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dc.contributor.authorGreen, Damian J.
dc.contributor.authorFrayo, Shani L.
dc.contributor.authorLin, Yukang
dc.contributor.authorHamlin, Donald K.
dc.contributor.authorFisher, Darrell R.
dc.contributor.authorFrost, Sofia H.L.
dc.contributor.authorKenoyer, Aimee L.
dc.contributor.authorHylarides, Mark D.
dc.contributor.authorGopal, Ajay K.
dc.contributor.authorGooley, Theodore A.
dc.contributor.authorOrozco, Johnnie J.
dc.contributor.authorTill, Brian G.
dc.contributor.authorO'Steen, Shyril
dc.contributor.authorOrcutt, Kelly Davis
dc.contributor.authorWilbur, D. Scott
dc.contributor.authorWittrup, Karl Dane
dc.contributor.authorPress, Oliver W.
dc.date.accessioned2020-06-03T15:00:57Z
dc.date.available2020-06-03T15:00:57Z
dc.date.issued2016-09
dc.date.submitted2016-08
dc.identifier.issn0008-5472
dc.identifier.issn1538-7445
dc.identifier.urihttps://hdl.handle.net/1721.1/125642
dc.description.abstractStreptavidin (SA)-biotin pretargeted radioimmunotherapy (PRIT) that targets CD20 in non-Hodgkin lymphoma (NHL) exhibits remarkable efficacy in model systems, but SA immunogenicity and interference by endogenous biotin may complicate clinical translation of this approach. In this study, we engineered a bispecific fusion protein (FP) that evades the limitations imposed by this system. Briefly, one arm of the FP was an anti-human CD20 antibody (2H7), with the other arm of the FP an anti-chelated radiometal trap for a radiolabeled ligand (yttrium[Y]-DOTA) captured by a very high-affinity anti-Y-DOTA scFv antibody (C825). Head-to-head biodistribution experiments comparing SA-biotin and bispecific FP (2H7-Fc-C825) PRIT in murine subjects bearing human lymphoma xenografts demonstrated nearly identical tumor targeting by each modality at 24 hours. However, residual radioactivity in the blood and normal organs was consistently higher following administration of 1F5-SA compared with 2H7-Fc-C825. Consequently, tumor-to-normal tissue ratios of distribution were superior for 2H7-Fc-C825 (P < 0.0001). Therapy studies in subjects bearing either Ramos or Granta subcutaneous lymphomas demonstrated that 2H7-Fc-C825 PRIT is highly effective and significantly less myelosuppressive than 1F5-SA (P < 0.0001). All animals receiving optimal doses of 2H7-Fc-C825 followed by 90Y-DOTA were cured by 150 days, whereas the growth of tumors in control animals progressed rapidly with complete morbidity by 25 days. In addition to demonstrating reduced risk of immunogenicity and an absence of endogenous biotin interference, our findings offer a preclinical proof of concept for the preferred use of bispecific PRIT in future clinical trials, due to a slightly superior biodistribution profile, less myelosuppression, and superior efficacy.en_US
dc.language.isoen
dc.publisherAmerican Association for Cancer Research (AACR)en_US
dc.relation.isversionofhttps://dx.doi.org/10.1158/0008-5472.can-16-0571en_US
dc.rightsCreative Commons Attribution-Noncommercial-Share Alikeen_US
dc.rights.urihttp://creativecommons.org/licenses/by-nc-sa/4.0/en_US
dc.sourcePMCen_US
dc.titleComparative Analysis of Bispecific Antibody and Streptavidin-Targeted Radioimmunotherapy for B-cell Cancersen_US
dc.typeArticleen_US
dc.identifier.citationGreen, Damian J. et al., "Comparative Analysis of Bispecific Antibody and Streptavidin-Targeted Radioimmunotherapy for B-cell Cancers" Cancer Research 76, 22 (November 2016): 6669–6679 ©2016 AACR.en_US
dc.contributor.departmentMassachusetts Institute of Technology. Department of Chemical Engineeringen_US
dc.contributor.departmentMassachusetts Institute of Technology. Department of Biological Engineeringen_US
dc.relation.journalCancer Researchen_US
dc.eprint.versionAuthor's final manuscripten_US
dc.type.urihttp://purl.org/eprint/type/JournalArticleen_US
eprint.statushttp://purl.org/eprint/status/PeerRevieweden_US
dc.date.updated2019-09-13T17:24:49Z
dspace.date.submission2019-09-13T17:24:52Z
mit.journal.volume76en_US
mit.journal.issue22en_US
mit.metadata.statusComplete


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