Microdeletions in 9q33.3-q34.11 in five patients with intellectual disability, microcephaly, and seizures of incomplete penetrance: is STXBP1 not the only causative gene?

Julia K Ehret,Eva Rossier,Benno Röthlisberger,Michael Bonin,Andreas Dufke,Alexander M Zink,Stefanie Schön,Nicola Dennert,Elisabeth Mangold,Eva Wohlleber,Hartmut Engels,Ute Grasshoff,Kirsten Cremer,Ghislaine Plessis,Isabel Filges,Jennifer A Lee,Elodie Lacaze,Johannes P Zimmermann,Guillaume Jedraszak,Andrea Bevot,Joris Andrieux,Peter Miny,Jéssica Becker ,A De Broca ,Michèle Mathieu‐Dramard ,Markus M Nöthen

doi:10.1186/s13039-015-0178-8

Abstract

BackgroundMost microdeletions involving chromosome sub-bands 9q33.3-9q34.11 to this point have been detected by analyses focused on STXBP1, a gene known to cause early infantile epileptic encephalopathy 4 and other seizure phenotypes. Loss-of-function mutations of STXBP1 have also been identified in some patients with intellectual disability without epilepsy. Consequently, STXBP1 is widely assumed to be the gene causing both seizures and intellectual disability in patients with 9q33.3-q34.11 microdeletions.ResultsWe report five patients with overlapping microdeletions of chromosome 9q33.3-q34.11, four of them previously unreported. Their common clinical features include intellectual disability, psychomotor developmental delay with delayed or absent speech, muscular hypotonia, and strabismus. Microcephaly and short stature are each present in four of the patients. Two of the patients had seizures. De novo deletions range from 1.23 to 4.13 Mb, whereas the smallest deletion of 432 kb in patient 3 was inherited from her mother who is reported to have mild intellectual disability. The smallest region of overlap (SRO) of these deletions in 9q33.3 does not encompass STXBP1, but includes two genes that have not been previously associated with disease, RALGPS1 and GARNL3.Sequencing of the two SRO genes RALGPS1 and GARNL3 in at least 156 unrelated patients with mild to severe idiopathic intellectual disability detected no causative mutations. Gene expression analyses in our patients demonstrated significantly reduced expression levels of GARNL3, RALGPS1 and STXBP1 only in patients with deletions of the corresponding genes. Thus, reduced expression of STXBP1 was ruled out as a cause for seizures in our patient whose deletion did not encompass STXBP1.ConclusionsWe suggest that microdeletions of this region on chromosome 9q cause a clinical spectrum including intellectual disability, developmental delay especially concerning speech, microcephaly, short stature, mild dysmorphisms, strabismus, and seizures of incomplete penetrance, and may constitute a new contiguous gene deletion syndrome which cannot completely be explained by deletion of STXBP1.Electronic supplementary materialThe online version of this article (doi:10.1186/s13039-015-0178-8) contains supplementary material, which is available to authorized users.

Highlights

Most microdeletions involving chromosome sub-bands 9q33.3-9q34.11 to this point have been detected by analyses focused on STXBP1, a gene known to cause early infantile epileptic encephalopathy 4 and other seizure phenotypes
Previously, microdeletions affecting the chromosomal region 9q33.3-q34.11 have been reported in association with early infantile epileptic encephalopathy 4 (EIEE4, or Ohtahara syndrome, OMIM #612164)
The STXBP1 gene was identified as a causative gene and loss-offunction mutations of STXBP1 have been shown to cause Epileptic Encephalopathy 4 (EIEE4) [1], West syndrome [2], other seizure phenotypes [3], non-syndromic epilepsy [4], and intellectual disability (ID)

Summary

Introduction

Most microdeletions involving chromosome sub-bands 9q33.3-9q34.11 to this point have been detected by analyses focused on STXBP1, a gene known to cause early infantile epileptic encephalopathy 4 and other seizure phenotypes. Loss-of-function mutations of STXBP1 have been identified in some patients with intellectual disability without epilepsy. The STXBP1 gene was identified as a causative gene and loss-offunction mutations of STXBP1 have been shown to cause EIEE4 [1], West syndrome [2], other seizure phenotypes [3], non-syndromic epilepsy [4], and intellectual disability (ID). We present the clinical and genetic characterization of five patients whose common clinical features include intellectual disability (ID), psychomotor developmental delay (DD) with delayed or absent speech, muscular hypotonia, strabismus, dysmorphisms and other recurrent findings. For these patients, we have identified overlapping microdeletions of chromosome 9q33.3-q34.11 by molecular karyotyping. The smallest region of overlap (SRO) concerning these common clinical features contains only two RefSeq genes, which has implications regarding the potential role STXBP1 may or may not play in our patients’ phenotypes

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