Abstract

Treatment of two human leukemia cell lines with 1.25% dimethyl sulfoxide at 37 °C results in a rapid increase in the number of transferrin receptors on the cell surface detected by fluoroscein-labeled anti-transferrin receptor antibodies. Both HL-60 cells, a human myeloid cell line, and K562 cells, a human erythroid—myeloid cell line, showed a 25–65% increase in cell surface transferrin binding in parallel experiments. Scatchard plot analysis of the data indicates that the number of receptors increases while the affinity of transferrin for the receptor remains the same. This rapid increase in the number of receptors at the cell surface appears to be due to a slowing of endocytosis rather than an increase in externalization of the receptor.

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