Your search keyword '"Plumb DA"' showing total 15 results

1. Elf3 Contributes to Cartilage Degradation in vivo in a Surgical Model of Post-Traumatic Osteoarthritis.

Author

Wondimu EB, Culley KL, Quinn J, Chang J, Dragomir CL, Plumb DA, Goldring MB, and Otero M

Subjects

Animals, Cartilage, Articular pathology, Chondrocytes metabolism, DNA-Binding Proteins physiology, Disease Models, Animal, Gene Expression Regulation, Interleukin-1beta metabolism, Male, Matrix Metalloproteinase 13 metabolism, Menisci, Tibial pathology, Mice, Mice, Knockout, Models, Anatomic, Nitric Oxide Synthase Type II metabolism, Osteoarthritis physiopathology, Transcription Factors physiology, Cartilage metabolism, DNA-Binding Proteins metabolism, Osteoarthritis metabolism, Transcription Factors metabolism

Abstract

The E-74 like factor 3 (ELF3) is a transcription factor induced by inflammatory factors in various cell types, including chondrocytes. ELF3 levels are elevated in human cartilage from patients with osteoarthritis (OA), and ELF3 contributes to the IL-1β-induced expression of genes encoding Mmp13, Nos2, and Ptgs2/Cox2 in chondrocytes in vitro. Here, we investigated the contribution of ELF3 to cartilage degradation in vivo, using a mouse model of OA. To this end, we generated mouse strains with cartilage-specific Elf3 knockout (Col2Cre:Elf3 f/f ) and Comp-driven Tet-off-inducible Elf3 overexpression (TRE-Elf3:Comp-tTA). To evaluate the contribution of ELF3 to OA, we induced OA in 12-week-old Col2Cre:Elf3 f/f and 6-month-old TRE-Elf3:Comp-tTA male mice using the destabilization of the medial meniscus (DMM) model. The chondrocyte-specific deletion of Elf3 led to decreased levels of IL-1β- and DMM-induced Mmp13 and Nos2 mRNA in vitro and in vivo, respectively. Histological grading showed attenuation of cartilage loss in Elf3 knockout mice compared to wild type (WT) littermates at 8 and 12 weeks following DMM surgery that correlated with reduced collagenase activity. Accordingly, Elf3 overexpression led to increased cartilage degradation post-surgery compared to WT counterparts. Our results provide evidence that ELF3 is a central contributing factor for cartilage degradation in post-traumatic OA in vivo.

Published

2018

2. Erratum: PIM1 kinase regulates cell death, tumor growth and chemotherapy response in triple-negative breast cancer.

Author

Brasó-Maristany F, Filosto S, Catchpole S, Marlow R, Quist J, Francesch-Domenech E, Plumb DA, Zakka L, Gazinska P, Liccardi G, Meier P, Gris-Oliver A, Cheang MCU, Perdrix-Rosell A, Shafat M, Noël E, Patel N, McEachern K, Scaltriti M, Castel P, Noor F, Buus R, Mathew S, Watkins J, Serra V, Marra P, Grigoriadis A, and Tutt AN

Published

2017

3. Erratum: PIM1 kinase regulates cell death, tumor growth and chemotherapy response in triple-negative breast cancer.

Author

Brasó-Maristany F, Filosto S, Catchpole S, Marlow R, Quist J, Francesch-Domenech E, Plumb DA, Zakka L, Gazinska P, Liccardi G, Meier P, Gris-Oliver A, Cheang MC, Perdrix-Rosell A, Shafat M, Noël E, Patel N, McEachern K, Scaltriti M, Castel P, Noor F, Buus R, Mathew S, Watkins J, Serra V, Marra P, Grigoriadis A, and Tutt AN

Published

2017

4. Progressive cell-mediated changes in articular cartilage and bone in mice are initiated by a single session of controlled cyclic compressive loading.

Author

Ko FC, Dragomir CL, Plumb DA, Hsia AW, Adebayo OO, Goldring SR, Wright TM, Goldring MB, and van der Meulen MC

Subjects

Adaptation, Physiological, Animals, Male, Mice, Inbred C57BL, Osteophyte etiology, Synovial Membrane physiology, Weight-Bearing, Bone and Bones physiology, Cartilage, Articular physiology, Osteoarthritis, Knee etiology

Abstract

We previously showed that repetitive cyclic loading of the mouse knee joint causes changes that recapitulate the features of osteoarthritis (OA) in humans. By applying a single loading session, we characterized the temporal progression of the structural and compositional changes in subchondral bone and articular cartilage. We applied loading during a single 5-minute session to the left tibia of adult (26-week-old) C57Bl/6 male mice at a peak load of 9.0N for 1,200 cycles. Knee joints were collected at times 0, 1, and 2 weeks after loading. The changes in articular cartilage and subchondral bone were analyzed by histology, immunohistochemistry (caspase-3 and cathepsin K), and microcomputed tomography. At time 0, no change was evident in chondrocyte viability or cartilage or subchondral bone integrity. However, cartilage pathology demonstrated by localized thinning and proteoglycan loss occurred at 1 and 2 weeks after the single session of loading. Transient cancellous bone loss was evident at 1 week, associated with increased osteoclast number. Bone loss was reversed to control levels at 2 weeks. We observed formation of fibrous and cartilaginous tissues at the joint margins at 1 and 2 weeks. Our findings demonstrate that a single session of noninvasive loading leads to the development of OA-like morphological and cellular alterations in articular cartilage and subchondral bone. The loss in subchondral trabecular bone mass and thickness returns to control levels at 2 weeks, whereas the cartilage thinning and proteoglycan loss persist. © 2016 Orthopaedic Research Society. Published by Wiley Periodicals, Inc. J Orthop Res 34:1941-1949, 2016., (© 2016 Orthopaedic Research Society. Published by Wiley Periodicals, Inc.)

Published

2016

5. PIM1 kinase regulates cell death, tumor growth and chemotherapy response in triple-negative breast cancer.

Author

Brasó-Maristany F, Filosto S, Catchpole S, Marlow R, Quist J, Francesch-Domenech E, Plumb DA, Zakka L, Gazinska P, Liccardi G, Meier P, Gris-Oliver A, Cheang MC, Perdrix-Rosell A, Shafat M, Noël E, Patel N, McEachern K, Scaltriti M, Castel P, Noor F, Buus R, Mathew S, Watkins J, Serra V, Marra P, Grigoriadis A, and Tutt AN

Subjects

Animals, Apoptosis drug effects, Biphenyl Compounds pharmacology, Cell Line, Tumor, Cell Proliferation drug effects, Cell Survival drug effects, Cell Survival genetics, DNA Copy Number Variations, Female, Gene Knockdown Techniques, Humans, Mice, Mitochondria metabolism, Myeloid Cell Leukemia Sequence 1 Protein metabolism, Neoplasm Transplantation, Protein Kinase Inhibitors pharmacology, Proto-Oncogene Mas, Proto-Oncogene Proteins c-bcl-2 metabolism, Proto-Oncogene Proteins c-myc metabolism, Proto-Oncogene Proteins c-pim-1 antagonists & inhibitors, Real-Time Polymerase Chain Reaction, Thiazolidines pharmacology, Xenograft Model Antitumor Assays, Apoptosis genetics, Cell Proliferation genetics, Gene Expression Regulation, Neoplastic, Proto-Oncogene Proteins c-pim-1 genetics, Triple Negative Breast Neoplasms genetics

Abstract

Triple-negative breast cancers (TNBCs) have poor prognosis and lack targeted therapies. Here we identified increased copy number and expression of the PIM1 proto-oncogene in genomic data sets of patients with TNBC. TNBC cells, but not nonmalignant mammary epithelial cells, were dependent on PIM1 for proliferation and protection from apoptosis. PIM1 knockdown reduced expression of the anti-apoptotic factor BCL2, and dynamic BH3 profiling of apoptotic priming revealed that PIM1 prevents mitochondrial-mediated apoptosis in TNBC cell lines. In TNBC tumors and their cellular models, PIM1 expression was associated with several transcriptional signatures involving the transcription factor MYC, and PIM1 depletion in TNBC cell lines decreased, in a MYC-dependent manner, cell population growth and expression of the MYC target gene MCL1. Treatment with the pan-PIM kinase inhibitor AZD1208 impaired the growth of both cell line and patient-derived xenografts and sensitized them to standard-of-care chemotherapy. This work identifies PIM1 as a malignant-cell-selective target in TNBC and the potential use of PIM1 inhibitors for sensitizing TNBC to chemotherapy-induced apoptotic cell death.

Published

2016

6. Mouse models of osteoarthritis: surgical model of posttraumatic osteoarthritis induced by destabilization of the medial meniscus.

Author

Culley KL, Dragomir CL, Chang J, Wondimu EB, Coico J, Plumb DA, Otero M, and Goldring MB

Subjects

Animals, Humans, Mice, Tibial Meniscus Injuries, Arthritis, Experimental pathology, Arthritis, Experimental physiopathology, Knee Injuries complications, Knee Injuries pathology, Knee Injuries physiopathology, Menisci, Tibial pathology, Menisci, Tibial physiopathology, Osteoarthritis, Knee etiology, Osteoarthritis, Knee pathology, Osteoarthritis, Knee physiopathology

Abstract

The surgical model of destabilization of the medial meniscus (DMM) has become a gold standard for studying the onset and progression of posttraumatic osteoarthritis (OA). The DMM model mimics clinical meniscal injury, a known predisposing factor for the development of human OA, and permits the study of structural and biological changes over the course of the disease. In addition, when applied to genetically modified or engineered mouse models, this surgical procedure permits dissection of the relative contribution of a given gene to OA initiation and/or progression. This chapter describes the requirements for the surgical induction of OA in mouse models, and provides guidelines and tools for the subsequent histological, immunohistochemical, and molecular analyses. Methods for the assessment of the contributions of selected genes in genetically modified strains are also provided.

Published

2015

7. ADAM17 controls endochondral ossification by regulating terminal differentiation of chondrocytes.

Author

Hall KC, Hill D, Otero M, Plumb DA, Froemel D, Dragomir CL, Maretzky T, Boskey A, Crawford HC, Selleri L, Goldring MB, and Blobel CP

Subjects

ADAM Proteins genetics, ADAM17 Protein, Animals, Apoptosis, Bone and Bones metabolism, Bone and Bones pathology, Calcification, Physiologic, Cartilage metabolism, Cartilage pathology, Cell Differentiation, Cell Proliferation, Cells, Cultured, Chondrocytes metabolism, Chondrocytes pathology, ErbB Receptors metabolism, Gene Deletion, Growth Plate metabolism, Growth Plate pathology, Heparin-binding EGF-like Growth Factor, Hypertrophy metabolism, Hypertrophy pathology, Intercellular Signaling Peptides and Proteins metabolism, Male, Mice, Osteoclasts cytology, Osteoclasts metabolism, Osteoclasts pathology, ADAM Proteins metabolism, Chondrocytes cytology, Osteogenesis

Abstract

Endochondral ossification is a highly regulated process that relies on properly orchestrated cell-cell interactions in the developing growth plate. This study is focused on understanding the role of a crucial regulator of cell-cell interactions, the membrane-anchored metalloproteinase ADAM17, in endochondral ossification. ADAM17 releases growth factors, cytokines, and other membrane proteins from cells and is essential for epidermal growth factor receptor (EGFR) signaling and for processing tumor necrosis factor alpha. Here, we report that mice lacking ADAM17 in chondrocytes (A17ΔCh) have a significantly expanded zone of hypertrophic chondrocytes in the growth plate and retarded growth of long bones. This abnormality is caused by an accumulation of the most terminally differentiated type of chondrocytes that produces a calcified matrix. Inactivation of ADAM17 in osteoclasts or endothelial cells does not affect the zone of hypertrophic chondrocytes, suggesting that the main role of ADAM17 in the growth plate is in chondrocytes. This notion is further supported by in vitro experiments showing enhanced hypertrophic differentiation of primary chondrocytes lacking Adam17. The enlarged zone of hypertrophic chondrocytes in A17ΔCh mice resembles that described in mice with mutant EGFR signaling or lack of its ligand transforming growth factor α (TGFα), suggesting that ADAM17 regulates terminal differentiation of chondrocytes during endochondral ossification by activating the TGFα/EGFR signaling axis.

Published

2013

8. In vivo cyclic compression causes cartilage degeneration and subchondral bone changes in mouse tibiae.

Author

Ko FC, Dragomir C, Plumb DA, Goldring SR, Wright TM, Goldring MB, and van der Meulen MC

Subjects

Adaptation, Physiological, Animals, Arthritis, Experimental diagnostic imaging, Biomechanical Phenomena, Cartilage diagnostic imaging, Disease Models, Animal, Male, Mice, Mice, Inbred C57BL, Osteoarthritis diagnostic imaging, Stress, Mechanical, Tibia diagnostic imaging, Tomography, X-Ray Computed, Arthritis, Experimental pathology, Cartilage pathology, Osteoarthritis pathology, Tibia pathology

Abstract

Objective: Alterations in the mechanical loading environment in joints may have both beneficial and detrimental effects on articular cartilage and subchondral bone, and may subsequently influence the development of osteoarthritis (OA). Using an in vivo tibial loading model, the aim of this study was to investigate the adaptive responses of cartilage and bone to mechanical loading and to assess the influence of load level and duration., Methods: Cyclic compression at peak loads of 4.5N and 9.0N was applied to the left tibial knee joint of adult (26-week-old) C57BL/6 male mice for 1, 2, and 6 weeks. Only 9.0N loading was utilized in young (10-week-old) mice. Changes in articular cartilage and subchondral bone were analyzed by histology and micro-computed tomography., Results: Mechanical loading promoted cartilage damage in both age groups of mice, and the severity of joint damage increased with longer duration of loading. Metaphyseal bone mass increased with loading in young mice, but not in adult mice, whereas epiphyseal cancellous bone mass decreased with loading in both young and adult mice. In both age groups, articular cartilage thickness decreased, and subchondral cortical bone thickness increased in the posterior tibial plateau. Mice in both age groups developed periarticular osteophytes at the tibial plateau in response to the 9.0N load, but no osteophyte formation occurred in adult mice subjected to 4.5N peak loading., Conclusion: This noninvasive loading model permits dissection of temporal and topographic changes in cartilage and bone and will enable investigation of the efficacy of treatment interventions targeting joint biomechanics or biologic events that promote OA onset and progression., (Copyright © 2013 by the American College of Rheumatology.)

Published

2013

9. E74-like factor 3 (ELF3) impacts on matrix metalloproteinase 13 (MMP13) transcriptional control in articular chondrocytes under proinflammatory stress.

Author

Otero M, Plumb DA, Tsuchimochi K, Dragomir CL, Hashimoto K, Peng H, Olivotto E, Bevilacqua M, Tan L, Yang Z, Zhan Y, Oettgen P, Li Y, Marcu KB, and Goldring MB

Subjects

Animals, Cartilage, Articular pathology, Chondrocytes pathology, DNA-Binding Proteins genetics, Gene Expression Regulation, Enzymologic drug effects, Gene Expression Regulation, Enzymologic genetics, Humans, Inflammation genetics, Inflammation metabolism, Inflammation pathology, Interleukin-1beta pharmacology, Matrix Metalloproteinase 13 genetics, Mice, Mice, Knockout, Osteoarthritis genetics, Osteoarthritis pathology, Proto-Oncogene Proteins genetics, Proto-Oncogene Proteins c-ets, Response Elements genetics, Stress, Physiological drug effects, Stress, Physiological genetics, Transcription Factor AP-1 genetics, Transcription Factor AP-1 metabolism, Transcription Factors genetics, Cartilage, Articular metabolism, Chondrocytes metabolism, DNA-Binding Proteins metabolism, Matrix Metalloproteinase 13 biosynthesis, Osteoarthritis metabolism, Proto-Oncogene Proteins metabolism, Transcription Factors metabolism, Transcription, Genetic

Abstract

Matrix metalloproteinase (MMP)-13 has a pivotal, rate-limiting function in cartilage remodeling and degradation due to its specificity for cleaving type II collagen. The proximal MMP13 promoter contains evolutionarily conserved E26 transformation-specific sequence binding sites that are closely flanked by AP-1 and Runx2 binding motifs, and interplay among these and other factors has been implicated in regulation by stress and inflammatory signals. Here we report that ELF3 directly controls MMP13 promoter activity by targeting an E26 transformation-specific sequence binding site at position -78 bp and by cooperating with AP-1. In addition, ELF3 binding to the proximal MMP13 promoter is enhanced by IL-1β stimulation in chondrocytes, and the IL-1β-induced MMP13 expression is inhibited in primary human chondrocytes by siRNA-ELF3 knockdown and in chondrocytes from Elf3(-/-) mice. Further, we found that MEK/ERK signaling enhances ELF3-driven MMP13 transactivation and is required for IL-1β-induced ELF3 binding to the MMP13 promoter, as assessed by chromatin immunoprecipitation. Finally, we show that enhanced levels of ELF3 co-localize with MMP13 protein and activity in human osteoarthritic cartilage. These studies define a novel role for ELF3 as a procatabolic factor that may contribute to cartilage remodeling and degradation by regulating MMP13 gene transcription.

Published

2012

10. Human chondrocyte cultures as models of cartilage-specific gene regulation.

Author

Otero M, Favero M, Dragomir C, Hachem KE, Hashimoto K, Plumb DA, and Goldring MB

Subjects

Cartilage cytology, Cartilage Oligomeric Matrix Protein, Cell Separation methods, Chondrocytes cytology, DNA Methylation, Extracellular Matrix Proteins metabolism, Glycoproteins metabolism, Humans, Matrilin Proteins, RNA, Messenger genetics, RNA, Messenger metabolism, Transcription, Genetic, Cartilage metabolism, Chondrocytes metabolism, Gene Expression Regulation, Primary Cell Culture methods

Abstract

The human adult articular chondrocyte is a unique cell type that has reached a fully differentiated state as an end point of development. Within the cartilage matrix, chondrocytes are normally quiescent and maintain the matrix constituents in a low-turnover state of equilibrium. Isolated chondrocytes in culture have provided useful models to study cellular responses to alterations in the environment such as those occurring in different forms of arthritis. However, expansion of primary chondrocytes in monolayer culture results in the loss of phenotype, particularly if high cell density is not maintained. This chapter describes strategies for maintaining or restoring differentiated phenotype by culture in suspension, gels, or scaffolds. Techniques for assessing phenotype involving primarily the analysis of synthesis of cartilage-specific matrix proteins as well as the corresponding mRNAs are also described. Approaches for studying gene regulation, including transfection of promoter-driven reporter genes with expression vectors for transcriptional and signaling regulators, chromatin immunoprecipitation, and DNA methylation are also described.

Published

2012

11. Roles of inflammatory and anabolic cytokines in cartilage metabolism: signals and multiple effectors converge upon MMP-13 regulation in osteoarthritis.

Author

Goldring MB, Otero M, Plumb DA, Dragomir C, Favero M, El Hachem K, Hashimoto K, Roach HI, Olivotto E, Borzì RM, and Marcu KB

Subjects

Animals, Chondrocytes metabolism, Chondrocytes pathology, Disease Models, Animal, Disease Progression, Extracellular Matrix metabolism, Homeostasis, Humans, Matrix Metalloproteinase 13 genetics, Mice, Osteoarthritis genetics, Phenotype, Cartilage metabolism, Cytokines metabolism, Inflammation Mediators metabolism, Matrix Metalloproteinase 13 metabolism, Osteoarthritis enzymology, Osteoarthritis pathology, Signal Transduction

Abstract

Human cartilage is a complex tissue of matrix proteins that vary in amount and orientation from superficial to deep layers and from loaded to unloaded zones. A major challenge to efforts to repair cartilage by stem cell-based and other tissue engineering strategies is the inability of the resident chondrocytes to lay down new matrix with the same structural and resilient properties that it had upon its original formation. This is particularly true of the collagen network, which is susceptible to cleavage once proteoglycans are depleted. Thus, a thorough understanding of the similarities and particularly the marked differences in mechanisms of cartilage remodeling during development, osteoarthritis, and aging may lead to more effective strategies for preventing cartilage damage and promoting repair. To identify and characterize effectors or regulators of cartilage remodeling in these processes, we are using culture models of primary human and mouse chondrocytes and cell lines and mouse genetic models to manipulate gene expression programs leading to matrix remodeling and subsequent chondrocyte hypertrophic differentiation, pivotal processes which both go astray in OA disease. Matrix metalloproteinases (MMP)-13, the major type II collagen-degrading collagenase, is regulated by stress-, inflammation-, and differentiation-induced signals that not only contribute to irreversible joint damage (progression) in OA, but importantly, also to the initiation/onset phase, wherein chondrocytes in articular cartilage leave their natural growth- and differentiation-arrested state. Our work points to common mediators of these processes in human OA cartilage and in early through late stages of OA in surgical and genetic mouse models.

Published

2011

12. Collagen XXVII organises the pericellular matrix in the growth plate.

Author

Plumb DA, Ferrara L, Torbica T, Knowles L, Mironov A Jr, Kadler KE, Briggs MD, and Boot-Handford RP

Subjects

Amino Acid Sequence, Animals, Base Sequence, Female, Fibrillar Collagens chemistry, Fibrillar Collagens genetics, Male, Mice, Mutation, Phenotype, Extracellular Matrix metabolism, Fibrillar Collagens metabolism, Growth Plate cytology, Growth Plate metabolism

Abstract

In order to characterise the function of the novel fibrillar type XXVII collagen, a series of mice expressing mutant forms of the collagen were investigated. Mice harboring a glycine to cysteine substitution in the collagenous domain were phenotypically normal when heterozygote and displayed a mild disruption of growth plate architecture in the homozygous state. Mice expressing an 87 amino acid deletion in the collagenous domain of collagen XXVII were phenotypically normal as heterozygotes whereas homozygotes exhibited a severe chondrodysplasia and died perinatally from a lung defect. Animals expressing the 87 amino acid deletion targeted specifically to cartilage were viable but severely dwarfed. The pericellular matrix of proliferative chondrocytes was disrupted and the proliferative cells exhibited a decreased tendency to flatten and form vertical columns. Collagen XXVII plays an important structural role in the pericellular extracellular matrix of the growth plate and is required for the organisation of the proliferative zone.

Published

2011

13. GADD45beta enhances Col10a1 transcription via the MTK1/MKK3/6/p38 axis and activation of C/EBPbeta-TAD4 in terminally differentiating chondrocytes.

Author

Tsuchimochi K, Otero M, Dragomir CL, Plumb DA, Zerbini LF, Libermann TA, Marcu KB, Komiya S, Ijiri K, and Goldring MB

Subjects

Activating Transcription Factor 1 metabolism, Animals, Cell Differentiation physiology, Cell Line, Tumor, Cyclic AMP Response Element-Binding Protein metabolism, Gene Expression Regulation, Developmental, Growth Plate cytology, Growth Plate embryology, Growth Plate physiology, Humans, MAP Kinase Kinase 3 metabolism, MAP Kinase Kinase 6 metabolism, MAP Kinase Kinase Kinase 1 metabolism, MAP Kinase Kinase Kinase 4 metabolism, Matrix Metalloproteinase 13 genetics, Mice, Mice, Inbred C57BL, Promoter Regions, Genetic physiology, Teratocarcinoma, Transcription Factor AP-1 metabolism, Transcription, Genetic physiology, p38 Mitogen-Activated Protein Kinases metabolism, Antigens, Differentiation metabolism, CCAAT-Enhancer-Binding Protein-beta metabolism, Chondrocytes cytology, Chondrocytes physiology, Collagen Type X genetics, MAP Kinase Signaling System physiology

Abstract

GADD45beta (growth arrest- and DNA damage-inducible) interacts with upstream regulators of the JNK and p38 stress response kinases. Previously, we reported that the hypertrophic zone of the Gadd45beta(-/-) mouse embryonic growth plate is compressed, and expression of type X collagen (Col10a1) and matrix metalloproteinase 13 (Mmp13) genes is decreased. Herein, we report that GADD45beta enhances activity of the proximal Col10a1 promoter, which contains evolutionarily conserved AP-1, cAMP-response element, and C/EBP half-sites, in synergism with C/EBP family members, whereas the MMP13 promoter responds to GADD45beta together with AP-1, ATF, or C/EBP family members. C/EBPbeta expression also predominantly co-localizes with GADD45beta in the embryonic growth plate. Moreover, GADD45beta enhances C/EBPbeta activation via MTK1, MKK3, and MKK6, and dominant-negative p38alphaapf, but not JNKapf, disrupts the combined trans-activating effect of GADD45beta and C/EBPbeta on the Col10a1 promoter. Importantly, GADD45beta knockdown prevents p38 phosphorylation while decreasing Col10a1 mRNA levels but does not affect C/EBPbeta binding to the Col10a1 promoter in vivo, indicating that GADD45beta influences the transactivation function of DNA-bound C/EBPbeta. In support of this conclusion, we show that the evolutionarily conserved TAD4 domain of C/EBPbeta is the target of the GADD45beta-dependent signaling. Collectively, we have uncovered a novel molecular mechanism linking GADD45beta via the MTK1/MKK3/6/p38 axis to C/EBPbeta-TAD4 activation of Col10a1 transcription in terminally differentiating chondrocytes.

Published

2010

14. Collagen XXVII is developmentally regulated and forms thin fibrillar structures distinct from those of classical vertebrate fibrillar collagens.

Author

Plumb DA, Dhir V, Mironov A, Ferrara L, Poulsom R, Kadler KE, Thornton DJ, Briggs MD, and Boot-Handford RP

Subjects

Organ Specificity physiology, Time Factors, Collagen biosynthesis, Gene Expression Regulation, Developmental physiology, Organogenesis physiology

Abstract

We have generated an antiserum to the variable domain of mouse collagen XXVII, a recently discovered novel member of the fibrillar collagen family. Collagen XXVII protein was first detectable in the mouse at embryonic day 12.5 (E12.5). By E14.5, the protein localized to cartilage, developing dermis, cornea, the inner limiting membrane of the retina, and major arteries of the heart. However, at E18.5, collagen XXVII protein was no longer apparent in most tissues and appeared restricted mainly to cartilage where expression continued into adulthood. Type XXVII collagen immunolocalized to 10-nm-thick nonstriated fibrils that were distinct from fibrils formed by the classical fibrillar collagens. The transient nature of its expression and unusual fibrillar structure suggest that collagen XXVII plays a developmental role distinct from those of the classical fibrillar collagens.

Published

2007

15. A novel and highly conserved collagen (pro(alpha)1(XXVII)) with a unique expression pattern and unusual molecular characteristics establishes a new clade within the vertebrate fibrillar collagen family.

Author

Boot-Handford RP, Tuckwell DS, Plumb DA, Rock CF, and Poulsom R

Subjects

Amino Acid Sequence, Animals, Blotting, Western, Conserved Sequence, Gene Expression Regulation, Developmental, Humans, Mice, Molecular Sequence Data, Phylogeny, Protein Structure, Tertiary, RNA, Messenger analysis, Sequence Analysis, DNA, Takifugu, Vertebrates, Evolution, Molecular, Fibrillar Collagens chemistry, Fibrillar Collagens genetics

Abstract

The type XXVII collagen gene codes for a novel vertebrate fibrillar collagen that is highly conserved in man, mouse, and fish (Fugu rubripes). The pro(alpha)1(XXVII) chain has a domain structure similar to that of the type B clade chains (alpha1(V), alpha3(V), alpha1(XI), and alpha2(XI)). However, compared with other vertebrate fibrillar collagens (types I, II, III, V, and XI), type XXVII collagen has unusual molecular features such as no minor helical domain, a major helical domain that is short and interrupted, and a short chain selection sequence within the NC1 domain. Pro(alpha)1(XXVII) mRNA is 9 kb and expressed by chondrocytes but also by a variety of epithelial cell layers in developing tissues including stomach, lung, gonad, skin, cochlear, and tooth. By Western blotting, type XXVII antisera recognized multiple bands of 240-110 kDa in tissue extracts and collagenous bands of 150-140 kDa in the conditioned medium of the differentiating chondrogenic ATDC5 cell line. Phylogenetic analyses revealed that type XXVII, together with the closely related type XXIV collagen gene, form a new, third clade (type C) within the vertebrate fibrillar collagen family. Furthermore, the exon structure of the type XXVII collagen gene is similar to, but distinct from, those of the genes coding for the type A or B clade pro(alpha) chains.

Published

2003