Nonclinical Safety, Pharmacokinetics, and Pharmacodynamics of Atacicept

doi:10.1093/toxsci/kfn105

ToxSci Advance Access originally published online on June 2, 2008
Toxicological Sciences 2008 105(1):200-210; doi:10.1093/toxsci/kfn105

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Nonclinical Safety, Pharmacokinetics, and Pharmacodynamics of Atacicept

Michela Carbonatto^*, Ping Yu^*, Mauro Bertolino^*, Enrico Vigna^*, Stephanie Steidler^*, Laura Fava^*, Chiara Daghero^*, Bruno Roattino^*, Manuela Onidi^*, Michele Ardizzone^*, Sergio Peano^*, Jennifer Visich, Derek Janszen, Stacey Dillon and Rafael Ponce^,1

^* Merck Serono (Istituto di Ricerche Biomediche "Antoine Marxer" RBM SpA)—10010 Colleretto Giacosa, Italy ZymoGenetics, Inc., Seattle, Washington 98102

¹ To whom correspondence should be addressed at Preclinical Safety Assessment, ZymoGenetics, Inc., 1201 Eastlake Ave. E., Seattle, WA 98102. Fax: (206) 442-6608. E-mail: reap{at}zgi.com.

Received March 27, 2008; accepted May 18, 2008

Abstract

Atacicept, a soluble recombinant fusion protein of the humanimmunoglobulin (Ig) G₁ Fc and the extracellular domain of thehuman transmembrane activator and calcium modulator and cyclophylinligand interactor receptor, acts as an antagonist of both Blymphocyte stimulator and a proliferating–inducing ligand.Here we determined the nonclinical safety, pharmacokineticsand pharmacodynamics of atacicept in mice and cynomolgus monkeys.Subcutaneous atacicept treatment (twice weekly in cynomolgusmonkeys, three times weekly in mice) was generally safe andwell tolerated safe and well tolerated with dosing up to 10mg/kg every other day for up to 39 weeks or up to 80 mg/kg whendosed for 4 weeks. At a dose of 1 mg/kg subcutaneous (sc) bioavailabilityof atacicept in mice and monkeys was 76 and 92%, with a meanserum t_1/2 of 44 and 179 h, respectively. In accord with itsanticipated mechanism of action, repeated administration ofatacicept decreased serum IgG concentrations up to 50%, IgMconcentrations >99%, and circulating mature B-cell concentrationsup to 60%. These effects were dose-related but reversible, asdetermined in a 25-week follow-up period. Microscopically, Bcells numbers were reduced in the follicular marginal zone ofthe spleen and the mantle surrounding germinal centers of thelymph nodes. These data confirm the preclinical safety and thepharmacological activity of atacicept and support its clinicaldevelopment.

Key Words: autoimmune; toxicity; chronic; immunotoxicity; pharmaceuticals.

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