Selective alteration at the growth‐hormone‐ releasing‐hormone nerve terminals during aging in GHRH‐green fluorescent protein mice

Summary Growth hormone (GH) secretion decreases spontaneously during lifespan, and the resulting GH deficiency participates in aging‐related morbidity. This deficiency appears to involve a defect in the activity of hypothalamic GH‐releasing hormone (GHRH) neurons. Here, we investigated this hypothes...

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Bibliographic Details
Published in:Aging cell 2007-04, Vol.6 (2), p.197-207
Main Authors: Alonso, Gérard, Sanchez‐Hormigo, Angela, Loudes, Catherine, El Yandouzi, Taoufik, Carmignac, Danielle, Faivre‐Bauman, Annie, Recolin, Bénédicte, Epelbaum, Jacques, Robinson, Iain CAF, Mollard, Patrice, Méry, Pierre‐François
Format: Article
Language:English
Subjects:
action potential
Action Potentials
Afferent Pathways - physiology
Animals
autophagy
Cellular Senescence - physiology
Excitatory Postsynaptic Potentials
GABA
glutamate
Green Fluorescent Proteins - analysis
Green Fluorescent Proteins - genetics
Growth Hormone - physiology
Growth Hormone-Releasing Hormone - genetics
Growth Hormone-Releasing Hormone - metabolism
Male
Mice
Mice, Transgenic
Neurons - metabolism
Neurons - physiology
patch clamp
Patch-Clamp Techniques
Presynaptic Terminals - metabolism
Presynaptic Terminals - ultrastructure
synaptic vesicles
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Summary:Summary Growth hormone (GH) secretion decreases spontaneously during lifespan, and the resulting GH deficiency participates in aging‐related morbidity. This deficiency appears to involve a defect in the activity of hypothalamic GH‐releasing hormone (GHRH) neurons. Here, we investigated this hypothesis, as well as the underlying mechanisms, in identified GHRH neurons from adult (∼13 weeks old) and aged (∼100 weeks old) transgenic GHRH‐green fluorescent protein mice, using morphological, biochemical and electrophysiological methods. Surprisingly, the spontaneous action potential frequency was similar in adult and aged GHRH neurons studied in brain slices. This was explained by a lack of change in the intrinsic excitability, and simultaneous increases in both stimulatory glutamatergic‐ and inhibitory GABAergic‐synaptic currents of aged GHRH neurons. Aging did not decrease GHRH and enhanced green fluorescent protein contents, GHRH neuronal number or GHRH‐fibre distribution, but we found a striking enlargement of GHRH‐positive axons, suggesting neuropeptide accumulation. Unlike in adults, autophagic vacuoles were evident in aged GHRH‐axonal profiles using electron microscopy. Thus, GHRH neurons are involved in aging of the GH axis. Aging had a subtle effect at the nerve terminal level in GHRH neurons, contrasting with the view that neuronal aging is accompanied by more widespread damage.
ISSN:1474-9718
1474-9726
DOI:10.1111/j.1474-9726.2007.00276.x