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Please use this identifier to cite or link to this item: https://doi.org/10.18632/oncotarget.442
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dc.titleEngineering the First Chimeric Antibody in Targeting Intracellular PRL-3 Oncoprotein for Cancer Therapy in Mice
dc.contributor.authorGuo, Ke
dc.contributor.authorTang, Jing Ping
dc.contributor.authorJie, Li
dc.contributor.authorAl-Aidaroos, Abdul Qader O
dc.contributor.authorHong, Cheng William
dc.contributor.authorTan, Cheng Peow Bobby
dc.contributor.authorPark, Jung Eun
dc.contributor.authorVarghese, Leyon
dc.contributor.authorFeng, Zhiwei
dc.contributor.authorZhou, Jianbiao
dc.contributor.authorChng, Wee Joo
dc.contributor.authorZeng, Qi
dc.date.accessioned2021-10-19T07:25:36Z
dc.date.available2021-10-19T07:25:36Z
dc.date.issued2012-02-01
dc.identifier.citationGuo, Ke, Tang, Jing Ping, Jie, Li, Al-Aidaroos, Abdul Qader O, Hong, Cheng William, Tan, Cheng Peow Bobby, Park, Jung Eun, Varghese, Leyon, Feng, Zhiwei, Zhou, Jianbiao, Chng, Wee Joo, Zeng, Qi (2012-02-01). Engineering the First Chimeric Antibody in Targeting Intracellular PRL-3 Oncoprotein for Cancer Therapy in Mice. ONCOTARGET 3 (2) : 158-171. ScholarBank@NUS Repository. https://doi.org/10.18632/oncotarget.442
dc.identifier.issn19492553
dc.identifier.urihttps://scholarbank.nus.edu.sg/handle/10635/203816
dc.description.abstractAntibodies are considered as 'magic bullets' because of their high specificity. It is believed that antibodies are too large to routinely enter the cytosol, thus antibody therapeutic approach has been limited to extracellular or secreted proteins expressed by cancer cells. However, many oncogenic proteins are localized within the cell. To explore the possibility of antibody therapies against intracellular targets, we generated a chimeric antibody targeting the intracellular PRL-3 oncoprotein to assess its antitumor activities in mice. Remarkably, we observed that the PRL-3 chimeric antibody could efficiently and specifically reduce the formation of PRL-3 expressing metastatic tumors. We further found that natural killer (NK) cells were important in mediating the therapeutic effect, which was only observed in a nude mouse model (T-cell deficient), but not in a Severe Combined Immunodeficiency' (scid) mouse model (B- and T-cell deficient), indicating the anticancer effect also depends on host B-cell activity. Our study involving 377 nude and scid mice suggests that antibodies targeting intracellular proteins can be developed to treat cancer. © Zeng et al.
dc.language.isoen
dc.publisherIMPACT JOURNALS LLC
dc.sourceElements
dc.subjectScience & Technology
dc.subjectLife Sciences & Biomedicine
dc.subjectOncology
dc.subjectCell Biology
dc.subjectPRL-3 monoclonal antibody
dc.subjectPRL-3 mouse/human chimeric antibody
dc.subjectantibody therapy
dc.subjectintracellular oncoprotein
dc.subjectMONOCLONAL-ANTIBODIES
dc.subjectTYROSINE-PHOSPHATASE
dc.subjectMETASTASIS
dc.subjectMARKERS
dc.typeArticle
dc.date.updated2021-10-19T07:14:57Z
dc.contributor.departmentCANCER SCIENCE INSTITUTE OF SINGAPORE
dc.contributor.departmentDEAN'S OFFICE (MEDICINE)
dc.contributor.departmentYONG LOO LIN SCHOOL OF MEDICINE
dc.description.doi10.18632/oncotarget.442
dc.description.sourcetitleONCOTARGET
dc.description.volume3
dc.description.issue2
dc.description.page158-171
dc.description.placeUnited States
dc.published.statePublished
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