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Elena Koustova, Yoshitatsu Sei, Linda Fossom, Mei-Ling Wei, Peter N.R. Usherwood, N. Bradley Keele, Michael A. Rogawski, Anthony S. Basile
Published in Volume 107, Issue 6
J Clin Invest. 2001; 107(6):737–744 doi:10.1172/JCI11500
Abstract | Full text | PDF
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Figure 6

LP-BM5 brain IgG damages cerebellar granule neurons in vitro. In the absence of cyclothiazide (50 μM), LDH release into the medium (and associated neuron damage) did not exceed background levels (dashed line) after application of AMPA (a) or LP-BM5 brain IgG (b). AMPA or IgG in the presence of cyclothiazide dose dependently increased LDH release from granule neurons. The neurotoxicity induced by 100 μM AMPA or 900 ng IgG was suppressed by 10 μM NBQX (filled circles). IgG from control mouse brain in the presence of cyclothiazide (900 ng; open squares) did not increase neuronal damage above basal levels. MK-801 (5 μM) was present in all experiments.