Abstract
Ribosomal protein L3 (RPL3) is known to be an indispensable and essential component for the peptidyltransferase center. In the present study, we found a novel function of RPL3 using a Xenopus laevis oocyte expression system. When expressed in X. oocytes, RPL3 mediated the high affinity transport of [3H]digoxin (Km = 213.3 ± 46.8 nM) in a time-, concentration-, and sodium-dependent manners. The maximum velocity of the transport of [3H]digoxin via RPL3 produced at physiological pH. However, we did not observe RPL3-mediated transport of several organic solutes such as [14C]androstenedione, [3H]dexamethasone, [3H]dehydroepiandrosterone sulfate, [3H]L-tryptophan, [14C]L-ascorbic acid, [14C]α-ketoglutarate, [14C]glutarate, [3H]methotrexate, [3H]bumetanide, [3H]probenecid, [14C]salicylic acid, [14C]theophylline and [3H]valproate. Our results suggest that RPL3 functions as a drug carrier protein and may be involved in the digoxin toxicity in the human body.
