期刊
CEREBRAL CORTEX
卷 14, 期 7, 页码 791-802出版社
OXFORD UNIV PRESS INC
DOI: 10.1093/cercor/bhh039
关键词
alcohol; fetal alcohol syndrome; integrin; nCAM; parietal cortex; somatosensory cortex; TGF beta 1
资金
- NIAAA NIH HHS [AA06916, AA07568] Funding Source: Medline
Transforming growth factor (TGF) beta1 regulates cell migration of non-neural cells. Hence, two hypotheses were tested: (i) that TGFbeta1 affects cell migration and the expression of associated adhesion proteins in developing cortex; and (ii) that these effects are antagonized by ethanol. The effects of TGFbeta1 (2.5-40 ng/ml) and ethanol (400 mg/dl) on cell migration were examined in organotypic cultures from fetal rat brains. Migration was determined by tracing the movement of cells pulse-labeled with bromodeoxyuridine. Cell migration was altered by TGFbeta1 in a concentration-dependent manner: at low concentrations, cell migration was promoted whereas at high concentrations TGFbeta1 impeded migration. Ethanol treatment alone reduced the rate of migration. Interestingly, the rate of cell migration in slices treated with both TGFbeta1 and ethanol was the same as that in untreated cultures. The expression of cell adhesion proteins (nCAM, integrin alpha(3), alpha(v) and beta(1)) was differentially effected by TGFbeta1 and/or ethanol. TGFbeta1 increased the expression of these adhesion proteins in a progressive, concentration-dependent manner. Likewise, ethanol also increased adhesion protein expression, however, combined TGFbeta1 and ethanol treatment reduced expression. Collectively, the data show that TGFbeta1 alters cell migration in the developing cortex and that the TGFbeta1 system is a target of ethanol toxicity.
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