OVEREXPRESSION OF THE BETA-1 THYROID RECEPTOR INDUCES DIFFERENTIATIONIN NEURO-2A CELLS

To determine the functions of the alpha1 and beta1 thyroid hormone rec eptors (TRs) in neural differentiation, we have established stable tra nsfected neuronal cell lines (Neuro-2a) that overexpress either TRalph a1 or TRbeta1. 3,5,3'-Triiodothyronine (T3) treatment of cells that ov erexpress TRbeta1 blocks proliferation by an arrest of cells in G0/G1 and induces morphological and functional differentiation of Neuro-2a c ells as indicated by the marked increase in the number of perisomatal filopodia-like neurites and in acetylcholinesterase (AChE) activity. T he effect on AChE activity was dose-dependent, and the time-course ana lysis reveals that this effect occurs after 24 hr of T3 treatment, wit h a maximal increase occurring after 48 hr of treatment. The increase of AChE activity is paralleled by an increase of AChE mRNAs. Last, we present evidence that shows that the effects of T3 on differentiation are independent of its effect on proliferation. T3 had no effect on th e differentiation of Neuro-2a cells that overexpressed TRalpha1. Our r esults indicate that TRbeta1 may play a kev role in the effects of T3 in neuroblastoma cell differentiation.