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Rhythms in clock proteins in the mouse pars tuberalis depend on MT1 melatonin receptor signalling

Melatonin provides a rhythmic neuroendocrine output, driven by a central circadian clock that encodes information about phase and length of the night. In the hypophyseal pars tuberalis (PT), melatonin is crucial for rhythmic expression of the clock genes mPer1 and mCry1, and melatonin acting in the...

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Published in:	The European journal of neuroscience 2005-12, Vol.22 (11), p.2845-2854
Main Authors:	Jilg, Antje, Moek, Juliane, Weaver, David R., Korf, Horst-Werner, Stehle, Jörg H., Von Gall, Charlotte
Format:	Article
Language:	English
Subjects:	Animals ARNTL Transcription Factors Basic Helix-Loop-Helix Transcription Factors - biosynthesis Basic Helix-Loop-Helix Transcription Factors - genetics BMAL1 Circadian Rhythm - physiology circadian rhythms CLOCK CLOCK Proteins Feedback - physiology Immunohistochemistry In Situ Hybridization mCRY1 mCRY2 Mice Mice, Knockout mPER1 mPER2 Nerve Tissue Proteins - metabolism pituitary Pituitary Gland, Posterior - physiology Receptor, Melatonin, MT1 - genetics Receptor, Melatonin, MT1 - physiology RNA - biosynthesis Signal Transduction - physiology Suprachiasmatic Nucleus - physiology Trans-Activators - genetics Trans-Activators - physiology
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creator	Jilg, Antje Moek, Juliane Weaver, David R. Korf, Horst-Werner Stehle, Jörg H. Von Gall, Charlotte
description	Melatonin provides a rhythmic neuroendocrine output, driven by a central circadian clock that encodes information about phase and length of the night. In the hypophyseal pars tuberalis (PT), melatonin is crucial for rhythmic expression of the clock genes mPer1 and mCry1, and melatonin acting in the PT influences prolactin secretion from the pars distalis. To examine further the possibility of a circadian clockwork functioning in the PT, and the impact of melatonin on this tissue, we assessed circadian clock proteins by immunohistochemistry and compared the diurnal expression in the PT of wild type (WT), and MT1 melatonin receptor‐deficient (MT1–/–) mice. While in the PT of WT mice mPER1, mPER2, and mCRY1 showed a pronounced rhythm, mCRY2, CLOCK, and BMAL1 were constitutively present. Despite reported differences in maximal levels and timing of mCry1, mPer1, and mPer2 RNAs, the corresponding protein levels peaked simultaneously during late day, suggesting a codependency for their stabilization and/or nuclear entry. MT1–/– mice had reduced levels of mPER1, mCRY1, CLOCK and BMAL1, consistent with the earlier reported reduction in mRNA expression of these clock genes. Surprisingly, mPER2‐immunoreaction was constitutively low, although mPer2 was rhythmically expressed in the PT of MT1–/– mice. This suggests that mPER2 is degraded due to the reduced levels of its stabilizing interaction partners mPER1 and mCRY1. The results show that melatonin, acting through the MT1, determines availability of the circadian proteins mPER1, mPER2 and mCRY1 and thus plays a crucial role in regulating rhythmicity in PT cells.
doi_str_mv	10.1111/j.1460-9568.2005.04485.x
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MT1–/– mice had reduced levels of mPER1, mCRY1, CLOCK and BMAL1, consistent with the earlier reported reduction in mRNA expression of these clock genes. Surprisingly, mPER2‐immunoreaction was constitutively low, although mPer2 was rhythmically expressed in the PT of MT1–/– mice. This suggests that mPER2 is degraded due to the reduced levels of its stabilizing interaction partners mPER1 and mCRY1. 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MT1–/– mice had reduced levels of mPER1, mCRY1, CLOCK and BMAL1, consistent with the earlier reported reduction in mRNA expression of these clock genes. Surprisingly, mPER2‐immunoreaction was constitutively low, although mPer2 was rhythmically expressed in the PT of MT1–/– mice. This suggests that mPER2 is degraded due to the reduced levels of its stabilizing interaction partners mPER1 and mCRY1. 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In the hypophyseal pars tuberalis (PT), melatonin is crucial for rhythmic expression of the clock genes mPer1 and mCry1, and melatonin acting in the PT influences prolactin secretion from the pars distalis. To examine further the possibility of a circadian clockwork functioning in the PT, and the impact of melatonin on this tissue, we assessed circadian clock proteins by immunohistochemistry and compared the diurnal expression in the PT of wild type (WT), and MT1 melatonin receptor‐deficient (MT1–/–) mice. While in the PT of WT mice mPER1, mPER2, and mCRY1 showed a pronounced rhythm, mCRY2, CLOCK, and BMAL1 were constitutively present. Despite reported differences in maximal levels and timing of mCry1, mPer1, and mPer2 RNAs, the corresponding protein levels peaked simultaneously during late day, suggesting a codependency for their stabilization and/or nuclear entry. MT1–/– mice had reduced levels of mPER1, mCRY1, CLOCK and BMAL1, consistent with the earlier reported reduction in mRNA expression of these clock genes. Surprisingly, mPER2‐immunoreaction was constitutively low, although mPer2 was rhythmically expressed in the PT of MT1–/– mice. This suggests that mPER2 is degraded due to the reduced levels of its stabilizing interaction partners mPER1 and mCRY1. The results show that melatonin, acting through the MT1, determines availability of the circadian proteins mPER1, mPER2 and mCRY1 and thus plays a crucial role in regulating rhythmicity in PT cells.</abstract><cop>Oxford, UK</cop><pub>Blackwell Publishing Ltd</pub><pmid>16324119</pmid><doi>10.1111/j.1460-9568.2005.04485.x</doi><tpages>10</tpages></addata></record>
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subjects	Animals ARNTL Transcription Factors Basic Helix-Loop-Helix Transcription Factors - biosynthesis Basic Helix-Loop-Helix Transcription Factors - genetics BMAL1 Circadian Rhythm - physiology circadian rhythms CLOCK CLOCK Proteins Feedback - physiology Immunohistochemistry In Situ Hybridization mCRY1 mCRY2 Mice Mice, Knockout mPER1 mPER2 Nerve Tissue Proteins - metabolism pituitary Pituitary Gland, Posterior - physiology Receptor, Melatonin, MT1 - genetics Receptor, Melatonin, MT1 - physiology RNA - biosynthesis Signal Transduction - physiology Suprachiasmatic Nucleus - physiology Trans-Activators - genetics Trans-Activators - physiology
title	Rhythms in clock proteins in the mouse pars tuberalis depend on MT1 melatonin receptor signalling
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