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Altered expression of circadian clock gene, mPer1, in mouse brain and kidney under morphine dependence and withdrawal

Every physiological function in the human body exhibits some form of circadian rhythmicity. Under pathological conditions, however, circadian rhythmicity may be dusrupted. Patients infected with HIV or addicted to drugs of abuse often suffer from sleep disorders and altered circadian rhythms. Early...

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Autores principales: Wang, Xiaojia, Wang, Yueqi, Xin, Haoyang, Liu, Yanyou, Wang, Yuhui, Zheng, Hang, Jiang, Zhou, Wan, Chaomin, Wang, Zhengrong, Ding, Jian M
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2006
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1563481/
https://www.ncbi.nlm.nih.gov/pubmed/16925815
http://dx.doi.org/10.1186/1740-3391-4-9
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author Wang, Xiaojia
Wang, Yueqi
Xin, Haoyang
Liu, Yanyou
Wang, Yuhui
Zheng, Hang
Jiang, Zhou
Wan, Chaomin
Wang, Zhengrong
Ding, Jian M
author_facet Wang, Xiaojia
Wang, Yueqi
Xin, Haoyang
Liu, Yanyou
Wang, Yuhui
Zheng, Hang
Jiang, Zhou
Wan, Chaomin
Wang, Zhengrong
Ding, Jian M
author_sort Wang, Xiaojia
collection PubMed
description Every physiological function in the human body exhibits some form of circadian rhythmicity. Under pathological conditions, however, circadian rhythmicity may be dusrupted. Patients infected with HIV or addicted to drugs of abuse often suffer from sleep disorders and altered circadian rhythms. Early studies in Drosophila suggested that drug seeking behavior might be related to the expression of certain circadian clock genes. Our previous research showed that conditioned place preference with morphine treatment was altered in mice lacking the Period-1 (mPer1) circadian clock gene. Thus, we sought to investigate whether morphine treatment could alter the expression of mPer1, especially in brain regions outside the SCN and in peripheral tissues. Our results using Western blot analysis showed that the mPER1 immunoreactivity exhibited a strong circadian rhythm in the brains of the control (Con), morphine-dependent (MD), and morphine-withdrawal (MW) mice. However, the phase of the circadian rhythm of mPER1 expression in the brains of MD mice significantly differed from that of the Con mice (p < 0.05). In contrast to mPER1 expression in the brain, the circadian rhythm of mPER1 immunoreactivity in the kidneys was abolished after morphine administration, whereas the Con mice maintained robust circadian rhythmicity of mPER1 in the kidney. Therefore, the effect of morphine on the circadian clock gene mPer1 may vary among different organs, resulting in desynchronization of circadian function between the SCN and peripheral organs.
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spelling pubmed-15634812006-09-09 Altered expression of circadian clock gene, mPer1, in mouse brain and kidney under morphine dependence and withdrawal Wang, Xiaojia Wang, Yueqi Xin, Haoyang Liu, Yanyou Wang, Yuhui Zheng, Hang Jiang, Zhou Wan, Chaomin Wang, Zhengrong Ding, Jian M J Circadian Rhythms Research Every physiological function in the human body exhibits some form of circadian rhythmicity. Under pathological conditions, however, circadian rhythmicity may be dusrupted. Patients infected with HIV or addicted to drugs of abuse often suffer from sleep disorders and altered circadian rhythms. Early studies in Drosophila suggested that drug seeking behavior might be related to the expression of certain circadian clock genes. Our previous research showed that conditioned place preference with morphine treatment was altered in mice lacking the Period-1 (mPer1) circadian clock gene. Thus, we sought to investigate whether morphine treatment could alter the expression of mPer1, especially in brain regions outside the SCN and in peripheral tissues. Our results using Western blot analysis showed that the mPER1 immunoreactivity exhibited a strong circadian rhythm in the brains of the control (Con), morphine-dependent (MD), and morphine-withdrawal (MW) mice. However, the phase of the circadian rhythm of mPER1 expression in the brains of MD mice significantly differed from that of the Con mice (p < 0.05). In contrast to mPER1 expression in the brain, the circadian rhythm of mPER1 immunoreactivity in the kidneys was abolished after morphine administration, whereas the Con mice maintained robust circadian rhythmicity of mPER1 in the kidney. Therefore, the effect of morphine on the circadian clock gene mPer1 may vary among different organs, resulting in desynchronization of circadian function between the SCN and peripheral organs. BioMed Central 2006-08-22 /pmc/articles/PMC1563481/ /pubmed/16925815 http://dx.doi.org/10.1186/1740-3391-4-9 Text en Copyright © 2006 Wang et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Wang, Xiaojia
Wang, Yueqi
Xin, Haoyang
Liu, Yanyou
Wang, Yuhui
Zheng, Hang
Jiang, Zhou
Wan, Chaomin
Wang, Zhengrong
Ding, Jian M
Altered expression of circadian clock gene, mPer1, in mouse brain and kidney under morphine dependence and withdrawal
title Altered expression of circadian clock gene, mPer1, in mouse brain and kidney under morphine dependence and withdrawal
title_full Altered expression of circadian clock gene, mPer1, in mouse brain and kidney under morphine dependence and withdrawal
title_fullStr Altered expression of circadian clock gene, mPer1, in mouse brain and kidney under morphine dependence and withdrawal
title_full_unstemmed Altered expression of circadian clock gene, mPer1, in mouse brain and kidney under morphine dependence and withdrawal
title_short Altered expression of circadian clock gene, mPer1, in mouse brain and kidney under morphine dependence and withdrawal
title_sort altered expression of circadian clock gene, mper1, in mouse brain and kidney under morphine dependence and withdrawal
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1563481/
https://www.ncbi.nlm.nih.gov/pubmed/16925815
http://dx.doi.org/10.1186/1740-3391-4-9
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