The first familial NSD2 cases with a novel variant in a Chinese father and daughter with atypical WHS facial features and a 7.5-year follow-up of growth hormone therapy

Hu, Xuyun; Wu, Di; Li, Yuchuan; Wei, Liya; Li, Xiaoqiao; Qin, Miao; Li, Hongdou; Li, Mengting; Chen, Shaoke; Gong, Chunxiu; Shen, Yiping

doi:10.1186/s12920-020-00831-9

Cited by 7 publications

(11 citation statements)

References 22 publications

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“…A comparison of our patient's features and the genetic result with the literature describing cases that only affect NSD2 (WHSC1) indicated that variants and deletions that only affect NSD2 manifest as mild WHS phenocopies (see Zanoni et al 1 describing 18 original patients, 13 previously published patients, [3][4][5][6][7][8][9] and the patient of our work).…”

supporting

confidence: 54%

“…Interestingly, his father carrying the same NSD2 variant showed mild intellectual disability presenting a seizure after a fever episode as a child, during which encephalitis was suspected, but no definite diagnosis was made. 9 Because of the very low frequency of seizures in NSD2related disorders in comparison with WHS, several genes included in the deleted region have been described as candidates. LETM1 has been considered as one of the candidates, but some patients with deletions in LETM1 do not present seizures.…”

mentioning

confidence: 99%

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Correspondence on “Loss-of-function and missense variants in NSD2 cause decreased methylation activity and are associated with a distinct developmental phenotype” by Zanoni et al

Cueto‐González

Fernández-Álvarez

Valenzuela

et al. 2022

Genetics in Medicine

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supporting

confidence: 54%

mentioning

confidence: 99%

Correspondence on “Loss-of-function and missense variants in NSD2 cause decreased methylation activity and are associated with a distinct developmental phenotype” by Zanoni et al

Cueto‐González

Fernández-Álvarez

Valenzuela

et al. 2022

Genetics in Medicine

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“…Hence, the clinical spectrum of NSD2 deletion encompasses: prenatal and postnatal growth restriction [ 14 ], microcephaly, developmental delay [ 15 ], congenital heart defects and several phenotypic traits, including hypertelorism, upward-slanting palpebral fissures, prominent nasal bridge, abnormal teething and micrognathia. Cleft palate has been described in fourteen patients [ 16 – 21 ].…”

Section: Discussionmentioning

confidence: 99%

From Wolf-Hirschhorn syndrome to NSD2 haploinsufficiency: a shifting paradigm through the description of a new case and a review of the literature

et al. 2022

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Background Wolf-Hirschhorn syndrome (WHS) is a well-defined disorder, whose core phenotype encompasses growth restriction, facial gestalt, intellectual disability and seizures. Nevertheless, great phenotypic variability exists due to the variable extent of the responsible 4p deletion. In addition, exome sequencing analyses, recently identified two genes, namely NSD2 and NELFA, whose loss-of-function variants contribute to a clinical spectrum consistent with atypical or partial WHS. The observation of patients exhibiting clinical features resembling WHS, with only mild developmental delay and without the typical dysmorphic features, carrying microdeletions sparing NSD2, has lead to the hypothesis that NSD2 is responsible for the intellectual disability and the facial gestalt of WHS. While presenting some of the typical findings of WHS (intellectual disability, facial gestalt, microcephaly, growth restriction and congenital heart defects), NSD2-deleted children tend to display a milder spectrum of skeletal abnormalities, usually consisting of clinodactyly, and do not exhibit seizures. We describe the clinical picture of a child with WHS due to a de novo mutation of NSD2 and discuss the clinical and diagnostic implications. Case presentation A 6-year-old boy was evaluated for a history of intrauterine growth restriction, low birth weight, neonatal hypotonia, and psychomotor delay. No episodes of seizure were reported. At physical examination, he displayed marphanoid habitus, muscle hypotrophy and facial dysmorphisms consisting in high frontal hairline, upslanting palpebral fissures and full lips with bifid ugula. Cryptorchidism, shawl scrotum, mild clinodactyly of the right little finger and bilateral syndactyly of the II and III toes with sandal gap were also noted. The radiographic essay demonstrated delayed bone age and echocardiography showed mild mitral prolapse. Whole genome sequencing analysis revealed a heterozygous de novo variant of NSD2 (c.2523delG). Conclusions Full WHS phenotype likely arises from the cumulative effect of the combined haploinsufficiency of several causative genes mapping within the 4p16.3 region, as a contiguous genes syndrome, with slightly different phenotypes depending on the specific genes involved in the deletion. When evaluating children with pictures resembling WHS, in absence of seizures, clinicians should consider this differential diagnosis.

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“…The WHS core phenotype (pre and postnatal growth delay, distinctive craniofacial features, intellectual disability, and seizures) is due to haploinsufficiency of several closely linked genes as opposed to a single gene (Battaglia, 2021;Maas et al, 2008;Zollino et al, 2008). This view is now clearly supported by the recognition of a number of individuals carrying a pathogenic variant of WHSC1 (NSD2) (loss of function, missense, truncating), or CTBP1, showing much of the core phenotype of the syndrome (developmental delay and failure to thrive; or intellectual disability and subtle dysmorphic features; or prenatal growth delay and intellectual disability) (Beck et al, 2016;Boczek et al, 2018;Derar et al, 2019;Hu et al, 2020;Jiang et al, 2019;Lozier et al, 2018) (Figures 5 and 6). The observation of such individuals has become possible with the wider employment of ES in the genetic testing of persons with neurodevelopmental disorders.…”

Section: Clinical Exome Sequencing Periodmentioning

confidence: 99%

The delineation of the Wolf‐Hirschhorn syndrome over six decades: Illustration of the ongoing advances in phenotype analysis and cytogenomic technology

Battaglia

Carey

2021

American J of Med Genetics Pt A

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Since Hirschhorn's description in 1961, the history and chronology of the clinical, cytogenetic, and molecular characterization of Wolf-Hirschhorn syndrome (WHS) elegantly demonstrates the remarkable advances in genetic technology over the last six decades that have paralleled the delineation of the phenotype. After mention in the Human Chromosome Newsletter of a child with a visible deletion of the top of a B chromosome group, 4-5, Hirschhorn and colleagues companioned their report with that of Wolf et al. in Humangenetik in 1965, and the condition was recognized and named. The 1960-1970s witnessed the description of many of the now classic chromosome disorders, including WHS, while HRB allowed for the recognition of chromosome syndromes with smaller deletions/duplications. FISH probes, developed in the next two decades, enabled the characterization of the critical region of WHS and improved clinical diagnosis with subtelomeric probes. Cytogenomic microarray in the early-mid 2000s led to both improved diagnosis of WHS patients and documentation of microdeletions of <5 megabases, helping to characterize the critical regions for specific component phenotypes (e.g., seizures, face). Recently exome sequencing technology has led to the discovery of WHS patients with WHSC1 loss of function variants, displaying some cardinal features of the phenotype (face, growth, and developmental delay).

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The first familial NSD2 cases with a novel variant in a Chinese father and daughter with atypical WHS facial features and a 7.5-year follow-up of growth hormone therapy

Cited by 7 publications

References 22 publications

Correspondence on “Loss-of-function and missense variants in NSD2 cause decreased methylation activity and are associated with a distinct developmental phenotype” by Zanoni et al

Correspondence on “Loss-of-function and missense variants in NSD2 cause decreased methylation activity and are associated with a distinct developmental phenotype” by Zanoni et al

From Wolf-Hirschhorn syndrome to NSD2 haploinsufficiency: a shifting paradigm through the description of a new case and a review of the literature

The delineation of the Wolf‐Hirschhorn syndrome over six decades: Illustration of the ongoing advances in phenotype analysis and cytogenomic technology

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