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15 results on '"Willson, Tracy A."'

1. Regulation of hematopoietic stem cells by their mature progeny

Author

de Graaf, Carolyn A., Kauppi, Maria, Baldwin, Tracey, Hyland, Craig D., Metcalf, Donald, Willson, Tracy A., Carpinelli, Marina R., Smyth, Gordon K., Alexander, Warren S., and Hilton, Douglas J.

Subjects
Bone marrow cells -- Properties, Hematopoietic stem cells -- Research, Science and technology
Abstract

Thrombopoietin (TPO), acting through its receptor Mpl, has two major physiological roles: ensuring production of sufficient platelets via stimulation of megakaryocyte production and maintaining hematopoietic stem cell (HSC) quiescence. Mpl also controls circulating TPO concentration via receptor-mediated internalization and degradation. Here, we demonstrate that the megakaryocytosis and increased platelet mass in mice with mutations in the Myb or p300 genes causes reduced circulating TPO concentration and TPO starvation of the stem-cell compartment, which is exacerbated because these cells additionally exhibit impaired responsiveness to TPO. HSCs from [Myb.sup.Plt4/Plt4] mice show altered expression of TPO-responsive genes and, like HSCs from Tpo and Mpl mutant mice, exhibit increased cycling and a decline in the number of HSCs with age. These studies suggest that disorders of platelet number can have profound effects on the HSC compartment via effects on the feedback regulation of circulating TPO concentration. doi: 10.1073/pnas.1016166108

Published
2010

2. Deficiency of 5-hydroxyisourate hydrolase causes hepatomegaly and hepatocellular carcinoma in mice

Author

Stevenson, William S., Hyland, Craig D., Zhang, Jian-Guo, Morgan, Phillip O., Willson, Tracy A., Gill, Anthony, Hilton, Adrienne A., Viney, Elizabeth M., Bahlo, Melanie, Masters, Seth L., Hennebry, Sarah, Richardson, Samantha J., Nicola, Nicos A., Metcalf, Donald, Hilton, Douglas J., Roberts, Andrew W., and Alexander, Warren S.

Subjects
Hepatoma -- Causes of, Uric acid -- Health aspects, Hepatomegaly -- Causes of, Hydrolases -- Health aspects, Enzymes -- Health aspects, Science and technology
Abstract

With the notable exception of humans, uric acid is degraded to (S)-allantoin in a biochemical pathway catalyzed by urate oxidase, 5hydroxyisourate (HIU) hydrolase, and 2-oxo-4-hydroxy-4-carboxy-5ureidoimidazoline decarboxylase in most vertebrate species. A point mutation in the gene encoding mouse HIU hydrolase, Urah, that perturbed uric acid metabolism within the liver was discovered during a mutagenesis screen in mice. The predicted substitution of cysteine for tyrosine in a conserved helical region of the mutantencoded HIU hydrolase resulted in undetectable protein expression. Mice homozygous for this mutation developed elevated platelet counts secondary to excess thrombopoietin production and hepatomegaly. The majority of homozygous mutant mice also developed hepatocellular carcinoma, and tumor development was accelerated by exposure to radiation. The development of hepatomegaly and liver tumors in mice lacking Urah suggests that uric acid metabolites may be toxic and that urate oxidase activity without HIU hydrolase function may affect liver growth and transformation. The absence of HIU hydrolase in humans predicts slowed metabolism of HIU after clinical administration of exogenous urate oxidase in conditions of uric acid-related pathology. The data suggest that prolonged urate oxidase therapy should be combined with careful assessment of toxicity associated with extrahepatic production of uric acid metabolites. N-ethyl-N-nitrosourea mutagenesis | uric acid | 5-hydroxyisourate hydrolase | hepatocellular carcinoma | thrombopoietin doi/ 10.1073/pnas.1010390107

Published
2010

3. Suppressor of cytokine signaling (SOCS)-5 is a potential negative regulator of epidermal growth factor signaling

Author

Nicholson, Sandra E., Metcalf, Donald, Sprigg, Naomi S., Columbus, Ruth, Walker, Francesca, Silva, Anabel, Cary, Dale, Willson, Tracy A., Zhang, Jian-Guo, Hilton, Douglas J., Alexander, Warren S., and Nicola, Nicos A.

Subjects
Epidermal growth factor -- Research, Proteins -- Research, Cellular control mechanisms -- Research, Science and technology
Abstract

The suppressors of cytokine signaling (SOCS) proteins are a family of SH2 domain-containing intracellular inhibitors of cytokine signal transduction that act by several different mechanisms. Recent evidence suggests that the action of the SOCS proteins may extend beyond the cytokine receptors to signaling initiated by members of the tyrosine kinase receptor family. In this study, the ability of SOCS-5 to negatively regulate signaling cascades downstream of the epidermal growth factor receptor (EGF-R) has been examined by using an EGF-responsive cell line engineered to constitutively express the EGF-R and SOCS-5 or SOCS-5 mutants. SOCS-5 associated with the EGF-R complex in an EGF-independent manner, and the mitogenic response to EGF of all SOCS-5-expressing cell lines was dramatically inhibited when compared with control cell lines. Furthermore, this effect was abrogated after deletion of the SOCS-5 SOCS box. This result suggests that the inhibition of signaling occurs through enhanced proteasomal degradation of the EGF-R through SOCS box recruitment of E3 ubiquitin ligase activity.

Published
2005

4. Development of hydrocephalus in mice lacking SOCS7

Author

Krebs, Danielle L., Metcalf, Donald, Merson, Tobias D., Voss, Anne K., Thomas, Tim, Zhang, Jian-Guo, Rakar, Steven, O'Bryan, Moira K., Willson, Tracy A., Viney, Elizabeth M., Mielke, Lisa A., Nicola, Nicos A., Hilton, Douglas J., and Alexander, Warren S.

Subjects
Hydrocephalus -- Research, Hydrocephalus -- Causes of, Cytokines -- Research, Cytokines -- Genetic aspects, Gene targeting, Science and technology
Abstract

SOCS7 is a member of the suppressor of cytokine signaling (SOCS) family of proteins (SOCS1-SOCS7 and CIS). SOCS proteins are composed of an N-terminal domain of variable length, a central Src homology 2 domain, and a C-terminal SOCS box. Biochemical and genetic studies have revealed that SOCS1, SOCS2, SOCS3, and CIS play an important role in the termination of cytokine and growth factor signaling. However, the biological actions of other SOCS proteins are less well defined. To investigate the physiological role of SOCS7, we have used gene targeting to generate mice that lack expression of the Socs7 gene. [Socs7.sup.-/-] mice were born in expected numbers, were fertile, and did not exhibit defects in hematopoiesis or circulating glucose or insulin concentrations. However, [Socs7.sup.-/-] mice were 7-10% smaller than their wild-type littermates, and within 15 weeks of age [approximately equal to] 50% of the [Socs7.sup.-/-] mice died as a result of hydrocephalus that was characterized by cranial distortion, dilation of the ventricular system, reduced thickness of the cerebral cortex, and disorganization of the subcommissural organ. In situ hybridization studies revealed prominent expression of Socs7 in the brain, suggestive of an important functional role of SOCS7 in this organ.

Published
2004

5. Suppressor screen in [Mpl.sup.-/-] mice: c-Myb mutation causes supraphysiological production of platelets in the absence of thrombopoietin signaling

Author

Carpinelli, Marina R., Hilton, Douglas J., Metcalf, Donald, Antonchuk, Jennifer L., Hyland, Craig D., Mifsud, Sandra L., Di Rago, Ladina, Hilton, Adrienne A., Willson, Tracy A., Roberts, Andrew W., Ramsay, Robert G., Nicola, Nicos A., and Alexander, Warren S.

Subjects
Genetics -- Research, Science and technology
Abstract

Genetic screens in lower organisms, particularly those that identify modifiers of preexisting genetic defects, have been used successfully to order components of complex signaling pathways. To date, similar suppressor screens have not been used in vertebrate. To define the molecular pathways regulating platelet production, we have executed a large-scale modifier screen with genetically thrombocytopenic [Mpl.sup.-/-] mice by using N-ethyl-N-nitrosourea mutagenesis. Here we show that mutations in the c-Myb gene cause a myeloproliferative syndrome and supraphysiological expansion of megakaryocyte and platelet production in the absence of thrombopoietin signaling. This screen demonstrates the utility of large-scale N-ethyl-N-nitrosourea mutagenesis suppressor screens in mice for the simultaneous discovery and in vivo validation of targets for therapeutic discovery in diseases for which mouse models are available.

Published
2004

6. The SOCS box of suppressor of cytokine signaling-1 is important for inhibition of cytokine action in vivo

Author

Zhang, Jian-Guo, Metcalf, Donald, Rakar, Steven, Asimakis, Maria, Greenhalgh, Christopher J., Willson, Tracy A., Starr, Robyn, Nicholson, Sandra E., Carter, Wendy, Alexander, Warren S., Hilton, Douglas J., and Nicola, Nicos A.

Subjects
Cytokines -- Genetic aspects, Inflammation -- Genetic aspects, Science and technology
Abstract

Suppressor of Cytokine Signaling-1 (SOCS-1) is an essential physiological inhibitor of IFN-[gamma] signaling. Mice lacking this gene die in the early postnatal period from a disease characterized by hyper-responsiveness to endogenous IFN-[gamma]. The SOCS box is a C-terminal domain shared with over 30 other proteins that links SOCS proteins to an E3 ubiquitin ligase activity and the proteasome, but whether it contributes to inhibition of cytokine signaling is currently disputed. We have deleted only the SOCS box of the SOCS-1 gene in mice and show that such mice have an increased responsiveness to IFN-y and slowly develop a fatal inflammatory disease. These results demonstrate that deletion of the SOCS box leads to a partial loss of function of SOCS-1.

Published
2001

7. Gigantism in mice lacking suppressor of cytokine signalling-2

Author

Metcalf, Donald, Greenhalgh, Christopher J., Viney, Elizabeth, Willson, Tracy A., Starr, Robyn, Nicola, Nicos A., Hilton, Douglas J., and Alexander, Warren S.

Subjects
Environmental issues, Science and technology, Zoology and wildlife conservation
Abstract

Author(s): Donald Metcalf; Christopher J. Greenhalgh; Elizabeth Viney; Tracy A. Willson; Robyn Starr; Nicos A. Nicola; Douglas J. Hilton; Warren S. Alexander (corresponding author) Suppressor of cytokine signalling-2 (SOCS-2) is [...]

Published
2000
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8. The conserved SOCS box motif in suppressors of cytokine signaling binds to elongins B and C and may couple bound proteins to proteasomal degradation

Author

Zhang, Jian-Guo, Farley, Alison, Nicholson, Sandra E., Willson, Tracy A., Zugaro, Lisa M., Simpson, Richard J., Moritz, Robert L., Cary, Dale, Richardson, Rachael, Hausmann, George, Kile, Benjamin J., Kent, Stephen B.H., Alexander, Warren S., Metcalf, Donald, Hilton, Douglas J., Nicola, Nicos A., and Baca, Manuel

Subjects
Cytokines -- Research, Proteins -- Research, Science and technology
Abstract

The suppressors of cytokine signaling (SOCS) family of proteins act as intracellular inhibitors of several cytokine signal transduction pathways. Their expression is induced by cytokine activation of the Janus kinase/signal transducer and activator of transcription (JAK/STAT) pathway and they act as a negative feedback loop by subsequently inhibiting the JAK/STAT pathway either by direct interaction with activated JAKs or with the receptors. These interactions are mediated at least in part by the SH2 domain of SOCS proteins but these proteins also contain a highly conserved C-terminal homology domain termed the SOCS box. Here we show that the SOCS box mediates interactions with elongins B and C, which in turn may couple SOCS proteins and their substrates to the proteasomal protein degradation pathway. Analogous to the family of F-box-containing proteins, it appears that the SOCS proteins may act as adaptor molecules that target activated cell signaling proteins to the protein degradation pathway.

Published
1999

9. Liver degeneration and lymphoid deficiencies in mice lacking suppressor of cytokine signaling-1

Author

Starr, Robyn, Metcalf, Donald, Elefanty, Andrew G., Brysha, Marta, Willson, Tracy A., Nicola, Nicos A., Hilton, Douglas J., and Alexander, Warren S.

Subjects
Cellular signal transduction -- Research, Cytokines -- Physiological aspects, Interleukin-6 -- Research, Liver diseases -- Research, Mice -- Physiological aspects, Science and technology
Abstract

SOCS-1, a member of the suppressor of cytokine signaling (SOCS) family, was identified in a genetic screen for inhibitors of interleukin 6 signal transduction. SOCS-1 transcription is induced by cytokines, and the protein binds and inhibits Janus kinases and reduces cytokine-stimulated tyrosine phosphorylation of signal transducers and activators of transcription 3 and the gp130 component of the interleukin 6 receptor. Thus, SOCS-1 forms part of a feedback loop that modulates signal transduction from cytokine receptors. To examine the role of SOCS-1 in vivo, we have used gene targeting to generate mice lacking this protein. SOCS-[1.sup.-/-] mice exhibited stunted growth and died before weaning with fatty degeneration of the liver and monocytic infiltration of several organs. In addition, the thymus of SOCS-[1.sup.-/-] mice was reduced markedly in size, and there was a progressive loss of maturing B lymphocytes in the bone marrow, spleen, and peripheral blood. Thus, SOCS-1 is required for in vivo regulation of multiple cell types and is indispensable for normal postnatal growth and survival.

Published
1998

10. Twenty proteins containing a C-terminal SOCS box form five structural classes

Author

Hilton, Douglas J., Richardson, Rachael T., Alexander, Warren S., Viney, Elizabeth M., Willson, Tracy A., Sprigg, Naomi S., Starr, Robyn, Nicholson, Sandra E., Metcalf, Donald, and Nicola, Nicos A.

Subjects
Proteins -- Research, Cytokines -- Research, Cellular signal transduction -- Research, Suppressor cells -- Research, Science and technology
Abstract

The four members of the recently identified suppressor of cytokines signaling family (SOCS-1, SOCS-2, SOCS-3, and CIS, where CIS is cytokine-inducible SH2-containing protein) appear, by various means, to negatively regulate cytokine signal transduction. Structurally, the SOCS proteins are composed of an N-terminal region of variable length and amino acid composition, a central SH2 domain, and a previously unrecognized C-terminal motif that we have called the SOCS box. By using the SOCS box amino acid sequence consensus, we have searched DNA databases and have identified a further 16 proteins that contain this motif. These proteins fall into five classes based on the protein motifs found N-terminal of the SOCS box. In addition to four new SOCS proteins (SOCS-4 to SOCS-7) containing an SH2 domain and a SOCS box, we describe three new families of proteins that contain either WD-40 repeats (WSB-1 and -2), SPRY domains (SSB-1 to -3) or ankyrin repeats (ASB-1 to -3) N-terminal of the SOCS box. In addition, we show that a class of small GTPases also contains a SOCS box. The expression of representative members of each class of proteins differs markedly, as does the regulation of expression by cytokines. The function of the WSB, SSB, and ASB protein families remains to be determined.

Published
1998

11. A family of cytokine-inducible inhibitors of signalling

Author

Starr, Robyn, Willson, Tracy A., Viney, Elizabeth M., Murray, Leecia J.L., Rayner, John R., Jenkins, Brendan J., Gonda, Thomas J., Alexander, Warren S., Metcalf, Donald, Nicola, Nicos A., and Hilton, Douglas J.

Subjects
Cytokines -- Research, Cell research -- Observations, Cancer -- Research, Environmental issues, Science and technology, Zoology and wildlife conservation
Abstract

Cellular responses ,such as differentiation and proliferation, are regulated by cytokines, which activate members of the JAK family of cytoplasmic tyrosine kinases via receptor aggregation. An expression cloning technique has been used to clone a complementary DNA (cDNA) encoding a protein SOCS-1, that has been found to be related to other full-length cDNAs encoding related proteins, termed SOCS-2 and SOCS-3. Transcription of the SOC family suggests that they may regulate cytokine signal transduction.

Published
1997

12. Leptin can induce proliferation, differentiation, and functional activation of hemopoietic cells

Author

Gainsford, Timothy, Willson, Tracy A., Metcalf, Donald, Handman, Emanuela, McFarlane, Clare, Ng, Ashley, Nicola, Nicos A., Alexander, Warren S., and Hilton, Douglas J.

Subjects
Leptin -- Physiological aspects, Hematopoietic stem cells -- Physiological aspects, Hematopoiesis -- Physiological aspects, Science and technology
Abstract

Many cytokines exert their biological effect through members of the hemopoietin receptor family. Using degenerate oligonucleotides to the common WSXWS motif, we have cloned from human hemopoietic cell cDNA libraries various forms of the receptor that was recently shown to bind the obesity hormone, leptin. mRNAs encoding long and short forms of the human leptin receptor were found to be coexpressed in a range of human and murine hemopoietic organs, and a subset of cells from these tissues bound leptin at the cell surface. Ectopic expression in murine Ba/F3 and M1 cell lines revealed that the long, but not the short, form of the leptin receptor can signal proliferation and differentiation, respectively. In cultures of murine or human marrow cells, human leptin exhibited no capacity to stimulate cell survival or proliferation, but it enhanced cytokine production and phagocytosis of Leishmania parasites by murine peritoneal macrophages. Our data provide evidence that, in addition to its role in fat regulation, leptin may also be able to regulate aspects of hemopoiesis and macrophage function.

Published
1996

14. Suppressor of cytokine signaling-3 preferentially binds to the SHP-2-binding site on the shared cytokine receptor subunit gp130

Author

Nicholson, Sandra E., De Souza, David, Fabri, Louis J., Corbin, Jason, Willson, Tracy A., Zhang, Jian-Guo, Silva, Anabel, Asimakis, Maria, Farley, Alison, Nash, Andrew D., Metcalf, Donald, Hilton, Douglas J., Nicola, Nicos A., and Baca, Manuel

Subjects
Biochemistry -- Research, Cytokines -- Research, Ligands -- Research, Tyrosine -- Analysis, Phosphatases -- Analysis, Proteins -- Analysis, Science and technology
Abstract

Suppressor of cytokine signaling-3 (SOCS-3) is one member of a family of intracellular inhibitors of signaling pathways initiated by cytokines that use, among others, the common receptor subunit gp130. The SH2 domain of SOCS-3 has been shown to be essential for this inhibitory activity, and we have used a quantitative binding analysis of SOCS-3 to synthetic phosphopeptides to map the potential sites of interaction of SOCS-3 with different components of the gp130 signaling pathway. The only high-affinity ligand found corresponded to the region of gp130 centered around phosphotyrosine-757 (pY757), previously shown to be a docking site for the tyrosine phosphatase SHP-2. By contrast, phosphopeptides corresponding to other regions within gp130, Janus kinase, or signal transducer and activator of transcription proteins bound to SOCS-3 with weak or undetectable affinity. The significance of pY757 in gp130 as a biologically relevant SOCS-3 docking site was investigated by using transfected 293T fibroblasts. Although SOCS-3 inhibited signaling in cells transfected with a chimeric receptor containing the wild-type gp130 intracellular domain, inhibition was considerably impaired for a receptor carrying a Y [right arrow] F point mutation at residue 757. Taken together, these data suggest that the mechanism by which SOCS-3 inhibits the gp130 signaling pathway depends on recruitment to the phosphorylated gp130 receptor, and that some of the negative regulatory roles previously attributed to the phosphatase SHP-2 might in fact be caused by the action of SOCS-3.

Published
2000

15. Myeloid leukaemia inhibitory factor maintains the developmental potential of embryonic stem cells

Author

Williams, R. Lindsay, Hilton, Douglas J., Pease, Shirley, Willson, Tracy A., Stewart, Colin L., Gearing, David P., Wagner, Erwin F., Metcalf, Donald, Nicolai, Nicos A., and Gough, Nicholas M.

Subjects
Cell differentiation -- Research, Stem cells -- Research, Mice as laboratory animals -- Research, Environmental issues, Science and technology, Zoology and wildlife conservation
Published
1988

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