Journal
JOURNAL OF CELLULAR AND MOLECULAR MEDICINE
Volume 5, Issue 4, Pages 417-428Publisher
CAROL DAVILA UNIV PRESS
DOI: 10.1111/j.1582-4934.2001.tb00177.x
Keywords
Fas (APO-1/CD95); apoptosis; human development; brain primary culture; TUNEL; annexin V; caspase-8; neurons; glial cells
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Fas (APO-1/CD95) is an important apoptotic mediator for both immune and nervous systems. In the present study, we have investigated the expression and function of Fas in human embryonic/fetal brain primary cultures from 12 human embryos and fetuses with gestational ages between 5 to 22 weeks. Anti-Fas fluorescent antibody was used for labeling of Fas positive cells and for quantitation of Fas expression in brain cultures. To demonstrate that Fas receptor is functional in human embryonic/fetal brain cells, anti-Human-Fas monoclonal antibody (0.5 mug/ml) was used to induce apoptosis in brain primary cultures. Apoptosis was investigated by flow-cytometry and fluorescent microscopy using TUNEL and annexin V labeling. Fas was found to be expressed in the embryonic/fetal human primary brain cultures, on neuronal and glial cells or their precursors, varying with gestational ages. Cross-linking of Fas induced apoptosis in brain cultures indicating that Fas receptor functions as a death receptor. We also showed that cell death triggered through Fas receptor was caspase dependent, hence it was blocked by a selective caspase-8 inhibitor (IETD-fmk). These results suggest that Fas is involved in neuronal apoptosis in the developing human brain.
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