Characterization of the Thermoregulatory Response to Pituitary Adenylate Cyclase-Activating Polypeptide in Rodents

被引:0
作者
Eszter Banki
Eszter Pakai
Balazs Gaszner
Csaba Zsiboras
Andras Czett
Paras Rahul Parkash Bhuddi
Hitoshi Hashimoto
Gabor Toth
Andrea Tamas
Dora Reglodi
Andras Garami
机构
[1] University of Pecs,Department of Anatomy PTE
[2] University of Pecs,MTA “Lendulet” PACAP Research Team, Medical School
[3] Osaka University,Department of Pathophysiology and Gerontology, Medical School
[4] University of Szeged,Graduate School of Pharmacological Sciences
来源
Journal of Molecular Neuroscience | 2014年 / 54卷
关键词
PACAP; Hyperthermia; Thermoregulation; Locomotor activity; Autonomic thermoeffectors;
D O I
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学科分类号
摘要
Administration of the long form (38 amino acids) of pituitary adenylate cyclase-activating polypeptide (PACAP38) into the central nervous system causes hyperthermia, suggesting that PACAP38 plays a role in the regulation of deep body temperature (Tb). In this study, we investigated the thermoregulatory role of PACAP38 in details. First, we infused PACAP38 intracerebroventricularly to rats and measured their Tb and autonomic thermoeffector responses. We found that central PACAP38 infusion caused dose-dependent hyperthermia, which was brought about by increased thermogenesis and tail skin vasoconstriction. Compared to intracerebroventricular administration, systemic (intravenous) infusion of the same dose of PACAP38 caused significantly smaller hyperthermia, indicating a central site of action. We then investigated the thermoregulatory phenotype of mice lacking the Pacap gene (Pacap−/−). Freely moving Pacap−/− mice had higher locomotor activity throughout the day and elevated deep Tb during the light phase. When the Pacap−/− mice were loosely restrained, their metabolic rate and Tb were lower compared to their wild-type littermates. We conclude that PACAP38 causes hyperthermia via activation of the autonomic cold-defense thermoeffectors through central targets. Pacap−/− mice express hyperkinesis, which is presumably a compensatory mechanism, because under restrained conditions, these mice are hypometabolic and hypothermic compared to controls.
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页码:543 / 554
页数:11
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