Gene expression patterns in relation to the clinical phenotype in Klinefelter syndrome

Michael Zitzmann; Rebecca Bongers; Steffi Werler; Nadja Bogdanova; Joachim Wistuba; Sabine Kliesch; Jörg Gromoll; Frank Tüttelmann

doi:10.1210/jc.2014-2780

Gene expression patterns in relation to the clinical phenotype in Klinefelter syndrome

J Clin Endocrinol Metab. 2015 Mar;100(3):E518-23. doi: 10.1210/jc.2014-2780. Epub 2014 Dec 22.

Authors

Michael Zitzmann¹, Rebecca Bongers, Steffi Werler, Nadja Bogdanova, Joachim Wistuba, Sabine Kliesch, Jörg Gromoll, Frank Tüttelmann

Affiliation

¹ Centre of Reproductive Medicine and Andrology (M.Z., R.B., S.W., J.W., S.K., J.G.), and Institute for Human Genetics (N.B., F.T.), University of Münster, University Clinics, D-48149 Münster, Germany.

PMID: 25532039
DOI: 10.1210/jc.2014-2780

Abstract

Context: Klinefelter syndrome (KS) is the most common chromosome disorder in men (47,XXY), exhibiting a phenotype with marked variation and increased morbidity. The pathophysiological link between the supernumerary X chromosome and the clinical phenotype remains unknown.

Objective: To elucidate whether differential gene expression patterns can be detected in KS patients and whether these are related to inherent clinical features.

Design, setting, participants: EXAKT (Epigenetics, X-chromosomal Features and Clinical Applications in Klinefelter Syndrome Trial) is a Münster-based prospective project involving 132 Klinefelter men and their parents. A range of cardiovascular, inflammatory, and metabolic factors, in comparison to age-matched male (n = 50)/female controls (n = 50) and in relation to genetic features, is assessed.

Main outcomes and measures: Our predefined hypothesis was that differential gene expression patterns in blood cells exist in KS patients vs male controls and are related to the clinical phenotype.

Results: Differential expression of 36 X-chromosomal and autosomal genes put KS patients into a unique genetic setting vs male and female controls. The KS cohort exhibited increased insulin resistance, enhanced inflammatory and procoagulatory status, higher waist circumference, dyslipidemia, and a markedly shorter 12-lead electrocardiogram QTc interval (partly located within the pathological range) vs male controls (all P < .001). Clinical dyshomeostasis was associated with expression patterns of dysregulated genes (all P < .01). Parental origin of the supernumerary X chromosome was a confounder regarding insulin resistance and cardiac phenotype (P < .05). Results are considered preliminary because gene expression was measured in blood cells.

Conclusions: The supernumerary X chromosome contributes to a number of pathologies in KS. The pattern of gene expression is altered in KS, and the degree of differential gene expression is associated with the clinical phenotype.

Trial registration: ClinicalTrials.gov NCT01703676.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adult
Case-Control Studies
Chromosomes, Human, X / genetics
Cross-Sectional Studies
Epigenesis, Genetic
Female
Gene Expression
Gene Expression Profiling
Genetic Association Studies
Humans
Klinefelter Syndrome / genetics*
Male
Middle Aged
Phenotype
Young Adult

Associated data

ClinicalTrials.gov/NCT01703676