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Emma Timms

Ontario Institute for Cancer Research

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Featured researches published by Emma Timms.

Nature | 1999

OPGL is a key regulator of osteoclastogenesis, lymphocyte development and lymph-node organogenesis

Young-Yun Kong; Hiroki Yoshida; Ildiko Sarosi; Hong-Lin Tan; Emma Timms; Casey Capparelli; Sean Morony; Antonio J. Oliveira-dos-Santos; Gwyneth Van; Annick Itie; Wilson Khoo; Andrew Wakeham; Colin R. Dunstan; David L. Lacey; Tak W. Mak; William J. Boyle; Josef M. Penninger

The tumour-necrosis-factor-family molecule osteoprotegerin ligand (OPGL; also known as TRANCE, RANKL and ODF) has been identified as a potential osteoclast differentiation factor and regulator of interactions between T cells and dendritic cells in vitro. Mice with a disrupted opgl gene show severe osteopetrosis and a defect in tooth eruption, and completely lack osteoclasts as a result of an inability of osteoblasts to support osteoclastogenesis. Although dendritic cells appear normal, opgl-deficient mice exhibit defects in early differentiation of T and B lymphocytes. Surprisingly, opgl-deficient mice lack all lymph nodes but have normal splenic structure and Peyers patches. Thus OPGL is a new regulator of lymph-node organogenesis and lymphocyte development and is an essential osteoclast differentiation factor in vivo.

Cell | 1993

Normal B lymphocyte development but impaired T cell maturation in CD45-Exon6 protein tyrosine phosphatase-deficient mice

Kenji Kishihara; Josef Penninger; Valerie A. Wallace; Thomas M. Kündig; Kazuhiro Kawal; Andrew Wakeham; Emma Timms; Klaus Pfeffer; Pamela S. Ohashi; Matthew L. Thomas; Caren Furlonger; Christopher J. Paige; Tak W. Mak

The transmembrane tyrosine phosphatase CD45 is expressed in multiple isoforms on all nucleated hematopoietic cells, resulting from alternative splicing of variable exons. We generated mice with a mutation in the variable CD45 exon 6, using homologous recombination. In mice homozygous for the CD45-exon6 mutation, B cells and most T cells did not express CD45. Development of B cells appeared normal, although Ig mu-induced proliferation was completely abrogated. Thymocyte maturation was blocked at the transitional stage from immature CD4+CD8+ to mature CD4+ or CD8+ cells, and only a few T cells could be detected in peripheral lymphoid organs. Clonal deletion of superantigen-reactive T cells still occurred. Cytotoxic T cell responses to lymphocytic choriomeningitis virus were absent in CD45-exon6-/- mice. These data imply that CD45 is differentially required for the development and function of B and T lymphocytes.

Cell | 1996

Impaired Negative Selection of T Cells in Hodgkin's Disease Antigen CD30–Deficient Mice

Ryuichi Amakawa; Anne Hakem; Thomas M. Kündig; Toshifumi Matsuyama; John J.L. Simard; Emma Timms; Andrew Wakeham; Hans-Willi Mittruecker; Henrik Griesser; Hiroaki Takimoto; Rudolf Schmits; Arda Shahinian; Pamela S. Ohashi; Josef Penninger; Tak W. Mak

CD30 is found on Reed-Sternberg cells of Hodgkins disease and on a variety of non-Hodgkins lymphoma cells and is up-regulated on cells after Epstein-Barr virus, human T cell leukemia virus, and HIV infections. We report here that the thymus in CD30-deficient mice contains elevated numbers of thymocytes. Activation-induced death of thymocytes after CD3 cross-linking is impaired both in vitro and in vivo. Breeding the CD30 mutation separately into alpha beta TCR-or gamma delta TCR-transgenic mice revealed a gross defect in negative but not positive selection. Thus, like TNF-receptors and Fas/Apo-1, the CD30 receptor is involved in cell death signaling. It is also an important coreceptor that participates in thymic deletion.

Proceedings of the National Academy of Sciences of the United States of America | 1999

Tumor necrosis factor receptor family member RANK mediates osteoclast differentiation and activation induced by osteoprotegerin ligand

Hailing Hsu; David L. Lacey; Colin R. Dunstan; Irina Solovyev; Anne Colombero; Emma Timms; Hong-Lin Tan; Gary Elliott; Michael J. Kelley; Ildiko Sarosi; Ling Wang; Xing-Zhong Xia; Robin Elliott; Laura Chiu; Tabitha Black; Sheila Scully; Casey Capparelli; Sean Morony; Grant Shimamoto; Michael B. Bass; William J. Boyle

Nature | 1992

Profound block in thymocyte development in mice lacking p56lck.

T. J. Molina; Kenji Kishihara; D. P. Siderovskid; W. van Ewijk; A. Narendran; Emma Timms; Andrew Wakeham; Christopher J. Paige; K.-U. Hartmann; A. Veillette; D. Davidson; Tak W. Mak

Infection and Immunity | 1998

Effective and Long-Lasting Immunity against the Parasite Leishmania major in CD8-Deficient Mice

Magdalena Huber; Emma Timms; Tak W. Mak; Martin Röllinghoff; Michael Lohoff

Journal of Experimental Medicine | 1993

The induction of experimental autoimmune myocarditis in mice lacking CD4 or CD8 molecules [corrected]

Josef M. Penninger; N Neu; Emma Timms; Valerie A. Wallace; D R Koh; Kenji Kishihara; C Pummerer; T W Mak

Journal of Immunology | 1997

T cell development in mice expressing splice variants of the protein tyrosine phosphatase CD45.

Ivona Kozieradzki; Thomas M. Kündig; Kenji Kishihara; Christopher J. Ong; D Chiu; Valerie A. Wallace; Kazuhiro Kawai; Emma Timms; J Ionescu; Pamela S. Ohashi; Jamey D. Marth; T W Mak; Josef M. Penninger

European Journal of Immunology | 1995

T lymphocyte development in p56lck deficient mice: allelic exclusion of the TcR β locus is incomplete but thymocyte development is not restored by TcR β or TcR αβ transgenes

Valerie A. Wallace; Kazuhiro Kawai; Christiaan N. Levelt; Kenji Kishihara; Thierry Molina; Emma Timms; Hanspeter Pircher; Josef Penninger; Pamela S. Ohashi; Klaus Eichmann; Tak W. Mak

Journal of Experimental Medicine | 1992