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Temple syndrome: improving the recognition of an underdiagnosed chromosome 14 imprinting disorder: an analysis of 51 published cases

Temple syndrome: improving the recognition of an underdiagnosed chromosome 14 imprinting disorder: an analysis of 51 published cases
Temple syndrome: improving the recognition of an underdiagnosed chromosome 14 imprinting disorder: an analysis of 51 published cases
Chromosome 14 harbours an imprinted locus at 14q32. Maternal uniparental disomy of chromosome 14, paternal deletions and loss of methylation at the intergenic differentially methylated region (IG-DMR) result in a human phenotype of low birth weight, hypotonia, early puberty and markedly short adult stature. The analysis of the world literature of 51 cases identifies the key features that will enhance diagnosis and potentially improve treatment. We found a median birth weight SD score (SDS) of -1.88 and median adult final height of -2.04 SDS. Hypotonia and motor delay were reported in 93% and 83% of cases, respectively. Early puberty was reported in 86% of cases with the mean age of menarche at 10 years and 2 months of age. Small hands and feet were reported frequently (87% and 96%, respectively). Premature birth was common (30%) and feeding difficulties frequently reported (n = 22). There was evidence of mildly reduced intellectual ability (measured IQ 75–95). Obesity was reported in 49% of cases, and three patients developed type 2 diabetes mellitus. Two patients were reported to have recurrent hypoglycaemia, and one of these patients was subsequently demonstrated to be growth hormone deficient and started replacement therapy. We propose the use of the name ‘Temple syndrome’ for this condition and suggest that improved diagnosis and long-term monitoring, especially of growth and cardiovascular risk factors, is required.
imprinting, temple syndrome, UPD14mat, chromosome 14q32
0022-2593
495-501
Ioannides, Y.
4f1480c1-41af-42c4-89e1-08174cadda39
Lokulo-Sodipe, K.
d428f857-0e58-4964-b1f0-136af7432805
Mackay, D.J.G.
588a653e-9785-4a00-be71-4e547850ee4a
Davies, J.H.
9f18fcad-f488-4c72-ac23-c154995443a9
Temple, I.K.
d63e7c66-9fb0-46c8-855d-ee2607e6c226
Ioannides, Y.
4f1480c1-41af-42c4-89e1-08174cadda39
Lokulo-Sodipe, K.
d428f857-0e58-4964-b1f0-136af7432805
Mackay, D.J.G.
588a653e-9785-4a00-be71-4e547850ee4a
Davies, J.H.
9f18fcad-f488-4c72-ac23-c154995443a9
Temple, I.K.
d63e7c66-9fb0-46c8-855d-ee2607e6c226

Ioannides, Y., Lokulo-Sodipe, K., Mackay, D.J.G., Davies, J.H. and Temple, I.K. (2014) Temple syndrome: improving the recognition of an underdiagnosed chromosome 14 imprinting disorder: an analysis of 51 published cases. Journal of Medical Genetics, 51 (8), 495-501. (doi:10.1136/jmedgenet-2014-102396). (PMID:24891339)

Record type: Article

Abstract

Chromosome 14 harbours an imprinted locus at 14q32. Maternal uniparental disomy of chromosome 14, paternal deletions and loss of methylation at the intergenic differentially methylated region (IG-DMR) result in a human phenotype of low birth weight, hypotonia, early puberty and markedly short adult stature. The analysis of the world literature of 51 cases identifies the key features that will enhance diagnosis and potentially improve treatment. We found a median birth weight SD score (SDS) of -1.88 and median adult final height of -2.04 SDS. Hypotonia and motor delay were reported in 93% and 83% of cases, respectively. Early puberty was reported in 86% of cases with the mean age of menarche at 10 years and 2 months of age. Small hands and feet were reported frequently (87% and 96%, respectively). Premature birth was common (30%) and feeding difficulties frequently reported (n = 22). There was evidence of mildly reduced intellectual ability (measured IQ 75–95). Obesity was reported in 49% of cases, and three patients developed type 2 diabetes mellitus. Two patients were reported to have recurrent hypoglycaemia, and one of these patients was subsequently demonstrated to be growth hormone deficient and started replacement therapy. We propose the use of the name ‘Temple syndrome’ for this condition and suggest that improved diagnosis and long-term monitoring, especially of growth and cardiovascular risk factors, is required.

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Accepted/In Press date: 2 May 2014
e-pub ahead of print date: 2 June 2014
Published date: August 2014
Keywords: imprinting, temple syndrome, UPD14mat, chromosome 14q32
Organisations: Human Development & Health

Identifiers

Local EPrints ID: 365414
URI: http://eprints.soton.ac.uk/id/eprint/365414
DOI: doi:10.1136/jmedgenet-2014-102396
ISSN: 0022-2593
PURE UUID: 806d313b-7d95-4b5b-8360-41c1c6e670a8
ORCID for K. Lokulo-Sodipe: ORCID iD orcid.org/0000-0002-8169-3384
ORCID for D.J.G. Mackay: ORCID iD orcid.org/0000-0003-3088-4401
ORCID for I.K. Temple: ORCID iD orcid.org/0000-0002-6045-1781

Catalogue record

Date deposited: 04 Jun 2014 11:13
Last modified: 15 Mar 2024 03:01

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Contributors

Author: Y. Ioannides
Author: K. Lokulo-Sodipe ORCID iD
Author: D.J.G. Mackay ORCID iD
Author: J.H. Davies
Author: I.K. Temple ORCID iD

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