Novel complement regulatory mechanisms in disease

Detta är en avhandling från Department of Medical protein chemistry

Författare: Emelie Holmquist; Lunds Universitet.; Lund University.; Lunds Universitet.; Lund University.; [2015]

Nyckelord: Medicin och hälsovetenskap Medicinska grundvetenskaper Cell- och molekylärbiologi; Medical and Health Sciences Basic Medicine Cell and Molecular Biology; Medicin och hälsovetenskap Medicinska grundvetenskaper Immunologi inom det medicinska området; Medical and Health Sciences Basic Medicine Immunology in the medical area;

Sammanfattning: Breast cancer cells have receptors on their surface and in their cytoplasm and nucleus. Chemical messengers such as hormones bind to receptors, and this causes changes in the cell. Breast cancer cells may or may not have three important receptors: estrogen receptor (ER), progesterone receptor (PR), and HER2.
ER+ cancer cells (that is, cancer cells that have estrogen receptors) depend on estrogen for their growth, so they can be treated with drugs to block estrogen effects (e.g. tamoxifen), and generally have a better prognosis. Untreated, HER2+ breast cancers are generally more aggressive than HER2- breast cancers,[80][81] but HER2+ cancer cells respond to drugs such as the monoclonal antibody trastuzumab (in combination with conventional chemotherapy), and this has improved the prognosis significantly.[82] Cells that do not have any of these three receptor types (estrogen receptors, progesterone receptors, or HER2) are called triple-negative, although they frequently do express receptors for other hormones, such as androgen receptor and prolactin receptor.

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