Your search keyword '"Qing-Jun Meng"' showing total 81 results

1. Circadian Disruption Primes Myofibroblasts for Accelerated Activation as a Mechanism Underpinning Fibrotic Progression in Non-Alcoholic Fatty Liver Disease

Author

Hanley, Elliot Jokl, Jessica Llewellyn, Kara Simpson, Oluwatobi Adegboye, James Pritchett, Leo Zeef, Ian Donaldson, Varinder S. Athwal, Huw Purssell, Oliver Street, Lucy Bennett, Indra Neil Guha, Neil A. Hanley, Qing-Jun Meng, and Karen Piper

Subjects

circadian rhythm, CLOCK, fibrosis, NAFLD, liver disease

Abstract

Circadian rhythm governs many aspects of liver physiology and its disruption exacerbates chronic disease. CLOCKΔ19 mice disrupted circadian rhythm and spontaneously developed obesity and metabolic syndrome, a phenotype that parallels the progression of non-alcoholic fatty liver disease (NAFLD). NAFLD represents an increasing health burden with an estimated incidence of around 25% and is associated with an increased risk of progression towards inflammation, fibrosis and carcinomas. Excessive extracellular matrix deposition (fibrosis) is the key driver of chronic disease progression. However, little attention was paid to the impact of disrupted circadian rhythm in hepatic stellate cells (HSCs) which are the primary mediator of fibrotic ECM deposition. Here, we showed in vitro and in vivo that liver fibrosis is significantly increased when circadian rhythm is disrupted by CLOCK mutation. Quiescent HSCs from CLOCKΔ19 mice showed higher expression of RhoGDI pathway components and accelerated activation. Genes altered in this primed CLOCKΔ19 qHSC state may provide biomarkers for early liver disease detection, and include AOC3, which correlated with disease severity in patient serum samples. Integration of CLOCKΔ19 microarray data with ATAC-seq data from WT qHSCs suggested a potential CLOCK regulome promoting a quiescent state and downregulating genes involved in cell projection assembly. CLOCKΔ19 mice showed higher baseline COL1 deposition and significantly worse fibrotic injury after CCl4 treatment. Our data demonstrate that disruption to circadian rhythm primes HSCs towards an accelerated fibrotic response which worsens liver disease.

Published

2023

2. Subtype-specific circadian clock dysregulation modulates breast cancer biology, invasiveness, and prognosis

Author

Jan A Hammarlund, Shi-Yang Li, Gang Wu, Jia-wen Lian, Sacha J Howell, Rob Clarke, Antony Adamson, Cátia F. Gonçalves, John B Hogenesch, Qing-Jun Meng, and Ron C Anafi

Subjects

Article

Abstract

SummaryStudies in shift workers and model organisms link circadian disruption to breast cancer. However, molecular rhythms in non-cancerous and cancerous human breast tissues are largely unknown. We reconstructed rhythms informatically, integrating locally collected, time-stamped biopsies with public datasets. For non-cancerous tissue, the inferred order of core-circadian genes matches established physiology. Inflammatory, epithelial-mesenchymal transition (EMT), and estrogen responsiveness pathways show circadian modulation. Among tumors, clock correlation analysis demonstrates subtype-specific changes in circadian organization. Luminal A organoids and informatic ordering of Luminal A samples exhibit continued, albeit disrupted rhythms. However, CYCLOPS magnitude, a measure of global rhythm strength, varied widely among Luminal A samples. Cycling of EMT pathway genes was markedly increased in high-magnitude Luminal A tumors. Patients with high-magnitude tumors had reduced 5-year survival. Correspondingly, 3D Luminal A cultures show reduced invasion following molecular clock disruption. This study links subtype-specific circadian disruption in breast cancer to EMT, metastatic potential, and prognosis.

Published

2023

3. Tick Tock, the Cartilage Clock

Author

Natalie Rogers and Qing-Jun Meng

Subjects

Rheumatology, Biomedical Engineering, Orthopedics and Sports Medicine

Published

2023

4. The clock transcription factor BMAL1 is a key regulator of extracellular matrix homeostasis and cell fate in the intervertebral disc

Author

Michal Dudek, Honor Morris, Natalie Rogers, Dharshika RJ Pathiranage, Danny Chan, Karl E Kadler, Judith Hoyland, and Qing-Jun Meng

Abstract

The circadian clock in mammals temporally coordinates physiological and behavioural processes to anticipate daily rhythmic changes in their environment. Chronic disruption to circadian rhythms (e.g., through ageing or shift work) is thought to contribute to a multitude of diseases, including degeneration of the musculoskeletal system. The intervertebral disc (IVD) in the spine contains circadian clocks which control ∼6% of the transcriptome in a rhythmic manner, including key genes involved in extracellular matrix (ECM) homeostasis. However, it remains largely unknown to what extent the local IVD molecular clock is required to drive rhythmic gene transcription and IVD physiology. In this work, we identified profound age-related changes of ECM microarchitecture and an endochondral ossification-like phenotype in the annulus fibrosus (AF) region of the IVD in theCol2a1-Bmal1knockout mice. Circadian time series RNA-Seq of the whole IVD inBmal1knockout revealed loss of circadian patterns in gene expression, with an unexpected emergence of 12-hour ultradian rhythms, including FOXO transcription factors. Further RNA sequencing of the AF tissue identified region-specific changes in gene expression, evidencing a loss of AF phenotype markers and a dysregulation of ECM and FOXO pathways inBmal1knockout mice. Consistent with an up-regulation of FOXO1 mRNA and protein levels inBmal1knockout IVDs, inhibition of FOXO1 in AF cells suppressed their osteogenic differentiation. Collectively, these data highlight the importance of the local molecular clock mechanism in the maintenance of the cell fate and ECM homeostasis of the IVD. Further studies may identify potential new molecular targets for alleviating IVD degeneration.

Published

2023

5. Circadian time series proteomics reveals daily dynamics in cartilage physiology

Author

Venkatesh Mallikarjun, Dharshika Pathiranage, Qing-Jun Meng, John F. Bateman, Constanza Angelucci, Ping Wang, Shireen R. Lamandé, Judith A. Hoyland, Karl E. Kadler, Michal Dudek, Craig Lawless, Raymond P. Boot-Handford, and Joe Swift

Subjects

0301 basic medicine, Proteomics, Cartilage, Articular, Circadian clock, Biomedical Engineering, Osteoarthritis, Biology, Article, 03 medical and health sciences, 0302 clinical medicine, Chondrocytes, Rheumatology, Tandem Mass Spectrometry, Circadian Clocks, Gene expression, medicine, Animals, Orthopedics and Sports Medicine, Circadian rhythm, RNA, Messenger, 030203 arthritis & rheumatology, Mice, Knockout, Mice, Inbred BALB C, Cartilage, Femur Head, Period Circadian Proteins, medicine.disease, Cell biology, Biomarker (cell), CTGF, 030104 developmental biology, medicine.anatomical_structure, Chromatography, Liquid

Abstract

Summary Objective Cartilage in joints such as the hip and knee experiences repeated phases of heavy loading and low load recovery during the 24-h day/night cycle. Our previous work has shown 24 h rhythmic changes in gene expression at transcript level between night and day in wild type mouse cartilage which is lost in a circadian clock knock-out mouse model. However, it remains unknown to what extent circadian rhythms also regulate protein level gene expression in this matrix rich tissue. Methods We investigated daily changes of protein abundance in mouse femoral head articular cartilage by performing a 48-h time-series LC-MS/MS analysis. Results Out of the 1,177 proteins we identified across all time points, 145 proteins showed rhythmic changes in their abundance within the femoral head cartilage. Among these were molecules that have been implicated in key cartilage functions, including CTGF, MATN1, PAI-1 and PLOD1 & 2. Pathway analysis revealed that protein synthesis, cytoskeleton and glucose metabolism exhibited time-of-day dependent functions. Analysis of published cartilage proteomics datasets revealed that a significant portion of rhythmic proteins were dysregulated in osteoarthritis and/or ageing. Conclusions Our circadian proteomics study reveals that articular cartilage is a much more dynamic tissue than previously thought, with chondrocytes driving circadian rhythms not only in gene transcription but also in protein abundance. Our results clearly call for the consideration of circadian timing mechanisms not only in cartilage biology, but also in the pathogenesis, treatment strategies and biomarker detection in osteoarthritis.

Published

2021

6. Synthetic gene circuits for preventing disruption of the circadian clock due to interleukin-1–induced inflammation

Author

Lara Pferdehirt, Anna R. Damato, Michal Dudek, Qing-Jun Meng, Erik D. Herzog, and Farshid Guilak

Subjects

Cartilage, Articular, Inflammation, Mice, Multidisciplinary, Circadian Clocks, Induced Pluripotent Stem Cells, Genes, Synthetic, Animals, Circadian Rhythm, Interleukin-1

Abstract

The circadian clock regulates tissue homeostasis through temporal control of tissue-specific clock-controlled genes. In articular cartilage, disruptions in the circadian clock are linked to a procatabolic state. In the presence of inflammation, the cartilage circadian clock is disrupted, which further contributes to the pathogenesis of diseases such as osteoarthritis. Using synthetic biology and tissue engineering, we developed and tested genetically engineered cartilage from murine induced pluripotent stem cells (miPSCs) capable of preserving the circadian clock in the presence of inflammation. We found that circadian rhythms arise following chondrogenic differentiation of miPSCs. Exposure of tissue-engineered cartilage to the inflammatory cytokine interleukin-1 (IL-1) disrupted circadian rhythms and degraded the cartilage matrix. All three inflammation-resistant approaches showed protection against IL-1–induced degradation and loss of circadian rhythms. These synthetic gene circuits reveal a unique approach to support daily rhythms in cartilage and provide a strategy for creating cell-based therapies to preserve the circadian clock.

Published

2022

7. The dynamic kidney matrisome - is the circadian clock in control?

Author

Rebecca Preston, Qing-Jun Meng, and Rachel Lennon

Subjects

Mammals, Mice, Basement membrane, Circadian Clocks, Glomerulus, Animals, Homeostasis, Extracellular matrix, Circadian clock, Kidney, Molecular Biology, Circadian Rhythm, Extracellular Matrix

Abstract

The circadian clock network in mammals is responsible for the temporal coordination of numerous physiological processes that are necessary for homeostasis. Peripheral tissues demonstrate circadian rhythmicity and dysfunction of core clock components has been implicated in the pathogenesis of diseases that are characterized by abnormal extracellular matrix, such as fibrosis (too much disorganized matrix) and tissue breakdown (too little matrix). Kidney disease is characterized by proteinuria, which along with the rate of filtration, displays robust circadian oscillation. Clinical observation and mouse studies suggest the presence of 24 h kidney clocks responsible for circadian oscillation in kidney function. Recent experimental evidence has also revealed that cell-matrix interactions and the biomechanical properties of extracellular matrix have key roles in regulating peripheral circadian clocks and this mechanism appears to be cell- and tissue-type specific. Thus, establishing a temporally resolved kidney matrisome may provide a useful tool for studying the two-way interactions between the extracellular matrix and the intracellular time-keeping mechanisms in this critical niche tissue. This review summarizes the latest genetic and biochemical evidence linking kidney physiology and disease to the circadian system with a particular focus on the extracellular matrix. We also review the experimental approaches and methodologies required to dissect the roles of circadian pathways in specific tissues and outline the translational aspects of circadian biology, including how circadian medicine could be used for the treatment of kidney disease.

Published

2022

8. Mmp14 is required for matrisome homeostasis and circadian rhythm in fibroblasts

Author

Ching-Yan Chloé Yeung, Richa Garva, Adam Pickard, Yinhui Lu, Venkatesh Mallikarjun, Joe Swift, Susan H. Taylor, Jyoti Rai, David R. Eyre, Mayank Chaturvedi, Yoshifumi Itoh, Qing-Jun Meng, Cornelia Mauch, Paola Zigrino, and Karl E. Kadler

Abstract

The circadian clock in tendon regulates the daily rhythmic synthesis of collagen-I and the appearance and disappearance of small-diameter collagen fibrils in the extracellular matrix. How the fibrils are assembled and removed is not fully understood. Here, we first showed that the collagenase, membrane type I-matrix metalloproteinase (MT1-MMP, encoded byMmp14), is regulated by the circadian clock in postnatal mouse tendon. Next, we generated tamoxifen-inducedCol1a2-Cre-ERT2::Mmp14KO mice (Mmp14conditional knockout (CKO)). The CKO mice developed hind limb dorsiflexion and thickened tendons, which accumulated narrow-diameter collagen fibrils causing ultrastructural disorganization. Mass spectrometry of control tendons identified 1195 proteins of which 212 showed time-dependent abundance. InMmp14CKO mice 19 proteins had reversed temporal abundance and 176 proteins lost time dependency. Among these, the collagen crosslinking enzymes lysyl oxidase-like 1 (LOXL1) and lysyl hydroxylase 1 (LH1; encoded byPlod2) were elevated and had lost time-dependent regulation. High-pressure chromatography confirmed elevated levels of hydroxylysine aldehyde (pyridinoline) crosslinking of collagen in CKO tendons. As a result, collagen-I was refractory to extraction. We also showed that CRISPR-Cas9 deletion ofMmp14from cultured fibroblasts resulted in loss of circadian clock rhythmicity of period 2 (PER2), and recombinant MT1-MMP was highly effective at cleaving soluble collagen-I but less effective at cleaving collagen pre-assembled into fibrils. In conclusion, our study shows that circadian clock-regulatedMmp14controls the rhythmic synthesis of small diameter collagen fibrils, regulates collagen crosslinking, and its absence disrupts the circadian clock and matrisome in tendon fibroblasts.

Published

2022

9. Circadian control of the secretory pathway maintains collagen homeostasis

Author

Antony Adamson, Joan Chang, David F. Holmes, Qing-Jun Meng, Joe Swift, Oliver E. Jensen, Ching-Yan Chloé Yeung, Adam Pickard, Venkatesh Mallikarjun, Karl E. Kadler, Tom Shearer, Ben Calverley, Helena Raymond-Hayling, Yinhui Lu, and Richa Garva

Subjects

Pyrrolidines, Transgene, Circadian clock, Carbazoles, Vesicular Transport Proteins, Mice, Transgenic, Thiophenes, 03 medical and health sciences, 0302 clinical medicine, Circadian Clocks, Collagen network, Animals, Homeostasis, Circadian rhythm, Secretory pathway, 030304 developmental biology, Sulfonamides, 0303 health sciences, Secretory Pathway, Chemistry, Endoplasmic reticulum, Aryl Hydrocarbon Receptor Nuclear Translocator, Cell Biology, Cyclic Nucleotide Phosphodiesterases, Type 4, Extracellular Matrix, Cell biology, Procollagen peptidase, 030220 oncology & carcinogenesis, Collagen, SEC Translocation Channels

Abstract

Collagen is the most abundant secreted protein in vertebrates and persists throughout life without renewal. The permanency of collagen networks contrasts with both the continued synthesis of collagen throughout adulthood and the conventional transcriptional/translational homeostatic mechanisms that replace damaged proteins with new copies. Here, we show circadian clock regulation of endoplasmic reticulum-to-plasma membrane procollagen transport by the sequential rhythmic expression of SEC61, TANGO1, PDE4D and VPS33B. The result is nocturnal procollagen synthesis and daytime collagen fibril assembly in mice. Rhythmic collagen degradation by CTSK maintains collagen homeostasis. This circadian cycle of collagen synthesis and degradation affects a pool of newly synthesized collagen, while maintaining the persistent collagen network. Disabling the circadian clock causes abnormal collagen fibrils and collagen accumulation, which are reduced in vitro by the NR1D1 and CRY1/2 agonists SR9009 and KL001, respectively. In conclusion, our study has identified a circadian clock mechanism of protein homeostasis wherein a sacrificial pool of collagen maintains tissue function.

Published

2020

10. Quantification of protein abundance and interaction defines a mechanism for operation of the circadian clock

Author

James S Bagnall, Alex A Koch, Nicola J Smyllie, Nicola Begley, Antony D Adamson, Jennifer L Fribourgh, David G Spiller, Qing-Jun Meng, Carrie L Partch, Korbinian Strimmer, Thomas A House, Michael H Hastings, and Andrew SI Loudon

Subjects

chromosomes, endocrine system, Mouse, Circadian Clocks/genetics, Lydia Becker Institute, ARNTL Transcription Factors/genetics, CLOCK Proteins, General Biochemistry, Genetics and Molecular Biology, live-cell imaging, modelling, Circadian Clocks, ResearchInstitutes_Networks_Beacons/lydia_becker_institute_of_immunology_and_inflammation, cell biology, single cell quantification, Genetics, Animals, DNA binding, CLOCK Proteins/genetics, Thomas Ashton Institute, Mammals, General Immunology and Microbiology, Mammals/metabolism, General Neuroscience, ARNTL Transcription Factors, General Medicine, ResearchInstitutes_Networks_Beacons/thomas_ashton_institute, Circadian Rhythm, circadian, FRAP, gene expression, Generic health relevance, Biochemistry and Cell Biology, Circadian Rhythm/genetics, Sleep Research

Abstract

The mammalian circadian clock exerts control of daily gene expression through cycles of DNA binding. Here, we develop a quantitative model of how a finite pool of BMAL1 protein can regulate thousands of target sites over daily time scales. We used quantitative imaging to track dynamic changes in endogenous labelled proteins across peripheral tissues and the SCN. We determine the contribution of multiple rhythmic processes coordinating BMAL1 DNA binding, including cycling molecular abundance, binding affinities, and repression. We find nuclear BMAL1 concentration determines corresponding CLOCK through heterodimerisation and define a DNA residence time of this complex. Repression of CLOCK:BMAL1 is achieved through rhythmic changes to BMAL1:CRY1 association and high-affinity interactions between PER2:CRY1 which mediates CLOCK:BMAL1 displacement from DNA. Finally, stochastic modelling reveals a dual role for PER:CRY complexes in which increasing concentrations of PER2:CRY1 promotes removal of BMAL1:CLOCK from genes consequently enhancing ability to move to new target sites.

Published

2022

11. Author response: Quantification of protein abundance and interaction defines a mechanism for operation of the circadian clock

Author

James S Bagnall, Alex A Koch, Nicola J Smyllie, Nicola Begley, Antony D Adamson, Jennifer L Fribourgh, David G Spiller, Qing-Jun Meng, Carrie L Partch, Korbinian Strimmer, Thomas A House, Michael H Hastings, and Andrew SI Loudon

Published

2022

12. Highly sensitive detection of low-concentration sodium chloride solutions based on polymeric nanofilms coated long period fiber grating

Author

Qiu-Shun, Li, Yan, Yang, Yong-Dong, Du, Lei, Cai, Yao-Hong, Ma, Jun-Hui, Yang, Mingyu, Li, Qing-Jun, Meng, Qing-Ai, Liu, and Wen-Fei, Dong

Subjects

Analytical Chemistry

Abstract

Long period fiber gratings (LPFGs) have special advantages in the detection of salt concentrations due to small volume, corrosion resistance and immunity to electromagnetic interference. However, it is very difficult to distinguish low-concentration salt solutions with usual LPFGs owing to the poor sensitivity. In this paper, the detection capability of the LPFG to low-concentration salt solutions was significantly improved by assembling salt-containing poly (diallyldimethylammonium chloride) (PDDA) and salt-containing poly (sodium-p-styrenesulfonate) (PSS). Experimental results showed that, the responsive wavelength range of the LPFG was remarkably broadened in low-concentration salt solutions after assembling nanofilms. The suitable detection range of the PDDA/PSS films coated LPFG for salt concentrations was 0-3%. In such a range, the average refractive index sensitivity and the average salinity sensitivity of the LPFG was as high as 29545.9 nm/RIU and 52.2 nm/% respectively. Compared with the LPFG without nanofilms, the discrimination ability of the PDDA/PSS films coated LPFG to 0-3% salt solutions increased by 568 times. The analysis demonstrated that PDDA and salt in the assembly solutions played a pivotal role in the above effects. The proposed sensor has extensive application prospects in the monitoring of salt concentration in many fields such as seawater, food processing, fermentation process, etc.

Published

2023

13. Directed differentiation of hPSCs through a simplified lateral plate mesoderm protocol for generation of articular cartilage progenitors

Author

Christopher A. Smith, Paul A. Humphreys, Mark A. Naven, Steven Woods, Fabrizio E. Mancini, Julieta O’Flaherty, Qing-Jun Meng, and Susan J. Kimber

Subjects

Cartilage, Articular, Pluripotent Stem Cells, Mesoderm, Multidisciplinary, Osteoarthritis, Humans, Cell Differentiation, Chondrogenesis

Abstract

Developmentally, the articular joints are derived from lateral plate (LP) mesoderm. However, no study has produced both LP derived prechondrocytes and preosteoblasts from human pluripotent stem cells (hPSC) through a common progenitor in a chemically defined manner. Differentiation of hPSCs through the authentic route, via an LP-osteochondral progenitor (OCP), may aid understanding of human cartilage development and the generation of effective cell therapies for osteoarthritis. We refined our existing chondrogenic protocol, incorporating knowledge from development and other studies to produce a LP-OCP from which prechondrocyte- and preosteoblast-like cells can be generated. Results show the formation of an OCP, which can be further driven to prechondrocytes and preosteoblasts. Prechondrocytes cultured in pellets produced cartilage like matrix with lacunae and superficial flattened cells expressing lubricin. Additionally, preosteoblasts were able to generate a mineralised structure. This protocol can therefore be used to investigate further cartilage development and in the development of joint cartilage for potential treatments.

Published

2023

14. Mechanical loading and hyperosmolarity as a daily resetting cue for skeletal circadian clocks

Author

Dong Wang, Judith A. Hoyland, Craig Lawless, Liu Yang, Cátia F. Gonçalves, Farshid Guilak, Dharshika Pathiranage, Qing-Jun Meng, Michal Dudek, and Zhuojing Luo

Subjects

CLOCK, Clock phase, Rhythm, Flexibility (anatomy), medicine.anatomical_structure, Osmotic concentration, Circadian clock, medicine, Circadian rhythm, Biology, Neuroscience, Sensory cue

Abstract

In mammals, temporally coordinated daily rhythms of behaviour and physiology are generated by a multi-oscillatory circadian system, entrained through cyclic environmental cues (e.g. light). Presence of niche-dependent physiological time cues has been proposed, which would allow local tissues flexibility of adopting a different phase relationship if circumstances require. Up till now, such tissue-unique stimuli have remained elusive. Here we show that cycles of mechanical loading and osmotic stimuli within physiological range drive rhythmic expression of clock genes and reset clock phase and amplitude in cartilage and intervertebral disc tissues. Hyperosmolarity (and not hypo-osmolarity) resets clocks in young and ageing skeletal tissues through mTORC2-AKT-GSK3β pathway, leading to genome-wide induction of rhythmic genes. These results suggest diurnal patterns of mechanical loading and consequent daily surges in extracellular osmolarity as a bona fide tissue niche-specific time cue to maintain skeletal circadian rhythms in sync. One-Sentence Summary Circadian clocks in aneural skeletal tissues sense the passage of time through rhythmic patterns of loading and osmolarity.

Published

2021

15. Quantification of circadian interactions and protein abundance defines a mechanism for operational stability of the circadian clock

Author

Michael H. Hastings, Korbinian Strimmer, Andrew S. I. Loudon, Nicola J. Smyllie, Alex A. Koch, Thomas House, Nicola Begley, Carrie L. Partch, Antony Adamson, David G. Spiller, Qing-Jun Meng, Jennifer L. Fribourgh, and James Bagnall

Subjects

PER2, endocrine system, chemistry.chemical_compound, Chemistry, Gene expression, Circadian clock, Circadian rhythm, Gene, Psychological repression, DNA, Atomic clock, Cell biology

Abstract

The mammalian circadian clock exerts substantial control of daily gene expression through cycles of DNA binding. Understanding of mechanisms driving the circadian clock is hampered by lack of quantitative data, without which predictive mathematical models cannot be developed. Here we develop a quantitative understanding of how a finite pool of BMAL1 protein can regulate thousands of target sites over daily time scales. We have used fluorescent correlation spectroscopy (FCS) to track dynamic changes in CRISPR-modified fluorophore-tagged proteins in time and space in single cells across SCN and peripheral tissues. We determine the contribution of multiple rhythmic processes in coordinating BMAL1 DNA binding, including the roles of cycling molecular abundance, binding affinities and two repressive modes of action. We find that nuclear BMAL1 protein numbers determine corresponding nuclear CLOCK concentrations through heterodimerization and define a DNA residence time of 2.6 seconds for this complex. Repression of CLOCK:BMAL1 is in part achieved through rhythmic changes to BMAL1:CRY1 affinity as well as a high affinity interaction between PER2:CRY1 which mediates CLOCK:BMAL1 displacement from DNA. Finally, stochastic modelling of these data reveals a dual role for PER:CRY complexes in which increasing concentrations of PER2:CRY1 promotes removal of BMAL1:CLOCK from genes consequently enhancing ability to move to new target sites.

Published

2021

16. Restoring the dampened expression of the core clock molecule BMAL1 protects against compression-induced intervertebral disc degeneration

Author

Dong Wang, Pandi Peng, Michal Dudek, Xueyu Hu, Xiaolong Xu, Qiliang Shang, Di Wang, Haoruo Jia, Han Wang, Bo Gao, Chao Zheng, Jianxin Mao, Chu Gao, Xin He, Pengzhen Cheng, Huanbo Wang, Jianmin Zheng, Judith A. Hoyland, Qing-Jun Meng, Zhuojing Luo, and Liu Yang

Subjects

endocrine system, Histology, Physiology, Endocrinology, Diabetes and Metabolism

Abstract

The circadian clock participates in maintaining homeostasis in peripheral tissues, including intervertebral discs (IVDs). Abnormal mechanical loading is a known risk factor for intervertebral disc degeneration (IDD). Based on the rhythmic daily loading pattern of rest and activity, we hypothesized that abnormal mechanical loading could dampen the IVD clock, contributing to IDD. Here, we investigated the effects of abnormal loading on the IVD clock and aimed to inhibit compression-induced IDD by targeting the core clock molecule brain and muscle Arnt-like protein-1 (BMAL1). In this study, we showed that BMAL1 KO mice exhibit radiographic features similar to those of human IDD and that BMAL1 expression was negatively correlated with IDD severity by systematic analysis based on 149 human IVD samples. The intrinsic circadian clock in the IVD was dampened by excessive loading, and BMAL1 overexpression by lentivirus attenuated compression-induced IDD. Inhibition of the RhoA/ROCK pathway by Y-27632 or melatonin attenuated the compression-induced decrease in BMAL1 expression. Finally, the two drugs partially restored BMAL1 expression and alleviated IDD in a diurnal compression model. Our results first show that excessive loading dampens the circadian clock of nucleus pulposus tissues via the RhoA/ROCK pathway, the inhibition of which potentially protects against compression-induced IDD by preserving BMAL1 expression. These findings underline the importance of the circadian clock for IVD homeostasis and provide a potentially effective therapeutic strategy for IDD.

Published

2021

17. Post Radical Nephroureterectomy Cystoscopic Surveillance and Usage of a Nomogram as a Predictor for Intravesical Recurrence

Author

Qing Jun Meng, Aravind Raveendran, Yu Dong Tian, Lin Gang Cui, Teng Li, and Yin Sheng Wei

Subjects

Urinary tract urethral cancer, Radical nephroureterectomy, Intravesical recurrence, Cytoscopic surveillance, Nomograms

Abstract

Intravesical recurrence post radical nephroureterectomy (RNU) is a frequent event requiring intense cystoscopic surveillance. This study includes cystoscopic surveillance and usage of variable predictors for intravesical recurrence after radical nephroureterectomy. The current investigation objective was to recognize intravesical recurrence indicators and build up a tool to allow risk delineated methodology supporting patient advising for cystoscopic surveillance and post-operative intravesical MMC administration. With a median follow-up of 36 months, intravesical recurrence occurred in 59 patients. IVR after RNU was noted in 59 patients after a median follow-up of 36 months. The probability of intravesical recurrence is 28.6%.The recurrent bladder tumors were managed with endoscopic resection and intravesical chemoimmunotherapy following the standard protocol. The recurrent bladder tumors showed the following characteristics: 3.4%, 3.4%, 8.5%, 37.3%, and 47.5% of tumors were in Ta, T1, T2, T3, and T4stages, respectively. One patient underwent radical cystectomy after a refractory muscle-invasive bladder tumor, and contralateral UTUC developed. Two patients had partial cystectomy after multiple endoscopic resections of T1 tumor, and intravesical chemotherapy failed. For 59 patients who developed bladder recurrence, the optimal cut-off point of early recurrence was determined to be six months after surgery (p=0.042). End-stage renal disease history and surgical margin positive patient has later bladder recurrence.

Published

2021

18. Tissue physiology revolving around the clock: circadian rhythms as exemplified by the intervertebral disc

Author

Judith A. Hoyland, Cátia F. Gonçalves, Qing-Jun Meng, Michal Dudek, and Honor Morris

Subjects

musculoskeletal diseases, 0301 basic medicine, Aging, Immunology, Circadian clock, Degeneration (medical), General Biochemistry, Genetics and Molecular Biology, Shift work, 03 medical and health sciences, 0302 clinical medicine, Rheumatology, medicine, Immunology and Allergy, Animals, Homeostasis, Humans, Circadian rhythm, Intervertebral Disc, business.industry, Intervertebral disc, musculoskeletal system, Low back pain, Spinal column, Circadian Rhythm, 030104 developmental biology, medicine.anatomical_structure, Ageing, medicine.symptom, business, Neuroscience, 030217 neurology & neurosurgery

Abstract

Circadian clocks in the brain and peripheral tissues temporally coordinate local physiology to align with the 24 hours rhythmic environment through light/darkness, rest/activity and feeding/fasting cycles. Circadian disruptions (during ageing, shift work and jet-lag) have been proposed as a risk factor for degeneration and disease of tissues, including the musculoskeletal system. The intervertebral disc (IVD) in the spine separates the bony vertebrae and permits movement of the spinal column. IVD degeneration is highly prevalent among the ageing population and is a leading cause of lower back pain. The IVD is known to experience diurnal changes in loading patterns driven by the circadian rhythm in rest/activity cycles. In recent years, emerging evidence indicates the existence of molecular circadian clocks within the IVD, disruption to which accelerates tissue ageing and predispose animals to IVD degeneration. The cell-intrinsic circadian clocks in the IVD control key aspects of physiology and pathophysiology by rhythmically regulating the expression of ~3.5% of the IVD transcriptome, allowing cells to cope with the drastic biomechanical and chemical changes that occur throughout the day. Indeed, epidemiological studies on long-term shift workers have shown an increased incidence of lower back pain. In this review, we summarise recent findings of circadian rhythms in health and disease, with the IVD as an exemplar tissue system. We focus on rhythmic IVD functions and discuss implications of utilising biological timing mechanisms to improve tissue health and mitigate degeneration. These findings may have broader implications in chronic rheumatic conditions, given the recent findings of musculoskeletal circadian clocks.

Published

2020

19. Quantitative live imaging of Venus::BMAL1 in a mouse model reveals complex dynamics of the master circadian clock regulator

Author

Michael H. Hastings, Johanna E. Chesham, Nan Yang, Honor Morris, Neil E. Humphreys, Judith A. Hoyland, Dharshika Pathiranage, Andrew S. I. Loudon, David G. Spiller, Michal Dudek, Nicola J. Smyllie, Egor Zindy, Antony Adamson, Qing-Jun Meng, James Bagnall, Cátia F. Gonçalves, and Kramer, Achim

Subjects

Aging, Cancer Research, Circadian clock, Regulator, Endogeny, QH426-470, Biochemistry, Mice, 0302 clinical medicine, Cryptochrome, Animal Cells, Medicine and Health Sciences, Cells, Cultured, Genetics (clinical), Connective Tissue Cells, Feedback, Physiological, Mammals, Microscopy, 0303 health sciences, Chronobiology, Suprachiasmatic nucleus, ARNTL Transcription Factors, Brain, Eukaryota, Light Microscopy, Recombinant Proteins, Circadian Rhythm, Circadian Rhythms, Circadian Oscillators, Liver, Connective Tissue, Vertebrates, Single-Cell Analysis, Anatomy, Cellular Types, Research Article, Sciences exactes et naturelles, endocrine system, Imaging Techniques, Fluorescence Recovery after Photobleaching, Biology, Research and Analysis Methods, Rodents, 03 medical and health sciences, Chondrocytes, Bacterial Proteins, Fluorescence Imaging, Genetics, Animals, Circadian rhythm, Muscle, Skeletal, Molecular Biology, Transcription factor, Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, Organisms, Biology and Life Sciences, Cell Biology, Luminescent Proteins, Biological Tissue, Cartilage, Microscopy, Fluorescence, Protein Biosynthesis, Amniotes, Neuroscience, 030217 neurology & neurosurgery

Abstract

Evolutionarily conserved circadian clocks generate 24-hour rhythms in physiology and behaviour that adapt organisms to their daily and seasonal environments. In mammals, the suprachiasmatic nucleus (SCN) of the hypothalamus is the principal co-ordinator of the cell-autonomous clocks distributed across all major tissues. The importance of robust daily rhythms is highlighted by experimental and epidemiological associations between circadian disruption and human diseases. BMAL1 (a bHLH-PAS domain-containing transcription factor) is the master positive regulator within the transcriptional-translational feedback loops (TTFLs) that cell-autonomously define circadian time. It drives transcription of the negative regulators Period and Cryptochrome alongside numerous clock output genes, and thereby powers circadian time-keeping. Because deletion of Bmal1 alone is sufficient to eliminate circadian rhythms in cells and the whole animal it has been widely used as a model for molecular disruption of circadian rhythms, revealing essential, tissue-specific roles of BMAL1 in, for example, the brain, liver and the musculoskeletal system. Moreover, BMAL1 has clock-independent functions that influence ageing and protein translation. Despite the essential role of BMAL1 in circadian time-keeping, direct measures of its intra-cellular behaviour are still lacking. To fill this knowledge-gap, we used CRISPR Cas9 to generate a mouse expressing a knock-in fluorescent fusion of endogenous BMAL1 protein (Venus::BMAL1) for quantitative live imaging in physiological settings. The Bmal1Venus mouse model enabled us to visualise and quantify the daily behaviour of this core clock factor in central (SCN) and peripheral clocks, with single-cell resolution that revealed its circadian expression, anti-phasic to negative regulators, nuclear-cytoplasmic mobility and molecular abundance., Author summary Cell-autonomous circadian clocks are transcriptional/translational feedback loops that co-ordinate almost all mammalian physiology and behaviour. Although their genetic basis is well understood, we are largely ignorant of the natural behaviour of clock proteins and how they work within these loops. This is particularly true for the essential transcriptional activator BMAL1. To address this, we created and validated a mouse carrying a fully functional knock-in allele that encodes a fluorescent fusion of BMAL1 (Venus::BMAL1). Quantitative live imaging in tissue explants and cells, including the central clock of the suprachiasmatic nucleus (SCN), revealed the circadian expression, nuclear-cytoplasmic mobility, fast kinetics and surprisingly low molecular abundance of endogenous BMAL1, providing significant quantitative insights into the intracellular mechanisms of circadian timing at single-cell resolution.

Published

2020

20. Knockdown of cytokeratin 8 overcomes chemoresistance of chordoma cells by aggravating endoplasmic reticulum stress through PERK/eIF2α arm of unfolded protein response and blocking autophagy

Author

Liu Yang, Qing-Jun Meng, Jianhui Wang, Di Wang, Pandi Peng, Dong Wang, Zhuojing Luo, Peiran Zhang, Chao Zheng, and Xiaolong Xu

Subjects

musculoskeletal diseases, Cancer Research, Eukaryotic Initiation Factor-2, Immunology, Article, Cellular and Molecular Neuroscience, Autophagy, Chordoma, Bone cancer, medicine, Animals, Humans, lcsh:QH573-671, Gene knockdown, lcsh:Cytology, Chemistry, Keratin-8, Endoplasmic reticulum, Cell Biology, Endoplasmic Reticulum Stress, medicine.disease, Cancer therapeutic resistance, Apoptosis, Cell culture, Unfolded Protein Response, Cancer research, Unfolded protein response, Keratin 8

Abstract

Chordoma is a malignant primary osseous spinal tumor with pronounced chemoresistance. However, the mechanisms of how chordoma cells develop chemoresistance are still not fully understood. Cytokeratin 8 (KRT8) is a molecular marker of notochordal cells, from which chordoma cells were believed to be originated. In this study, we showed that either doxorubicin or irinotecan promoted KRT8 expression in both CM319 and UCH1 cell lines, accompanied by an increased unfolded protein response and autophagy activity. Then, siRNA-mediated knockdown of KRT8 chemosensitized chordoma cells in vitro. Mechanistic studies showed that knockdown of KRT8 followed by chemotherapy aggravated endoplasmic reticulum stress through PERK/eIF2α arm of unfolded protein response and blocked late-stage autophagy. Moreover, suppression of the PERK/eIF2α arm of unfolded protein response using PERK inhibitor GSK2606414 partially rescued the apoptotic chordoma cells but did not reverse the blockage of the autophagy flux. Finally, tumor xenograft model further confirmed the chemosensitizing effects of siKRT8. This study represents the first systematic investigation into the role of KRT8 in chemoresistance of chordoma and our results highlight a possible strategy of targeting KRT8 to overcome chordoma chemoresistance.

Published

2019

21. Circadian time series proteomics reveals daily dynamics in cartilage physiology

Author

Joe Swift, Ping Wang, Shireen R. Lamandé, Michal Dudek, Judith A. Hoyland, Craig Lawless, Jayalath P.D. Ruckshanthi, Qing-Jun Meng, Constanza Angelucci, John F. Bateman, Karl E. Kadler, and Venkatesh Mallikarjun

Subjects

030203 arthritis & rheumatology, 0303 health sciences, Cartilage, Osteoarthritis, Biology, medicine.disease, Proteomics, Biomarker (cell), Cell biology, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Gene expression, medicine, Protein biosynthesis, Circadian rhythm, Cytoskeleton, 030304 developmental biology

Abstract

ObjectivesArticular cartilage undergoes cyclical heavy loading and low load recovery during the 24-hour day/night cycle. We investigated the daily changes of protein abundance in mouse femoral head articular cartilage by performing 24-hour time-series proteomics study.MethodsTandem mass spectrometry analysis was used to quantify proteins extracted from mouse cartilage. Bioinformatics analysis was performed to quantify rhythmic changes in protein abundance. Primary chondrocytes were isolated and cultured for independent validation of selected rhythmic proteins.Results145 rhythmic proteins were detected. Among these were key cartilage molecules including CCN2, MATN1, PAI-1 and PLOD1 & 2. Pathway analysis revealed that proteins related to protein synthesis, cytoskeleton and glucose metabolism exhibited time-of-day dependent peaks in their abundance. Meta-analysis of published proteomics datasets from articular cartilage revealed that numerous rhythmic proteins were dysregulated in osteoarthritis and/or ageing.ConclusionsOur circadian proteomics study revealed that articular cartilage is a much more dynamic tissue than previously thought. Chondrocytes exhibit circadian rhythms not only in gene expression but also in protein abundance. Our results clearly call for the consideration of circadian timing in understanding cartilage biology, osteoarthritis pathogenesis, treatment strategies and biomarker detection.

Published

2019

22. Preservation of circadian rhythms by the protein folding chaperone, BiP

Author

Richa Garva, Adam Pickard, Peter Arvan, Ben Calverley, Karl E. Kadler, Joan Chang, Qing-Jun Meng, and Nissrin Alachkar

Subjects

collagen, Protein Folding, Circadian clock, Mice, Transgenic, Endoplasmic Reticulum, 4PBA, Per2::luc, UDCA, Mice, 03 medical and health sciences, 0302 clinical medicine, Fibrosis, medicine, Animals, Homeostasis, Circadian rhythm, Endoplasmic Reticulum Chaperone BiP, Heat-Shock Proteins, 030304 developmental biology, 0303 health sciences, Chemistry, Research, medicine.disease, Circadian Rhythm, Cell biology, 030220 oncology & carcinogenesis, Cancer cell, Unfolded protein response, Protein folding, Chemical chaperone, ER stress

Abstract

Dysregulation of collagen synthesis is associated with disease progression in cancer and fibrosis. Collagen synthesis is coordinated with the circadian clock, which in cancer cells is, curiously, deregulated by endoplasmic reticulum (ER) stress. We hypothesized interplay between circadian rhythm, collagen synthesis, and ER stress in normal cells. Here we show that fibroblasts with ER stress lack circadian rhythms in gene expression upon clock-synchronizing time cues. Overexpression of binding immunoglobulin protein (BiP) or treatment with chemical chaperones strengthens the oscillation amplitude of circadian rhythms. The significance of these findings was explored in tendon, where we showed that BiP expression is ramped preemptively prior to a surge in collagen synthesis at night, thereby preventing protein misfolding and ER stress. In turn, this forestalls activation of the unfolded protein response in order for circadian rhythms to be maintained. Thus, targeting ER stress could be used to modulate circadian rhythm and restore collagen homeostasis in disease.—Pickard, A., Chang, J., Alachkar, N., Calverley, B., Garva, R., Arvan, P., Meng, Q.-J., Kadler, K. E. Preservation of circadian rhythms by the protein folding chaperone, BiP.

Published

2019

23. Circadian rhythms in skin and other elastic tissues

Author

Mark Naven, Louise Hopkinson, Sarah A. Hibbert, Alexander Eckersley, Mike Bell, Victoria L. Newton, Matiss Ozols, Michael J. Sherratt, and Qing-Jun Meng

Subjects

0301 basic medicine, medicine.medical_treatment, Extracellular matrix, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Homeostasis, Humans, Circadian rhythm, Molecular Biology, Skin, Extracellular Matrix Proteins, biology, Cartilage, Elastic Tissue, Chronotherapy (treatment scheduling), Cell biology, Circadian Rhythm, Extracellular Matrix, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, biology.protein, Wound healing, Elastin, Elastic fiber

Abstract

Circadian rhythms are daily oscillations that, in mammals, are driven by both a master clock, located in the brain, and peripheral clocks in cells and tissues. Approximately 10% of the transcriptome, including extracellular matrix components, is estimated to be under circadian control. Whilst it has been established that certain collagens and extracellular matrix proteases are diurnally regulated (for example in tendon, cartilage and intervertebral disc) the role played by circadian rhythms in mediating elastic fiber homeostasis is poorly understood. Skin, arteries and lungs are dynamic, resilient, elastic fiber-rich organs and tissues. In skin, circadian rhythms influence cell migration and proliferation, wound healing and susceptibility of the tissues to damage (from protease activity, oxidative stress and ultraviolet radiation). In the cardiovascular system, blood pressure and heart rate also follow age-dependent circadian rhythms whilst the lungs exhibit diurnal variations in immune response. In order to better understand these processes it will be necessary to characterise diurnal changes in extracellular matrix biology. In particular, given the sensitivity of peripheral clocks to external factors, the timed delivery of interventions (chronotherapy) has the potential to significantly improve the efficacy of treatments designed to repair and regenerate damaged cutaneous, vascular and pulmonary tissues.

Published

2019

24. Influence of the extracellular matrix on cell-intrinsic circadian clocks

Author

Charles H. Streuli and Qing-Jun Meng

Subjects

Circadian clock, CLOCK Proteins, Biology, Mechanotransduction, Cellular, Extracellular matrix, 03 medical and health sciences, 0302 clinical medicine, Circadian Clocks, medicine, Animals, Homeostasis, Humans, Protein Isoforms, Circadian rhythm, Mechanotransduction, Fibroblast, Tissue homeostasis, 030304 developmental biology, Feedback, Physiological, Mammals, Regulation of gene expression, 0303 health sciences, ARNTL Transcription Factors, Period Circadian Proteins, Cell Biology, Epithelium, Circadian Rhythm, Extracellular Matrix, Cryptochromes, Eukaryotic Cells, medicine.anatomical_structure, Cellular Microenvironment, Gene Expression Regulation, 030220 oncology & carcinogenesis, Neuroscience

Abstract

Cell-autonomous circadian clocks coordinate tissue homeostasis with a 24-hourly rhythm. The molecular circadian clock machinery controls tissue- and cell type-specific sets of rhythmic genes. Disruptions of clock mechanisms are linked to an increased risk of acquiring diseases, especially those associated with aging, metabolic dysfunction and cancer. Despite rapid advances in understanding the cyclic outputs of different tissue clocks, less is known about how the clocks adapt to their local niche within tissues. We have discovered that tissue stiffness regulates circadian clocks, and that this occurs in a cell-type-dependent manner. In this Review, we summarise new work linking the extracellular matrix with differential control of circadian clocks. We discuss how the changes in tissue structure and cellular microenvironment that occur throughout life may impact on the molecular control of circadian cycles. We also consider how altered clocks may have downstream impacts on the acquisition of diseases.

Published

2019

25. Timing metabolism in cartilage and bone: links between circadian clocks and tissue homeostasis

Author

Qing-Jun Meng and Cátia F. Gonçalves

Subjects

0301 basic medicine, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Cartilage, Circadian clock, Osteoporosis, 030209 endocrinology & metabolism, Metabolism, Osteoarthritis, Biology, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Endocrinology, medicine.anatomical_structure, Internal medicine, medicine, Circadian rhythm, Neuroscience, Homeostasis, Tissue homeostasis

Abstract

The circadian system in mammals is responsible for the temporal coordination of multiple physiological and behavioural processes that are necessary for homeostasis. In the skeleton, it has long been known that metabolic functions of chondrocytes, osteoblasts and osteoclasts exhibit intrinsic circadian rhythms. In addition, results from animal models reveal a close connection between the disruption of circadian rhythms and skeletal disorders such as rheumatoid arthritis, osteoarthritis and osteoporosis. In this review, we summarise the latest insights into the genetic and biochemical mechanisms linking cartilage and bone physiology to the circadian clock system. We also discuss how this knowledge can be utilised to improve human health.

Published

2019

26. Application of Mosaic Instruments on Back-up Panel in Nuclear Power Plant

Author

Hong-Tao Sun, Qing-Jun Meng, Zhi-Guo Ma, Fu-Ju Xie, and Chao Gao

Subjects

Electrical isolation, Operability, Computer science, Process (engineering), law, Interface (computing), Nuclear power plant, Systems engineering, Mosaic (geodemography), Dimension (data warehouse), Control room, law.invention

Abstract

The mosaic instruments installed on the back-up panel (BUP) have uniform dimensions and are demonstrated to be not only a modern style of main control room (MCR) but also conveniently installed, maintained and powerfully extended. As the human-machine interface equipments, mosaic instrument needs to consider the requirement of human factors (operability, readability, prevention of malfunction) and independence (physical separation and electrical isolation) in the nuclear power plant (NPP) designing process in order to insure the NPP in safe status This paper mainly introduces the type and dimension character of the mosaic instruments and describe the human factors engineering, independence application characters that how to meet the standard requirements when the mosaic instruments are used on BUP in main control room of NPP. As the development of nuclear industry, for the NPP, the application of mosaic instruments will be a new choice.

Published

2019

27. The brain–joint axis in osteoarthritis: nerves, circadian clocks and beyond

Author

Francis Berenbaum and Qing-Jun Meng

Subjects

0301 basic medicine, Nervous system, Aging, Hypothalamo-Hypophyseal System, medicine.medical_specialty, Circadian clock, Pituitary-Adrenal System, Inflammation, Review, Autonomic Nervous System, 03 medical and health sciences, Metabolic Diseases, Rheumatology, Circadian Clocks, Internal medicine, Osteoarthritis, Journal Article, medicine, Humans, Circadian rhythm, business.industry, Circadian Rhythm, Vagus nerve, Autonomic nervous system, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Reflex, Cholinergic, Joints, medicine.symptom, business, Neuroscience

Abstract

Osteoarthritis (OA) is a prevalent and debilitating joint disease for which ageing, obesity and chronic inflammation are known risk factors. The central, peripheral and autonomic nervous systems are essential in all metabolic systems, and emerging evidence suggests a role for these systems in OA. In the past few years, metabolic diseases, such as obesity or diabetes, have been linked to disruption of circadian rhythms that are tightly regulated by the nervous system, whereas inflammatory and autoimmune diseases are known to be linked to disruption of the cholinergic vagus nerve reflex. Interestingly, metabolism, inflammation and circadian rhythms have all been linked to the development and progression of OA. This article reviews current knowledge of the direct and indirect roles of the nervous system and circadian system in the initiation and/or progression of OA, and highlights the directions for future research in this emerging field.

Published

2016

28. Disrupted circadian clocks and altered tissue mechanics in primary human breast tumours

Author

Miles Howe, Eleanor Broadberry, Charles H. Streuli, Qing-Jun Meng, James C. McConnell, Egor Zindy, Nan Yang, Rachel Waddington, Angela Leek, Jack Williams, and Leena Dennis Joseph

Subjects

0301 basic medicine, Circadian clock, Primary Cell Culture, Breast Neoplasms, Epithelial cells, Biology, lcsh:RC254-282, Epithelium, Cohort Studies, Circadian clocks, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Stroma, medicine, Tumor Cells, Cultured, Humans, Circadian rhythm, Breast, RNA, Messenger, Mammographic density, Tissue homeostasis, Aged, Cancer, ARNTL Transcription Factors, Sciences bio-médicales et agricoles, Middle Aged, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, 3. Good health, CLOCK, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cancer research, Female, Collagen, Research Article

Abstract

Background Circadian rhythms maintain tissue homeostasis during the 24-h day-night cycle. Cell-autonomous circadian clocks play fundamental roles in cell division, DNA damage responses and metabolism. Circadian disruptions have been proposed as a contributing factor for cancer initiation and progression, although definitive evidence for altered molecular circadian clocks in cancer is still lacking. In this study, we looked at circadian clocks in breast cancer. Methods We isolated primary tumours and normal tissues from the same individuals who had developed breast cancer with no metastases. We assessed circadian clocks within primary cells of the patients by lentiviral expression of circadian reporters, and the levels of clock genes in tissues by qPCR. We histologically examined collagen organisation within the normal and tumour tissue areas, and probed the stiffness of the stroma adjacent to normal and tumour epithelium using atomic force microscopy. Results Epithelial ducts were disorganised within the tumour areas. Circadian clocks were altered in cultured tumour cells. Tumour regions were surrounded by stroma with an altered collagen organisation and increased stiffness. Levels of Bmal1 messenger RNA (mRNA) were significantly altered in the tumours in comparison to normal epithelia. Conclusion Circadian rhythms are suppressed in breast tumour epithelia in comparison to the normal epithelia in paired patient samples. This correlates with increased tissue stiffness around the tumour region. We suggest possible involvement of altered circadian clocks in the development and progression of breast cancer. Electronic supplementary material The online version of this article (10.1186/s13058-018-1053-4) contains supplementary material, which is available to authorized users.

Published

2018

29. Circadian control of the secretory pathway is a central mechanism in tissue homeostasis

Author

Oliver E. Jensen, Venkatesh Mallikarjun, Joe Swift, Ching-Yan Chloé Yeung, Tom Shearer, Helena Raymond-Hayling, Yinhui Lu, Karl E. Kadler, Ben Calverley, David F. Holmes, Qing-Jun Meng, Antony Adamson, Adam Pickard, Richa Garva, and Joan Chang

Subjects

0303 health sciences, Chemistry, Circadian clock, Fibril, Cell biology, 03 medical and health sciences, Procollagen peptidase, 0302 clinical medicine, Collagen network, Circadian rhythm, 030217 neurology & neurosurgery, Tissue homeostasis, Homeostasis, Secretory pathway, 030304 developmental biology

Abstract

Collagen is the most abundant secreted protein in vertebrates that persists throughout life without renewal. The unchanging nature of collagen contrasts with observed continued collagen synthesis throughout adulthood and with conventional transcriptional and translational homeostatic mechanisms that replace damaged proteins with new copies. Here we show circadian clock regulation of procollagen transport from ER-to-Golgi and Golgi-to-plasma membrane by sequential rhythmic expression of SEC61, TANGO1, PDE4D and VPS33B. The result is nocturnal procollagen synthesis and daytime collagen fibril assembly in mice. Rhythmic collagen degradation by CTSK maintains collagen homeostasis. This circadian cycle of collagen synthesis, assembly and degradation affects only a pool of newly-synthesized collagen whilst maintaining the persistent collagen network. Disabling the circadian clock causes collagen accumulation and abnormal fibrilsin vivo. In conclusion, our study has identified a circadian clock mechanism of protein homeostasis in which a sacrificial pool of collagen is synthesized and removed to maintain tissue function.

Published

2018

30. The chondrocyte clock gene Bmal1 controls cartilage homeostasis and integrity

Author

Jayalath P.D. Ruckshanthi, Qing-Jun Meng, Ding Jin, Xin Li, Michal Dudek, Raymond P. Boot-Handford, Ping Wang, Nan Yang, Hikari Yoshitane, Nicole Gossan, Ilaria Bellantuono, Yoshitaka Fukada, Maya Boudiffa, and Hee Jeong Im

Subjects

Cartilage, Articular, Male, 0301 basic medicine, endocrine system, Circadian clock, Osteoarthritis, Biology, Bioinformatics, Chondrocyte, Mice, 03 medical and health sciences, Chondrocytes, Research Support, N.I.H., Extramural, Transforming Growth Factor beta, Journal Article, medicine, Animals, Homeostasis, Humans, Circadian rhythm, Tissue homeostasis, Mice, Knockout, NFATC Transcription Factors, Sequence Analysis, RNA, Cartilage homeostasis, Research Support, Non-U.S. Gov't, Cartilage, ARNTL Transcription Factors, General Medicine, medicine.disease, Circadian Rhythm, Cell biology, CLOCK, 030104 developmental biology, medicine.anatomical_structure, Research Support, U.S. Gov't, Non-P.H.S, Research Article

Abstract

Osteoarthritis (OA) is the most prevalent and debilitating joint disease, and there are currently no effective disease-modifying treatments available. Multiple risk factors for OA, such as aging, result in progressive damage and loss of articular cartilage. Autonomous circadian clocks have been identified in mouse cartilage, and environmental disruption of circadian rhythms in mice predisposes animals to OA-like damage. However, the contribution of the cartilage clock mechanisms to the maintenance of tissue homeostasis is still unclear. Here, we have shown that expression of the core clock transcription factor BMAL1 is disrupted in human OA cartilage and in aged mouse cartilage. Furthermore, targeted Bmal1 ablation in mouse chondrocytes abolished their circadian rhythm and caused progressive degeneration of articular cartilage. We determined that BMAL1 directs the circadian expression of many genes implicated in cartilage homeostasis, including those involved in catabolic, anabolic, and apoptotic pathways. Loss of BMAL1 reduced the levels of phosphorylated SMAD2/3 (p-SMAD2/3) and NFATC2 and decreased expression of the major matrix-related genes Sox9, Acan, and Col2a1, but increased p-SMAD1/5 levels. Together, these results define a regulatory mechanism that links chondrocyte BMAL1 to the maintenance and repair of cartilage and suggest that circadian rhythm disruption is a risk factor for joint diseases such as OA.

Published

2015

31. Environmental Disruption of Circadian Rhythm Predisposes Mice to Osteoarthritis-Like Changes in Knee Joint

Author

Andre J. van Wijnen, Xin Li, Fred W. Turek, Keith C. Summa, Michael B. Ellman, Qing-Jun Meng, Ali Keshavarizian, Di Chen, Christopher B. Forsyth, Robin M. Voigt, Ranjan Kc, Gary S. Stein, Hee Jeong Im, and Martha Hotz Vitaterna

Subjects

medicine.medical_specialty, Anabolism, Physiology, Cartilage, Clinical Biochemistry, Stimulation, Cell Biology, Osteoarthritis, Biology, medicine.disease, Pathophysiology, medicine.anatomical_structure, Endocrinology, Internal medicine, medicine, Circadian rhythm, Signal transduction, Homeostasis

Abstract

Circadian rhythm dysfunction is linked to many diseases, yet pathophysiological roles in articular cartilage homeostasis and degenerative joint disease including osteoarthritis (OA) remains to be investigated in vivo. Here, we tested whether environmental or genetic disruption of circadian homeostasis predisposes to OA-like pathological changes. Male mice were examined for circadian locomotor activity upon changes in the light:dark (LD) cycle or genetic disruption of circadian rhythms. Wild-type (WT) mice were maintained on a constant 12 hour:12 hour LD cycle (12:12 LD) or exposed to weekly 12 hour phase shifts. Alternatively, male circadian mutant mice (ClockΔ19 or Csnk1etau mutants) were compared with age-matched WT littermates that were maintained on a constant 12:12 LD cycle. Disruption of circadian rhythms promoted osteoarthritic changes by suppressing proteoglycan accumulation, upregulating matrix-degrading enzymes and downregulating anabolic mediators in the mouse knee joint. Mechanistically, these effects involved activation of the PKCδ-ERK-RUNX2/NFκB and β-catenin signaling pathways, stimulation of MMP-13 and ADAMTS-5, as well as suppression of the anabolic mediators SOX9 and TIMP-3 in articular chondrocytes of phase-shifted mice. Genetic disruption of circadian homeostasis does not predispose to OA-like pathological changes in joints. Our results, for the first time, provide compelling in vivo evidence that environmental disruption of circadian rhythms is a risk factor for the development of OA-like pathological changes in the mouse knee joint.

Published

2015

32. Overview of Development of NPP Advanced Main Control Room Console

Author

Yong-Bin Sun, Zhi-Bin Liu, and Qing-Jun Meng

Subjects

Computer science, Cathode ray tube, law, Control system, Nuclear power plant, Protection system, Control room, Automotive engineering, law.invention

Abstract

The development of advanced Main Control Room (MCR) console of the Nuclear Power Plant (NPP) in the world is overviewed, and the brief introduction of corresponding techniques used in the various NPP MCR consoles is given. The design input and output of procedure and demands, methods of the design research of advanced main control room are issued in detail, especially for the MCR console, which is to be incorporated in the new generation of Chinese nuclear power plant with computerized reactor, control system, protection system, Cathode Ray Tube (CRT) display and soft operation. The results of the comparison of MCR technology can provide a reference for the MCR console development trend.

Published

2017

33. Involvement of posttranscriptional regulation of Clock in the emergence of circadian clock oscillation during mouse development

Author

Moe Hisatomi, Yoshiki Tsuchiya, Masayuki Hara, Qing-Jun Meng, Munehiro Ohashi, Yasuhiro Umemura, Nobuya Koike, Yoichi Minami, and Kazuhiro Yagita

Subjects

0301 basic medicine, Cellular differentiation, Circadian clock, CLOCK, CLOCK Proteins, Biology, 03 medical and health sciences, Mice, Circadian Clocks, Oscillation (cell signaling), Animals, Circadian rhythm, RNA, Messenger, Oscillating gene, Molecular clock, General, Genetics, Multidisciplinary, RNA-Binding Proteins, Cell Differentiation, Mouse Embryonic Stem Cells, Period Circadian Proteins, Embryonic stem cell, Cell biology, Circadian Rhythm, 030104 developmental biology, PNAS Plus, Gene Expression Regulation, embryonic structures, Ontogeny, biology.protein, Posttranscriptional regulation, Protein Processing, Post-Translational, Dicer

Abstract

Circadian clock oscillation emerges in mouse embryo in the later developmental stages. Although circadian clock development is closely correlated with cellular differentiation, the mechanisms of its emergence during mammalian development are not well understood. Here, we demonstrate an essential role of the posttranscriptional regulation of Clock subsequent to the cellular differentiation for the emergence of circadian clock oscillation in mouse fetal hearts and mouse embryonic stem cells (ESCs). In mouse fetal hearts, no apparent oscillation of cell-autonomous molecular clock was detectable around E10, whereas oscillation was clearly visible in E18 hearts. Temporal RNA-sequencing analysis using mouse fetal hearts reveals many fewer rhythmic genes in E10–12 hearts (63, no core circadian genes) than in E17–19 hearts (483 genes), suggesting the lack of functional circadian transcriptional/translational feedback loops (TTFLs) of core circadian genes in E10 mouse fetal hearts. In both ESCs and E10 embryos, CLOCK protein was absent despite the expression of Clock mRNA, which we showed was due to Dicer/Dgcr8-dependent translational suppression of CLOCK. The CLOCK protein is required for the discernible molecular oscillation in differentiated cells, and the posttranscriptional regulation of Clock plays a role in setting the timing for the emergence of the circadian clock oscillation during mammalian development.

Published

2017

34. Epithelial and stromal circadian clocks are inversely regulated by their mechano-matrix environment

Author

Jack, Williams, Nan, Yang, Amber, Wood, Egor, Zindy, Qing-Jun, Meng, and Charles H, Streuli

Subjects

Short Report, Epithelial Cells, Period Circadian Proteins, Fibroblasts, Mechanotransduction, Cellular, Circadian clocks, Mice, Mammary Glands, Animal, Cellular Microenvironment, Circadian gene expression, Animals, RNA, Female, Breast, Stromal Cells, Epidermis, Lung, Skin

Abstract

The circadian clock is an autonomous molecular feedback loop inside almost every cell in the body. We have shown that the mammary epithelial circadian clock is regulated by the cellular microenvironment. Moreover, a stiff extracellular matrix dampens the oscillations of the epithelial molecular clock. Here, we extend this analysis to other tissues and cell types, and identify an inverse relationship between circadian clocks in epithelia and fibroblasts. Epithelial cells from mammary gland, lung and skin have significantly stronger oscillations of clock genes in soft 3D microenvironments, compared to stiff 2D environments. Fibroblasts isolated from the same tissues show the opposite response, exhibiting stronger oscillations and more prolonged rhythmicity in stiff microenvironments. RNA analysis identified that a subset of mammary epithelial clock genes, and their regulators, are upregulated in 3D microenvironments in soft compared to stiff gels. Furthermore, the same genes are inversely regulated in fibroblasts isolated from the same tissues. Thus, our data reveal for the first time an intrinsic difference in the regulation of circadian genes in epithelia and fibroblasts., Highlighted Article: Cell-matrix interactions are known to control circadian clocks. Here, we discovered that the matrix inversely regulates epithelia and fibroblasts.

Published

2017

35. The Risks and Solutions of Green Financial Management in Application

Author

Qing-Jun Meng, Li Tao, and Yong-Jun Tang

Subjects

Financial management, Finance, business.industry, Business, Business risks, SWOT analysis

Published

2017

36. Circadian control of tissue homeostasis and adult stem cells

Author

Qing-Jun Meng, Peggy Janich, and Salvador Aznar Benitah

Subjects

Mechanism (biology), Cellular differentiation, Cell Cycle, Circadian clock, Cell Differentiation, Cell Biology, Biology, Cell cycle, Circadian Rhythm, Cell biology, Adult Stem Cells, Organ Specificity, Circadian Clocks, Animals, Homeostasis, Humans, Suprachiasmatic Nucleus, Circadian rhythm, Tissue homeostasis, Adult stem cell

Abstract

The circadian timekeeping mechanism adapts physiology to the 24-hour light/dark cycle. However, how the outputs of the circadian clock in different peripheral tissues communicate and synchronize each other is still not fully understood. The circadian clock has been implicated in the regulation of numerous processes, including metabolism, the cell cycle, cell differentiation, immune responses, redox homeostasis, and tissue repair. Accordingly, perturbation of the machinery that generates circadian rhythms is associated with metabolic disorders, premature ageing, and various diseases including cancer. Importantly, it is now possible to target circadian rhythms through systemic or local delivery of time cues or compounds. Here, we summarize recent findings in peripheral tissues that link the circadian clock machinery to tissue-specific functions and diseases.

Published

2014

37. The circadian clock regulates rhythmic activation of the NRF2/glutathione-mediated antioxidant defense pathway to modulate pulmonary fibrosis

Author

Keiko Taguchi, Qing-Jun Meng, Hikari Yoshitane, Jefferson Y. Chan, Yoshitaka Fukada, Aya Sagami, Dharshika Pathiranage, Andrew S. I. Loudon, Gijsbertus T. J. van der Horst, Nan Yang, Vanja Pekovic-Vaughan, David A. Bechtold, Baoqiang Guo, Julie E. Gibbs, Masayuki Yamamoto, and Molecular Genetics

Subjects

Pulmonary Fibrosis, Circadian clock, Pharmacology, Inbred C57BL, medicine.disease_cause, Medical and Health Sciences, environment and public health, E-Box Elements, chemistry.chemical_compound, Idiopathic pulmonary fibrosis, Mice, 0302 clinical medicine, Isothiocyanates, Pulmonary fibrosis, 2.1 Biological and endogenous factors, Homeostasis, Aetiology, Promoter Regions, Genetic, Lung, 0303 health sciences, Biological Sciences, respiratory system, Glutathione, 3. Good health, medicine.anatomical_structure, Sulfoxides, Respiratory, Female, Sleep Research, Protein Binding, Research Paper, medicine.medical_specialty, NF-E2-Related Factor 2, 1.1 Normal biological development and functioning, Biology, Bleomycin, digestive system, NRF2, Promoter Regions, 03 medical and health sciences, Genetic, SDG 3 - Good Health and Well-being, Underpinning research, Internal medicine, Circadian Clocks, Genetics, medicine, Animals, Anticarcinogenic Agents, Circadian rhythm, 030304 developmental biology, Psychology and Cognitive Sciences, medicine.disease, respiratory tract diseases, Mice, Inbred C57BL, Oxidative Stress, Endocrinology, chemistry, Gene Expression Regulation, 030217 neurology & neurosurgery, Oxidative stress, Developmental Biology

Abstract

The disruption of the NRF2 (nuclear factor erythroid-derived 2-like 2)/glutathione-mediated antioxidant defense pathway is a critical step in the pathogenesis of several chronic pulmonary diseases and cancer. While the mechanism of NRF2 activation upon oxidative stress has been widely investigated, little is known about the endogenous signals that regulate the NRF2 pathway in lung physiology and pathology. Here we show that an E-box-mediated circadian rhythm of NRF2 protein is essential in regulating the rhythmic expression of antioxidant genes involved in glutathione redox homeostasis in the mouse lung. Using an in vivo bleomycin-induced lung fibrosis model, we reveal a clock “gated” pulmonary response to oxidative injury, with a more severe fibrotic effect when bleomycin was applied at a circadian nadir in NRF2 levels. Timed administration of sulforaphane, an NRF2 activator, significantly blocked this phenotype. Moreover, in the lungs of the arrhythmic ClockΔ19 mice, the levels of NRF2 and the reduced glutathione are constitutively low, associated with increased protein oxidative damage and a spontaneous fibrotic-like pulmonary phenotype. Our findings reveal a pivotal role for the circadian control of the NRF2/glutathione pathway in combating oxidative/fibrotic lung damage, which might prompt new chronotherapeutic strategies for the treatment of human lung diseases, including idiopathic pulmonary fibrosis.

Published

2014

38. microRNA-455 is regulated in a circadian manner and targets a number of components of the circadian rhythm

Author

R. Horne, Qing-Jun Meng, Ian M. Clark, and Tracey E. Swingler

Subjects

Rheumatology, microRNA, Biomedical Engineering, Orthopedics and Sports Medicine, Circadian rhythm, Biology, Neuroscience

Published

2018

39. Research on the Color-Difference Evaluation of Food Package Printing Matter Based on the Human Visual Characteristics

Author

Zhi Jian Li and Qing Jun Meng

Subjects

Spatial filter, Color difference, Computer science, business.industry, media_common.quotation_subject, General Medicine, Color space, Field (computer science), Image (mathematics), medicine.anatomical_structure, Component (UML), medicine, Contrast (vision), Human eye, Computer vision, Artificial intelligence, business, media_common

Abstract

In order to improve for the inadequacy of traditional evaluation methods, this paper researched a kind of color-difference evaluation method for the food package printing matter based on human visual characteristics. Research method is as follow: the reference image and the target image were transformed to the opposite color space, and were dealt with the human eye Contrast Sensitive Function (CSF) spatial filter. The modified three opposite color component of images were transformed into the CIE XYZ space image after CSF spatial filtering processed; finally the image was transformed to the CIELAB space image. The color-difference of the target image was calculated according to color-difference formula. The color-difference result of image is the calculation result with human visual characteristics filtering processed; it combines subjective evaluation with objective evaluation. The research could provide practical and effective evaluation method for the field of food package printing matter.

Published

2013

40. Research on Fracture Surface Morphology and Tensile Properties of Cellulose-Based Green Food Packaging Membrane Materials

Author

Qing Jun Meng and Zhi Jian Li

Subjects

chemistry.chemical_compound, Membrane, Materials science, Morphology (linguistics), chemistry, Scanning electron microscope, Ultimate tensile strength, General Medicine, Cellulose, Phase inversion (chemistry), Elongation, Composite material, Dissolution

Abstract

The Green food-packaging membranes were prepared with N-methylmorpholine-N-oxide (NMMO) as the major solvent by using L-S phase inversion technique. Scanning electron microscopy (SEM) was adopted to characterize fracture surface morphology of membrane, and tensile machine was adopted to test the membrane strength performance. Research results show with the concentration of cellulose increases from 5% to 9%, structure of membrane becomes compact, aperture size becomes small and even, value of tensile strength increases 59.6%, and value of elongation increases 67.5%. With dissolving temperature increases from 100°C to 120°C, structure of membrane becomes loose, pore size becomes big and uneven, value of tensile strength decreases 19.2%, and value of elongation decreases 13.1%. The research can provide the theoretical reference for optimizing technology, adjusting the structure of membrane, and improving the performances of membrane.

Published

2013

41. Research on the Whiteness of Eye-Protection Wrapping Paper

Author

Qing Jun Meng and Zhi Jian Li

Subjects

Engineering drawing, Aesthetics, law, Computer science, media_common.quotation_subject, Quality (business), General Medicine, Eye protection, Gift wrapping, media_common, law.invention

Abstract

Whiteness of wrapping paper is the main affecting factor of printed matter color rendition, the higher the whiteness, the better the results of color rendition. But the result of pursuiting high whiteness is that human eyes are harmed by the photic stimulation of paper-based printed matter. To solve the mentioned above problem, this paper preliminary researches the correlation between paper whiteness and asthenopia, the correlation between printing quality and paper whiteness, for finding out appropriate whiteness that can meet the eyes comfort and have better printing quality. Results show the asthenopia occurs easier as whiteness of wrapping paper increases. Besides, the paper samples with the whiteness values as 89.4% and 96.2% have the better printing quality, and the samples with the whiteness values as 84.6% have the worse printing quality relatively, but the quality gap is not big. Results show the whiteness of samples is between 84.6% and 89.4%, human eyes dont feel asthenopia and the printing quality is better. The research results can provide the theoretical basis for printing and packaging enterprises to choose paper which are suitable for printing packing and have eye-protection function, and contribute to the human eye protection.

Published

2013

42. The Circadian Clock in Murine Chondrocytes Regulates Genes Controlling Key Aspects of Cartilage Homeostasis

Author

Raymond P. Boot-Handford, John F. Bateman, Hugh D. Piggins, Magnus Rattray, Nicole Gossan, Leo A. H. Zeef, Alun T. L. Hughes, Christopher B. Little, Qing-Jun Meng, Lynn Rowley, and James Hensman

Subjects

Cartilage, Articular, Male, medicine.medical_specialty, Immunology, Circadian clock, Biology, RAR-related orphan receptor alpha, Cell Line, Chondrocyte Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, Chondrocytes, Rheumatology, Internal medicine, Circadian Clocks, Osteoarthritis, medicine, Immunology and Allergy, Animals, Homeostasis, Humans, Pharmacology (medical), Circadian rhythm, 030304 developmental biology, 0303 health sciences, NPAS2, Cartilage homeostasis, Period Circadian Proteins, Arthritis, Experimental, CLOCK, Endocrinology, Gene Expression Regulation, 030217 neurology & neurosurgery, PER1

Abstract

The circadian clock governs ∼24-hour cycles in physiology through rhythmic control of tissue-specific sets of clock-controlled genes (CCGs), which allows precise orchestration of organ function (1). In mammals (including humans), the circadian system is organized in a hierarchical manner. The suprachiasmatic nuclei of the hypothalamus receive information from external time cues (predominantly, the light/dark cycle) and synchronize peripheral clocks in most major body organs through neuronal or systemic factors (2–3). The molecular basis of the circadian clock relies on the rhythmic activity of evolutionarily conserved clock genes and proteins, including those for transcriptional activators (Clock/Npas2 and Bmal1), transcriptional repressors (Per1/2 and Cry1/2), and nuclear hormone receptors (Nr1d1/2 [Rev-Erbα/β] and Rora/Rorg) (1). This transcriptional–translational feedback loop controls expression of downstream CCGs to regulate tissue-specific physiology. Disruption of the circadian rhythm (attributable to, for example, effects of aging or shift work) has been correlated with an increased risk of various human diseases, including obesity, diabetes, cardiovascular disease, and cancer (4). Articular cartilage is a specialized load-bearing tissue comprising an abundant extracellular matrix, which is produced and maintained by a sparse population of chondrocytes. As the only cell type residing in this tissue, chondrocytes have a poor capacity for endogenous repair, and there is little evidence of cell division throughout adult life (5). Deterioration in chondrocyte function and survival accompanies the damage and loss of cartilage, a common outcome in degenerative and inflammatory joint diseases such as osteoarthritis (OA) and rheumatoid arthritis (RA). Several physiologic processes in cartilage exhibit diurnal variation, including the processes of matrix synthesis, the growth rate in the growth plate, and mineralization (6,7). Mice with mutations in clock genes show altered regulation of bone volume (9), retarded long bone growth (10), and increased susceptibility to inflammatory arthritis (11), providing in vivo evidence for the importance of the molecular clock in the skeletal system. Moreover, in patients with OA and those with RA, there is a clear circadian rhythm in the severity of pain and stiffness and the extent of manual dexterity (12–13). Expression of clock genes has been shown in bone and joint tissues (11,14) and in isolated chondrocytes (10–16), but no studies have directly examined the detailed mechanisms, inputs, or targets of the cartilage circadian clock, and none have examined how the clock changes during aging and in the pathogenesis of joint disease. In the present study, we demonstrate the presence of self-sustained, functional circadian clocks in mouse cartilage tissue, primary chondrocytes, and a human chondrosarcoma cell line. Circadian transcriptome profiling revealed rhythmic expression of ∼3.9% of the genes expressed in mouse cartilage, including key genes associated with tissue homeostasis. In addition, circadian rhythms in the cartilage from aged mice were significantly dampened. Finally, the expression of key circadian clock genes was altered in articular cartilage from mice with experimentally induced OA. Taken together, our results implicate chondrocyte circadian clocks as a key regulator of cartilage homeostasis, and suggest that changes in circadian regulation may play a role in the pathogenesis of joint disease.

Published

2013

43. Research on the Influence of Paper Smoothness on the Color Effect

Author

Qing Jun Meng and Zhi Jian Li

Subjects

Smoothness (probability theory), business.industry, Computer science, Papermaking, General Engineering, Process (computing), Color effect, Color printing, Gamut, Computer graphics (images), Computer vision, Artificial intelligence, business, Hue

Abstract

Smoothness directly influences the color effect of printed matter, so it is very significant for researching the influence of paper smoothness on color effect of printed matter. This article researchs the relationships between the paper smoothness and the color effect of printed matter through experiments. The results show that, hue error of printed matter decreases with increased smoothness, color gamut of printed matter increases with increased smoothness, the glossiness of printed matter increases with increased smoothness, and color effect of printed matter better with increased smoothness. The results could provide a theoretical reference for papermaking enterprises to optimize the process of papermaking and produce suitable paper for color printing.

Published

2013

44. Circadian clocks and breast cancer

Author

Charles H. Streuli, Qing-Jun Meng, Jack Williams, and Victoria Blakeman

Subjects

0301 basic medicine, medicine.medical_specialty, Epithelial-Mesenchymal Transition, Circadian clock, Breast Neoplasms, Review, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Surgical oncology, Circadian Clocks, Internal medicine, Journal Article, Animals, Humans, Medicine, Breast, Epithelial–mesenchymal transition, Circadian rhythm, Oncology & Carcinogenesis, Regulation of gene expression, business.industry, Suprachiasmatic nucleus, Cancer, medicine.disease, Circadian Rhythm, 3. Good health, Cell Transformation, Neoplastic, 030104 developmental biology, Endocrinology, Gene Expression Regulation, Organ Specificity, 030220 oncology & carcinogenesis, Female, Suprachiasmatic Nucleus, business, Neuroscience, 1112 Oncology And Carcinogenesis

Abstract

Circadian clocks respond to environmental time cues to coordinate 24-hour oscillations in almost every tissue of the body. In the breast, circadian clocks regulate the rhythmic expression of numerous genes. Disrupted expression of circadian genes can alter breast biology and may promote cancer. Here we overview circadian mechanisms, and the connection between the molecular clock and breast biology. We describe how disruption of circadian genes contributes to cancer via multiple mechanisms, and link this to increased tumour risk in women who work irregular shift patterns. Understanding the influence of circadian rhythms on breast cancer could lead to more efficacious therapies, reformed public health policy and improved patient outcome.

Published

2016

45. Circadian Clocks in Articular Cartilage and Bone: A Compass in the Sea of Matrices

Author

Qing-Jun Meng and Nan Yang

Subjects

0301 basic medicine, Cartilage, Articular, Aging, Physiology, Circadian clock, Long bone, Review, Osteoarthritis, Biology, Bone tissue, Chondrocyte, Bone and Bones, Extracellular matrix, 03 medical and health sciences, Chondrocytes, Physiology (medical), Circadian Clocks, Journal Article, medicine, Animals, Humans, Cartilage, Anatomy, medicine.disease, Cell biology, Resorption, Circadian Rhythm, 030104 developmental biology, medicine.anatomical_structure

Abstract

Temporally coordinated resorption and synthesis is the key to maintaining healthy bones. Articular cartilage is a highly specialized connective tissue within the joints that lines the surface of a long bone. Emerging evidence has suggested a critical role of the circadian system in controlling cartilage and bone biology. Articular cartilage is sparsely populated with chondrocytes, surrounded by abundant extracellular matrices that are synthesized and maintained solely by chondrocytes. Once damaged, the articular cartilage tissue has poor capacity for endogenous repair, leaving the joints prone to osteoarthritis, an age-related painful condition that affects millions of individuals worldwide. An important question is how articular cartilage has evolved its remarkable capacity to maintain homeostasis and withstand daily biomechanical challenges associated with resting/activity cycles. Equally important is how this avascular and aneural tissue senses time and uses this information to coordinate daily phases of metabolic activity and tissue remodeling/repair. Bone tissue derived from cartilage has similarly sparse populations of resident cells living in dense and largely mineralized matrices. We discuss recent progress on circadian clocks in these matrix-rich skeletal tissues and highlight avenues for future research.

Published

2016

46. Visualizing and Quantifying Intracellular Behavior and Abundance of the Core Circadian Clock Protein PERIOD2

Author

Johanna E. Chesham, Raymond P. Boot-Handford, Nicola J. Smyllie, Michael R. H. White, David G. Spiller, Michael H. Hastings, Toke P. Krogager, Andrew S. I. Loudon, Elizabeth S. Maywood, Qing-Jun Meng, James Boyd, Ben Saer, and Violetta Pilorz

Subjects

0301 basic medicine, endocrine system, Circadian clock, Biology, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, Circadian Clocks, Report, Journal Article, Animals, CLOCK Proteins, Circadian rhythm, Oscillating gene, Genetics, Agricultural and Biological Sciences(all), Suprachiasmatic nucleus, Biochemistry, Genetics and Molecular Biology(all), Period Circadian Proteins, Bacterial circadian rhythms, Cell biology, PER2, CLOCK, 030104 developmental biology, Suprachiasmatic Nucleus, General Agricultural and Biological Sciences, 030217 neurology & neurosurgery

Abstract

Summary Transcriptional-translational feedback loops (TTFLs) are a conserved molecular motif of circadian clocks. The principal clock in mammals is the suprachiasmatic nucleus (SCN) of the hypothalamus. In SCN neurons, auto-regulatory feedback on core clock genes Period (Per) and Cryptochrome (Cry) following nuclear entry of their protein products is the basis of circadian oscillation [1, 2]. In Drosophila clock neurons, the movement of dPer into the nucleus is subject to a circadian gate that generates a delay in the TTFL, and this delay is thought to be critical for oscillation [3, 4]. Analysis of the Drosophila clock has strongly influenced models of the mammalian clock, and such models typically infer complex spatiotemporal, intracellular behaviors of mammalian clock proteins. There are, however, no direct measures of the intracellular behavior of endogenous circadian proteins to support this: dynamic analyses have been limited and often have no circadian dimension [5, 6, 7]. We therefore generated a knockin mouse expressing a fluorescent fusion of native PER2 protein (PER2::VENUS) for live imaging. PER2::VENUS recapitulates the circadian functions of wild-type PER2 and, importantly, the behavior of PER2::VENUS runs counter to the Drosophila model: it does not exhibit circadian gating of nuclear entry. Using fluorescent imaging of PER2::VENUS, we acquired the first measures of mobility, molecular concentration, and localization of an endogenous circadian protein in individual mammalian cells, and we showed how the mobility and nuclear translocation of PER2 are regulated by casein kinase. These results provide new qualitative and quantitative insights into the cellular mechanism of the mammalian circadian clock., Graphical Abstract, Highlights • Reporter mouse is used for real-time fluorescent imaging of mammalian clock protein PER2 • In contrast to Drosophila, localization of PER2 is not subject to circadian gating • Circadian abundance, mobility, and intracellular dynamics of native PER2 are quantified • Casein kinase1 controls nucleocytoplasmic mobility of PER2 alongside circadian period, Smyllie et al. use a fluorescent reporter mouse to image the circadian dynamics of PER2, a key component of the circadian clock in the suprachiasmatic nucleus and fibroblasts. They reveal marked divergence of the mechanisms of mouse and fly clock cells, and they provide quantitative data to support reappraisal of current models of the mammalian clock.

Published

2016

47. Circadian clocks, ageing and age-related diseases

Author

Qing-Jun Meng

Subjects

Ageing, Age related, Circadian clock, Physiology, General Medicine, Biology

Published

2016

48. The intervertebral disc contains intrinsic circadian clocks that are regulated by age and cytokines and linked to degeneration

Author

Michal, Dudek, Nan, Yang, Jayalath Pd, Ruckshanthi, Jack, Williams, Elzbieta, Borysiewicz, Ping, Wang, Antony, Adamson, Jian, Li, John F, Bateman, Michael R, White, Raymond P, Boot-Handford, Judith A, Hoyland, and Qing-Jun, Meng

Subjects

Mice, Knockout, Aging, Nucleus Pulposus, Tumor Necrosis Factor-alpha, Interleukin-1beta, Age Factors, NF-kappa B, Temperature, ARNTL Transcription Factors, CLOCK Proteins, Intervertebral Disc Degeneration, Period Circadian Proteins, Transfection, Circadian Rhythm, Tissue Culture Techniques, Mice, Circadian Clocks, Animals, Humans, Intervertebral Disc, Transcriptome, Cells, Cultured, Signal Transduction

Abstract

The circadian clocks are internal timing mechanisms that drive ∼24-hour rhythms in a tissue-specific manner. Many aspects of the physiology of the intervertebral disc (IVD) show clear diurnal rhythms. However, it is unknown whether IVD tissue contains functional circadian clocks and if so, how their dysregulation is implicated in IVD degeneration.Clock gene dynamics in ex vivo IVD explants (from PER2:: luciferase (LUC) reporter mice) and human disc cells (transduced with lentivirus containingHere we show the existence of the circadian rhythm in mouse IVD tissue and human disc cells. This rhythm is dampened with ageing in mice and can be abolished by treatment with interleukin-1β but not tumour necrosis factor α. Time-series RNAseq revealed 607 genes with 24-hour patterns of expression representing several essential pathways in IVD physiology. Mice with conditional knockout ofWe have established autonomous circadian clocks in mouse and human IVD cells which respond to age and cytokines, and control key pathways involved in the homeostasis of IVDs. Genetic disruption to the mouse IVD molecular clock predisposes to IVD degeneration. These results support the concept that disruptions to circadian rhythms may be a risk factor for degenerative IVD disease and low back pain.

Published

2016

49. Effective Dot Area’s Calculating Based on YNSN Model

Author

Chen Fei Zhao, Qing Jun Meng, Qing Han, and Cong Cong Chi

Subjects

Optics, business.industry, Range (statistics), Mode (statistics), General Medicine, Dot gain, business, Reflectivity, Visible spectrum, Mathematics

Abstract

Yule-Nielsen neugebauer spectrum(YNSN) model can describe the relation between dot area and spectrum reflectance, which can calculate the effective dot area. The modified index in the model still can’t be determined. The reciprocal of paper’s spectral reflectance at the range of visible light is adopted as the modified index in YNSN model in order to reduce the optical dot gain. By experiment, the modified YNSN mode can be used to calculate the effective dot area of light color. The research has a certain significance for controlling and testing printing color.

Published

2012

50. The Impact of Offset Paper on Ink Transfer Rate and Ink Absorption Rate

Author

Qing Jun Meng, Liang Liu, and Zhi Jian Li

Subjects

Absorption rate, Materials science, Offset (computer science), Inkwell, Transfer (computing), ComputingMethodologies_DOCUMENTANDTEXTPROCESSING, ComputingMethodologies_IMAGEPROCESSINGANDCOMPUTERVISION, General Engineering, Composite material, ComputingMethodologies_COMPUTERGRAPHICS

Abstract

The ink transfer rate and ink absorption rate directly affects the quality of printing matter, so it is very important to know the influence factors of the ink transfer rate and ink absorption rate. This paper studied on the impact of offset paper smoothness and offset paper absorbency on the ink transfer rate, the impact of offset paper compactness and offset paper absorbency on the ink absorption rate. The results show that ink transfer rate is affected by offset paper smoothness within a certain range. The ink transfer rate is affected greatly by offset paper absorbency. The ink absorption rate is greatly affected by offset paper compactness and absorbency.

Published

2012