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Vol. 301, Issue 2, 467-477, May 2002
Department of Biopharmaceutics and Drug Metabolism, Graduate School
of Pharmaceutical Sciences, Kyoto University, Sakyo-ku, Kyoto, Japan
(Y.Y., K.S., K.Y., Y.T.); Department of Drug Delivery Research,
Graduate School of Pharmaceutical Sciences, Kyoto University, Sakyo-ku,
Kyoto, Japan (M.N., F.Y., M.H.)
In vivo disposition characteristics of succinylated (Suc-) proteins
were studied after intravenous injection in mice in relation to their
molecular characteristics as negatively charged macromolecules. Recombinant superoxide dismutase (SOD; molecular mass, 32 kDa), bovine serum albumin (BSA; molecular mass, 67 kDa), and bovine IgG
(molecular mass, 150 kDa) were used to produce succinylated derivatives
with different degrees of modification. 111In-labeled
Suc-SODs were rapidly excreted into the urine with no significant
hepatic uptake. In contrast, 111In-Suc-BSA and Suc-IgG were
significantly taken up by liver nonparenchymal cells via scavenger
receptors (SRs) according to the degree of succinylation and the dose
injected. Interestingly, highly succinylated BSAs exhibited significant
accumulation in the kidney at higher doses when the hepatic uptake was
saturated. Pharmacokinetic analysis demonstrated that the hepatic
uptake of succinylated proteins depended on the molecular size and the
estimated surface density of succinylated amino residues. Further
analysis based on a physiological pharmacokinetic model, involving a
saturable process with Michaelis-Menten kinetics, revealed that the
surface density of negative charges was correlated with the affinity of
larger succinylated proteins for the hepatic SRs. Thus, the present
study has provided useful basic information for a therapeutic strategy
and the molecular design of succinylated proteins for use as drug
carriers and therapeutic agents per se for SR-mediated targeting in vivo.
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