Anna Poluha scite author profile

Infantile myofibromatosis (IM), which is typically diagnosed in young children, comprises a wide clinical spectrum ranging from inconspicuous solitary soft tissue nodules to multiple disseminated tumors resulting in life-threatening complications. Familial IM follows an autosomal dominant mode of inheritance and is linked to PDGFRB germline variants. Somatic PDGFRB variants were also detected in solitary and multifocal IM lesions. PDGFRB variants associated with IM constitutively activate PDGFRB kinase activity in the absence of its ligand. Germline variants have lower activating capabilities than somatic variants and, thus, require a second cis-acting hit for full receptor activation. Typically, these mutant receptors remain sensitive to tyrosine kinase inhibitors such as imatinib. The SIOPE Host Genome Working Group, consisting of pediatric oncologists, clinical geneticists and scientists, met in January 2020 to discuss recommendations for genetic testing and surveillance for patients who are diagnosed with IM or have a family history of IM/PDGFRB germline variants. This report provides a brief review of the clinical manifestations and genetics of IM and summarizes our interdisciplinary recommendations.

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Novel 14q11.2 microduplication including the CHD8 and SUPT16H genes associated with developmental delay

Smyk¹,

Poluha²,

Jaszczuk³

et al. 2016

American J of Med Genetics Pt A

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Neurodevelopmental disorders have long been associated with chromosomal abnormalities, including microdeletions and microduplications. Submicroscopic 14q11.2 deletions involving the CHD8 and SUPT16H genes have been reported in patients with developmental delay (DD)/intellectual disability (ID) or autism spectrum disorders (ASDs) and/or macrocephaly. Recently, disruptive CHD8 mutations were described in patients with similar phenotypes further showing pivotal role of CHD8 gene in the pathogenesis of DD/ID or ASDs. We report here the first case of ~445 kb de novo microduplication, encompassing the minimal critical 14q11.2 deletion region, in 8-year-old boy showing DD, cognitive impairment and facial dysmorphism. Our results suggest that gain of the chromosomal region 14q11.2 is causative for clinical findings present in the patient.

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Molecular and clinical characterization of new patient with 1,08 Mb deletion in 10p15.3 region

Poluha

Bernaciak²,

Jaszczuk

et al. 2017

Mol Cytogenet

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Background: Three distinct contiguous gene deletion syndromes are located at 10p chromosomal region. The deletion, involving 10p15.3 region, has been characterized by (DeScipio et al., Am J Med Genet A 158A:2152-61, 2012. However, because of the variation in size of the described deletions and lack of knowledge about the involved genes, the correlation between genotypes and patients' phenotypes remains unknown. Conclusions: This case shows the importance of collection of more patients with deletion in order to obtain a more precise physical map of 10p region.

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Anna Poluha

Phenotype and genotype in 103 patients with tricho-rhino-phalangeal syndrome

Genetic testing and surveillance in infantile myofibromatosis: a report from the SIOPE Host Genome Working Group

Novel 14q11.2 microduplication including the CHD8 and SUPT16H genes associated with developmental delay

Molecular and clinical characterization of new patient with 1,08 Mb deletion in 10p15.3 region

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