Literature DB >> 22453096

Minipig as a potential translatable model for monoclonal antibody pharmacokinetics after intravenous and subcutaneous administration.

Yanan Zheng1, Devin B Tesar1, Lisa Benincosa2, Herbert Birnböck3, C Andrew Boswell4, Daniela Bumbaca4, Kyra J Cowan4, Dimitry M Danilenko4, Ann L Daugherty5, Paul J Fielder4, Hans Peter Grimm3, Amita Joshi4, Nicole Justies3, Gerry Kolaitis2, Nicholas Lewin-Koh4, Jing Li4, Sami McVay4, Jennifer O'Mahony4, Michael Otteneder3, Michael Pantze3, Wendy S Putnam4, Zhihua J Qiu4, Jane Ruppel4, Thomas Singer3, Oliver Stauch3, Frank-Peter Theil4, Jennifer Visich4, Jihong Yang4, Yong Ying4, Leslie A Khawli4, Wolfgang F Richter3.   

Abstract

Subcutaneous (SC) delivery is a common route of administration for therapeutic monoclonal antibodies (mAbs) with pharmacokinetic (PK)/pharmacodynamic (PD) properties requiring long-term or frequent drug administration. An ideal in vivo preclinical model for predicting human PK following SC administration may be one in which the skin and overall physiological characteristics are similar to that of humans. In this study, the PK properties of a series of therapeutic mAbs following intravenous (IV) and SC administration in Göttingen minipigs were compared with data obtained previously from humans. The present studies demonstrated: (1) minipig is predictive of human linear clearance; (2) the SC bioavailabilities in minipigs are weakly correlated with those in human; (3) minipig mAb SC absorption rates are generally higher than those in human and (4) the SC bioavailability appears to correlate with systemic clearance in minipigs. Given the important role of the neonatal Fc-receptor (FcRn) in the PK of mAbs, the in vitro binding affinities of these IgGs against porcine, human and cynomolgus monkey FcRn were tested. The result showed comparable FcRn binding affinities across species. Further, mAbs with higher isoelectric point tended to have faster systemic clearance and lower SC bioavailability in both minipig and human. Taken together, these data lend increased support for the use of the minipig as an alternative predictive model for human IV and SC PK of mAbs.

Entities:  

Keywords:  animal model; mAb IgG; minipig; neonatal Fc receptor (FcRn); pharmacokinetics; subcutaneous bioavailability

Mesh:

Substances:

Year:  2012        PMID: 22453096      PMCID: PMC3361660          DOI: 10.4161/mabs.4.2.19387

Source DB:  PubMed          Journal:  MAbs        ISSN: 1942-0862            Impact factor:   5.857


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