Your search keyword '"Waterhouse NJ"' showing total 5 results

1. Cellular settings mediating Src Substrate switching between focal adhesion kinase tyrosine 861 and CUB-domain-containing protein 1 (CDCP1) tyrosine 734.

Author

Wortmann A, He Y, Christensen ME, Linn M, Lumley JW, Pollock PM, Waterhouse NJ, and Hooper JD

Subjects

Antigens, Neoplasm, Binding Sites, Cell Adhesion, Cell Line, Tumor, Cell Membrane metabolism, Disease Progression, Fibroblasts metabolism, Gene Silencing, HeLa Cells, Humans, Microscopy, Confocal methods, Phosphorylation, Antigens, CD chemistry, Cell Adhesion Molecules chemistry, Focal Adhesion Protein-Tyrosine Kinases chemistry, Neoplasm Proteins chemistry, Tyrosine chemistry, src-Family Kinases metabolism

Abstract

Reciprocal interactions between Src family kinases (SFKs) and focal adhesion kinase (FAK) are critical during changes in cell attachment. Recently it has been recognized that another SFK substrate, CUB-domain-containing protein 1 (CDCP1), is differentially phosphorylated during these events. However, the molecular processes underlying SFK-mediated phosphorylation of CDCP1 are poorly understood. Here we identify a novel mechanism in which FAK tyrosine 861 and CDCP1-Tyr-734 compete as SFK substrates and demonstrate cellular settings in which SFKs switch between these sites. Our results show that stable CDCP1 expression induces robust SFK-mediated phosphorylation of CDCP1-Tyr-734 with concomitant loss of p-FAK-Tyr-861 in adherent HeLa cells. SFK substrate switching in these cells is dependent on the level of expression of CDCP1 and is also dependent on CDCP1-Tyr-734 but is independent of CDCP1-Tyr-743 and -Tyr-762. In HeLa CDCP1 cells, engagement of SFKs with CDCP1 is accompanied by an increase in phosphorylation of Src-Tyr-416 and a change in cell morphology to a fibroblastic appearance dependent on CDCP1-Tyr-734. SFK switching between FAK-Tyr-861 and CDCP1-Tyr-734 also occurs during changes in adhesion of colorectal cancer cell lines endogenously expressing these two proteins. Consistently, increased p-FAK-Tyr-861 levels and a more epithelial morphology are seen in colon cancer SW480 cells silenced for CDCP1. Unlike protein kinase Cδ, FAK does not appear to form a trimeric complex with Src and CDCP1. These data demonstrate novel aspects of the dynamics of SFK-mediated cell signaling that may be relevant during cancer progression.

Published

2011

2. A central role for Bid in granzyme B-induced apoptosis.

Author

Waterhouse NJ, Sedelies KA, Browne KA, Wowk ME, Newbold A, Sutton VR, Clarke CJ, Oliaro J, Lindemann RK, Bird PI, Johnstone RW, and Trapani JA

Subjects

Animals, BH3 Interacting Domain Death Agonist Protein, Bone Marrow Cells cytology, Bone Marrow Cells metabolism, Cell Death, Cell Proliferation, Cells, Cultured, Chromium metabolism, Cytochromes c metabolism, Dendrites metabolism, Dendritic Cells, Dose-Response Relationship, Drug, Fibroblasts metabolism, Granzymes, Intracellular Membranes metabolism, Lymphocytes metabolism, Lymphoma, B-Cell metabolism, Membrane Potentials, Mice, Mice, Inbred C57BL, Mitochondria metabolism, Time Factors, Apoptosis, Carrier Proteins physiology, Serine Endopeptidases metabolism

Abstract

Granzyme B, a protease released from cytotoxic lymphocytes, has been proposed to induce target cell death by cleaving and activating the pro-apoptotic Bcl-2 family member Bid. It has also been proposed that granzyme B can induce target cell death by activating caspases directly, by cleaving caspase substrates, and/or by cleaving several non-caspase substrates. The relative importance of Bid in granzyme B-induced cell death has therefore remained unclear. Here we report that cells isolated from various tissues of Bid-deficient mice were resistant to granzyme B-induced cell death. Consistent with the proposed role of Bid in regulating mitochondrial outer membrane permeabilization, cytochrome c remained in the mitochondria of Bid-deficient cells treated with granzyme B. Unlike wild type cells, Bid-deficient cells survived and were then able to proliferate normally, demonstrating the critical role for Bid in mediating granzyme B-induced apoptosis.

Published

2005

3. Granzyme M mediates a novel form of perforin-dependent cell death.

Author

Kelly JM, Waterhouse NJ, Cretney E, Browne KA, Ellis S, Trapani JA, and Smyth MJ

Subjects

Animals, Apoptosis, Blotting, Western, Caspases metabolism, Cell Death, Cell Line, Chromium metabolism, DNA Fragmentation, Dose-Response Relationship, Drug, Enzyme Activation, Erythrocytes metabolism, Granzymes, HeLa Cells, Humans, Iodine metabolism, Jurkat Cells, K562 Cells, Killer Cells, Natural metabolism, Lymphocytes metabolism, Membrane Glycoproteins metabolism, Mitochondria metabolism, Perforin, Pore Forming Cytotoxic Proteins, Proto-Oncogene Proteins c-bcl-2 metabolism, Recombinant Proteins metabolism, Serine Endopeptidases metabolism, Sheep, Time Factors, Serine Endopeptidases physiology

Abstract

Cell death is mediated by cytotoxic lymphocytes through various granule serine proteases released with perforin. The unique protease activity, restricted expression, and distinct gene locus of granzyme M suggested this enzyme might have a novel biological function or trigger a novel form of cell death. Herein, we demonstrate that in the presence of perforin, the protease activity of granzyme M rapidly and effectively induces target cell death. In contrast to granzyme B, cell death induced by granzyme M does not feature obvious DNA fragmentation, occurs independently of caspases, caspase activation, and perturbation of mitochondria and is not inhibited by overexpression of Bcl-2. These data raise the likelihood that granzyme M represents a third major and specialized perforin-dependent cell death pathway that plays a significant role in death mediated by NK cells.

Published

2004

4. Granzyme B-mediated apoptosis proceeds predominantly through a Bcl-2-inhibitable mitochondrial pathway.

Author

Pinkoski MJ, Waterhouse NJ, Heibein JA, Wolf BB, Kuwana T, Goldstein JC, Newmeyer DD, Bleackley RC, and Green DR

Subjects

Amino Acid Sequence, Cytochrome c Group metabolism, Enzyme Activation, Granzymes, Humans, Hydrolysis, Jurkat Cells, Kinetics, Molecular Sequence Data, Apoptosis drug effects, Mitochondria physiology, Proto-Oncogene Proteins c-bcl-2 physiology, Serine Endopeptidases pharmacology

Abstract

Cytotoxic T lymphocytes kill virus-infected and tumor cell targets through the concerted action of proteins contained in cytolytic granules, primarily granzyme B and perforin. Granzyme B, a serine proteinase with substrate specificity similar to the caspase family of apoptotic cysteine proteinases, is capable of cleaving and activating a number of death proteins in target cells. Despite the ability to engage the death pathway at multiple entry points, the preferred mechanism for rapid induction of apoptosis by granzyme B has yet to be clearly established. Here we use time lapse confocal microscopy to demonstrate that mitochondrial cytochrome c release is the primary mode of granzyme B-induced apoptosis and that Bcl-2 is a potent inhibitor of this pivotal event. Caspase activation is not required for cytochrome c release, an activity that correlates with cleavage and activation of Bid, which we have found to be cleaved more readily by granzyme B than either caspase-3 or caspase-8. Bcl-2 blocks the rapid destruction of targets by granzyme B by blocking mitochondrial involvement in the process.

Published

2001

5. Bax-induced caspase activation and apoptosis via cytochrome c release from mitochondria is inhibitable by Bcl-xL.

Author

Finucane DM, Bossy-Wetzel E, Waterhouse NJ, Cotter TG, and Green DR

Subjects

Animals, Cell Line, Cysteine Proteinase Inhibitors pharmacology, Cytochrome c Group antagonists & inhibitors, Enzyme Activation, Humans, Mice, Mice, Inbred BALB C, Proto-Oncogene Proteins antagonists & inhibitors, bcl-2-Associated X Protein, bcl-X Protein, Apoptosis, Caspases metabolism, Cytochrome c Group metabolism, Mitochondria, Liver enzymology, Proto-Oncogene Proteins metabolism, Proto-Oncogene Proteins c-bcl-2 metabolism

Abstract

A growing body of evidence supports a role for mitochondria and mitochondria-derived factors in the cell death process. In particular, much attention has focused on cytochrome c, a key component of the electron transport chain, that has been reported to translocate from the mitochondria to the cytosol in cells undergoing apoptosis. The mechanism for this release is, as yet, unknown. Here we report that ectopic expression of Bax induces apoptosis with an early release of cytochrome c preceding many apoptosis-associated morphological alterations as well as caspase activation and subsequent substrate proteolysis. A loss of mitochondrial transmembrane potential was detected in vivo, although no mitochondrial swelling or loss of transmembrane potential was observed in isolated mitochondria treated with Bax in vitro. Caspase inhibitors, such as endogenous XIAP and synthetic peptide benzyloxycarbonyl-Val-Ala-Asp-fluoromethyl ketone (zVAD-fmk), although capable of altering the kinetics and perhaps mode of cell death, had no influence on this release, suggesting that if cytochrome c plays a role in caspase activation it must precede this step in the apoptotic process. Mitochondrial permeability transition was also shown to be significantly prevented by caspase inhibition, indicating that the translocation of cytochrome c from mitochondria to cytosol is not a consequence of events requiring mitochondrial membrane depolarization. In contrast, Bcl-xL was capable of preventing cytochrome c release while also significantly inhibiting cell death. It would therefore appear that the mitochondrial release of factors such as cytochrome c represents a critical step in committing a cell to death, and this release is independent of permeability transition and caspase activation but is inhibited by Bcl-xL.

Published

1999