TY - JOUR
T1 - A cytotoxic humanized anti-ganglioside antibody produced in a murine cell line defective of N-glycolylated-glycoconjugates
AU - Fernández-Marrero, Yuniel
AU - Roque-Navarro, Lourdes
AU - Hernández, Tays
AU - Dorvignit, Denise
AU - Molina-Pérez, Marively
AU - González, Addys
AU - Sosa, Katya
AU - López-Requena, Alejandro
AU - Pérez, Rolando
AU - Mateo de Acosta, Cristina
PY - 2011/12
Y1 - 2011/12
N2 - Gangliosides containing the N-glycolyl (NGc) form of sialic acid are tumor-associated antigens and promising candidates for cancer therapy. We previously generated the murine 14F7 monoclonal antibody (mAb), specific for the N-glycolyl-GM3 ganglioside (NGcGM3), which induced an oncosis-like type of cell death on malignant cell lines expressing this antigen and recognized breast carcinoma by immunoscintigraphy in cancer patients. As humanization is expected to enhance its use for human cancer therapy, herein we describe the design and generation of two humanized versions of the 14F7 mAb by disrupting potential human T cell epitopes on its variable region. No differences in antigen reactivity or cytotoxic properties were detected among the variants tested and with respect to the chimeric counterpart. Humanized 14F7 genes were transfected into the NGcGM3-expressing NS0 cell line. Therefore, in the industrial scaling-up of the transfectoma in serum-free medium, cell viability was lost due to the cytotoxic effect of the secreted antibody. This shortcoming was solved by knocking down the CMP- N-acetylneuraminic acid hydroxylase enzyme, thus impairing the synthesis of NGc-glycoconjugates. Humanized 14F7 mAb is of potential value for the therapy of NGcGM3-expressing tumors.
AB - Gangliosides containing the N-glycolyl (NGc) form of sialic acid are tumor-associated antigens and promising candidates for cancer therapy. We previously generated the murine 14F7 monoclonal antibody (mAb), specific for the N-glycolyl-GM3 ganglioside (NGcGM3), which induced an oncosis-like type of cell death on malignant cell lines expressing this antigen and recognized breast carcinoma by immunoscintigraphy in cancer patients. As humanization is expected to enhance its use for human cancer therapy, herein we describe the design and generation of two humanized versions of the 14F7 mAb by disrupting potential human T cell epitopes on its variable region. No differences in antigen reactivity or cytotoxic properties were detected among the variants tested and with respect to the chimeric counterpart. Humanized 14F7 genes were transfected into the NGcGM3-expressing NS0 cell line. Therefore, in the industrial scaling-up of the transfectoma in serum-free medium, cell viability was lost due to the cytotoxic effect of the secreted antibody. This shortcoming was solved by knocking down the CMP- N-acetylneuraminic acid hydroxylase enzyme, thus impairing the synthesis of NGc-glycoconjugates. Humanized 14F7 mAb is of potential value for the therapy of NGcGM3-expressing tumors.
KW - Cmah
KW - Cytotoxic antibody
KW - Gangliosides
KW - Humanization
KW - N-glycolyl-GM3
KW - ShRNA
UR - http://www.scopus.com/inward/record.url?scp=80054944831&partnerID=8YFLogxK
U2 - 10.1016/j.imbio.2011.07.004
DO - 10.1016/j.imbio.2011.07.004
M3 - Article
C2 - 21802167
AN - SCOPUS:80054944831
SN - 0171-2985
VL - 216
SP - 1239
EP - 1247
JO - Immunobiology
JF - Immunobiology
IS - 12
ER -