective and promising substance improving synaptic plasticity and, consecutively, cognitive function. It is expected that both substances are improving synaptic plasticity as well as alertness. Changes in alertness may be a precondition for improvement of cognition. Trial registration: The clinical trial is registered in ClinicalTrials.gov (NCT03504501; https://www.clinicaltrials.gov; date of registration: 04/11/2018) and in EudraCT (number 2016–005022-10). [ABSTRACT FROM AUTHOR]

Published

2023

145. Hypertrophic cardiomyopathy in an adult patient with Noonan syndrome with multiple lentigines.

Author

Rivero‐García, Pamela, Campuzano‐Estrada, Isabel del Carmen, and Hernandez‐Felix, Jorge Humberto

Subjects

*NOONAN syndrome, *HYPERTROPHIC cardiomyopathy, *APICAL hypertrophic cardiomyopathy, *LENTIGO, *SHORT stature, *TAKOTSUBO cardiomyopathy, *PECTUS excavatum

Abstract

Key Clinical Message: Noonan syndrome with multiple lentigines (NSML) is a rare RASopathy caused by pathogenic variants (PV) predominantly in PTPN11 gene. We report a 54‐year‐old male with apical hypertrophic cardiomyopathy, who was diagnosed with NSML due to his short stature, multiple lentigines, winged neck, pectus excavatum, and a heterozygous PV in PTPN11 c.836A > ¡G. [ABSTRACT FROM AUTHOR]

Published

2023

146. Obliterated cavum septi pellucidi: Clinical significance and role of fetal magnetic resonance.

Author

Fantasia, Ilaria, Ciardo, Claudia, Bracalente, Gabriella, Filippi, Elisa, Murru, Flora Maria, Spezzacatene, Anita, Bin, Maura, Mendez Quintero, Olivia, Montaguti, Elisa, Lees, Christoph, Papanikolaou, Katherine, Pilu, Gianluigi, Prefumo, Federico, Thilaganathan, Baskaran, and Stampalija, Tamara

Subjects

*FETAL MRI, *MAGNETIC resonance, *FETAL ultrasonic imaging, *PRENATAL diagnosis, *NOONAN syndrome

Abstract

Introduction: The objective of this study was to describe a cohort of fetuses with an ultrasound prenatal diagnosis of obliterated cavum septi pellucidi (oCSP) with the aim to explore the rate of associated malformations, the progression during pregnancy and the role of fetal magnetic resonance imaging (MRI). Material and methods: This was a retrospective multicenter international study of fetuses diagnosed with oCSP in the second trimester with available fetal MRI and subsequent ultrasound and/or fetal MRI follow-up in the third trimester. Where available, postnatal data were collected to obtain information on neurodevelopment. Results: We identified 45 fetuses with oCSP at 20.5 weeks (interquartile range 20.1-21.1). oCSP was apparently isolated at ultrasound in 89% (40/45) and fetal MRI found additional findings in 5% (2/40) of cases, including polymicrogyria and microencephaly. In the remaining 38 fetuses, fetal MRI found a variable amount of fluid in CSP in 74% (28/38) and no fluid in 26% (10/38). Ultrasound follow-up at or after 30 weeks confirmed the diagnosis of oCSP in 32% (12/38) while fluid was visible in 68% (26/38). At follow-up MRI, performed in eight pregnancies, there were periventricular cysts and delayed sulcation with persistent oCSP in one case. Among the remaining cases with normal follow-up ultrasound and fetal MRI findings, the postnatal outcome was normal in 89% of cases (33/37) and abnormal in 11% (4/37): two with isolated speech delay, and two with neurodevelopmental delay secondary to postnatal diagnosis of Noonan syndrome at 5 years in one case and microcephaly with delayed cortical maturation at 5 months in the other. Conclusions: Apparently isolated oCSP at mid-pregnancy is a transient finding with the visualization of the fluid later in pregnancy in up to 70% of cases. At referral, associated defects can be found in around 11% of cases at ultrasound and 8% at fetal MRI indicating the need for a detailed evaluation by expert physicians when oCSP is suspected. [ABSTRACT FROM AUTHOR]

Published

2023

147. The molecular functions of RIT1 and its contribution to human disease.

Author

Van, Richard, Cuevas-Navarro, Antonio, Castel, Pau, and McCormick, Frank

Subjects

Biochemistry and Cell Biology, Biological Sciences, Cancer, Rare Diseases, Aetiology, 2.1 Biological and endogenous factors, Animals, Disease Models, Animal, Humans, Mutation, Neoplasms, Noonan Syndrome, ras Proteins, GTPases, cancer, point mutations, stress response, Chemical Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology, Biochemistry and cell biology

Abstract

RIT1 is a member of the Ras family of GTPases that direct broad cellular physiological responses through tightly controlled signaling networks. The canonical Ras GTPases are well-defined regulators of the RAF/MEK/ERK pathway and mutations in these are pathogenic in cancer and a class of developmental disorders termed RASopathies. Emerging clinical evidences have now demonstrated a role for RIT1 in RASopathies, namely Noonan syndrome, and various cancers including lung adenocarcinoma and myeloid malignancies. While RIT1 has been mostly described in the context of neuronal differentiation and survival, the mechanisms underlying aberrant RIT1-mediated signaling remain elusive. Here, we will review efforts undertaken to characterize the biochemical and functional properties of the RIT1 GTPase at the molecular, cellular, and organismal level, as well as provide a phenotypic overview of different human conditions caused by RIT1 mutations. Deeper understanding of RIT1 biological function and insight to its pathogenic mechanisms are imperative to developing effective therapeutic interventions for patients with RIT1-mutant Noonan syndrome and cancer.

Published

2020

148. Advancing RAS/RASopathy therapies: An NCI‐sponsored intramural and extramural collaboration for the study of RASopathies

Author

Gross, Andrea M, Frone, Megan, Gripp, Karen W, Gelb, Bruce D, Schoyer, Lisa, Schill, Lisa, Stronach, Beth, Biesecker, Leslie G, Esposito, Dominic, Hernandez, Edjay Ralph, Legius, Eric, Loh, Mignon L, Martin, Staci, Morrison, Deborah K, Rauen, Katherine A, Wolters, Pamela L, Zand, Dina, McCormick, Frank, Savage, Sharon A, Stewart, Douglas R, Widemann, Brigitte C, and Yohe, Marielle E

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Orphan Drug, Cancer, Heart Disease, Prevention, Cardiovascular, Congenital Heart Disease, Neurofibromatosis, Genetics, Pediatric, Neurosciences, Rare Diseases, Congenital Structural Anomalies, Clinical Research, Pediatric Cancer, 2.1 Biological and endogenous factors, Biomarkers, Tumor, Costello Syndrome, Ectodermal Dysplasia, Facies, Failure to Thrive, Heart Defects, Congenital, Humans, Intersectoral Collaboration, Molecular Targeted Therapy, Mutation, National Cancer Institute (U.S.), Neurofibromatosis 1, Noonan Syndrome, Research Report, Signal Transduction, United States, ras Proteins, cardiofaciocutaneous syndrome, Costello syndrome, Noonan syndrome, Ras, MAP kinase pathway, RASopathies, Ras/MAP kinase pathway, Clinical sciences

Abstract

RASopathies caused by germline pathogenic variants in genes that encode RAS pathway proteins. These disorders include neurofibromatosis type 1 (NF1), Noonan syndrome (NS), cardiofaciocutaneous syndrome (CFC), and Costello syndrome (CS), and others. RASopathies are characterized by heterogenous manifestations, including congenital heart disease, failure to thrive, and increased risk of cancers. Previous work led by the NCI Pediatric Oncology Branch has altered the natural course of one of the key manifestations of the RASopathy NF1. Through the conduct of a longitudinal cohort study and early phase clinical trials, the MEK inhibitor selumetinib was identified as the first active therapy for the NF1-related peripheral nerve sheath tumors called plexiform neurofibromas (PNs). As a result, selumetinib was granted breakthrough therapy designation by the FDA for the treatment of PN. Other RASopathy manifestations may also benefit from RAS targeted therapies. The overall goal of Advancing RAS/RASopathy Therapies (ART), a new NCI initiative, is to develop effective therapies and prevention strategies for the clinical manifestations of the non-NF1 RASopathies and for tumors characterized by somatic RAS mutations. This report reflects discussions from a February 2019 initiation meeting for this project, which had broad international collaboration from basic and clinical researchers and patient advocates.

Published

2020

149. The sixth international RASopathies symposium: Precision medicine-From promise to practice.

Author

Gripp, Karen W, Schill, Lisa, Schoyer, Lisa, Stronach, Beth, Bennett, Anton M, Blaser, Susan, Brown, Amanda, Burdine, Rebecca, Burkitt-Wright, Emma, Castel, Pau, Darilek, Sandra, Dias, Alwyn, Dyer, Tuesdi, Ellis, Michelle, Erickson, Gregg, Gelb, Bruce D, Green, Tamar, Gross, Andrea, Ho, Alan, Holder, James Lloyd, Inoue, Shin-Ichi, Jelin, Angie C, Kennedy, Annie, Klein, Richard, Kontaridis, Maria I, Magoulas, Pilar, McConnell, Darryl B, McCormick, Frank, Neel, Benjamin G, Prada, Carlos E, Rauen, Katherine A, Roberts, Amy, Rodriguez-Viciana, Pablo, Rosen, Neal, Rumbaugh, Gavin, Sablina, Anna, Solman, Maja, Tartaglia, Marco, Thomas, Angelica, Timmer, William C, Venkatachalam, Kartik, Walsh, Karin S, Wolters, Pamela L, Yi, Jae-Sung, Zenker, Martin, and Ratner, Nancy

Subjects

Humans, Genetic Diseases, Inborn, ras Proteins, Mitogen-Activated Protein Kinase Kinases, Signal Transduction, Germ-Line Mutation, Costello syndrome, Noonan syndrome, RASopathy, cardio-facio-cutaneous syndrome, kinases, neurofibromatosis, Rare Diseases, Genetics, Good Health and Well Being, Clinical Sciences

Abstract

The RASopathies are a group of genetic disorders that result from germline pathogenic variants affecting RAS-mitogen activated protein kinase (MAPK) pathway genes. RASopathies share RAS/MAPK pathway dysregulation and share phenotypic manifestations affecting numerous organ systems, causing lifelong and at times life-limiting medical complications. RASopathies may benefit from precision medicine approaches. For this reason, the Sixth International RASopathies Symposium focused on exploring precision medicine. This meeting brought together basic science researchers, clinicians, clinician scientists, patient advocates, and representatives from pharmaceutical companies and the National Institutes of Health. Novel RASopathy genes, variants, and animal models were discussed in the context of medication trials and drug development. Attempts to define and measure meaningful endpoints for treatment trials were discussed, as was drug availability to patients after trial completion.

Published

2020

150. Prenatal diagnosis of euploid increased nuchal translucency on fetal ultrasound (II): RASopathy disorders – Prenatal ultrasound findings and genotype–phenotype correlations

Author

Chih-Ping Chen

Subjects

increased nuchal translucency, noonan syndrome, prenatal diagnosis, rasopathy disorder, ultrasound, Medical technology, R855-855.5

Abstract

Prenatal diagnosis of euploid increased nuchal translucency (NT) remains a challenge to obstetricians and genetic counselors, although increased euploid NT at prenatal diagnosis can be associated with a favorable outcome. Prenatal diagnosis of euploid increased NT should include a differential diagnosis of pathogenetic copy number variants and RASopathy disorders (RDs) including Noonan syndrome. Therefore, chromosomal microarray analysis, whole-exome sequencing, RASopathy-disorder testing, and protein-tyrosine phosphatase nonreceptor type 11 gene testing may be necessary under such a circumstance. In this report, a comprehensive review of RDs with its prenatal ultrasound findings and genotype-phenotype correlations is presented.

Published

2023