Engineered humanized diabodies for microPET imaging of prostate stem cell antigen-expressing tumors

doi:10.1093/protein/gzn055

PEDS Advance Access published online on October 28, 2008
Protein Engineering Design and Selection, doi:10.1093/protein/gzn055

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Engineered humanized diabodies for microPET imaging of prostate stem cell antigen-expressing tumors

Jeffrey V. Leyton¹, Tove Olafsen¹, Mark A. Sherman³, Karl B. Bauer¹, Patrick Aghajanian¹, Robert E. Reiter² and Anna M. Wu¹^,4

¹Crump Institute for Molecular Imaging, Department of Molecular and Medical Pharmacology, David Geffen School of Medicine at UCLA, 700 Westwood Plaza ²Department of Urology, UCLA, Center for the Health Sciences, 10833 Le Conte Ave., Los Angeles, CA 90095 ³Division Information Sciences, City of Hope National Medical Center, City of Hope, 1500 East Duarte Rd, Duarte, CA 91010, USA

⁴ To whom correspondence should be addressed. E-mail: awu{at}mednet.ucla.edu

We have previously demonstrated preclinical in vivo targetingof prostate stem cell antigen (PSCA) using a humanized anti-PSCA2B3 monoclonal antibody (mAb). However, humanization resultedin 5-fold loss of apparent affinity relative to the parentalmAb (1 nM). In this study, diabodies (scFv dimers of 55 kDa)were generated from 2B3 including variants with different linkerlengths as well as back-mutations to original murine residuesto improve affinity. Parental 2B3 (p2B3) and back-mutated 2B3(bm2B3) diabodies (Dbs) with five- or eight-amino acid linkers(p2B3-Db5, p2B3-Db8, bm2B3-Db5 and bm2B3-Db8) were evaluatedfor binding to PSCA by flow cytometry and affinities were determinedby surface plasmon resonance. Back-mutation restored the affinityfrom 5.4 to 1.9 nM. Stability, evaluated by size exclusion,revealed that diabodies with eight-residue linkers existed asa mixture of dimeric and monomeric species at low concentrations( $≤$ 1 mg/ml). Shortening the linker from eight to five residuesimproved dimer stability, notably in the bm2B3-Db8 comparedwith bm2B3-Db5. Both p2B3-Db8 and bm2B3-Db8 were radioiodinatedwith ¹²⁴I and evaluated by serial micro-positron emission tomographyimaging in mice bearing LAPC-9 human prostate cancer xenografts.Localization in LAPC-9 xenografts was seen at 4 h, whereas at20 h most of the activity had cleared from the tumor. Highesttumor-to-background contrast ratios and best images were obtainedat 12 h. Although the higher affinity bm2B3-Db8 demonstratedimproved tumor retention at later time points (20 h), it didnot improve tumor targeting or imaging compared with p2B3-Db8at 12 h.

Keywords: affinity maturation/diabody/PET/prostate cancer/PSCA

Received September 15, 2008; revised September 15, 2008; accepted September 18, 2008.

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