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Identification and characterization of fully human anti-CD22 monoclonal antibodies

Author:

Xiao, X.

Ho, M.

Zhu, Z.

Pastan, I.

Dimitrov, D. S.
Author Address

Protein Interactions Group, CCRNP, NCI-Frederick, NIH, Frederick, MD 21702-1201, USA. xiaox@ncifcrf.gov

1. Year: 2009
2. Date: May-Jun
3. Epub Date: 1/13/2010
Journal: Mabs
1. Volume: 1
2. Issue: 3
3. Pages: 297-303
Type of Article: Article
ISSN: 1942-0870 (Electronic);1942-0862 (Linking)

Abstract:

CD22 is a member of the B cell receptor family and is implicated in B cell function and development. It is expressed on multiple forms of B cell lymphoma and is an attractive cancer therapeutic target. We report here the identification of two fully human anti-CD22 antibodies using phage display methodology. Both antibodies exhibit specific binding to cell surface-associated CD22 in multiple B cell lines. Through ELISA using mammalian cell-expressed sub-domains of CD22 as binding antigen, we mapped the binding epitopes of the newly identified CD22 antibodies to be within the Ig-like domains 5 to 7 of CD22. Their epitopes do not overlap with those of several therapeutic antibodies currently in preclinical or clinical development. These antibodies have potential as cancer therapeutic candidates and research reagents.

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External Sources

View record in PubMed
PMID: 20065646
View record in PubMed Central
PMCID: PMC2726586

Library Notes

Fiscal Year: FY2008-2009

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