Decreased cholesterol synthesis as a possible aetiological factor in malformations of Trisomy 18

Wayne W.K. Lam; J. Kirk; N. Manning; W. Reardon; R. I. Kelley; D. FitzPatrick

doi:10.1016/j.ejmg.2005.05.011

Decreased cholesterol synthesis as a possible aetiological factor in malformations of Trisomy 18

Wayne W.K. Lam, J. Kirk, N. Manning, W. Reardon, R. I. Kelley, D. FitzPatrick

Kennedy Krieger Institute

Research output: Contribution to journal › Article › peer-review

12 Scopus citations

Abstract

We report a series of neonates and foetuses with trisomy 18 and abnormally low cholesterol levels and propose that down regulation of cholesterol synthesis in trisomy 18 is, in part, responsible for its phenotype. Cholesterol is a major structural lipid of cell membranes, as well as the precursor of steroid hormones and bile acids. Several human malformation syndromes have been identified biochemically as disorders of cholesterol biosynthesis. Trisomy 18, a multi-system malformation syndrome, has clinical features that overlap with those of disorders of cholesterol biosynthesis and dysregulation of this pathway may have a role in the developmental pathology.

Original language	English (US)
Pages (from-to)	195-199
Number of pages	5
Journal	European Journal of Medical Genetics
Volume	49
Issue number	2
DOIs	https://doi.org/10.1016/j.ejmg.2005.05.011
State	Published - Mar 2006

Keywords

Cholesterol
Edwards
Smith-Lemli-Opitz
Sterol biosynthesis
Trisomy 18

ASJC Scopus subject areas

Genetics
Genetics(clinical)

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10.1016/j.ejmg.2005.05.011

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title = "Decreased cholesterol synthesis as a possible aetiological factor in malformations of Trisomy 18",

abstract = "We report a series of neonates and foetuses with trisomy 18 and abnormally low cholesterol levels and propose that down regulation of cholesterol synthesis in trisomy 18 is, in part, responsible for its phenotype. Cholesterol is a major structural lipid of cell membranes, as well as the precursor of steroid hormones and bile acids. Several human malformation syndromes have been identified biochemically as disorders of cholesterol biosynthesis. Trisomy 18, a multi-system malformation syndrome, has clinical features that overlap with those of disorders of cholesterol biosynthesis and dysregulation of this pathway may have a role in the developmental pathology.",

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T1 - Decreased cholesterol synthesis as a possible aetiological factor in malformations of Trisomy 18

AU - Lam, Wayne W.K.

AU - Kirk, J.

AU - Manning, N.

AU - Reardon, W.

AU - Kelley, R. I.

AU - FitzPatrick, D.

PY - 2006/3

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N2 - We report a series of neonates and foetuses with trisomy 18 and abnormally low cholesterol levels and propose that down regulation of cholesterol synthesis in trisomy 18 is, in part, responsible for its phenotype. Cholesterol is a major structural lipid of cell membranes, as well as the precursor of steroid hormones and bile acids. Several human malformation syndromes have been identified biochemically as disorders of cholesterol biosynthesis. Trisomy 18, a multi-system malformation syndrome, has clinical features that overlap with those of disorders of cholesterol biosynthesis and dysregulation of this pathway may have a role in the developmental pathology.

AB - We report a series of neonates and foetuses with trisomy 18 and abnormally low cholesterol levels and propose that down regulation of cholesterol synthesis in trisomy 18 is, in part, responsible for its phenotype. Cholesterol is a major structural lipid of cell membranes, as well as the precursor of steroid hormones and bile acids. Several human malformation syndromes have been identified biochemically as disorders of cholesterol biosynthesis. Trisomy 18, a multi-system malformation syndrome, has clinical features that overlap with those of disorders of cholesterol biosynthesis and dysregulation of this pathway may have a role in the developmental pathology.

KW - Cholesterol

KW - Edwards

KW - Smith-Lemli-Opitz

KW - Sterol biosynthesis

KW - Trisomy 18

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Decreased cholesterol synthesis as a possible aetiological factor in malformations of Trisomy 18

Abstract

Keywords

ASJC Scopus subject areas

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