Cathepsin V, a Novel and Potent Elastolytic Activity Expressed in Activated Macrophages

Yasuda, Yoh; Li, Zhenqiang; Greenbaum, Doron C.; Bogyo, Matthew; Weber, Ekkehard; Brὂmme, Dieter

doi:10.1074/jbc.m403986200

Cited by 173 publications

(142 citation statements)

References 54 publications

(53 reference statements)

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“…The findings of this study indicate the novel role of cathepsin V in secretory vesicles for producing active neuropeptides, which contrasts with the well known function of cathepsin V in lysosomes (11,45). This study shows that human neuroblastoma cells contain cathepsin V in secretory vesicles as well as lysosomes.…”

Section: Substratecontrasting

confidence: 50%

Human Cathepsin V Protease Participates in Production of Enkephalin and NPY Neuropeptide Neurotransmitters

Funkelstein

Koch

et al. 2012

Journal of Biological Chemistry

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Background: Proteases are required to generate peptide neurotransmitters. Results: Human cathepsin V participates in the production of enkephalin and NPY peptide neurotransmitters illustrated by gene expression and silencing. Conclusion: Human cathepsin V participates in producing enkephalin and NPY neurotransmitters in secretory vesicles. Significance: Elucidation of human-specific proteases participating in peptide neurotransmitter production is essential for understanding human health and disease.

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Section: Substratecontrasting

confidence: 50%

Human Cathepsin V Protease Participates in Production of Enkephalin and NPY Neuropeptide Neurotransmitters

Funkelstein

Koch

et al. 2012

Journal of Biological Chemistry

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“…After protein transfer and blocking of nonspecific binding sites for 2 hours with 5% skimmed milk in PBST, membranes were incubated overnight at 4°C with the rabbit polyclonal antibodies to cath-D (1: 7500), 22 cath-B (both 1:500), and cath-H (1:10,000) and mAbs to cath-K (1:200), cath-V (1:500). Also, we used the two mAbs specific for procath-L (2D4 at 1:500) and all three cath-L forms (33/1 at 1:500), 23,24 respectively. Secondary horseradish peroxidase-conjugated goat antirabbit and rabbit anti-mouse Igs were used at 1:20,000 for 1 hour at room temperature, respectively.…”

Section: Western Blot Analysismentioning

confidence: 99%

Relaxin Enhances the Oncogenic Potential of Human Thyroid Carcinoma Cells

Hombach‐Klonisch

Białek

Trojanowicz

et al. 2006

The American Journal of Pathology

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The role of members of the insulin-like superfamily in human thyroid carcinoma is primarily unknown. Here we demonstrate the presence of RLN2 relaxin and relaxin receptor LGR7 in human papillary, follicular, and undifferentiated anaplastic thyroid carcinoma suggesting a specific involvement of relaxin-LGR7 signaling in thyroid carcinoma. Stable transfectants of the LGR7-positive human follicular thyroid carcinoma cell lines FTC-133 and FTC-238 that secrete bioactive proRLN2 revealed this hormone to act as a multifunctional endocrine factor in thyroid carcinoma cells. Although RLN2 did not act as a mitogen, it acted as an autocrine/paracrine factor and significantly increased anchorage-independent growth and thyroid carcinoma cell motility and invasiveness through elastin matrices. In recent years, the multifunctional peptide hormone relaxin has been identified as an important endocrine player in the reproductive tract, cardiovascular/neural systems, and oncology.1,2 The thyroid was once considered to be a relaxin target tissue with relaxin reported to increase thyroid weight, radioactive iodine uptake, and protein-bound iodination in rats.3,4 Likely because of the crude relaxin preparations used at the time, these results could not be confirmed. 5 No further investigations were reported thereafter using highly purified relaxin preparations to validate a potential role of relaxin in thyroid tissues and thyroid cell lines. Some 40 years later, the discovery of the G-protein-coupled relaxin-like receptors LGR7 and LGR8 revealed the presence of transcripts for both LGR7 (relaxin receptor) and LGR8 (INSL3/relaxin receptor) in the thyroid gland. 6 -8 Relaxin and the relaxin-like INSL3 have been shown to activate cAMP-dependent signaling pathways by binding to either LGR7 or LGR8. 8 -12 We recently demonstrated the expression and regulation of INSL3 and LGR8 transcripts in human thyroid carcinoma cell lines, identifying hyper-and neoplastic human thyrocytes as a new source and target of the actions of INSL3 and a novel INSL3 splice variant. 8,13 Although still primarily undefined, relaxin appears to have oncogenic potential in various organs and tissues, including the human thyroid.14 -17 Relaxin affects proliferation and differentiation of MCF-7 human carcinoma cells in a concentration-dependent manner 18 and can modify the extracellular matrix by affecting the expresSupported by the Deutsche Forschungsgemeinschaft (grants KL1249/5-1

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“…MMPs degrade fibrillar elements such as fibrillar collagens and elastin, and nonfibrillar elements (nonfibrillar collagens, glycoproteins, and proteoglycans) such as type IV collagen, the proteoglycan perlecan or glycoproteins laminin and entactin, all constitu- 43 Recently, cathepsin V has been identified in atherosclerotic plaque specimens and exhibits the most potent elastase activity yet described among human proteases. 35 The plasminogen system degrades laminin, fibronectin, vitronectin, and proteoglycans. Neutrophil elastase degrades collagen, elastin, laminin, fibronectin, and proteoglycan.…”

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confidence: 99%

Extracellular Proteases in Atherosclerosis and Restenosis

García‐Touchard

Henry

Sangiorgi

et al. 2005

ATVB

146

101

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Abstract-Extracellular proteolysis plays a key role in many pathophysiologic processes including cancer, inflammatory diseases, and cardiovascular conditions such as atherosclerosis and restenosis. Whereas matrix metalloproteinases are their best known member, many others are becoming better known. The extracellular proteases are a complex and heterogeneous superfamily of enzymes. They include metalloproteinases (matrix metalloproteinases, adamalysins, or pappalysins), serine proteases (elastase, coagulation factors, plasmin, tissue plasminogen activator, urokinase plasminogen activator), and the cysteine proteases (such cathepsins). In addition to their matrix degradation capabilities, they have other less well known biologic functions that include angiogenesis, growth factor bioavailability, cytokine modulation, receptor shedding, enhancing cell migration, proliferation, invasion, and apoptosis. This review discusses extracellular proteases relevant to the vasculature, their classification and function, and how protease disorders contribute to arterial plaque growth, including chronic atherosclerosis, acute coronary syndromes, restenosis, and vascular remodeling. These broad extracellular protease functions make them potentially interesting therapeutic targets. Key Words: acute coronary syndromes Ⅲ aneurysms Ⅲ athersclerosis Ⅲ proteases Ⅲ restenosis E xtracellular proteolysis is important to many biological processes including tissue remodeling, wound healing, and embryogenesis. It also has a key role in pathophysiologic processes including cancer, chronic inflammatory diseases, and cardiovascular conditions such as atherosclerosis and restenosis.Extracellular proteases (ECP) form a heterogeneous family that is becoming increasingly well understood. Whereas matrix metalloproteinases are the best described, many others are also becoming known. For example, a new protease family, the pappalysins, is now included. Other enzymes such as cysteine proteases were previously considered intracellular enzymes but have recently been shown to function in the extracellular space. In parallel with these discoveries, ECP have generated special interest because they degrade extracellular matrix (ECM). Although recent attention has focused on their impact in vulnerable plaques, promoting weakness and rupture, they are also involved in many other important biological functions.This review discusses extracellular proteases relevant to the vasculature, their function, and how protease disorders contribute to multiple stages of arterial plaque growth, including chronic atherosclerosis, acute coronary syndromes (ACS), restenosis, and vascular remodeling. Extracellular Protease ClassificationProteases or peptidases are enzymes that hydrolyze peptide bonds. They are classified as endopeptidases (cleaving the inner regions of peptide chains) and exopeptidases, which act at or near the peptide ends, liberating a single, dipeptide, or a tripeptide amino acid residue. Endopeptidases are the principal enzymes degrading extracellular prote...

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Cathepsin V, a Novel and Potent Elastolytic Activity Expressed in Activated Macrophages

Cited by 173 publications

References 54 publications

Human Cathepsin V Protease Participates in Production of Enkephalin and NPY Neuropeptide Neurotransmitters

Human Cathepsin V Protease Participates in Production of Enkephalin and NPY Neuropeptide Neurotransmitters

Relaxin Enhances the Oncogenic Potential of Human Thyroid Carcinoma Cells

Extracellular Proteases in Atherosclerosis and Restenosis

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