Publications by authors named "Nicholas Totty"

We have used global protein expression analysis to characterize the pathways of dexamethasone-mediated apoptosis and resistance in myeloma. Analysis of MM.1S cells by two-dimensional polyacrylamide gel electrophoresis (2D-PAGE) identified a series of proteins that were up- and downregulated following dexamethasone treatment.

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We have used an affinity purification method to identify substrates of protein kinase B/Akt. One protein that associates with 14-3-3 in an Akt-dependent manner is shown here to be the Yes-associated protein (YAP), which is phosphorylated by Akt at serine 127, leading to binding to 14-3-3. Akt promotes YAP localization to the cytoplasm, resulting in loss from the nucleus where it functions as a coactivator of transcription factors including p73.

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Cell surface antigen CD109 is a glycosylphosphatidylinositol (GPI)-linked glycoprotein of approximately 170 kd found on a subset of hematopoietic stem and progenitor cells and on activated platelets and T cells. Although it has been suggested that T-cell CD109 may play a role in antibody-inducing T-helper function and it is known that platelet CD109 carries the Gov alloantigen system, the role of CD109 in hematopoietic cells remains largely unknown. As a first step toward elucidating the function of CD109, we have isolated and characterized a human CD109 cDNA from KG1a and endothelial cells.

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Article Synopsis
  • IAPs (inhibitor-of-apoptosis proteins) help regulate cell death by inhibiting caspases, which are enzymes that facilitate apoptosis.
  • Reaper family proteins and Smac/DIABLO can bind to IAPs, preventing them from blocking caspases and promoting apoptosis in both flies and mammals.
  • The study identified Omi/HtrA2 as a new protein that binds to the IAP XIAP, has a role in apoptosis, and is released from mitochondria during cell death, suggesting it functions similarly to the Reaper family proteins.
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