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| Martin Poenie | |
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Associate Professor Ph.D. Stanford, 1986 Office PAT 543C
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| T cells are an important part of our immune system and are distinctive
because they carry out their function by interacting with other cells
in a highly specific and directional manner. They can either kill
other cells by secreting cytotoxic substances or they can help other
cells by secreting special growth factors. In order to carry out these
functions, they form a specialized junction with their target cell
called an immune synapse. Subsequently, they move the microtubule
organizing center up close to the synapse and established a special
secretory zone. Finally, they deliver the contents of their secretory
vesicles to this secretory zone. We have been studying how T cells polarize their cytoskeleton in response to antigenic target cells. As part of this effort we have developed a new form of light microscopy called modulated polarization microscopy (MPM) that makes it possible to see cytoskeletal movements in living T cells. Studies using MPM provided important new insights into how this process works and given us clues about microtubules are anchored at the synapse. Currently we are studying how microtubules interact with the synapse and in particular how microtubule motor proteins become anchored there. |
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