Most leukemic cell lines and primary blood samples originated from cells that were moving throughout the circulatory system. Isn't it likely that culturing them in a still setting may be altering their properties (transcription, differentiation, etc.)? Why are there so few culture systems available or used in the literature that account for this difference? After all, the goal is to make the model as similar to actual physiology as possible, correct? I haven't been able to ever find any material on this topic; any input would be useful.

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