Size matters: Large copy number losses in Hirschsprung disease patients reveal genes involved in enteric nervous system development

Kuil, Laura E.; MacKenzie, Katherine C.; Tang, Clara Sze-Man; Windster, Jonathan D; Le, Thuy Linh; Karim, Anwarul; Graaf, Bianca M. de; Helm, Robert van der; Bever, Yolande van; Sloots, Cornelius E. J.; Meeussen, Conny; Tibboel, Dick; Klein, Annelies de; Wijnen, René; Amiel, Jeanne; Lyonnet, Stanislas; García-Barceló, María-Mercé; Tam, Paul Kwong Hang; Alves, Maria M.; Brooks, Alice S.; Hofstra, Robert M.W.; Brosens, Erwin

doi:10.1371/journal.pgen.1009698

Cited by 20 publications

(9 citation statements)

References 100 publications

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“…Moreover, there was one LoF variant (D737 TUBB NM_178014.4:c.623_624del (p.Tyr208Ter)) in the gene which is characterized by high LoF intolerance (pLI = 0.98). HGMD reports only 14 variants, of which there are 12 missense pathogenic variants and whole gene deletion and frameshift deletion with supposed deleterious effects in patients with Hirschsprung disease [ 39 ].…”

Section: Discussionmentioning

confidence: 99%

Complex Diagnostics of Non-Specific Intellectual Developmental Disorder

Levchenko

Дадали

Bessonova

et al. 2022

IJMS

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Intellectual development disorder (IDD) is characterized by a general deficit in intellectual and adaptive functioning. In recent years, there has been a growing interest in studying the genetic structure of IDD. Of particular difficulty are patients with non-specific IDD, for whom it is impossible to establish a clinical diagnosis without complex genetic diagnostics. We examined 198 patients with non-specific IDD from 171 families using whole-exome sequencing and chromosome microarray analysis. Hereditary forms of IDD account for at least 35.7% of non-specific IDD, of which 26.9% are monogenic forms. Variants in the genes associated with the BAF (SWI/SNF) complex were the most frequently identified. We were unable to identify phenotypic features that would allow differential diagnosis of monogenic and microstructural chromosomal rearrangements in non-specific IDD at the stage of clinical examination, but due to its higher efficiency, exome sequencing should be the diagnostic method of the highest priority study after the standard examination of patients with NIDD in Russia.

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Section: Discussionmentioning

confidence: 99%

Complex Diagnostics of Non-Specific Intellectual Developmental Disorder

Levchenko

Дадали

Bessonova

et al. 2022

IJMS

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“…Uveal melanoma cell lines have been authenticated previously by single polymorphism analysis and AmpFLSTR™ Identi ler™ Plus PCR Ampli cation Kit (Thermo Fisher, Bleiswijk, The Netherlands) followed by sequencing. Additionally, we performed single nucleotide polymorphism analysis on CLR4059 and GM21808 with the In nium™ Global Screening Array-24 v3.0 BeadChip according to the manufacturer's protocols and guidelines (Illumina, San Diego, CA, USA) and analysis methods described previously [31].…”

Section: Cell Culture Conditionsmentioning

confidence: 99%

Uveal Melanoma zebrafish xenograft models illustrate the mutation status-dependent effect of compound synergism or antagonism

Bosch,

Kilic,

Brosens

2024

Preprint

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Purpose Uveal melanoma (UM) is the most common primary intraocular malignancy with a high probability of metastatic disease. Although excellent treatment option for primary UM are available, therapy for metastatic disease remain limited. Drug discovery studies using mouse models have thus far failed to provide therapeutic solutions, highlighting the need for novel models. Here, we optimize zebrafish xenografts as a potential model for drug discovery by showcasing the behavior of multiple cell lines and novel findings on mutation-dependent compound synergism/antagonism using Z-Tada; an algorithm to objectively characterize output measurements. Methods Prognostic relevant primary and metastatic UM cell lines or healthy melanocytes were inoculated at three distinct inoculation sites. Standardized quantifications independent of inoculation site were obtained using Z-Tada; an algorithm to measure tumor burden and the number, size and distance of disseminated tumor cells. Sequentially, we utilized this model to validate combinatorial synergism or antagonism seen in vitro. Results Detailed analysis of 691 zebrafish xenografts demonstrated perivitelline space inoculation provided robust data with high probability of cell dissemination. Cell lines with more invasive behavior (SF3B1mut and BAP1mut) behaved most aggressive in this model. Combinatorial drug treatment illustrated synergism or antagonism is mutation-dependent, which were confirmed in vivo. Combinatorial treatment differed per xenograft-model, as it either inhibited overall tumor burden or cell dissemination. Conclusion Perivitelline space inoculation provides robust zebrafish xenografts with the ability for high-throughput drug screening and robust data acquisition using Z-Tada. This model demonstrates that drug discovery for uveal melanoma must take mutational subclasses into account, especially in combinatorial treatment discoveries.

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“…We also used available in-house RNA sequencing data from human intestine at embryonic weeks 12, 14 and 16 [49]. Enteric nervous genes expression prioritization has been described previously [50].…”

Section: Data Analysis and Selection Of Somatic Variantsmentioning

confidence: 99%

The Somatic Mutation Paradigm in Congenital Malformations: Hirschsprung Disease as a Model

MacKenzie

Garritsen

Chauhan

et al. 2021

IJMS

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Patients with Hirschsprung disease (HSCR) do not always receive a genetic diagnosis after routine screening in clinical practice. One of the reasons for this could be that the causal mutation is not present in the cell types that are usually tested—whole blood, dermal fibroblasts or saliva—but is only in the affected tissue. Such mutations are called somatic, and can occur in a given cell at any stage of development after conception. They will then be present in all subsequent daughter cells. Here, we investigated the presence of somatic mutations in HSCR patients. For this, whole-exome sequencing and copy number analysis were performed in DNA isolated from purified enteric neural crest cells (ENCCs) and blood or fibroblasts of the same patient. Variants identified were subsequently validated by Sanger sequencing. Several somatic variants were identified in all patients, but causative mutations for HSCR were not specifically identified in the ENCCs of these patients. Larger copy number variants were also not found to be specific to ENCCs. Therefore, we believe that somatic mutations are unlikely to be identified, if causative for HSCR. Here, we postulate various modes of development following the occurrence of a somatic mutation, to describe the challenges in detecting such mutations, and hypothesize how somatic mutations may contribute to ‘missing heritability’ in developmental defects.

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Size matters: Large copy number losses in Hirschsprung disease patients reveal genes involved in enteric nervous system development

Cited by 20 publications

References 100 publications

Complex Diagnostics of Non-Specific Intellectual Developmental Disorder

Complex Diagnostics of Non-Specific Intellectual Developmental Disorder

Uveal Melanoma zebrafish xenograft models illustrate the mutation status-dependent effect of compound synergism or antagonism

The Somatic Mutation Paradigm in Congenital Malformations: Hirschsprung Disease as a Model

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