3q27.3-q29 duplication and 2q37.2-q37.3 deletion rare in a female child with developmental delay and hypotonia in Manaus, Brazil

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DOI:

https://doi.org/10.18316/sdh.v10i2.8274

Palavras-chave:

SNP array, Duplication, Deletion, Pathogenic Variants.

Resumo

Introduction

Cytogenomic analyses play a fundamental role in the detection of genetic disorders in patients with developmental delay, and are an excellent diagnostic method.

Objective

Report the case in a female child with developmental delay and hypotonia and relate the existence of copy-number variations to understand their contribution to the appearance of the phenotype.

Methods

This is an case report. Anamnesis, female with 10 months of age at first appointment. Mother reported uneventful pregnancy with obstructed cesarean delivery and neonatal jaundice. She is the only child of a non-consanguineous, common characteristics of developmental delay and hypotonia. Physical examination, patient presented developmental delay, hypotonia, loose skin, hyperextensible joints, micrognathia, ankyloglossia, umbilical hernia, camptodactyly and involuntary convulsive seizures. Cytogenomic analysis, SNP Array.

Results

SNP array revealed a duplication in 3q27.3.3q29 and a deletion in 2q37.2.2q37.3, both considered pathogenic.

Conclusion

Among the pathogenic variants, already known duplications syndromes were observed, as well as changes that are not described in the literature. The altered regions contain genes that are sensitive to dosage and/or gene haploinsufficiency, contributed to the phenotype of the patient. SNP array proved to be paramount in the diagnostic elucidation of patient, and made it possible to therapeutic management and genetic counseling.

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Publicado

2022-05-27

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