Dorothy Levis scite author profile

Immunotherapy has revolutionized cancer therapy. Two recently FDA-approved immunotherapies for B-cell malignancies target CD19, in the form of a Bispecific T-Cell Engager (BiTE) antibody construct or chimeric antigen receptor T (CAR-T) cells. Blinatumomab, an FDA-approved BiTE, binds to CD19 on B cells and to CD3 on T cells, mediating effector-target cell contact and T-cell activation that results in effective elimination of target B cells. Although CD19 is expressed by essentially all B-cell malignancies at clinical presentation, relapses with loss or reduction in CD19 surface expression are increasingly recognized as a cause of treatment failure. Therefore, there is a clear need to develop therapeutics for alternate targets. We have developed a novel BiTE consisting of humanized anti-CD22 and anti-CD3 single chain variable fragments. Target binding of the anti-CD22 and anti-CD3 moieties was confirmed by flow cytometry. CD22-BiTE promoted in vitro cell-mediated cytotoxicity in a dose and effector: target (E:T)-dependent fashion. Additionally, in an established acute lymphoblastic leukemia (ALL) xenograft mouse model, CD22-BiTE demonstrated tumor growth inhibition, comparable to blinatumomab. Further, the combination of blinatumomab and CD22-BiTE yielded increased efficacy in vivo when compared to the single agents. In conclusion, we report here the development of a new BiTE with cytotoxic activity against CD22+ cells which could represent an alternate or complementary therapeutic option for B-cell malignancies.

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22-P

Jackowski

Kuchipudi

Levis

et al. 2013

Human Immunology

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19-P Examining varibility in unacceptable antigen calls between histocompatibility labs within a given UNOS region: A sharing among friends

DiPaola¹,

Levis²,

Teresi³

et al. 2011

Human Immunology

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47-P: Titer of Antibodies Can Be Estimated from Median Channel Shifts of Positive Flow Crossmatches

Rosenberg

Jackowski

et al. 2010

Human Immunology

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Dorothy Levis

Multi-Array Antibody Screening in Detecting Antibodies to Mismatched HLA in Patients Awaiting a Second Transplant

A Novel bispecific T-cell engager (BiTE) targeting CD22 and CD3 has both in vitro and in vivo activity and synergizes with blinatumomab in an acute lymphoblastic leukemia (ALL) tumor model

22-P

19-P Examining varibility in unacceptable antigen calls between histocompatibility labs within a given UNOS region: A sharing among friends

47-P: Titer of Antibodies Can Be Estimated from Median Channel Shifts of Positive Flow Crossmatches

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