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Xenobiotica
the fate of foreign compounds in biological systems
Volume 38, 2008 - Issue 10
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Research Article

PEGylation of somatropin (recombinant human growth hormone): Impact on its clearance in humans

, , , , , & show all
Pages 1340-1351 | Received 06 Apr 2008, Accepted 18 Aug 2008, Published online: 16 Oct 2008
 

Abstract

1. PHA-794428 is a PEGylated version of somatropin (human growth hormone). The pharmacokinetics of PHA-794428 have been studied in humans following single subcutaneous administration (dose range 10–500 µg kg−1). In the same study the pharmacokinetics of somatropin were also determined following a 3.6 mg (51 µg kg−1) subcutaneous dose. Comparison of the pharmacokinetics of both molecules indicates that PEGylation of somatropin with a 40 kD PEG results in a ten- to 20-fold increase in area under the curve and a similar increase in half-life when compared with somatropin in human (at equivalent subcutaneous doses).

2. Literature data indicate that somotropin is cleared by two mechanisms. The first processes is clearance by glomerular filtration. This is a passive, non-capacity-limited process. A second, capacity-limited, process is mediated by interaction with growth hormone receptors present in a number of tissues including the liver. It is hypothesized that PHA-794428 shares the same clearance mechanisms. However, the addition of the PEG moiety has modulated the clearance by both of these processes. Pharmacokinetic modelling of human serum concentration data obtained for these molecules strongly supports this hypothesis. The renal clearance is reduced due to the increased size of the molecule (Cl/F reduced from 9.6 to 0.1 l h−1 for somatropin and PHA-794428, respectively). In addition, the reduction in growth hormone receptor affinity has reduced the clearance mediated by interaction with this receptor (somatropin Km = 3.6 µg l−1 and Vmax = 104 µg h−1/PHA-794428 Km = 53 µg l−1 and Vmax = 84 µg h−1).

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