18q deletion syndrome

Changed by Frank Gaillard, 13 Mar 2019

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18q-deletion syndrome is a rare chromosomal anomaly where there is a deletion of part of the long arm of chromosome 18. Associated symptoms and findings vary widely, as do their severity. Characteristic clinical features include short stature, mental retardation, hypotonia, facial and distal skeletal abnormalities.

Clinical presentation

The presence of the syndrome is usually evident at or soon after birth. Although there is significant phenotypic variation, some features are relatively constant and include ¹:

decreased growth
craniofacial dysmorphism
- midface hypoplasia
- frontal bossing
- "carp-like" mouth
genital hypoplasia
limb abnormalities
- clubfoot
- syndactyly
- short thumbs
neurological abnormalities
- developmental delay and mental retardation
- ocular movement disorders
- seizures
- autism

Pathology

Chromosome 18q syndrome appears to result from a spontaneous, sporadic chromosomal error during very early embryonic development.

Radiographic features

MRI

The appearance of the brain on MRI is dominated by hypomyelination and abnormal white matter, particularly posteriorly and in the periventricular region. It is characterised by bilateral symmetric deep white matter hyperintensity on T2-weighted images, with associated involvement of the subcortical white matter also frequently encountered ^1,2. The brainstem and cerebellum are usually spared.

MR spectroscopy

MRS demonstrates elevated white matter choline and alpha-glutamate concentrations (resonates at 3.75 ppm) ³.

-</ul><h4>Pathology</h4><p>Chromosome 18q syndrome appears to result from a spontaneous, sporadic chromosomal error during very early embryonic development.</p><h4>Radiographic features</h4><h5>MRI</h5><p>The appearance of the brain on MRI is dominated by <a title="Hypomyelinating disorders" href="/articles/hypomyelinating-disorders">hypomyelination</a> and abnormal white matter, particularly posteriorly and in the periventricular region. It is characterised by bilateral symmetric deep white matter hyperintensity on T2-weighted images, with associated involvement of the subcortical white matter also frequently encountered <sup>1,2</sup>. The brainstem and cerebellum are usually spared.</p><h6>MR spectroscopy</h6><p>MRS demonstrates elevated white matter choline and alpha-glutamate concentrations (resonates at 3.75 ppm) <sup>3</sup>. </p>
+</ul><h4>Pathology</h4><p>Chromosome 18q syndrome appears to result from a spontaneous, sporadic chromosomal error during very early embryonic development.</p><h4>Radiographic features</h4><h5>MRI</h5><p>The appearance of the brain on MRI is dominated by <a href="/articles/hypomyelinating-disorders">hypomyelination</a> and abnormal white matter, particularly posteriorly and in the periventricular region. It is characterised by bilateral symmetric deep white matter hyperintensity on T2-weighted images, with associated involvement of the subcortical white matter also frequently encountered <sup>1,2</sup>. The brainstem and cerebellum are usually spared.</p><h6>MR spectroscopy</h6><p>MRS demonstrates elevated white matter choline and alpha-glutamate concentrations (resonates at 3.75 ppm) <sup>3</sup>. </p>

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