2.1.4 Parts of the brain affected: Hypothalamus

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Retinoid receptor expression and metabolism in the hypothalamus

Components of the metabolic pathway for retinoids have been identified in adult brain tissues, suggesting that all-trans-retinoic acid (ATRA) can be synthesized in discrete regions of the brain. The distribution of retinoid receptor proteins in the adult nervous system is different from that seen during development; and suggests that retinoid signalling is likely to have a physiological role in adult cortex, amygdala, hypothalamus, hippocampus, striatum and associated brain regions [1].

The retinoid X receptor and retinoid signaling in the neuroendocrine hypothalamus associated with adaptations to season and body-weight

Siberian hamsters were maintained in long or short photoperiods that generate physiological states of obesity or leanness. Microarray expression analysis first identified CRBP1 as a photoperiod-responsive gene, and then further studies using in situ hybridization and immunocytochemistry revealed that expression levels of several related retinoid-signaling genes were modulated in response to photoperiod changes. Genes of the retinoid-signaling pathway, encoding nuclear receptors (RXR/RAR) and retinoid binding proteins (CRBP1 and CRABP2) are photoperiodically regulated in the dorsal tuberomamillary nucleus (DTM): Their expression is significantly lower in short photoperiods and parallels body weight decreases. Studies in pinealectomized hamsters confirm that the pineal melatonin rhythm is necessary for these seasonal changes, and studies in testosterone-treated hamsters reveal that these changes in gene expression are not the secondary consequence of photoperiod-induced changes in steroid levels. Comparative studies using Syrian hamsters, which show divergent seasonal body weight responses to Siberian hamsters when exposed to short photoperiods, showed a distinct pattern of changes in retinoid gene expression in the DTM in response to a change in photoperiod. The DTM may be an important integrating center for photoperiodic control of seasonal physiology and suggest that the changes in retinoid X receptor gamma expression may be associated with seasonal changes in body weight and energy metabolism [2].

Retinoic acid involved in rat GnRH release in the hypothalamus

Insulin signaling in the hypothalamus

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References:

[1] Lane MA, Bailey SJ. Role of retinoid signalling in the adult brain. (2005) Prog Neurobiol. Mar;75(4):275-93.
[2] Ross AW, Webster CA, Mercer JG, Moar KM, Ebling FJ, Schuhler S, Barrett P, Morgan PJ.
Photoperiodic regulation of hypothalamic retinoid signaling: association of retinoid X receptor gamma with body weight.
(2004) Endocrinology. Jan;145(1):13-20.
www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=pubmed&dopt=Abstract&list_uids=14681212

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Endocrinology. 2005 Jul 7; [Epub ahead of print] Related Articles, Links


Consumption of a fat-rich diet activates a pro-inflammatory response and induces insulin resistance in the hypothalamus.

De Souza CT, Araujo EP, Bordin S, Ashimine R, Zollner RL, Boshero AC, Saad MJ, Velloso LA.

Departments of Internal Medicine and Physiology and Biophysics, State University of Campinas, 13084-970, Campinas - SP; Department of Physiology and Biophysics, University of Sao Paulo, 05508-900, Sao Paulo - SP, Brazil.

Obesity has reached epidemic proportions in several regions of the world. General changes in lifestyle, including consumption of fat-rich food, are among the most important factors leading to an unprecedented increase in the prevalence of this disease. Weight gain results from an imbalance between caloric intake and energy expenditure. Both of these parameters are under the tight control of specialized neurons of the hypothalamus that respond to peripheral anorexigenic and adipostatic signals carried by leptin and insulin. Here we show, by macroarray analysis, that high-fat feeding (hyperlipidic diet - HL) induces the expression of several pro-inflammatory cytokines and inflammatory responsive proteins in hypothalamus. This phenomenon is accompanied by increased activation of JNK and NFkappaB. In addition, HL feeding leads to impaired functional and molecular activation of the insulin-signaling pathway, which is paralleled by increased serine phosphorylation of the insulin receptor and IRS-2. Intracerebroventricular (icv) treatment of HL rats with a specific inhibitor of JNK (SP600125) restores insulin signaling and leads to a reduced caloric intake and weight loss. We conclude that HL feeding induces a local pro-inflammatory status in the hypothalamus, which results in impaired anorexigenic insulin signaling.

PMID: 16002529 [PubMed - as supplied by publisher]

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Brain Res Mol Brain Res. 1998 Feb;54(1):74-84. Related Articles, Links


Retinoic acid regulates gonadotropin-releasing hormone (GnRH) release and gene expression in the rat hypothalamic fragments and GT1-1 neuronal cells in vitro.

Cho S, Cho H, Geum D, Kim K.

Department of Molecular Biology, Seoul National University, South Korea.

The present study attempts to examine the possible involvement of retinoic acid (RA) in the regulation of gonadotropin-releasing hormone (GnRH) release and gene expression in the rat hypothalamic fragments and GT1-1 neuronal cells in vitro. During a short-term period (2h), RA (0.01-1 microM) increased GnRH release in a dose-related manner. Time-course experiments showed that RA rapidly increased GnRH release by 30 min in both cells. RA-induced GnRH release was slowly attenuated in the next incubation period in hypothalamic fragments, but rapidly returned to control levels in GT-1 cells. In hypothalamic fragments, GnRH mRNA levels decreased, but in GT1-1 cells, no change in GnRH mRNA levels was observed. We then extended the incubation time to see any changes in GnRH mRNA levels by RA in GT1-1 cells. In a long term (up to 48 h), RA increased GnRH mRNA levels in a dose- and time-related manner. Significant increase in GnRH mRNA levels by RA (at higher than 10 nM) was observed within 12h. Transient transfection experiments with a luciferase reporter vector containing more than 3 kb of the rat GnRH 5'-flanking region (-3002 to +88) revealed that RA also increased the rat GnRH promoter activity in a similar dose-and time-dependent manner, suggesting that increases in GnRH mRNA levels are attributable, at least in part, to the enhanced gene transcription. The promoter analysis with the 5'-deletional constructs demonstrated that cis-elements responsible for the RA action may reside within -1640/-1438 of the rat GnRH promoter, where multiple direct or palindromic arrangements of the AGGTCA-related sequences exist. We also showed that GT1-1 cells as well as the hypothalamic tissues express mRNA for multiple subtypes of retinoid receptors, and that reporter plasmids with three copies of the strong retinoic acid response element (RARE) were activated by 80 folds upon treatment with RA in GT1-1 cells, suggesting that retinoid receptors in GT1-1 cells are functional. Taken together, the present study strongly suggests that RA is an important regulator of the GnRH neurons.

PMID: 9526050 [PubMed - indexed for MEDLINE]

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ISOTRETINOIN and depression risk : suggestion to reproduct study about this hypothesis, in order to infirm or confirm it.

cf mail sent to pharmaco-epidemiologics searchers :
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- ALL THIS SITE IS IN THIS PDF : Last version of "State of the knowledge about the side effects of Roaccutane
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