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Vol. 26, Issue 2, 126-131, February 1998
Drug metabolism and Pharmacokinetics Lab., Chugai Pharmaceutical
Co., Ltd.(M.K., K.M., H.K., A.O., K.K.) and
Faculty of Pharmaceutical
Sciences, University of Tokyo (Y.K., Y.S)
We examined the pharmacokinetics of recombinant human
erythropoietin (rh-EPO) in genetically anemic mice
(W/Wv genotype) to clarify its disposition
mechanism in hematopoietic injury such as occurs in aplastic anemia.
After rh-EPO was administered to W/Wv and
control (+/+ genotype) mice once a day for 1 week at different doses,
both the hematocrit (Hct) and tissue uptake clearance (CLup) of
125I-rh-EPO by spleen and bone marrow in the
femur were estimated on the eighth day. The hematocrit increased on
eighth day, depending on the dose administered. Compared with +/+ mice
10 times more rh-EPO was needed in W/Wv mice to
produce an almost equivalent pharmacological effect. In +/+ mice, the
CLup of 125I-rh-EPO by spleen increased to
4-fold that of controls after treatment with rh-EPO, 4.8 µg/kg,
whereas that by bone marrow remained unchanged, irrespective of the
dose administered. On the other hand, the increase in both the Hct and
CLup in spleen was minimal in W/Wv mice. The
CLup by bone marrow and spleen in both types of mice showed saturation
with similar Km values
(389-619 pM), comparable with the dissociation constant of the EPO
receptor. In addition, the Hct correlated with the sum of the CLup by
bone marrow and spleen in both types of mice, and the correlation lines were superimposable. These results suggest that the pharmacological receptors govern the saturable tissue uptake not only in normal mice
but also in those that are anemic.
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