De novo microdeletion of 5q14.3 excluding <i>MEF2C</i> in a patient with infantile spasms, microcephaly, and agenesis of the corpus callosum

Shimojima, Keiko; Okumura, Akihisa; Mori, Hiromu; Abe, Shinpei; Ikeno, Mitsuru; Shimizu, Toshiaki; Yamamoto, Toshiyuki

doi:10.1002/ajmg.a.35490

Cited by 24 publications

(40 citation statements)

References 13 publications

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“…An abnormal corpus callosum morphology was seen in 12/13 patients. Corpus callosum dysgenesis has been described in the literature in various CNVs, and has been specifically described in most of our patients' chromosomal microdeletion/microduplication syndromes: 1p36 deletion, 5q14 deletion, 15q13 deletion, 18q21 deletion, 14q32 duplication, Wolf‐Hirschhorm syndrome, 1q43q44 deletion, and 21q22 deletion (Ballif et al, ; Edwards, Sherr, Barkovich, & Richards, ; Gillentine & Schaaf, ; Heide et al, ; Hotz et al, ; Oegema et al, ; Õiglane‐Shlik et al, ; Ramaswamy et al, ; Shimojima et al, ; Verbrugge et al, ; Villa et al, ). A study on the role of chromosomal micro‐rearrangements in patients with both corpus callosum abnormality and intellectual disability, found that 13% had CNVs as the probable cause of their disorder (Heide et al, ).…”

Section: Discussionmentioning

confidence: 66%

Brain white matter abnormalities associated with copy number variants

Vigdorovich

Ben-Sira

Blumkin

et al. 2019

American J of Med Genetics Pt A

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White matter (WM) signal abnormalities are demonstrated in various neurodevelopmental disorders on brain magnetic resonance imaging (MRI). The pattern of WM abnormalities can aid in the diagnostic process. This study aims to characterize the WM changes found in microdeletion/microduplication syndromes. Thirteen patients with neurodevelopmental disorders due to copy number variations were collected from a cohort of children with evidence of WM abnormalities on brain MRI, in two medical centers. A pediatric neuroradiologist blindly interpreted the MRI scans.Clinical and genetic findings were retrospectively extracted from the medical records. WM changes included: multifocal (10/13) periventricular (12/13) and subcortical (5/13) signal abnormalities and WM volume loss (6/13). Dysgenesis of the corpus callosum was depicted in 12/13. The main clinical features were: global developmental delay (13/13), hypotonia (11/13), epilepsy (10/13), dysmorphic features (9/13), microcephaly (6/13), short stature (6/13), and systemic involvement (6/13). We showed that different chromosomal micro-rearrangement syndromes share similar MRI patterns of nonspecific multifocal predominantly periventricular WM changes associated with corpus callosum dysgenesis with or without WM and gray matter loss. Hence, the association of these features in a patient evaluated for global developmental delay/intellectual disability suggests a chromosomal micro-rearrangement syndrome, and a chromosomal microarray analysis should be performed.

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Section: Discussionmentioning

confidence: 66%

Brain white matter abnormalities associated with copy number variants

Vigdorovich

Ben-Sira

Blumkin

et al. 2019

American J of Med Genetics Pt A

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“…8,9 A neurocutaneous syndrome involving intracranial and dermatologic vascular malformations has also been described. 4,5,7,[13][14][15] However, MEF2C lies outside the deleted region in at least 5 reported cases of 5q14.3 deletion syndrome, 8,9,16,17 so a role for other genes at the 5q14.3 locus is likely. Current literature points to MEF2C (OMIM 600662) haploinsufficiency playing the most important role, largely based on identification of intragenic mutations of this gene in patients with intellectual disability, stereotypies, and infantile-onset epilepsy, which may include infantile spasms, and myoclonic, atonic, generalized tonicclonic, focal impaired awareness, atypical absence, and hemiclonic seizures.…”

mentioning

confidence: 99%

“…Current literature points to MEF2C (OMIM 600662) haploinsufficiency playing the most important role, largely based on identification of intragenic mutations of this gene in patients with intellectual disability, stereotypies, and infantile-onset epilepsy, which may include infantile spasms, and myoclonic, atonic, generalized tonicclonic, focal impaired awareness, atypical absence, and hemiclonic seizures. 4,5,7,[13][14][15] However, MEF2C lies outside the deleted region in at least 5 reported cases of 5q14.3 deletion syndrome, 8,9,16,17 so a role for other genes at the 5q14.3 locus is likely.…”

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confidence: 99%

ADGRV1 is implicated in myoclonic epilepsy

et al. 2017

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Our data suggest that the ADGRV1 variation contributes to epilepsy with myoclonic seizures, although the inheritance pattern may be complex in many cases. In patients with 5q14.3 deletion and epilepsy, ADGRV1 haploinsufficiency likely contributes to seizure development. The latter is a shift from current thinking, as MEF2C haploinsufficiency has been considered the main cause of epilepsy in 5q14.3 deletion syndrome. In cases of 5q14.3 deletion and epilepsy, seizures likely occur due to haploinsufficiency of one or both of ADGRV1 and MEF2C.

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“…[4] Down's syndrome is the most common chromosomal abnormality reported in patients with IS; however, many other types of chromosomal abnormalities have been reported, including 1p36 deletion, 17p 13.3 microdeletion, 22q, XXY [4] , partial 2p trisomy, 4p trisomy, 7q trisomy, 7q duplication, 15p tetrasomy, 15q duplication, 18p monosomy, 18q duplication, 21 trisomy, t (12;21), t (X; 18)(p22;p11.2), t (6;14)(q27;q13.3), t (1;Y), and disomy for Xq26.3-qter [2,3] , 5q14.3, 7q11.23-q21.1, tetrasomy 12p, 15q13.3, 16p13.11 microdeletion, 17q21.31 microdeletion, and 19p13 deletion. [5][6][7][8] It was once presumed that the chromosomal abnormality, trisomy 7q33->qter and monosomy 9 pter->p23, found in a child was probably the etiology for the IS and multiple anomalies, and the epilepsy is most likely resulted from the distal 7q duplication and not distal 9p deletion. [9] Epilepsy was once associated with chromosome 7 abnormities: Trisomy of the short-arm of chromosome 7 was formerly reported to be associated with epileptic crises [10] and long-arm deletion of chromosome 7 was also previously found to be associated with IS.…”

Section: Discussionmentioning

confidence: 99%

Infantile spasms in a boy with an abnormal karyotype (46, XY, der(9)t(7;9)(p15;p22)pat)

Zhong

Dong

et al. 2014

Neurol India

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Infantile spasm (IS) is an epilepsy syndrome affecting infants and young toddlers and many causes have been reported, including occasional chromosomal abnormalities. We describe a 6-month-oldboy who experienced his first seizure at 5 months of age. The seizures were characterized by brief head nods and forceful flexion of the trunk and limbs. The patient has been developmentally delayed since birth and had deteriorated remarkably in the last month. Interictal electroencephalography showed modified hypsarrhythmia. Magnetic resonance imaging showed delayed myelination and widened brain extracellular space. Chromosomal analysis revealed the karyotype 46, XY, der(9) t(7;9)(p15;p22) pat. His father has the asymptomatic reciprocal translocation t(7;9)(p15;p22). This chromosomal abnormality is probably the etiology for the ISs and severe developmental anomalies in this patient. Chromosomal analysis may be done in patients with IS with no obvious cause.

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De novo microdeletion of 5q14.3 excluding MEF2C in a patient with infantile spasms, microcephaly, and agenesis of the corpus callosum

Cited by 24 publications

References 13 publications

Brain white matter abnormalities associated with copy number variants

Brain white matter abnormalities associated with copy number variants

ADGRV1 is implicated in myoclonic epilepsy

Infantile spasms in a boy with an abnormal karyotype (46, XY, der(9)t(7;9)(p15;p22)pat)

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