Your search keyword '"cathepsin k"' showing total 4,376 results

101. METTL3 Modulates Ctsk + Lineage Supporting Cranial Osteogenesis via Hedgehog.

Author

Xu R, Sheng R, Lin W, Jiang S, Zhang D, Liu L, Lei K, Li X, Liu Z, Zhang X, Wang Y, Seriwatanachai D, Zhou X, and Yuan Q

Subjects

Animals, Mice, Cell Lineage, Cranial Sutures, Stem Cells, Zinc Finger Protein GLI1 metabolism, Zinc Finger Protein GLI1 genetics, Methyltransferases metabolism, Methyltransferases genetics, Osteogenesis physiology, Osteogenesis genetics, Hedgehog Proteins metabolism, Skull, Signal Transduction, Cathepsin K

Abstract

N6-methyladenosine (m 6 A) modification, a eukaryotic messenger RNA modification catalyzed by methyltransferase-like 3 (METTL3), plays a pivotal role in stem cell fate determination. Calvarial bone development and maintenance are orchestrated by the cranial sutures. Cathepsin K (CTSK)-positive calvarial stem cells (CSCs) contribute to mice calvarial ossification. However, the role of m 6 A modification in regulating Ctsk + lineage cells during calvarial development remains elusive. Here, we showed that METTL3 was colocalized with cranial nonosteoclastic Ctsk + lineage cells, which were also associated with GLI1 expression. During neonatal development, depletion of Mettl3 in the Ctsk + lineage cells delayed suture formation and decreased mineralization. During adulthood maintenance, loss of Mettl3 in the Ctsk + lineage cells impaired calvarial bone formation, which was featured by the increased bone porosity, enhanced bone marrow cavity, and decreased number of osteocytes with the less-developed cellular outline. The analysis of methylated RNA immunoprecipitation sequencing and RNA sequencing data indicated that loss of METTL3 reduced Hedgehog (Hh) signaling pathway. Restoration of Hh signaling pathway by crossing Sufu fl/+ alleles or by local administration of SAG21 partially rescued the abnormity. Our data indicate that METTL3 modulates Ctsk + lineage cells supporting calvarial bone formation by regulating the Hh signaling pathway, providing new insights for clinical treatment of skull vault osseous diseases., Competing Interests: Declaration of Conflicting InterestsThe authors declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article.

Published

2024

102. Inhibition of miR-29 Activity in the Myeloid Lineage Increases Response to Calcitonin and Trabecular Bone Volume in Mice.

Author

Shin, Bongjin, Hrdlicka, Henry C, Delany, Anne M, and Lee, Sun-Kyeong

Subjects

OSTEOCLASTS, TRANCE protein, CANCELLOUS bone, CALCITONIN receptors, CALCITONIN, KILLER cells, ENDOTHELIN receptors

Abstract

The miR-29-3p family (miR-29a, miR-29b, miR-29c) of microRNAs is increased during receptor activator of nuclear factor kappa-B ligand (RANKL)-induced osteoclastogenesis. In vivo, activation of a miR-29-3p tough decoy inhibitor in Cre recombinase under the control of the lysozyme 2 promoter-expressing cells (myeloid lineage) resulted in mice displaying enhanced trabecular and cortical bone volume because of decreased bone resorption. Calcitonin receptor (Calcr) is a miR-29 target that negatively regulates bone resorption. CALCR was significantly increased in RANKL-treated miR-29-decoy osteoclasts, and these cells were more responsive to the inhibitory effect of calcitonin on osteoclast formation. Further, cathepsin K (Ctsk), which is critical for resorption, was decreased in miR-29-decoy cells. CALCR is a Gs-coupled receptor and its activation raises cAMP levels. In turn, cAMP suppresses cathepsin K, and cAMP levels were increased in miR-29-decoy cells. siRNA-mediated knock-down of Calcr in miR-29 decoy osteoclasts allowed recovery of cathepsin K levels in these cells. Overall, using a novel knockin tough decoy mouse model, we identified a new role for miR-29-3p in bone homeostasis. In RANKL-driven osteoclastogenesis, as seen in normal bone remodeling, miR-29-3p promotes resorption. Consequently, inhibition of miR-29-3p activity in the myeloid lineage leads to increased trabecular and cortical bone. Further, this study documents an interrelationship between CALCR and CTSK in osteoclastic bone resorption, which is modulated by miR-29-3p. [ABSTRACT FROM AUTHOR]

Published

2021

103. Studies Conducted at Kyushu University on Extracellular Matrix Proteins Recently Published (Pathogenesis of human atheroma necrotic core: degradation of connective tissue fibers and possible involvement of cathepsin K).

Subjects

EXTRACELLULAR matrix proteins, PROTEOLYTIC enzymes, CYSTEINE proteinases, PEPTIDES, CONNECTIVE tissues, ATHEROSCLEROTIC plaque

Abstract

A recent study conducted at Kyushu University investigated the pathogenesis of human atheroma, a serious atherosclerotic lesion. The researchers examined the distribution of connective tissue fibers, such as collagen and elastic fibers, in different regions of atheroma. They found that the liponecrotic tissue in the necrotic core of atheroma is formed by the severe degradation of pre-existing connective tissue fibers, likely caused by proteolytic enzymes secreted by macrophage foam cells. This study provides insights into the formation of atheroma and the potential involvement of cathepsin K in the degradation of connective tissue fibers. [Extracted from the article]

Published

2024

104. New Findings from Jiujiang University Describe Advances in Osteoporosis (Synthesis and Biological Evaluation of Novel Piperidine-3-Carboxamide Derivatives as Anti-Osteoporosis Agents Targeting Cathepsin K).

Subjects

BIOSYNTHESIS, OSTEOPOROSIS, PROTEOLYTIC enzymes, CYSTEINE proteinases, METABOLIC bone disorders, OSTEOCLASTS

Abstract

The article reports on new advancements in osteoporosis research from Jiujiang University. The study focuses on novel piperidine-3-carboxamide derivatives designed to inhibit cathepsin K, a target for anti-osteoporosis treatment. Topics include the synthesis of these derivatives, the effectiveness of compound H-9 in bone resorption inhibition, and its potential for increasing bone mineral density in osteoporosis models.

Published

2024

105. New Heart Disease Study Findings Has Been Reported by a Researcher at University of Babylon (Assessment of Serum Cathepsin k and Lipid Profile in Chronic Coronary Syndrome Patients).

Published

2024

106. Decreased levels of cathepsin Z mRNA expressed by immune blood cells: diagnostic and prognostic implications in prostate cancer

Author

A.A.S. Batista, B.M. Franco, M.M. Perez, E.G. Pereira, T. Rodrigues, M.L. Wroclawski, F.L.A. Fonseca, and E.R. Suarez

Subjects

Cathepsin X, Cathepsin K, Prostate-specific antigen, Biopsy, Biomarker, Prostate cancer, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Cathepsin Z (CTSZ) is a cysteine protease responsible for the adhesion and migration of both immune and tumor cells. Due to its dual role, we hypothesized that the site of CTSZ expression could be determinant of the pro- or anti-tumorigenic effects of this enzyme. To test this hypothesis, we analyzed CTSZ expression data in healthy and tumor tissues by bioinformatics and evaluated the expression levels of CTSZ mRNA in the blood cells of prostate cancer (PCa) patients by qRT-PCR compared with healthy subjects, evaluating its diagnostic and prognostic implications for this type of cancer. Immune cells present in the blood of healthy patients overexpress CTSZ. In PCa, we found decreased CTSZ mRNA levels in blood cells, 75% lower than in healthy subjects, that diminished even more during biochemical relapse. CTSZ mRNA in the blood cells had an area under the curve for PCa diagnosis of 0.832, with a 93.3% specificity, and a positive likelihood ratio of 9.4. The site of CTSZ mRNA expression is fundamental to determine its final role as a protective determinant in PCa, such as CTSZ mRNA in the blood cells, or a malignant determinant, such as found for CTSZ expressed in high levels by different types of primary and metastatic tumors. Low CTSZ mRNA expression in the total blood is a possible PCa marker complementary to prostate-specific antigen (PSA) for biopsy decisions, with the potential to eliminate unnecessary biopsies.

Published

2021

107. Cathepsin K (Clone EPR19992) Demonstrates Uniformly Positive Immunoreactivity in Renal Oncocytoma, Chromophobe Renal Cell Carcinoma, and Distal Tubules.

Author

Iakymenko, Oleksii A., Delma, Katiana S., Jorda, Merce, and Kryvenko, Oleksandr N.

Subjects

*RENAL cell carcinoma, *KIDNEY tumors, *MOLECULAR cloning, *TRANSCRIPTION factors, *EOSINOPHILIA

Abstract

Introduction. Cathepsin K is overexpressed in several tumors associated with microphthalmia transcription factor (MiTF) family or mechanistic target of rapamycin (mTOR) upregulation. Among renal neoplasms, MiTF translocation renal cell carcinoma (RCC), perivascular epithelioid cell neoplasms (PEComa), and eosinophilic solid and cystic RCC have demonstrated Cathepsin K immunoreactivity. In this study, we demonstrate a uniform Cathepsin K expression in oncocytoma, chromophobe RCC (CHRCC), and distal tubules. Design. We stained 13 oncocytomas, 13 CHRCC, 14 clear cell RCC (CCRCC), 9 papillary RCC (PRCC), 9 PEComas, and 5 MiTF RCC. Additionally, we assessed immunoreactivity for Cathepsin K in non-neoplastic renal parenchyma. Immunolabeling was performed on regularly charged slides from formalin-fixed paraffin-embedded tissue with monoclonal anti-rabbit antibodies to human Cathepsin K (clone EPR19992, Abcam). Results. All oncocytomas demonstrated diffuse strong cytoplasmic immunolabeling. CHRCC demonstrated uniform less intense immunolabeling in all cases with membranous accentuation. The assessment of the non-neoplastic renal parenchyma in all cases showed strong cytoplasmic immunoreaction in distal tubules and proximal tubules stained faintly. Mesangial cells were not immunoreactive. All MiTF RCC and PEComas were immunoreactive for Cathepsin K, whereas CCRCC and PRCC were negative in all cases. Conclusions. In this study, we expand the spectrum of renal neoplasms reactive with a particular clone of Cathepsin K (EPR19992). Distal tubules are strongly immunoreactive for Cathepsin K. Our conclusions need to be taken into consideration when differential diagnosis includes MiTF RCC or PEComa and this Cathepsin K clone is included in the immunohistochemical panel. This newer antibody clone was not tested in prior publications, potentially explaining the difference in conclusions. [ABSTRACT FROM AUTHOR]

Published

2021

108. The genotypic and phenotypic spectrum of pycnodysostosis in Saudi Arabia: Novel variants and clinical findings.

Author

Mushiba, Aziza M., FAQEIH, EISSA, Saleh, Mohammed A., Ramzan, Khushnooda, Imtiaz, Faiqa, Al‐Owain, Mohammed, Alhashem, Amal M., and Alswaid, Abdulrahman

Abstract

Pycnodysostosis is characterized by short stature, osteosclerosis, acro‐osteolysis, increased tendency of fractures, and distinctive dysmorphic features. It is a rare autosomal recessive disease caused by biallelic CTSK mutations. The clinical details of 18 patients from Saudi Arabia were reviewed. Short stature, osteopetrosis, acro‐osteolysis, and distinctive facial dysmorphism were documented in all cases. Our results highlight the significant complications associated with this disease. The large anterior fontanelle is one of the cardinal signs of this disease; however, half of our patients had small fontanelles and a quarter had craniosynostosis, which caused optic nerve compression. Sleep apnea was of the major complications in three patients. Bone fracture can be a presenting symptom, and in our patients it mainly occurred after the age of 3 years. Bone marrow suppression was seen in a single patient of our cohort who was misdiagnosed initially with malignant osteopetrosis. In this study, we also describe two novel (c.5G > A [p.Trp2Ter], c.538G > A [p.Gly180Ser]) and two reported (c.244–29 A > G, c.830C > T [p.Ala277Val]) CTSK mutations. Our results indicate that the recurrent intronic variant, c.244–29 A > G is likely to be a founder mutation, as it was found in 78% (14/18 patients) of our cohort belonging to the same tribe. [ABSTRACT FROM AUTHOR]

Published

2021

109. Cathepsin K deficiency promotes alveolar bone regeneration by promoting jaw bone marrow mesenchymal stem cells proliferation and differentiation via glycolysis pathway.

Author

Zhang, Wuyang, Dong, Zhiwei, Li, Dengke, Li, Bei, Liu, Yuan, Zheng, Xueni, Liu, Hui, Zhou, Hongzhi, Hu, Kaijin, and Xue, Yang

Subjects

*GLYCOLYSIS, *MESENCHYMAL stem cell differentiation, *BONE regeneration, *BONE marrow, *MESENCHYMAL stem cells, *MONOCARBOXYLATE transporters

Abstract

Objectives: To clarify the possible role and mechanism of Cathepsin K (CTSK) in alveolar bone regeneration mediated by jaw bone marrow mesenchymal stem cells (JBMMSC). Materials and Methods: Tooth extraction models of Ctsk knockout mice (Ctsk‐/‐) and their wildtype (WT) littermates were used to investigate the effect of CTSK on alveolar bone regeneration. The influences of deletion or inhibition of CTSK by odanacatib (ODN) on proliferation and osteogenic differentiation of JBMMSC were assessed by CCK‐8, Western blot and alizarin red staining. To explore the differently expressed genes, RNA from WT and Ctsk‐/‐ JBMMSC was sent to RNA‐seq. ECAR, glucose consumption and lactate production were measured to identify the effect of Ctsk deficiency or inhibition on glycolysis. At last, we explored whether Ctsk deficiency or inhibition promoted JBMMSC proliferation and osteogenic differentiation through glycolysis. Results: We found out that Ctsk knockout could promote alveolar bone regeneration in vivo. In vitro, we confirmed that both Ctsk knockout and inhibition by ODN could promote proliferation of JBMMSC, up‐regulate expression of Runx2 and ALP, and enhance matrix mineralization. RNA‐seq results showed that coding genes of key enzymes in glycolysis were significantly up‐regulated in Ctsk‐/‐ JBMMSC, and Ctsk deficiency or inhibition could promote glycolysis in JBMMSC. After blocking glycolysis by 3PO, the effect of Ctsk deficiency or inhibition on JBMMSC's regeneration was blocked subsequently. Conclusions: Our findings revealed that Ctsk knockout or inhibition could promote alveolar bone regeneration by enhancing JBMMSC regeneration via glycolysis. These results shed new lights on the regulatory mechanism of CTSK on bone regeneration. [ABSTRACT FROM AUTHOR]

Published

2021

110. In vivo fluorescence reflectance imaging of protease activity in a mouse model of post-traumatic osteoarthritis

Author

Satkunananthan, PB, Anderson, MJ, De Jesus, NM, Haudenschild, DR, Ripplinger, CM, and Christiansen, BA

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Physical Injury - Accidents and Adverse Effects, Aging, 2.1 Biological and endogenous factors, Aetiology, Musculoskeletal, Animals, Anterior Cruciate Ligament Injuries, Bone Resorption, Cartilage, Articular, Cathepsin K, Disease Models, Animal, Female, Knee Injuries, Knee Joint, Male, Matrix Metalloproteinases, Mice, Molecular Imaging, Optical Imaging, Osteoarthritis, Knee, Peptide Hydrolases, X-Ray Microtomography, Fluorescence reflectance imaging, Post-traumatic osteoarthritis, Inflammation, Bone resorption, Protease, Cathepsin, Biomedical Engineering, Human Movement and Sports Sciences, Arthritis & Rheumatology, Clinical sciences, Sports science and exercise

Abstract

ObjectiveJoint injuries initiate a surge of inflammatory cytokines and proteases that contribute to cartilage and subchondral bone degeneration. Detecting these early processes in animal models of post-traumatic osteoarthritis (PTOA) typically involves ex vivo analysis of blood serum or synovial fluid biomarkers, or histological analysis of the joint. In this study, we used in vivo fluorescence reflectance imaging (FRI) to quantify protease, matrix metalloproteinase (MMP), and Cathepsin K activity in mice following anterior cruciate ligament (ACL) rupture. We hypothesized that these processes would be elevated at early time points following joint injury, but would return to control levels at later time points.DesignMice were injured via tibial compression overload, and FRI was performed at time points from 1 to 56 days after injury using commercially available activatable fluorescent tracers to quantify protease, MMP, and cathepsin K activity in injured vs uninjured knees. PTOA was assessed at 56 days post-injury using micro-computed tomography and whole-joint histology.ResultsProtease activity, MMP activity, and cathepsin K activity were all significantly increased in injured knees relative to uninjured knees at all time points, peaking at 1-7 days post-injury, then decreasing at later time points while still remaining elevated relative to controls.ConclusionsThis study establishes FRI as a reliable method for in vivo quantification of early biological processes in a translatable mouse model of PTOA, and provides crucial information about the time course of inflammation and biological activity following joint injury. These data may inform future studies aimed at targeting these early processes to inhibit PTOA development.

Published

2014

111. Cathepsin K maintains the compartment of bone marrow T lymphocytes in vivo.

Author

Hausinger, Renate, Hackl, Marianne, Jardon Alvarez, Ana, Kehr, Miriam, Romero Marquez, Sandra, Hettler, Franziska, Kehr, Christian, Grziwok, Sandra, Schreck, Christina, Peschel, Christian, Istvánffy, Rouzanna, and Oostendorp, Robert A. J.

Subjects

*T cells, *BONE marrow, *CELL proliferation, *BONE marrow cells, *HEMATOPOIETIC stem cells

Abstract

In this study, we investigated the influence of the loss of cathepsin K (Ctsk) gene on the hematopoietic system in vitro and in vivo. We found that cultures with lineage− SCA1+ KIT+ (LSK) cells on Ctsk deficient stromal cells display reduced colony formation and proliferation, with increased differentiation, giving rise to repopulating cells with reduced ability to repopulate the donor LSKs and T cell compartments in the bone marrow (BM). Subsequent in vivo experiments showed impairment of lymphocyte numbers, but, gross effects on early hematopoiesis or myelopoiesis were not found. Most consistently in in vivo experimental settings, we found a significant reduction of (donor) T cell numbers in the BM. Lymphocyte deregulation is also found in transplantation experiments, which revealed that Ctsk is required for optimal regeneration of small populations of T cells, particularly in the BM, but also of thymic B cells. Interestingly, cell nonautonomous Ctsk regulates both B and T cell numbers, but T cell numbers in the BM require an additional autonomous Ctsk‐dependent process. Thus, we show that Ctsk is required for the maintenance of hematopoietic stem cells in vitro, but in vivo, Ctsk deficiency most strongly affects lymphocyte homeostasis, particularly of T cells in the BM. [ABSTRACT FROM AUTHOR]

Published

2021

112. Uterine leiomyosarcomas with osteoclast-like giant cells associated with high expression of RUNX2 and RANKL.

Author

Terasaki, Mika, Terasaki, Yasuhiro, Wakamatsu, Kyoko, Kuwahara, Naomi, Yoneyama, Koichi, Kawase, Rieko, Kurose, Keisuke, Toda, Etsuko, Endo, Yoko, Kunugi, Shinobu, Kajimoto, Yusuke, and Shimizu, Akira

Abstract

Uterine leiomyosarcoma (ULMS) with osteoclast-like giant cells (OLGCs) has been reported as a rare phenomenon in ULMS, and its clinico-pathological features and tumorigenesis remain unclear. We recently reported high expression of receptor activator of nuclear factor κB ligand (RANKL) in ULMS with OLGCs. As osteoblasts produce RANKL, in this study, we analyzed the expression of Runt-related transcription factor 2 (RUNX2), a critical transcription factor for osteoblasts, and osteoclast-related proteins in three cases of ULMS with OLGCs as well as five conventional ULMSs and nine leiomyomas. Immunohistochemistry and real-time reverse transcription quantitative polymerase chain reaction analyses showed high expression of RUNX2 and RANKL in ULMS with OLGCs. In these cases, macrophages expressed receptor activator of nuclear factor κB (RANK), and OLGCs expressed osteoclast-related proteins (nuclear factor of activated T cells, cytoplasmic 1 (NFATc1), and cathepsin K). Accumulation sites of cathepsin K–positive OLGCs showed hemorrhagic appearance and degraded type IV collagen. We reviewed reported cases of ULMS with OLGCs, including ours, and found that they presented an aggressive course even at stage I. Furthermore, metastatic lesions showed similar histological features to those of OLGC association in ULMS. Here, we show that tumor cells in ULMS with OLGCs highly express RUNX2 and RANKL and that osteoclastic differentiation of macrophages occurs in the tumor tissue. [ABSTRACT FROM AUTHOR]

Published

2021

113. Preclinical evaluation of [11C]L‐235 as a radioligand for Positron Emission Tomography cathepsin K imaging in bone.

Author

Bennacef, Idriss, Rubins, Daniel, Riffel, Kerry, Williams, Mangay, Posavec, Diane J., Holahan, Marie A., Purcell, Mona L., Haley, Hyking D., Wolf, Mary, Stachel, Shawn J., Lubbers, Laura S., Wesolowski, Gregg A., Duong, Le T., Hamill, Terence G., Evelhoch, Jeffrey L., and Hostetler, Eric D.

Subjects

*POSITRON emission tomography, *RADIOACTIVE tracers, *ANIMAL young, *COMPUTED tomography, *DIAGNOSTIC imaging, *AUTORADIOGRAPHY

Abstract

The cathepsin K (CatK) enzyme is abundantly expressed in osteoclasts, and CatK inhibitors have been developed for the treatment of osteoporosis. In our effort to support discovery and clinical evaluations of a CatK inhibitor, we sought to discover a radioligand to determine target engagement of the enzyme by therapeutic candidates using positron emission tomography (PET). L‐235, a potent and selective CatK inhibitor, was labeled with carbon‐11. PET imaging studies recording baseline distribution of [11C]L‐235, and chase and blocking studies using the selective CatK inhibitor MK‐0674 were performed in juvenile and adult nonhuman primates (NHP) and ovariectomized rabbits. Retention of the PET tracer in regions expected to be osteoclast‐rich compared with osteoclast‐poor regions was examined. Increased retention of the radioligand was observed in osteoclast‐rich regions of juvenile rabbits and NHP but not in the adult monkey or adult ovariectomized rabbit. Target engagement of CatK was observed in blocking studies with MK‐0674, and the radioligand retention was shown to be sensitive to the level of MK‐0674 exposure. [11C]L‐235 can assess target engagement of CatK in bone only in juvenile animals. [11C]L‐235 may be a useful tool for guiding the discovery of CatK inhibitors. [ABSTRACT FROM AUTHOR]

Published

2021

114. Les traitements en cours de développement dans l'arthrose.

Author

Latourte, Augustin and Richette, Pascal

Abstract

Les traitements actuellement disponibles pour la prise en charge pharmacologique de l'arthrose sont limités, soit du fait d'une efficacité modeste, soit par un risque d'effets secondaires potentiellement dangereux dans une population âgée, souvent porteuse de comorbidités. La prévalence de l'arthrose ne cesse d'augmenter et le besoin de nouveaux traitements pour traiter les symptômes de l'arthrose, mais aussi pour ralentir ou stopper la progression de la maladie, est donc majeur. La meilleure compréhension de la physiopathologie de l'arthrose a permis l'identification de nouvelles cibles thérapeutiques, et certains traitements relatifs à ces cibles sont actuellement à l'étude dans des essais thérapeutiques de phase 2 ou 3. Citons notamment les anticorps anti-NGF, la sprifermine, les inhibiteurs de la voie Wnt ou de la cathepsine K, molécules qui ont donné des résultats parfois prometteurs. Leur profil de tolérance reste à préciser sur le long terme. Aussi, la balance bénéfice-risque des anticorps anti-NGF, inducteurs d'arthropathies rapidement progressives, reste à préciser. Ces nouveaux traitements pourraient toutefois offrir de nouvelles perspectives thérapeutiques pour les patients dans les prochaines années. The pharmalogical therapies currently available for the management of osteoarthritis are limited, either because of they have a modest effect-size, or because they can expose elder patients with often multiple comorbidities to a substantial risk of potentially dangerous side effects. The prevalence of osteoarthritis increases consistently, and there is therefore a major need for new treatments to treat the symptoms of osteoarthritis, but also to slow or stop the progression of the disease. The better understanding of the pathophysiology of osteoarthritis has led to the identification of new therapeutic targets, and some drugs related to these targets are currently being studied in phase 2 or 3 randomized controlled trials. These include anti-NGF antibodies, sprifermin, Wnt or cathepsin K inhibitors, some of which have shown promising results. Their long-term tolerance profile remains to be determined. Also, the benefit:risk ratio of anti-NGF antibodies, which induce rapidly progressive arthropathies, remains to be determined. These new treatments could, however, offer new therapeutic prospects for patients in the coming years. [ABSTRACT FROM AUTHOR]

Published

2021

115. The Mechanism Switching the Osteoclast From Short to Long Duration Bone Resorption

Author

Jean-Marie Delaisse, Kent Søe, Thomas Levin Andersen, Aleksandra Maria Rojek, and Niels Marcussen

Subjects

osteoporosis, ruffled border, resorption trenches, cathepsin K, collagen, sealing zone, Biology (General), QH301-705.5

Abstract

The current models of osteoclastic bone resorption focus on immobile osteoclasts sitting on the bone surface and drilling a pit into the bone matrix. It recently appeared that many osteoclasts also enlarge their pit by moving across the bone surface while resorbing. Drilling a pit thus represents only the start of a resorption event of much larger amplitude. This prolonged resorption activity significantly contributes to pathological bone destruction, but the mechanism whereby the osteoclast engages in this process does not have an answer within the standard bone resorption models. Herein, we review observations that lead to envision how prolonged resorption is possible through simultaneous resorption and migration. According to the standard pit model, the “sealing zone” which surrounds the ruffled border (i.e., the actual resorption apparatus), “anchors” the ruffled border against the bone surface to be resorbed. Herein, we highlight that continuation of resorption demands that the sealing zone “glides” inside the cavity. Thereby, the sealing zone emerges as the structure responsible for orienting and displacing the ruffled border, e.g., directing resorption against the cavity wall. Importantly, sealing zone displacement stringently requires thorough collagen removal from the cavity wall - which renders strong cathepsin K collagenolysis indispensable for engagement of osteoclasts in cavity-enlargement. Furthermore, the sealing zone is associated with generation of new ruffled border at the leading edge, thereby allowing the ruffled border to move ahead. The sealing zone and ruffled border displacements are coordinated with the migration of the cell body, shown to be under control of lamellipodia at the leading edge and of the release of resorption products at the rear. We propose that bone resorption demands more attention to osteoclastic models integrating resorption and migration activities into just one cell phenotype.

Published

2021

116. Serum concentration of matrix metalloproteinases and angiogenic factors in patients with venous leg ulcers.

Author

Kolano, Paweł, Bednarski, Igor A., Kraska-Gacka, Marzena, Narbutt, Joanna, and Lesiak, Aleksandra

Subjects

*SERUM, *MATRIX metalloproteinases, *VASCULAR endothelial growth factors, *CONTROL groups, *ENZYME-linked immunosorbent assay

Abstract

Introduction: Leg ulcers are a frequently observed medical problem affecting 3-5% of the general population over 65 years of age. The most common factor responsible for the development of leg ulcers is chronic venous insufficiency (CVI). It is believed that during the formation of an ulcer there are two processes occurring simultaneously, extracellular matrix (ECM) degradation and angiogenesis in which several proteins including matrix metalloproteinases, angiogenic and regulatory factors are engaged. Aim: To determine the serum concentration of matrix metalloproteinase-1 (MMP-1), -9 (MMP-9), tissue inhibitors of metalloproteinases-1 (TIMP-1), angiogenin and vascular endothelial growth factor (VEGF) in patients suffering from venous leg ulcers and in the healthy control group. Material and methods: The study group consisted of 71 Caucasians (39 patients, 32 controls). To evaluate the serum concentration of MMP-1, MMP-9, TIMP-1, VEGF and angiogenin, the ELISA technique was used. Results: Mean MMP-1 and MMP-9 concentrations in the study group were 14.16 ±2.98 and 12.45 ±3.85 ng/ml, respectively, and in controls 6.08 ±2.51 ng/ml and 6.77 ±2.41 ng/ml, respectively and both differences were statistically significant (p < 0.001). There was no significant difference between the study and the control group in TIMP-1 concentration. Mean VEGF and ANG concentrations in the study group were 589.3 ±346.2 pg/ml and 1802.0 ±415.7 pg/ml, respectively, and in controls 220.3 ±110.4 pg/ml and 1229.0 ±337.7 pg/ml, respectively and both differences were statistically significant (p < 0.001). Conclusions: Lack of significant differences in the concentration of TIMP-1 between the control and the study group confirms that proteolysis is a hallmark of CVI, but increased concentration of VEGF and angiogenin in the study group compared to the control group shows that angiogenesis occurs simultaneously with ECM remodelling. [ABSTRACT FROM AUTHOR]

Published

2021

117. Inhibitory effect of cathepsin K inhibitor (ODN-MK-0822) on invasion, migration and adhesion of human breast cancer cells in vitro.

Author

Vashum, Yaongamphi, Premsingh, Riya, Kottaiswamy, Amuthavalli, Soma, Mathangi, Padmanaban, Abirami, Kalaiselvan, Parkavi, and Samuel, Shila

Abstract

Approximately 90% of patients with advanced breast cancer develop bone metastases; an event that results in severe decrease of quality of life and a drastic deterioration in prognosis. Therefore, to increase the survival of breast cancer patients, the development of new therapeutic strategies to impair metastatic process and skeletal complications is critical. Previous studies on the role of cathepsin K (CTSK) in metastatic spreading led to several strategies for inhibition of this molecule such as MIV-711 (Medivir), balicatib and odanacatib (ODN) which were on trial in the past. The present study intended to assess the anti-metastatic efficacy of ODN in breast cancer cells. Human breast cancer cell lines MDA-MB-231 were treated with different concentrations of ODN and performed invasion, adhesion and migration assays and, RT-PCR and western blot to evaluate the effect of ODN on the metastatic potential of breast cancer cells. ODN markedly decreased wound healing cell migration, invasion and adhesion at a dose dependent manner. ODN inhibits cell invasion by decreasing the matrix metalloproteinase (MMP-9) with the upregulation of TIMP-1 expression. ODN effectively inhibited the phosphorylation of extracellular signal-regulated kinase (ERK), p38, and c-Jun N-terminal Kinase (JNK), and blocked the expression of β-integrins and FAK proteins. ODN also significantly inhibited PI3K downstream targets Rac1, Cdc42, paxillin and Src which are critical for cell adhesion, migration and cytoskeletal reorganization. ODN exerts anti-metastatic action through inhibition of signaling pathway for MMP-9, PI3K and MAPK. This indicates potential therapeutic effects of ODN in the treatment of metastatic breast cancer. [ABSTRACT FROM AUTHOR]

Published

2021

118. The Predictive Value of Osteocalcin, Granulin, Cathepsin K and Some Other Biomarkers in Women with Premature Ovarian Failure.

Author

Ibraheem, Mahmood Khalil, Mutazsabahahmied, Algburi, Firas Shawqi, and Alobaidi, Amina Hamed

Subjects

BLOOD serum analysis, BIOMARKERS, PREDICTIVE tests, OSTEOCALCIN, GROWTH factors, PHOSPHORUS, PROTEOLYTIC enzymes, WOMEN, VITAMIN D, PARATHYROID hormone, OVARIAN diseases, DESCRIPTIVE statistics, CALCIUM

Abstract

Background: Premature ovarian failure (POF), often and misleadingly referred to as 'premature menopause', is defined as a loss of ovarian activity before the age of 40 years and is characterized by irregular or absent periods and reduced fertility. Symptoms include those associated with the natural menopause (night sweats and vaginal dryness), and with the long-term adverse effects of estrogen deficiency (osteoporosis and cardiovascular disease): the latter is believed to explain the shorter life expectancy associated with POF. Aim: To determine the predictive value of serum osteocalcin(OC), granulin(GRN), cathepsin k (CTK), vitamin D, parathyroid hormones (PTH), calcium and phosphrus as biomarkers for POF. Method: Sixty (60) women with idiopathic POF with thirty (30) women as control groups were included in the study. Baseline investigation in all subjects included serum Osteocalcin(OC), granulin(GRN), cathepsin k (CTK), vitamin D, parathyroid hormones (PTH), calcium and phosphrus levels were estimated using the appropriate assays for each. Results: The mean serum levels of Osteocalcin, Ganulin, Parathyroid hormones, vitamin D and phosphorus, were significantly higher in women with POF, when compared to healthy controls (P=<0.05). However, mean serum levels of cathepsin k and calcium in POF group were non significant differences, when compared to healthy controls. Conclusion: Osteocalcin and granulin serum levels may be used as new biomarker for the diagnosis of premature ovarian failure. [ABSTRACT FROM AUTHOR]

Published

2021

119. Effects of IL-34 and anti-IL-34 neutralizing mAb on alveolar bone loss in a ligature-induced model of periodontitis.

Author

Duarte C, Yamada C, Ngala B, Garcia C, Akkaoui J, Birsa M, Ho A, Nusbaum A, AlQallaf H, John V, and Movila A

Subjects

Animals, Male, Mice, Antibodies, Monoclonal therapeutic use, Antibodies, Monoclonal pharmacology, Cathepsin K, Disease Models, Animal, Isoenzymes, Ligation, Macrophage Colony-Stimulating Factor, Mice, Inbred C57BL, Osteoclasts drug effects, Osteogenesis drug effects, RANK Ligand metabolism, Receptor, Macrophage Colony-Stimulating Factor antagonists & inhibitors, Signal Transduction, Tartrate-Resistant Acid Phosphatase metabolism, Alveolar Bone Loss metabolism, Antibodies, Neutralizing pharmacology, Interleukins metabolism, Periodontitis immunology

Abstract

Macrophage colony-stimulating factor (M-CSF) and interleukin-34 (IL-34) are ligands for the colony-stimulating factor-1  receptor (CSF-1r) expressed on the surface of monocyte/macrophage lineage cells. The importance of coordinated signaling between M-CSF/receptor activator of the nuclear factor kappa-Β ligand (RANKL) in physiological and pathological bone remodeling and alveolar bone loss in response to oral bacterial colonization is well established. However, our knowledge about the IL-34/RANKL signaling in periodontal bone loss remains limited. Recently published cohort studies have demonstrated that the expression patterns of IL-34 are dramatically elevated in gingival crevicular fluid collected from patients with periodontitis. Therefore, the present study aims to evaluate the effects of IL-34 on osteoclastogenesis in vitro and in experimental ligature-mediated model of periodontitis using male mice. Our initial in vitro study demonstrated increased RANKL-induced osteoclastogenesis of IL-34-primed osteoclast precursors (OCPs) compared to M-CSF-primed OCPs. Using an experimental model of ligature-mediated periodontitis, we further demonstrated elevated expression of IL-34 in periodontal lesions. In contrast, M-CSF levels were dramatically reduced in these periodontal lesions. Furthermore, local injections of mouse recombinant IL-34 protein significantly elevated cathepsin K activity, increased the number of tartrate-resistant acid phosphatase (TRAP)-positive osteoclasts and promoted alveolar bone loss in periodontitis lesions. In contrast, anti-IL-34 neutralizing monoclonal antibody significantly reduced the level of alveolar bone loss and the number of TRAP-positive osteoclasts in periodontitis lesions. No beneficial effects of locally injected anti-M-CSF neutralizing antibody were observed in periodontal lesions. This study illustrates the role of IL-34 in promoting alveolar bone loss in periodontal lesions and proposes the potential of anti-IL34 monoclonal antibody (mAb)-based therapeutic regimens to suppress alveolar bone loss in periodontitis lesions., (© 2023 The Authors. Molecular Oral Microbiology published by John Wiley & Sons Ltd.)

Published

2024

120. Establishment and validation of an efficient method for the 3D culture of osteoclasts in vitro.

Author

Faqeer A, Liu J, Zhang L, Wang C, Zhou G, and Zhang Y

Subjects

Animals, Cell Differentiation, Collagen, Mice, Cell Culture Techniques, Three Dimensional methods, Macrophages cytology, Cathepsin K, Cytokines metabolism, Cells, Cultured, Osteoclasts cytology, Hydrogels, Cell Culture Techniques

Abstract

Introduction: Osteoclasts (OCs) play a crucial role in maintaining bone health. Changes in OC activity are linked to different bone diseases, making them an intriguing focus for research. However, most studies on OCs have relied on 2D cultures, limiting our understanding of their behavior. Yet, there's a lack of knowledge regarding platforms that effectively support osteoclast formation in 3D cultures., Methods: In our investigation, we explored the capacity of collagen and GelMA hydrogels to facilitate osteoclast development in 3D culture settings. We assessed the osteoclast development by using different hydrogels and cell seeding strategies and optimizing cell seeding density and cytokine concentration. The osteoclast development in 3D cultures was further validated by biochemical assays and immunochemical staining., Results: Our findings revealed that 0.3 % (w/v) collagen was conducive to osteoclast formation in both 2D and 3D cultures, demonstrated by increased multinucleation and higher TRAP activity compared to 0.6 % collagen and 5 % to 10 % (w/v) GelMA hydrogels. Additionally, we devised a "sandwich" technique using collagen substrates and augmented the initial macrophage seeding density and doubling cytokine concentrations, significantly enhancing the efficiency of OC culture in 3D conditions. Notably, we validated osteoclasts derived from macrophages in our 3D cultures express key osteoclast markers like cathepsin K and TRAP., Conclusions: To conclude, our study contributes to establishing an effective method for cultivating osteoclasts in 3D environments in vitro. This innovative approach not only promises a more physiologically relevant platform to study osteoclast behavior during bone remodeling but also holds potential for applications in bone tissue engineering., Clinical Significance: This study introduces an efficient method for cultivating osteoclasts in 3D environments in vitro. It offers a more physiologically relevant platform to investigate osteoclast behavior and holds promise to advance research in bone biology and regenerative dentistry., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2024

121. Cathepsin K: The Action in and Beyond Bone

Author

Rongchen Dai, Zeting Wu, Hang Yin Chu, Jun Lu, Aiping Lyu, Jin Liu, and Ge Zhang

Subjects

Cathepsin K, osteoclast, bone resorption, osteoporosis, osteoarthritis, Cathepsin K inhibitor, Biology (General), QH301-705.5

Abstract

Cathepsin K (CatK) is one of the most potent proteases in lysosomal cysteine proteases family, of which main function is to mediate bone resorption. Currently, CatK is among the most attractive targets for anti-osteoporosis drug development. Although many pharmaceutical companies are working on the development of selective inhibitors for CatK, there is no FDA approved drug till now. Odanacatib (ODN) developed by Merck & Co. is the only CatK inhibitor candidate which demonstrated high therapeutic efficacy in patients with postmenopausal osteoporosis in Phase III clinical trials. Unfortunately, the development of ODN was finally terminated due to the cardio-cerebrovascular adverse effects. Therefore, it arouses concerns on the undesirable CatK inhibition in non-bone sites. It is known that CatK has far-reaching actions throughout various organs besides bone. Many studies have also demonstrated the involvement of CatK in various diseases beyond the musculoskeletal system. This review not only summarized the functional roles of CatK in bone and beyond bone, but also discussed the potential relevance of the CatK action beyond bone to the adverse effects of inhibiting CatK in non-bone sites.

Published

2020

122. Whole‐exome sequencing identified a novel variant in an Iranian patient affected by pycnodysostosis

Author

Ehsan Razmara, Homeyra Azimi, Amirreza Bitaraf, Mohammad Ali Daneshmand, Mohammad Galehdari, Maryam Dokhanchi, Elika Esmaeilzadeh‐Gharehdaghi, and Masoud Garshasbi

Subjects

cathepsin K, nonsense variant, pycnodysostosis, rare disease, whole‐exome sequencing, Genetics, QH426-470

Abstract

Abstract Background Whole‐exome sequencing (WES) has emerged as a successful diagnostic tool in molecular genetics laboratories worldwide. In this study, we aimed to find the potential genetic cause of skeletal disease, a heterogeneous disease, revealing the obvious short stature phenotype. In an Iranian family, we used solo‐WES in a suspected patient to decipher the potential genetic cause(s). Methods A comprehensive clinical and genotyping examination was applied to suspect the disease of the patient. The solo clinical WES was exploited, and the derived data were filtered according to the standard pipelines. In order to validate the WES finding, the region harboring the candidate variant in the CTSK gene was amplified from genomic DNA and sequenced directly by Sanger sequencing. Results Sequence analysis revealed a rare novel nonsense variant, p.(Trp320*); c.905G>A, in the CTSK gene (NM_000396.3). In silico analysis shed light on the contribution of the variant to the pathogenicity of pycnodysostosis. This variant was confirmed by Sanger sequencing and further clinical examinations of the patient confirmed the disease. Conclusion The present study shows a rare variant of the CTSK gene, which inherited as autosomal recessive, in an Iranian male patient with pycnodysostosis. Taken together, the novel nonsense CTSK variant meets the criteria of being likely pathogenic according to the American College of Medical Genetics and Genomics‐the Association for Molecular Pathology (ACMG‐AMP) variant interpretation guidelines.

Published

2020

123. Associations of Serum Cathepsin K and Polymorphisms in CTSK Gene With Bone Mineral Density and Bone Metabolism Markers in Postmenopausal Chinese Women

Author

Li-hong Gao, Shan-shan Li, Hua Yue, and Zhen-lin Zhang

Subjects

cathepsin K, bone mineral density, bone metabolic markers, SNPs, postmenopausal women, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Cathepsin K plays an important role in bone resorption. The reports of the association of serum cathepsin K with bone mineral density (BMD) and bone turnover markers are conflicting and the role of serum cathepsin K as a bone turnover marker is unclear. The aims of the study were as follows: (1) to investigate the association of serum cathepsin K with BMD and markers of bone turnover and (2) to evaluate the correlations of single-nucleotide polymorphisms (SNPs) within the CTSK gene with serum cathepsin K, BMD, and markers of bone metabolism in postmenopausal Chinese women. A cross-sectional study was conducted with 1752 postmenopausal Chinese women. Four tagging SNPs (rs12085336, rs12746973, rs4379678, and rs10847) of the CTSK gene were genotyped. Serum cathepsin K of 768 and markers of bone metabolism of 1752 including serum intact PTH, 25-hydroxyvitamin D [25(OH)D], procollagen type 1 N-terminal propeptide (P1NP), and β-CrossLaps of type I collagen containing cross- linked C-telopeptide (β-CTX) were measured. The BMD of the lumbar spine and proximal femur were measured by dual-energy X-ray absorptiometry (DXA). No significant relationship was detected between serum cathepsin K and age, BMI, BMD or bone metabolic markers (all P > 0.05) after adjustment for age and BMI. We failed to identify any significant association between the genotypes or haplotypes of CTSK and BMD, bone turnover markers, or serum cathepsin K. Neither serum cathepsin K nor CTSK gene polymorphisms was correlated with BMD or bone turnover markers. Genetic polymorphisms of CTSK may not be a major contributor to variations in the serum cathepsin K or BMD in postmenopausal Chinese women. The results implied that serum cathepsin K may not be viewed as a substitute for bone turnover markers.

Published

2020

124. Multitarget-Based Virtual Screening for Identification of Herbal Substances toward Potential Osteoclastic Targets

Author

Siripat Chaichit, Pathomwat Wongrattanakamon, Busaban Sirithunyalug, Piyarat Nimmanpipug, and Supat Jiranusornkul

Subjects

Cathepsin K, V-ATPase, integrin, virtual screening, multitarget, Technology, Engineering (General). Civil engineering (General), TA1-2040, Biology (General), QH301-705.5, Physics, QC1-999, Chemistry, QD1-999

Abstract

Osteoporosis is a complex bone disease indicating porous bone with low bone mass density and fragility. Cathepsin K, V-ATPase, and αVβ3 integrin are exhibited as novel targets for osteoporosis treatment. Our preliminary study uses a state-of-the-art method, including target-based virtual screening and clustering methods to determine promising candidates with multitarget properties. Phytochemicals with osteoprotective properties from the literature are used to elucidate the molecular interactions toward three targets. The binding scores of compounds are normalized and rescored. The K-means and hierarchical clustering methods are applied to filter and define the promising compounds, and the silhouette analysis is supposed to validate the clustering method. We explore 108 herbal compounds by virtual screening and the cluster approach, and find that rutin, sagittatoside A, icariin, and kaempferitrin showed strong binding affinities against Cathepsin K, V-ATPase, and αVβ3 integrin. Dockings of candidates toward three targets also provide the protein-ligand interactions and crucial amino acids for binding. Our study provides a straightforward and less time-consuming approach to exploring the new multitarget candidates for further investigations, using a combination of in silico methods.

Published

2022

125. Differentiation of Cells Isolated from Human Femoral Heads into Functional Osteoclasts

Author

Daniel R. Halloran, Brian Heubel, Connor MacMurray, Denise Root, Mark Eskander, Sean P. McTague, Heather Pelkey, and Anja Nohe

Subjects

bone, osteoclasts, TRAP, Cathepsin K, RAW 264.7 cells, osteoarthritis, Biology (General), QH301-705.5

Abstract

Proper formation of the skeleton during development is crucial for the mobility of humans and the maintenance of essential organs. The production of bone is regulated by osteoblasts and osteoclasts. An imbalance of these cells can lead to a decrease in bone mineral density, which leads to fractures. While many studies are emerging to understand the role of osteoblasts, less studies are present about the role of osteoclasts. This present study utilized bone marrow cells isolated directly from the bone marrow of femoral heads obtained from osteoarthritic (OA) patients after undergoing hip replacement surgery. Here, we used tartrate resistant acid phosphatase (TRAP) staining, Cathepsin K, and nuclei to identity osteoclasts and their functionality after stimulation with macrophage-colony stimulation factor (M-CSF) and receptor activator of nuclear factor kappa-β ligand (RANKL). Our data demonstrated that isolated cells can be differentiated into functional osteoclasts, as indicated by the 92% and 83% of cells that stained positive for TRAP and Cathepsin K, respectively. Furthermore, isolated cells remain viable and terminally differentiate into osteoclasts when stimulated with RANKL. These data demonstrate that cells isolated from human femoral heads can be differentiated into osteoclasts to study bone disorders during development and adulthood.

Published

2022

126. Nonclinical and clinical pharmacological characterization of the potent and selective cathepsin K inhibitor MIV-711

Author

Erik Lindström, Biljana Rizoska, Ian Henderson, Ylva Terelius, Markus Jerling, Charlotte Edenius, and Urszula Grabowska

Subjects

Cathepsin K, Osteoarthritis, CTX-I, NTX-I, CTX-II, Subchondral bone, Medicine

Abstract

Abstract Background Cathepsin K is an attractive therapeutic target for diseases in which bone resorption is excessive such as osteoporosis and osteoarthritis (OA). The current paper characterized the pharmacological profile of the potent and selective cathepsin K inhibitor, MIV-711, in vitro and in cynomolgus monkeys, and assessed translation to human based on a single dose clinical study in man. Methods The potency and selectivity of MIV-711 were assessed in vitro using recombinant enzyme assays and differentiated human osteoclasts. MIV-711 was administered to healthy cynomolgus monkeys (3–30 µmol/kg, p.o.). Plasma levels of MIV-711 and the bone resorption biomarker CTX-I were measured after single dose experiments, and urine levels of CTX-I, NTX-I and CTX-II biomarkers were measured after repeat dose experiments. The safety, pharmacokinetics and pharmacodynamics (serum CTX-I) of MIV-711 were assessed in human healthy subjects after single ascending doses from 20 to 600 mg. Results MIV-711 was a potent inhibitor of human cathepsin K (Ki: 0.98 nmol/L) with > 1300-fold selectivity towards other human cathepsins. MIV-711 inhibited human osteoclast-mediated bone resorption with an IC50 value of 43 nmol/L. Single oral doses of MIV-711 to monkeys reduced plasma levels of CTX-I in a dose-dependent fashion by up to 57% at trough. The effect on CTX-I was linearly correlated to the plasma exposure of MIV-711, while the efficacy duration outlasted plasma exposure. Repeat oral dosing with MIV-711 also reduced urinary levels of the bone resorption biomarkers CTX-I (by 93%) and NTX-I (by 71%) and the cartilage degradation biomarker CTX-II (by 71%). MIV-711 was safe and well-tolerated when given as single ascending doses to healthy subjects. MIV-711 reduced serum CTX-I levels in a dose-dependent manner by up to 79% at trough. The relationship between MIV-711 exposure and effects on these biomarkers in humans was virtually identical when compared to the corresponding monkey data. Conclusions MIV-711 is a potent and selective cathepsin K inhibitor with dose-dependent effects on biomarkers of bone and cartilage degradation in monkey and human. Taken together, MIV-711 shows promise for the treatment of bone and cartilage related disorders in humans, such as OA. Trial Registration EudraCT number 2011-003024-12, registered on June 22nd 2011

Published

2018

127. Relationship between bone remodeling markers, bone mineral density, and severity of coronary atherosclerosis in men with stable coronary heart disease

Author

T. A. Raskina, M. V. Letaeva, A. V. Voronkina, E. B. Malyuta, O. N. Khryachkova, and O. L. Barbarash

Subjects

coronary atherosclerosis, osteopenic syndrome, cathepsin k, osteopontin, c-terminal telopeptide of type i collagen, Medicine

Abstract

The development of atherosclerosis is a complex multifactorial process, in which the markers of bone formation and resorption play an important role and which is closely related to the calcification of the vessel intima and fibrous plaques.Objective: to assess the relationship between bone remodeling markers (cathepsin K, C-terminal telopeptide of type I collagen (CTX-I) and osteopontin), bone mineral density (BMD), and severity of coronary atherosclerosis in men with stable coronary heart disease (CHD).Patients and methods. The investigation enrolled 102 male patients with verified stable CHD. Coronary angiographic and densitometric findings and blood cathepsin K, osteopontin, and CTX-I concentrations were assessed.Results.The concentration of cathepsin K and CTX-I was significantly higher and that of osteopontin was significantly lower in patients with CHD than in men without CHD. There was no association of the level of bone remodeling markers with the type of coronary artery lesion and the severity of coronary atherosclerosis. Cathepsin K concentrations in patients with a high SYNTAX score of coronary atherosclerosis were shown to be 5.5 times lower in the presence of osteopenic syndrome (OPS) than in those with the similar severity of atherosclerosis and normal BMD. Analysis of osteopontin and CTX-I levels from the standpoint of the presence of OPS suggests that there are no differences in relation to both the type of coronary vessel lesion and its severity. Conclusion. Current data suggest that there are common mechanisms for the development of two socially significant conditions: atherosclerosis and osteoporosis (OP). The phenomenon of concomitant development of these diseases has been studied mainly in postmenopausal women. Today, however, OP is also increasingly found in men, associating with more severe manifestations of coronary atherosclerosis than in patients with no signs of osteopenia.

Published

2018

128. Cathepsin K associates with lymph node metastasis and poor prognosis in oral squamous cell carcinoma

Author

Frank K. Leusink, Eleftherios Koudounarakis, Michael H. Frank, Ronald Koole, Paul J. van Diest, and Stefan M. Willems

Subjects

Oral squamous cell carcinoma, Cathepsin K, Lymph node metastasis, Prognosis, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Lymph node metastasis (LNM) is a major determinant of prognosis and treatment planning of oral squamous cell carcinoma (OSCC). Cysteine cathepsins constitute a family of proteolytic enzymes with known role in the degradation of the extracellular matrix. Involvement in pathological processes, such as inflammation and cancer progression, has been proved. The aim of the study was to discover the clinicopathological and prognostic implications of cathepsin K (CTSK) expression in oral squamous cell carcinoma. Methods Eighty-three patients with primary OSCC, treated surgically between 1996 and 2000, were included. Gene expression data were acquired from a previously reported study. Human papilloma virus (HPV) status was previously determined by an algorithm for HPV-16. CTSK Protein expression was semi-quantitatively determined by immunohistochemistry in tumor and stromal cells. Expression data were correlated with various clinicopathological variables. Results Elevated gene and protein expression of CTSK were strongly associated to LNM and perineural invasion (p

Published

2018

129. The selective cathepsin K inhibitor MIV-711 attenuates joint pathology in experimental animal models of osteoarthritis

Author

Erik Lindström, Biljana Rizoska, Karin Tunblad, Charlotte Edenius, Alison M. Bendele, Don Maul, Michael Larson, Neha Shah, Valerie Yoder Otto, Chris Jerome, and Urszula Grabowska

Subjects

Cathepsin K, Osteoarthritis, HP-1, CTX-I, CTX-II, Subchondral bone, Medicine

Abstract

Abstract Background MIV-711 is a highly potent and selective cathepsin K inhibitor. The current article summarizes the therapeutic effects of MIV-711 on joint pathology in rabbits subjected to anterior cruciate ligament transection (ACLT), and the prophylactic effects on joint pathology in dogs subjected to partial medial meniscectomy, two surgical models of osteoarthritis (OA). Methods Starting 1 week after surgery, rabbits were dosed daily via oral gavage with either MIV-711 or vehicle (n = 7/group) for 7 weeks. The four treatment groups were: (1) sham + vehicle; (2) ACLT + vehicle; (3) ACLT + MIV-711, 30 µmol/kg and (4) ACLT + MIV-711, 100 µmol/kg. Subchondral bone and articular cartilage structures were assessed by µCT, histomorphometry, and scoring. Dogs subjected to partial medial meniscectomy received either MIV-711 (30 µmol/kg) or vehicle (n = 15/group) via oral gavage once daily, starting 1 day before meniscectomy, for 28 days. Cartilage degradation was assessed at the macroscopic and microscopic levels. The exposures of MIV-711 were assessed in both studies and biomarkers reflecting bone resorption (HP-1 in rabbits, CTX-I in dogs) and cartilage degradation (CTX-II) were measured. Results In ACLT rabbits, MIV-711 decreased HP-1 levels by up to 72% (p

Published

2018

130. Cathepsin K activity controls cardiotoxin‐induced skeletal muscle repair in mice

Author

Shinyu Ogasawara, Xian Wu Cheng, Aiko Inoue, Lina Hu, Limei Piao, Chenglin Yu, Hiroki Goto, Wenhu Xu, Guangxian Zhao, Yanna Lei, Guang Yang, Kaoru Kimura, Hiroyuki Umegaki, Guo‐Ping Shi, and Masafumi Kuzuya

Subjects

Cathepsin K, Apoptosis, Skeletal muscle, Injury, Remodelling, Fibrosis, Diseases of the musculoskeletal system, RC925-935, Human anatomy, QM1-695

Abstract

Abstract Background Cathepsin K (CatK) is a widely expressed cysteine protease that has gained attention because of its enzymatic and non‐enzymatic functions in signalling. Here, we examined whether CatK‐deficiency (CatK−/−) would mitigate injury‐related skeletal muscle remodelling and fibrosis in mice, with a special focus on inflammation and muscle cell apoptosis. Methods Cardiotoxin (CTX, 20 μM/200 μL) was injected into the left gastrocnemius muscle of male wild‐type (CatK+/+) and CatK−/− mice, and the mice were processed for morphological and biochemical studies. Results On post‐injection Day 14, CatK deletion ameliorated muscle interstitial fibrosis and remodelling and performance. At an early time point (Day 3), CatK−/− reduced the lesion macrophage and leucocyte contents and cell apoptosis, the mRNA levels of monocyte chemoattractant protein‐1, toll‐like receptor‐2 and toll‐like receptor‐4, and the gelatinolytic activity related to matrix metalloproteinase‐2/‐9. CatK deletion also restored the protein levels of caspase‐3 and cleaved caspase‐8 and the ratio of the BAX to the Bcl‐2. Moreover, CatK deficiency protected muscle fibre laminin and desmin disorder in response to CTX injury. These beneficial muscle effects were mimicked by CatK‐specific inhibitor treatment. In vitro experiments demonstrated that pharmacological CatK inhibition reduced the apoptosis of C2C12 mouse myoblasts and the levels of BAX and caspase‐3 proteins induced by CTX. Conclusions These results demonstrate that CatK plays an essential role in skeletal muscle loss and fibrosis in response to CTX injury, possibly via a reduction of inflammation and cell apoptosis, suggesting a novel therapeutic strategy for the control of skeletal muscle diseases by regulating CatK activity.

Published

2018

131. Advances in the discovery of cathepsin K inhibitors on bone resorption

Author

Jun Lu, Maolin Wang, Ziyue Wang, Zhongqi Fu, Aiping Lu, and Ge Zhang

Subjects

Cathepsin K, osteoclast, bone resorption, osteoporosis, cathepsin K inhibitors, Therapeutics. Pharmacology, RM1-950

Abstract

Cathepsin K (Cat K), highly expressed in osteoclasts, is a cysteine protease member of the cathepsin lysosomal protease family and has been of increasing interest as a target of medicinal chemistry efforts for its role in bone matrix degradation. Inhibition of the Cat K enzyme reduces bone resorption and thus, has rendered the enzyme as an attractive target for anti-resorptive osteoporosis therapy. Over the past decades, considerable efforts have been made to design and develop highly potent, excellently selective and orally applicable Cat K inhibitors. These inhibitors are derived from synthetic compounds or natural products, some of which have passed preclinical studies and are presently in clinical trials at different stages of advancement. In this review, we briefly summarised the historic development of Cat K inhibitors and discussed the relationship between structures of inhibitors and active sites in Cat K for the purpose of guiding future development of inhibitors.

Published

2018

132. Relation of bone mineral density with homocysteine and cathepsin K levels in postmenopausal women

Author

Madhukar Mittal, Rajeev Verma, Arvind Mishra, Ajay Singh, Vivek Kumar, K K Sawlani, M Kaleem Ahmad, Pratishtha Mishra, and Rishika Gaur

Subjects

Bone mineral density, cathepsin K, homocysteine, osteoporosis, postmenopausal, Diseases of the endocrine glands. Clinical endocrinology, RC648-665, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Background: Homocysteine (HCY) interferes with collagen cross-linking in bones and stimulates osteoclast activity. The activated osteoclasts secrete cathepsin K (CathK), a cysteine protease, in eminent quantity during bone resorption. Hyperhomocysteinemia may effect bone mineral density (BMD) through CathK. We, therefore, examined the relation between HCY and BMD along with CathK, 25-hydroxyvit-D (25[OH]D), intact parathyroid hormone (iPTH), and Vitamin B12. Materials and Methods: We recruited a total of 93 postmenopausal women between the age group of 45–60 years, attending the Endocrinology outpatient department at King George's Medical University, Lucknow. BMD was done by DXA scan using Hologic QDR1000 system. Based on the WHO criteria, patients were segregated into three groups as follows; normal bone mass, osteopenia, and osteoporosis. All women underwent routine biochemical laboratory parameters, HCY, Vitamin B12, and CathK levels. Results: Among 93 postmenopausal women, 56% (52) had osteoporosis. Nineteen percent (18) had normal BMD (mean age, 53.22 ± 8.5 years) and 23 (25%) had osteopenia (mean age 52.86 ± 6.67 years). The mean age in the osteoporetic group was 56.2 ± 6.9 years. The median (interquartile range) levels of HCY in the three groups were 14.5 μmol/L (12.2–24.7), 15.05 μmol/L (12.1–19.9) and 13.2 μmol/L (10.3–17.0), respectively. CathK levels were similar in three groups 7.6 ng/ml (7.0–80.5), 8.3 ng/ml (7.3–8.5), and 8.6 ng/ml (7.2–8.9). Both HCY and CathK were found positively associated with serum phosphorus (r = 0.584, P < 2.01 and r = 0.249, P < 0.05, respectively). Levels of HCY positively correlate with PTH (r = 0.303, P < 0.01) and inversely with Vitamin B12 (r = −0.248, P < 0.05). No significant association was seen between CathK level and 25(OH) D, iPTH, serum calcium. Conclusion: Low bone mass by DXA is a significant problem in postmenopausal females. HCY and CathK do not reliably correlate with bone loss in postmenopausal women although phosphorus metabolism may play a role.

Published

2018

133. Comparative evaluation of cathepsin K levels in gingival crevicular fluid among smoking and nonsmoking patients with chronic periodontitis

Author

Priya Lochana Gajendran, Harinath Parthasarathy, and Anupama Tadepalli

Subjects

Cathepsin K, gingival crevicular fluid, periodontitis, smoking, Dentistry, RK1-715

Abstract

Background: The aim of the study is to comparatively evaluate the levels of cathepsin K (CSTK) in gingival crevicular fluid (GCF) among smoking and nonsmoking patients with chronic periodontitis (CP). Materials and Methods: A total of 160 systemically healthy male patients were included in the study. Based on probing pocket depth, clinical attachment level, plaque index, and modified sulcular bleeding index, the patients were allotted into four groups: Group I - with forty subjects who were smokers with healthy periodontium, Group II - with forty nonsmoking subjects with healthy periodontium, Group III - forty patients who were smokers with CP, and Group IV - with forty nonsmoking CP patients. Those who claimed to have never smoked were recruited into the nonsmoker group, whereas subjects who reported smoking ≥10 cigarettes per day for more than 5 years were recruited into the smoker group. The GCF samples were collected using microcapillary pipettes and analyzed for levels of CSTK using enzyme-linked immunosorbent assay. Results: The GCF concentration of CSTK was expressed in pg/μl. The mean CSTK levels in the groups were Group I - 0.158 ± 0.043 pg/μl, Group II - 0.145 ± 0.026 pg/μl, Group III - 15.768 ± 12.40 pg/μl, and for Group IV - 11.59 ± 12.15 pg/μl, respectively. The levels of CSTK were statistically higher in Group III when compared with Group IV (P = 0.037) (P < 0.05). Conclusion: CSTK levels were significantly increased in smokers with CP than nonsmokers, suggesting a positive influence of smoking on CSTK which could possibly play a role in the increased susceptibility for osteoclastic bone destruction in smoker subjects.

Published

2018

134. Study Findings from Yanbian University Hospital Provide New Insights into Glucose Elevating Agents (Dipeptidyl Peptidase-4 Disturbs Adipocyte Differentiation Via the Negative Regulation of the Glucagon-like Peptide-1/adiponectin-cathepsin K...).

Abstract

A study conducted at Yanbian University Hospital in Jilin, China, has found that chronic psychosocial stress can lead to metabolic disorders. The study focused on the role of dipeptidyl peptidase-4 (DPP4) and cysteinyl cathepsin K (CTSK) in stress-related adipocyte differentiation. The researchers discovered that increased DPP4 activity in mice under chronic stress conditions negatively regulated the glucagon-like peptide-1 (GLP-1)/adiponectin-CTSK axis, leading to harmful changes in adipose tissue. However, DPP4 deletion and GLP-1 receptor activation were found to reverse these effects, suggesting that the DPP4/GLP-1 and adiponectin/CTSK axes could be potential therapeutic targets for individuals with stress-related metabolic disorders. [Extracted from the article]

Published

2024

135. Findings from State University of New York (SUNY) Buffalo Provides New Data on Life Science (Heparan Sulfate Selectively Inhibits the Collagenase Activity of Cathepsin K).

Abstract

New research from the State University of New York (SUNY) Buffalo provides new data on the life science topic of heparan sulfate selectively inhibiting the collagenase activity of cathepsin K. Cathepsin K is a cysteine protease that plays a role in bone resorption. The study found that heparan sulfate forms a stable complex with cathepsin K, inducing its dimerization. Heparan sulfate also has a dual role in regulating the enzymatic activity of cathepsin K, preserving its peptidase activity while inhibiting its collagenase activity. The researchers suggest that structurally defined heparan sulfate oligosaccharides could be explored as a new class of selective cathepsin K inhibitors for diseases involving excessive bone resorption. [Extracted from the article]

Published

2024

136. FDA grants Medivir's MIV-711 Rare Pediatric Disease Designation and Orphan Drug Designation for the treatment of Legg-Calve-Perthes Disease.

Abstract

Medivir AB, a pharmaceutical company, has received Rare Pediatric Disease Designation and Orphan Drug Designation from the FDA for its drug MIV-711, a selective cathepsin K inhibitor, for the treatment of Legg-Calve-Perthes Disease (LCPD). LCPD is a serious disease that primarily affects individuals aged from birth to 18 years and currently has no effective treatments. MIV-711 has shown promising results in preventing bone degradation and deformity in animal models and clinical studies, making it a potential treatment option for LCPD. The designation allows for fast track review and the possibility of receiving a Priority Review Voucher from the FDA. [Extracted from the article]

Published

2024

137. Glimpses into the molecular pathogenesis of Peyronie's disease.

Author

ten Dam, Evert-Jan P. M., van Driel, Mels F., de Jong, Igle Jan, Werker, Paul M. N., and Bank, Ruud A.

Subjects

*PENILE induration, *EXTRACELLULAR matrix proteins, *PENIS diseases, *WNT signal transduction, *COLLAGEN

Abstract

Peyronie's disease (PD) is a fibroproliferative disease of the penis. Since little is known about the molecular pathogenesis of PD, we compared the biochemical make-up of PD plaques with normal tunica albuginea to clarify pathological processes in the scarred tissue. Protein and mRNA levels were measured in plaques and in unaffected pieces of the tunica albuginea. We investigated the presence of myofibroblasts, the deposition of collagens, and some key elements of Wnt and YAP1 signaling at protein level. The expression of 45 genes, all related to collagen homeostasis and extracellular matrix proteins, was quantified. In plaques, more myofibroblasts were present, and we observed an activation of Wnt signaling and YAP1 signaling. Increased levels of the collagens types I and III confirm the fibrotic nature of plaques. The mRNA ratio of collagen types III, IV, and VI to type I was increased. The expression of lysyl hydroxylase 3 was higher, whereas a decreased expression level was seen for fibronectin and cathepsin K. The biochemical composition of plaques was different from unaffected tunica albuginea: the relative and absolute abundance of various extracellular matrix proteins were changed, as well as the quality of collagen and the level of the collagen-degrading enzyme cathepsin K. [ABSTRACT FROM AUTHOR]

Published

2020

138. Dopamine D1 receptor stimulates cathepsin K-dependent degradation and resorption of collagen I in lung fibroblasts.

Author

Diaz Espinosa, Ana M., Link, Patrick A., Sicard, Delphine, Jorba, Ignasi, Tschumperlin, Daniel J., and Haak, Andrew J.

Subjects

*COLLAGEN, *FIBROBLASTS, *ATOMIC force microscopy, *LUNGS, *DOPAMINE receptors, *EXTRACELLULAR matrix, *WOUND healing, *EXTRACELLULAR matrix proteins

Abstract

Matrix resorption is essential to the clearance of the extracellular matrix (ECM) after normal wound healing. A disruption in these processes constitutes a main component of fibrotic diseases, characterized by excess deposition and diminished clearance of fibrillar ECM proteins, such as collagen type I. The mechanisms and stimuli regulating ECM resorption in the lung remain poorly understood. Recently, agonism of dopamine receptor D1 (DRD1), which is predominantly expressed on fibroblasts in the lung, has been shown to accelerate tissue repair and clearance of ECM following bleomycin injury in mice. Therefore, we investigated whether DRD1 receptor signaling promotes the degradation of collagen type I by lung fibroblasts. For cultured fibroblasts, we found that DRD1 agonism enhances extracellular cleavage, internalization and lysosomal degradation of collagen I mediated by cathepsin K, which results in reduced stiffness of cell-derived matrices, as measured by atomic force microscopy. In vivo agonism of DRD1 similarly enhanced fibrillar collagen degradation by fibroblasts, as assessed by tissue labeling with a collagen-hybridizing peptide. Together, these results implicate DRD1 agonism in fibroblast-mediated collagen clearance, suggesting an important role for this mechanism in fibrosis resolution. [ABSTRACT FROM AUTHOR]

Published

2020

139. Identification of potential allosteric binding sites in cathepsin K based on intramolecular communication.

Author

Rocha, Gisele V., Bastos, Leonardo S., and Costa, Mauricio G. S.

Abstract

Network theory methods and molecular dynamics (MD) simulations are accepted tools to study allosteric regulation. Indeed, dynamic networks built upon correlation analysis of MD trajectories provide detailed information about communication paths between distant sites. In this context, we aimed to understand whether the efficiency of intramolecular communication could be used to predict the allosteric potential of a given site. To this end, we performed MD simulations and network theory analyses in cathepsin K (catK), whose allosteric sites are well defined. To obtain a quantitative measure of the efficiency of communication, we designed a new protocol that enables the comparison between properties related to ensembles of communication paths obtained from different sites. Further, we applied our strategy to evaluate the allosteric potential of different catK cavities not yet considered for drug design. Our predictions of the allosteric potential based on intramolecular communication correlate well with previous catK experimental and theoretical data. We also discuss the possibility of applying our approach to other proteins from the same family. [ABSTRACT FROM AUTHOR]

Published

2020

140. Management of chronic suppurative osteomyelitis in a patient with pycnodysostosis.

Author

Negromonte Gonçalves, Kalyne Kelly, Ribeiro de Lima, Caio Henrique, Gonçalves Silva, Caio César, Alves Diniz, Demóstenes, de Aguiar Soares Carneiro, Suzana Célia, and Cavalcanti do Egito Vasconcelos, Belmiro

Subjects

BIOPSY, CHRONIC diseases, FISTULA, PATIENT aftercare, LYSOSOMAL storage diseases, METRONIDAZOLE, OSTEOMYELITIS, SUBMANDIBULAR gland, TREATMENT effectiveness, CURETTAGE, CEFTRIAXONE

Abstract

Pycnodysostosis is a rare bone dysplasia that causes changes in the facial skeleton. Osteomyelitis is common in patients with this syndrome, and, among the gnathic bones, the mandible is the most commonly affected. This case report describes the treatment of a 46-year-old woman with pycnodysostosis that was associated with chronic suppurative osteomyelitis of 5 years' duration. The patient had no intraoral focus of infection or history of tooth extraction that would explain the clinical findings of pain and a left-sided submandibular fistula. After the patient received 8 days of antibiotic therapy consisting of ceftriaxone and metronidazole, surgical access was achieved through the left submandibular region, and biopsy and curettage of the lesion and excision of the associated fistula were performed. At the 2-year follow-up examination, there was no evidence of lesion recurrence. [ABSTRACT FROM AUTHOR]

Published

2020

141. A phase 1 pooled PK/PD analysis of bone resorption biomarkers for odanacatib, a Cathepsin K inhibitor.

Author

Zajic, Stefan, Stoch, S. Aubrey, McCrea, Jacqueline B., Witter, Rose, Fayad, Ghassan N., Martinho, Monika, and Stone, Julie A.

Abstract

To develop a framework for evaluating the resorption effects of Cathepsin K (CatK) inhibitors and to inform dose regimen selection, a pharmacokinetic/pharmacodynamic (PK/PD) model for odanacatib (ODN) was developed based upon data from Phase 1 studies. Pooled PK/PD data from 11 studies (N = 249) were fit reasonably to a population inhibitory sigmoid Emax model. Body weight on E0 (baseline uNTx/Cr, urinary N-terminal telopeptide normalized by creatinine) and age on Emax (fractional inhibition of the biomarker response) were significant covariates for biomarker response. Simulations of typical osteoporosis patients (by age, sex and weight) indicated minimal differences between sexes in concentration-uNTx/Cr relationship. There was no evidence that regimen (daily vs. weekly dosing) influenced the PK/PD relationship of resorption inhibition for odanacatib. PK/PD models based on data from odanacatib (ODN) Phase 1 studies demonstrated that uNTx/Cr was an appropriate bone resorption biomarker for assessment of the effects of a CatK inhibitor. The models also identified the determinants of response in the PK/PD relationship for ODN (body weight on E0 and age on Emax). [ABSTRACT FROM AUTHOR]

Published

2020

142. Abundant osteoclasts in the subchondral bone of the juvenile Thoroughbred metacarpus suggest an important role in joint maturation.

Author

Gilday, Rebecca, Richard, Hélène, Beauchamp, Guy, Fogarty, Ursula, and Laverty, Sheila

Abstract

Background: The administration of bisphosphonate medications, which target osteoclastic‐bone remodelling, to juvenile and adult racehorses is a matter of debate owing to concerns that these molecules remain bound to the bone‐mineralised matrix and may interfere with subsequent bone growth, adaptation to exercise and healing of bone microdamage in equine athletes. Osteoclasts participate in endochondral ossification, subchondral bone remodelling and bone repair. There is a knowledge gap on the role of equine osteoclast biology in the growth and maturation of joint surfaces and this information is important to inform judicious bisphosphonate use. Objectives: Measure and compare the osteoclast density in the subchondral bone of Thoroughbred (TB) distal third metacarpi (McIII) at different sites, varying depths from the articular surface and with age (0‐84 months). Study design: Ex vivo cadaveric study. Methods: McIIIs from foals, yearlings and adults were collected, fixed in formaldehyde and stored at 4°C. Sections were cut from the lateral hemi‐metacarpus, stained and scored for cartilage degeneration. Osteoclasts were counted on immunohistochemically (Cathepsin K) stained sections. Osteoclast density was compared in regions of interest (ROIs—the sagittal ridge, axial and abaxial condyle) and also at two depths (0‐3 mm and 3‐6 mm) into the subchondral bone below the osteochondral junction. Results: The osteoclast density was consistently highest in the subchondral cortical bone plate (0‐3 mm) when compared with the deeper trabecular bone in all age groups. Furthermore, the osteoclast density was significantly higher in juvenile Thoroughbreds (foals and yearlings) within both sites in the subchondral bone when compared with adults. Main limitations: The number of specimens available for study was restricted. Conclusions: Osteoclasts are important in normal McIII epiphyseal and articular surface maturation and have a propensity to localise at the osteochondral junction and subchondral cortical bone plate zone in juvenile Thoroughbreds. [ABSTRACT FROM AUTHOR]

Published

2020

143. 杜仲醇提取物可促进根尖周炎模型大鼠骨组织的愈合.

Author

大雷, 周守恒, 闫健伟, 李博, 许诺, 史春, and 高阳

Subjects

*PERIAPICAL periodontitis, *EUCOMMIA ulmoides, *BONES, *BONE resorption, *DENTAL pulp, *WESTERN diet

Abstract

BACKGROUND: Current research on Eucommia ulmoides Oliv. mainly focuses on its use in the treatment of osteoarthritis that Eucommia ulmoides Oliv. can enhance the healing ability of bone tissue. However, research on its bone repairability in periapical periodontitis has not been reported.OBJECTIVE: To study the effect of alcohol extract of Eucommia ulmoides Oliv. on cathepsin K expression in periapical periodontitis rats.METHODS:Twenty-four Sprague-Dawley rats were divided into normal control group (n=4) and apical periodontitis group (n=20). In the periapical periodontitis group, a periapical periodontitis model was established after exposure of the dental pulp in the first molar of the right mandible. The normal control group did not deal with any treatment.After 4 weeks of feeding, four rats from each group were taken for micro-CT detection.Bone destructionwas quantified to confirm whether the rat model of periapical periodontitis was successfully constructed. After 5 weeks of feeding, the remaining 16 rats with periapical periodontitis were equally randomized into alcohol extract group (given alcohol extract of Eucommia ulmoides Oliv. via intragastric administration, 5 mL/kg per day) and normal saline group (given the same dose of normal saline via intragastric administration every day). After 4 weeks of gavage, four mice from each group were selected to perform micro-CT examination. The ability of alcohol extract of Eucommia ulmoides Oliv. to repair periapical bone tissue was analyzed. First molars of the right mandible from the other four rats in each group were extracted to detect the expression of cathepsin K in the alveolar bone using immunohistochemical staining.RESULTS AND CONCLUSION: Micro-CT results showed that the rat model of periapical periodontitis was successfully constructed as there was a significant difference in the bone resorption volume between the normal control and apical periodontitis groups [(0.223±0.009) mm³ vs. (0.945±0.037) mm³, P=0.00]. After 4 weeks of gavage, the micro-CT results showed that the alcohol extract of Eucommia ulmoides Oliv. significantly reduced the bone resorption volume in the rat model of periapical periodontitis (P< 0.05). Immunohistochemistry results showed that the alcohol extract of Eucommia ulmoides Oliv. significantly inhibited the expression of cathepsin K, a marker of bone destruction, in the rat model of periapical periodontitis. Therefore, these findings indicate that the alcohol extract of Eucommia ulmoides Oliv. can inhibit the expression of cathepsin K and promote the healing of bone tissue in the rats with periapical periodontitis. [ABSTRACT FROM AUTHOR]

Published

2020

144. 绝经后骨质疏松症患者血清 β-CTX、CatheK 和 OPG水平变化及其临床意义.

Author

丁琦, 邢桂红, 秦晓丹, and 李飞

Abstract

Objective To observe the changes of serum β-collagen degradation products (β-CTX), cathepsin K (Cathe K), and osteoprotegerin (OPG) levels in postmenopausal osteoporosis (PMO) patients, and to discuss their clinical significance. Methods Sixty-four PMO patients (osteoporosis group, 34 patients with osteoporotic fracture and 30 patients without osteoporosis fracture), 43 patients with postmenopausal bone mass reduction (bone mass reduction group), and 42 patients with normal postmenopausal bone mass (bone mass normal group) were selected. After all subjects were enrolled, cubital vein was collected, serum was centrifuged and serum β-CTX, Cathe K and OPG were detected The effectiveness of serum β-CTX, Cathe K, and OPG in predicting osteoporotic fracture of PMO patients was assessed by using the receiver operating characteristic (ROC) curve. Results The levels of serum β-CTX and Cathe K in the osteoporosis group and the bone mass reduction group were higher than those in the bone mass normal group, and the levels of serum OPG were lower than those in the bone mass normal group, and the levels of serum β-CTX and Cathe K in the osteporosis group were higher than those in the bone mass reduction group, while the levels of serum OPG in the osteoporosis group were lower than those in the bone mass reduction group (all P < 0. 05). Serum β-CTX and Cathe K levels of PMO patients with osteoporotic fractures were higher than those without, and OPG levels were lower than those without (all P < 0. 05). ROC curve analysis showed that the area under the curve (AUC) of serum β-CTX in predicting osteoporotic fracture in PMO patients was 0.839 (95%C/: 0.756-0.903), and the optimal cut-off value was 7.84 µg/L, the prediction sensitivity was 77. 8% and specificity was 80. 7% ; the AUC of serum Cathe K in predicting osteoporotic fracture in PMO patients was 0. 821 (95% Cl: 0. 735-0. 889), and the optimal cut-off value was 33. 04 µg/L, the prediction sensitivity was 68. 3% and specificity was 89. 1 % ; the AUC of serum OPG in predicting osteoporotic fracture in PMO patients was 0. 824 (95% CI: 0. 739-0. 891), the optimal cut-off value was 3. 12 µg/L, and the prediction sensitivity was 78. 8% and speci一 如tywas 82. 0%; the combined prediction of serum β-CTX, Cathe K and OPG in PMO patients was 0. 945 (95% CI: 0. 909-0. 981), the sensitivity and specificity were 95. 7% and 90. 2%, respectively. The AUC of combined prediction of serum β-CTX, Cathe K, and OPG in predicting osteoporotic fracture of PMO patients was higher than that of serum 仕 CTX, Cathe Kand OPG alone (Z立148, 2. 581, and 3. 145, respectively, all P < 0. 05) . Conclusion Serum β-CTX and Cathe K levels in PMO patients increase significantly, while OPG levels decrease; serum β-CTX, Cathe K, and OPG can be used as biological indicators in predicting the occurrence of osteoporosis fracture in PMO patients, and the prediction efficiency of the three combined is higher [ABSTRACT FROM AUTHOR]

Published

2020

145. Function of Cathepsin K in the Central Nervous System of Male Mice is Independent of Its Role in the Thyroid Gland.

Author

Dauth, Stephanie, Rakov, Helena, Sîrbulescu, Ruxandra F., Ilieş, Iulian, Weber, Jonas, Batbajar Dugershaw, Battuja, Braun, Doreen, Rehders, Maren, Wirth, Eva K., Führer, Dagmar, Schweizer, Ulrich, and Brix, Klaudia

Subjects

*CENTRAL nervous system, *THYROID gland, *THYROTROPIN releasing factor, *NEURAL development, *CEREBELLAR cortex, *THYROID hormones, *MONOCARBOXYLATE transporters, *MICE

Abstract

Cathepsin K deficiency in male mice (Ctsk−/−) results in decreased numbers of hippocampal astrocytes and altered neuronal patterning as well as learning and memory deficits. Additionally, cathepsin K carries essential roles in the thyroid gland where it contributes to the liberation of thyroid hormones (TH). Because TH are essential for brain development, in particular for the cerebellum, we investigated whether cathepsin K's function in the thyroid is directly linked to the brain phenotype of Ctsk−/− mice. Serum levels of thyroid stimulating hormone, brain concentrations of free TH, and deiodinase 2 (Dio2) activity in brain parenchyma as well as cerebellar development were comparable in Ctsk−/− and WT animals, suggesting regular thyroid states and TH metabolism. Despite unaltered transcript levels, protein expression of two TH transporters was enhanced in specific brain regions in Ctsk−/− mice, suggesting altered TH supply to these regions. Thyrotropin releasing hormone (Trh) mRNA levels were enhanced threefold in the hippocampus of Ctsk−/− mice. In the striatum of Ctsk−/− mice the mRNA for Dio2 and hairless were approximately 1.3-fold enhanced, while mRNA levels for monocarboxylate transporter 8 and Trh were reduced to 60% and 40%, respectively, pointing to altered striatal physiology. We conclude that the role of cathepsin K in the thyroid gland is not directly associated with its function in the central nervous system (CNS) of mice. Future studies will show whether the brain region-specific alterations in Trh mRNA may eventually result in altered neuroprotection that could explain the neurobehavioral defects of Ctsk−/− mice. [ABSTRACT FROM AUTHOR]

Published

2020

146. Evolution of lung pathology in lymphangioleiomyomatosis: associations with disease course and treatment response.

Author

Miller, Suzanne, Stewart, Iain D, Clements, Debbie, Soomro, Irshad, Babaei‐Jadidi, Roya, and Johnson, Simon R

Subjects

THERAPEUTICS, DISEASE progression, NODULAR disease, LUNGS, MAST cells, RIBOSOMAL proteins, RIBOSOMES, OSTEOCLASTOGENESIS

Abstract

Lymphangioleiomyomatosis (LAM) is a rare multisystem disease with a variable clinical course. The lungs are infiltrated by nodules of LAM cells, stromal cells and inflammatory cells, causing lung cysts and respiratory failure. We used immunohistochemical markers in lung biopsy and transplant samples from a national cohort of women with LAM with linked clinical data to understand how LAM nodule cell populations changed with disease progression. Marker distribution was examined qualitatively by dual immunohistochemistry, and markers for LAM cells, fibroblasts, lymphatics, mast cells, proliferation, cathepsin K and mTOR pathway activity were quantitated in LAM nodules and compared with clinical features and prospective lung function loss. The LAM cell marker PNL2 was more extensively expressed in those with higher forced expiratory volume in one second (FEV1), higher diffusion in the lung for carbon monoxide (DLCO) and less extensive disease involvement whilst the converse was true for the protease cathepsin K. Each percentage increase in cathepsin K reactivity was associated with a 0.65% decrease in FEV1 (95% CI −1.11 to −0.18) and a 0.50% decrease in DLCO (95% CI −0.96 to −0.05). Higher reactivity to the mTOR complex 1 activation marker, phospho‐ribosomal protein S6, was associated with a better lung function response to rapamycin (p = 0.0001). We conclude that LAM nodules evolve with disease progression, with LAM cells becoming outnumbered by fibroblasts. Increasing cathepsin K expression is associated with more severe disease and lung function loss. Markers of mTOR activation predict the response to rapamycin, suggesting that more advanced LAM may be less mTOR responsive and treatments specifically targeted towards LAM associated fibroblasts may have roles as adjuncts to mTOR inhibition. [ABSTRACT FROM AUTHOR]

Published

2020

147. Fibroblast Growth Factor–21 Ameliorates Rheumatoid Arthritis by Maintaining Articular Integrity.

Author

Opoku, Yeboah Kwaku, Liu, Zhihang, Liu, Han, Afrifa, Justice, Koranteng, Harriet, Ren, Guiping, and Li, Deshan

Subjects

*RHEUMATOID arthritis, *SYNOVITIS, *FIBROBLAST growth factors, *DEGENERATION (Pathology), *TREATMENT effectiveness, *CARTILAGE regeneration, *OSTEOCLASTOGENESIS, *CARTILAGE

Abstract

Rheumatoid arthritis, a chronic degenerative autoimmune disease is hallmarked by tenacious inflammation of synovial membranes causing cartilage destruction and bone erosion. The search for effective therapies to mitigate its degenerative conditions remains partly elusive. Fibroblast growth factor 21 (FGF21) is known to modulate inflammation, playing a significant role in immune-mediated diseases such as rheumatoid arthritis. Here, we histopathologically evaluate the therapeutic efficacy of FGF21 in collagen-induced arthritis (CIA) mice. CIA mice were subcutaneously treated with FGF21 (3 mg/kg) for three consecutive weeks. Arthritic severity was scored followed by histopathological evaluation of the joints and immunohistochemistry using rabbit ant-cathepsin K, IL-10, MMP1, and 3 antibodies. Our data revealed that FGF21 significantly mitigated the severity of arthritis. Histopathologically, the articular structure was considerably enhanced by FGF21 through the reduction in the expression of cathepsin K and MMP3 whiles upregulating the expression of IL-10. Taken together, our findings suggest that FGF21 preserves the integrity of the articular structure thereby preventing cartilage and bone destruction in CIA mice. FGF21, therefore, has therapeutic prospects in the treatment of RA. [ABSTRACT FROM AUTHOR]

Published

2020

148. Cathepsin K regulates localization and secretion of Tartrate-Resistant Acid Phosphatase (TRAP) in TRAP-overexpressing MDA-MB-231 breast cancer cells.

Author

Reithmeier, Anja, Norgård, Maria, Ek-Rylander, Barbro, Näreoja, Tuomas, and Andersson, Göran

Subjects

*ACID phosphatase, *CYSTEINE proteinases, *CANCER cells, *BREAST cancer, *CANCER cell migration

Abstract

Background: Tartrate–resistant acid phosphatase (TRAP/ ACP5) belongs to the binuclear metallophosphatase family and is present in two isoforms. The primary translation product is an uncleaved TRAP 5a isoform with low phosphatase activity. TRAP 5a can be post-translationally processed to a cleaved TRAP 5b isoform with high phosphatase activity by e.g. cysteine proteinases, such as Cathepsin K (CtsK). The relevance of the phosphatase activity of TRAP 5b has been demonstrated for proliferation, migration and invasion of cancer cells. TRAP-overexpressing MDA-MB-231 breast cancer cells displayed higher levels of TRAP 5a and efficient processing of TRAP 5a to TRAP 5b protein, but no changes in levels of CtsK when compared to mock-transfected cells. In TRAP-overexpressing cells colocalization of TRAP 5a and proCtsK was augmented, providing a plausible mechanism for generation of TRAP 5b. CtsK expression has been associated with cancer progression and has been pharmacologically targeted in several clinical studies. Results: In the current study, CtsK inhibition with MK-0822/Odanacatib did not abrogate the formation of TRAP 5b, but reversibly increased the intracellular levels of a N-terminal fragment of TRAP 5b and reduced secretion of TRAP 5a reversibly. However, MK-0822 treatment neither altered intracellular TRAP activity nor TRAP-dependent cell migration, suggesting involvement of additional proteases in proteolytic processing of TRAP 5a. Notwithstanding, CtsK was shown to be colocalized with TRAP and to be involved in the regulation of secretion of TRAP 5a in a breast cancer cell line, while it still was not essential for processing of TRAP 5a to TRAP 5b isoform. Conclusion: In cancer cells multiple proteases are involved in cleaving TRAP 5a to high-activity phosphatase TRAP 5b. However, CtsK-inhibiting treatment was able to reduce secretion TRAP 5a from TRAP-overexpressing cancer cells. [ABSTRACT FROM AUTHOR]

Published

2020

149. Identification and characterization of a cathepsin K homologue that interacts with pathogen bacteria in black rockfish, Sebastes schlegelii.

Author

He, Shu-wen, Du, Xue, Wang, Guang-hua, Wang, Jing-jing, Xie, Bing, Gu, Qin-qin, Zhang, Min, and Gu, Han-jie

Subjects

*STRIPED bass, *VIBRIO anguillarum, *PEPTIDASE, *VIBRIO infections, *BACTERIAL diseases, *CATHEPSINS

Abstract

Cathepsin K belongs to the family of cysteine cathepsins. It is well known that the cysteine cathepsins participate in various physiological processes and host immune defense in mammals. However, in teleost fish, the function of cathepsin K is very limited. In the present study, a cathepsin K homologue (SsCTSK) from the teleost black rockfish (Sebastes schlegelii) was identified and examined at expression and functional levels. In silico analysis showed that three domains, including signal peptide, cathepsin propeptide inhibitor I29 domain, and functional domain Pept_C1, are existed in SsCTSK. SsCTSK also possesses a peptidase domain with three catalytically essential residues (Cys25, His162 and Asn183). Phylogenetic profiling indicated that SsCTSK was evolutionally close to the cathepsin K of other teleost fish. Expression of SsCTSK occurred in multiple tissues and was induced by bacterial infection. Purified recombinant SsCTSK (rSsCTSK) exhibited apparent maximal peptidase activity at 45 °C, and its enzymatic activity was remarkably declined in the presence of the cathepsin inhibitor E−64. Moreover, rSsCTSK possesses the ability to bind with PAMPs and bacteria. Finally, knockdown of SsCTSK expression facilitated bacterial invasion in black rockfish. Collectively, these results indicated that SsCTSK functions as a cysteine protease and may serves as a target for pathogen manipulation of host defense system. • Expression of SsCTSK was upregulated during Vibrio anguillarum infection. • rSsCTSK exhibited apparent peptidase activity. • rSsCTSK displayed apparent binding activities against LPS, PGN and different bacteria. • The knockdown of SsCTSK facilitated bacterial invasion in black rockfish. [ABSTRACT FROM AUTHOR]

Published

2020

150. Whole‐exome sequencing identified a novel variant in an Iranian patient affected by pycnodysostosis.

Author

Razmara, Ehsan, Azimi, Homeyra, Bitaraf, Amirreza, Daneshmand, Mohammad Ali, Galehdari, Mohammad, Dokhanchi, Maryam, Esmaeilzadeh‐Gharehdaghi, Elika, and Garshasbi, Masoud

Subjects

*EXOMES, *MEDICAL genetics, *MOLECULAR genetics, *MOLECULAR pathology, *SHORT stature, *MOLECULAR association, *RECESSIVE genes

Abstract

Background: Whole‐exome sequencing (WES) has emerged as a successful diagnostic tool in molecular genetics laboratories worldwide. In this study, we aimed to find the potential genetic cause of skeletal disease, a heterogeneous disease, revealing the obvious short stature phenotype. In an Iranian family, we used solo‐WES in a suspected patient to decipher the potential genetic cause(s). Methods: A comprehensive clinical and genotyping examination was applied to suspect the disease of the patient. The solo clinical WES was exploited, and the derived data were filtered according to the standard pipelines. In order to validate the WES finding, the region harboring the candidate variant in the CTSK gene was amplified from genomic DNA and sequenced directly by Sanger sequencing. Results: Sequence analysis revealed a rare novel nonsense variant, p.(Trp320*); c.905G>A, in the CTSK gene (NM_000396.3). In silico analysis shed light on the contribution of the variant to the pathogenicity of pycnodysostosis. This variant was confirmed by Sanger sequencing and further clinical examinations of the patient confirmed the disease. Conclusion: The present study shows a rare variant of the CTSK gene, which inherited as autosomal recessive, in an Iranian male patient with pycnodysostosis. Taken together, the novel nonsense CTSK variant meets the criteria of being likely pathogenic according to the American College of Medical Genetics and Genomics‐the Association for Molecular Pathology (ACMG‐AMP) variant interpretation guidelines. [ABSTRACT FROM AUTHOR]

Published

2020