Your search keyword '"Heger, Sabine"' showing total 3 results

1. Gene Expression Profiling of Hypothalamic Hamartomas: A Search for Genes Associated with Central Precocious Puberty.

Author

Parent, Anne-Simone, Matagne, Valerie, Westphal, Manfred, Heger, Sabine, Ojeda, Sergio, and Jung, Heike

Subjects

HYPOTHALAMIC hormones, GENE expression, HUMAN sexuality, PRECOCIOUS puberty, LUTEINIZING hormone releasing hormone, GENETICS

Abstract

Background: Hypothalamic hamartomas (HHs) are congenital lesions composed of neurons and astroglia. Frequently, HHs cause central precocious puberty (CPP) and/or gelastic seizures. Because HHs might express genes similar to those required for the initiation of normal puberty, we used cDNA arrays to compare the gene expression profile of an HH associated with CPP with three HHs not accompanied by sexual precocity. Methods: Global changes in gene expression were detected using Affymetrix arrays. The results were confirmed by semiquantitative PCR, which also served to examine the expression of selected genes in the hypothalamus of female monkeys undergoing puberty. Results: All HHs were associated with seizures. Ten genes whose expression was increased in the HH with CPP were identified. They encode proteins involved in three key cellular processes: transcriptional regulation, cell-cell signaling, and cell adhesiveness. They include IA-1 and MEF2A, two transcription factors required for neuronal development; mGluR1 and VILIP-1, which encode proteins involved in neuronal communication, and TSG-6 that encodes a protein involved in cell adhesiveness. Of these, expression of mGluR1 also increases in the female monkey hypothalamus at puberty. Conclusions: Increased expression of these genes in HHs may be relevant to the ability of some HHs to induce sexual precocity. Copyright © 2007 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2008

2. Early Onset of Puberty: Tracking Genetic and Environmental Factors.

Author

Parent, Anne-Simone, Rasier, Gregory, Gerard, Arlette, Heger, Sabine, Roth, Christian, Mastronardi, Claudio, Jung, Heike, Ojeda, Sergio R., and Bourguignon, Jean-Pierre

Subjects

PUBERTY, CRITICAL periods (Biology), SEX (Biology), GENETIC regulation, ADOLESCENCE

Abstract

Under physiological conditions, factors affecting the genetic control of hypothalamic functions are predominant in determining the individual variations in timing of pubertal onset. In pathological conditions, however, these variations can involve different genetic susceptibility and the interaction of environmental factors. The high incidence of precocious puberty in foreign children migrating to Belgium and the detection in their plasma of a long-lasting 1,1,1 -trichloro-2,2-bis(4-chlorophenyl) ethane (DDT) residue suggest the potential role of environmental endocrine disrupting chemicals in the early onset of puberty. This hypothesis was confirmed by experimental data showing that temporary exposure of immature female rats to DDT in vivo results in early onset of puberty. We compared the gene expression profile of hypothalamic hamartoma associated or not with precocious puberty in order to identify gene networks responsible for both hamartoma-dependent sexual precocity and the onset of normal human puberty. In conclusion, pathological variations in the timing of puberty may provide unique information about the interactions of either environmental conditions or genetic susceptibility with the hypothalamic mechanism controlling the onset of sexual maturation, as shown by examples of precocious puberty following exposure to endocrine disrupters or due to hypothalamic hamartoma. [ABSTRACT FROM AUTHOR]

Published

2005

3. The Neurobiology of Female Puberty.

Author

Ojeda, Sergio R., Prevot, Vincent, Heger, Sabine, Lomniczi, Alejandro, Dziedzic, Barbara, and Mungenast, Alison

Subjects

NEUROBIOLOGY, PUBERTY, NEUROGLIA, GROWTH factors, HYPOTHALAMUS

Abstract

In this review, studies are described indicating that the increase in pulsatile release of gonadotropin releasing hormone that signals the initiation of puberty requires both changes in transsynaptic communication and the activation of glia-to-neuron signaling pathways. The major players in the transsynaptic control of puberty are neurons that utilize excitatory and inhibitory amino acids as transmitters. Glial cells employ a combination of trophic factors and small cell-cell signaling molecules to regulate neuronal function and thus promote sexual development. A neuron-to-glia signaling pathway mediated by excitatory amino acids serves to coordinate the simultaneous activation of transsynaptic and glia-to-neuron communication required for the advent of sexual maturity. Copyright © 2003 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2003