To increase the bioavailability of quercetin (Q) contained in various plants, including tea, acetylated Q (pentaacetyl quercetin, Q-Ac5) was synthesized, and the bioavailabilities of Q and Q-Ac5 were compared. Q and Q-Ac5 were administered orally (330 μmol/kg body wt.) to rats (Sprague-Dawley, ♂, six weeks old), and the blood plasma was analyzed by HPLC-ECD (+800 mV). Both compounds were absorbed as conjugated forms, not as Q and isorhamnetin, which is a methylated Q metabolite, in the free form, and Q-Ac5 in the intact form. The peak concentration of total Q (Q administration, 34.91 ± 9.1 μM; Q-Ac5 administration, 6.98 ± 2.3 μM) reached at 15 min after oral administration. The area under the curve (AUC) value in the Q administration group was four times higher than that in the Q-Ac5 administration group. The absorption ratio of Q was not improved by acetylation. This result was different from the case of several phenolic compounds, in which the absorption ratio was improved by acetylation. This dissimilarity might be caused by the difference in various factors, such as solubility, type of vehicle, molecular weight, and structural distinction. Nevertheless, this study provides useful information in terms of new drug development and bioavailability improvement of phenolic compounds by acetylation.