Circadian clock characteristics are altered in human thyroid malignant nodules
T Mannic, P Meyer, F Triponez… - The Journal of …, 2013 - academic.oup.com
The Journal of Clinical Endocrinology & Metabolism, 2013•academic.oup.com
Context: The circadian clock represents the body's molecular time-keeping system. Recent
findings revealed strong changes of clock gene expression in various types of human
cancers. Objective: Due to emerging evidence on the connection between the circadian
oscillator, cell cycle, and oncogenic transformation, we aimed to characterize the circadian
clockwork in human benign and malignant thyroid nodules. Design: Clock transcript levels
were assessed by quantitative RT-PCR in thyroid tissues. To provide molecular …
findings revealed strong changes of clock gene expression in various types of human
cancers. Objective: Due to emerging evidence on the connection between the circadian
oscillator, cell cycle, and oncogenic transformation, we aimed to characterize the circadian
clockwork in human benign and malignant thyroid nodules. Design: Clock transcript levels
were assessed by quantitative RT-PCR in thyroid tissues. To provide molecular …
Context
The circadian clock represents the body's molecular time-keeping system. Recent findings revealed strong changes of clock gene expression in various types of human cancers.
Objective
Due to emerging evidence on the connection between the circadian oscillator, cell cycle, and oncogenic transformation, we aimed to characterize the circadian clockwork in human benign and malignant thyroid nodules.
Design
Clock transcript levels were assessed by quantitative RT-PCR in thyroid tissues. To provide molecular characteristics of human thyroid clockwork, primary thyrocytes established from normal or nodular thyroid tissue biopsies were subjected to in vitro synchronization with subsequent clock gene expression analysis by circadian bioluminescence reporter assay and by quantitative RT-PCR.
Results
The expression levels of the Bmal1 were up-regulated in tissue samples of follicular thyroid carcinoma (FTC), and in papillary thyroid carcinoma (PTC), as compared with normal thyroid and benign nodules, whereas Cry2 was down-regulated in FTC and PTC. Human thyrocytes derived from normal thyroid tissue exhibited high-amplitude circadian oscillations of Bmal1-luciferase reporter expression and endogenous clock transcripts. Thyrocytes established from FTC and PTC exhibited clock transcript oscillations similar to those of normal thyroid tissue and benign nodules (except for Per2 altered in PTC), whereas cells derived from poorly differentiated thyroid carcinoma exhibited altered circadian oscillations.
Conclusions
This is the first study demonstrating a molecular makeup of the human thyroid circadian clock. Characterization of the thyroid clock machinery alterations upon thyroid nodule malignant transformation contributes to understanding the connections between circadian clocks and oncogenic transformation. Moreover, it might help in improving the thyroid nodule preoperative diagnostics.
Oxford University Press
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