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Early and late passage C-6 glial cell growth: Similarities with primary glial cells in culture
Authors:Dimitra Mangoura MD PhD  Nikos Sakellaridis MD  PhD  Jackeline Jones  Antonia Vernadakis
Institution:(1) Department of Psychiatry and Pharmacology, University of Colorado School of Medicine, Denver, Colorado, USA;(2) Present address: Department of Pediatrics, Biochemistry & Molecular Biology, University of Chicago Medical School, Maryland Avenue, Box 82, 5841 S. Chicago, Illinois, 60637;(3) Present address: Department of Pharmacology and Toxicology, University of Indiana School of Medicine Northwest Center for Medical Education, 3400 Broadway Gary, Indiana, 46408;(4) Departments of Psychiatry and Pharmacology, University of Colorado School of Medicine, 9th Avenue, 4200 E Denver, CO, 80262
Abstract:Earlier studies in our laboratory have shown that C-6 glial cells in culture exhibit astrocytic properties with increasing cell passage. In this study, we tested the responsiveness of early and late passage C-6 glial cells to various cultures conditions: culture substrata (collagen, poly-L-lysine, plastic), or supplements for the culture medium, DMEM, fetal calf, or heat inactivated (HI) serum, or media conditioned from mouse neuroblastoma cells (NBCM) or primary chick embryo cultured neurons (NCM)]. Glutamine synthetase (GS) and cyclic nucleotide phosphohydrolase (CNP), astrocytic and oligodendrocytic glial markers, were used. Cell numer and protein content increased exponentially with days in culture regardless of the type of the substratum or cell passage. Differences in cell morphology among the three types of substratum were also reflected on GS activity, which rose by three-fold on culture day 3 for cells grown on collagen; thereafter, GS profiles were similar for all substrata. This early rise in GS is interpreted to reflect differential cell adhesion processes on the substrata; specifically, cell adhesion on the collagen stimulated differentiation into ldquoastrocytic phenotyperdquo.Analogous to immature glia cells in primary cultures, early passage C-6 glial cells responded to neuronal factors supplied either from NCM or NBCM by expressing reduced GS activity, the astrocytic marker and enhanced CNP activity, the oligodendrocytic marker. Thus, early passage cells can be induced to express either astrocytic or oligodendrocytic phenotype. In accordance with our previous reports on primary glial cells, late passage C-6 cells exhibit their usual astrocytic behavior, responding to serum factors with GS activity. Moreover, whereas NCM or NBCM alone markedly lowered GS activity, a combination with serum restored activity. The present findings confirm our previous observations and further establish the C-6 glial cells as a reliable model to study immature glia.Special issue dedicated to Dr. Paola S. Timiras.
Keywords:Glial cell  C-6 glioma cells  primary culture  glutamine synthetasc  CNP  cell passage
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