Role of tyrosine kinases in G-protein signaling /

Wan, Yong.

January 1997

Thesis (Ph. D.)--Cornell University, December, 1997. / Vita. Includes bibliographical references (leaves 96-113).

Tied together a molecular role for Tie1 in angiopoietin Tie2 signaling /

Seegar, Tom Conrad Maugans,

January 1900

Thesis (Ph.D.)--Virginia Commonwealth University, 2010. / Prepared for: Dept. of Biochemistry. Title from title-page of electronic thesis. Bibliography: leaves 106-117

The Met receptor tyrosine kinase in mammary gland tumorigenesis and development /

Petkiewicz, Stephanie L.

January 2007

The Met receptor tyrosine kinase (RTK) is expressed in the mammary gland under both normal and neoplastic conditions. Overexpression of the Met receptor is found in 15--20% of human breast cancers and is correlated with shortened disease-free interval and overall survival. In order to explore the role of dysregulated Met receptor signaling on the development of mammary tumors I have characterized a transgenic mouse model that expresses either wild type or a dysregulated Met receptor in the mammary epithelium under the control of the mouse mammary tumor virus promoter/enhancer (MMTV-Met). The Met receptor variants contained a mutation that results in decreased receptor ubiquitination and prolonged receptor signaling (Y1003F) or an activating mutation that was originally observed in patients with papillary renal carcinoma (M1250T) or both mutations (YF/MT). In vitro and in vivo transformation assays demonstrated that each mutation singly is weakly transforming, however, there was an additive effect on transformation when both mutations were present. This additive effect was observed in the transgenic mice where multiparous MMTV-Met-YF/MT mice developed tumors earlier and with much greater penetrance than did mice expressing either of the single mutants. This provides the first in vivo model that demonstrates a role for ubiquitination in suppression of transforming activity of an RTK. MMTV-Met-YF/MT tumors displayed a range of histological phenotypes but were mainly comprised of luminal lineage cells. Notably, MMTV-Met-M1250T tumors contained cells from both the basal and luminal populations, suggesting transformation of a progenitor cell. Progenitor cell transformation in RTK transgenic mouse models is uncommon and highlights distinct signaling differences and potentially lineage specificity of the two Met mutants. / Through assays of overexpression in vivo and inhibition in vitro, Met receptor signaling has been correlated with the development of the mammary gland. To examine the effects of loss of Met receptor signaling on mammary gland development I have utilized the Cre/LoxP1 recombination system to knock-out the Met receptor from the mammary epithelium. Mammary-specific Cre recombinase efficiently excised floxed DNA as visualized by activation of a beta-galactosidase reporter In Met+/+ glands, however, few beta-galactosidase positive cells are retained In the Mefl/fl glands and an intermediate number are retained in the Met fl/+ glands. This indicates that Met-null cells are selected against and supports a role for Met in the development of the mammary gland.

Receptor Protein-Tyrosine Kinases.

Mammary Tumor Virus, Mouse -- genetics.

Protein tyrosine kinases and the regulation of signalling and adhesion in Drosophila melanogaster /

Grabbe, Caroline,

January 2007

Diss. (sammanfattning) Umeå : Umeå Universitet, 2007. / Härtill 5 uppsatser.

C-SRC phosphorylation of P190 RHOGAP : regulation of P190/P120 RASGAP interaction /

Roof, Richard W.

January 1999

Thesis (Ph. D.)--University of Virginia, 1999. / Includes bibliographical references (p. 192-224). Also available online through Digital Dissertations.

Fms signal transduction, p150S̳h̳i̳p̳ : a signal transduction molecule with inositol 5-phosphatase activity /

Lioubin, Mario N.

January 1996

Thesis (Ph. D.)--University of Washington, 1996. / On t.p. "S̳h̳i̳p̳" is superscript. Vita. Includes bibliographical references (leaves [94]-105).

The role of cellular factors in modulation of entry by ovine betaretroviruses and murine gammaretroviruses /

Van Hoeven, Neal Scott.

January 2005

Thesis (Ph. D.)-- University of Washington, 2005. / Vita. Includes bibliographical references (leaves 126-142).

The Met receptor tyrosine kinase in mammary gland tumorigenesis and development /

Petkiewicz, Stephanie L.

January 2007

No description available.

Mammary Tumor Virus, Mouse -- genetics.

Receptor Protein-Tyrosine Kinases.

Differential regulation of c-Cbl and Cbl-b ubiquitin ligases downstream of the Met receptor tyrosine kinase

Durrant, Michael, 1982-

January 2007

The Cbl family of E3 ubiquitin ligases are important negative regulators of multiple receptor and cytoplasmic tyrosine kinases, and participate in a wide variety of cellular processes. Uncoupling of Cbl-mediated negative regulation allows activated receptor tyrosine kinases such as the Met receptor to escape degradation, enhancing their oncogenic potential in vitro and in vivo. Despite the consequences of loss of Cbl-mediated negative regulation for human disease, little is known about the mechanisms regulating Cbl protein levels themselves. / In this thesis work, I demonstrate a differential regulation of c-Cbl and Cbl-b downstream of the Met receptor tyrosine kinase. Cbl-b protein levels decrease in response to Met kinase activity, whereas c-Cbl levels remain stable. Cbl-b is partially degraded in a proteasome-dependant manner. This requires Cbl-b ubiquitin ligase activity and a carboxy terminal domain region located between the RING and UBA domains. I conclude that the regulation of c-Cbl and Cbl-b differs downstream of Met, and propose that negative regulation of Cbl-b by a dysregulated Met receptor may contribute to tumourigenesis.

Gene Expression Regulation, Neoplastic.

Ubiquitin-Protein Ligases -- metabolism.

Signal transduction in focal cerebral ischemia : experimental studies on VEGF, MAPK and Src family kinases /

Lennmyr, Fredrik,

January 2002

Diss. (sammanfattning) Uppsala : Univ., 2002. / Härtill 4 uppsatser.