Construction and evaluation of a novel humanized HER2-specific chimeric receptor.

[severe combined immunodeficiency]

The human epidermal growth factor receptor 2 (HER 2 ) represents one of the most studied tumor -associated antigens (TAAs ) for cancer immunotherapy . The monoclonal antibody (mAb ) trastuzumab has improved the outcomes of patients with HER 2 + breast cancer . However , a large number of HER 2 + tumors are not responsive to , or become resistant to , trastuzumab-based therapy , and thus more effective therapies targeting HER 2 are needed .H ER 2 -specific T cells were generated by the transfer of genes that encode chimeric antigen receptor (CAR ). Using a multistep overlap extension PCR method , we constructed a novel , humanized HER 2 CAR-containing , chA 21 single -chain variable fragment (scFv ) region of antigen-specific mAb and T -cell intracellular signaling chains made up of CD 28 and CD 3 ζ . An interferon γ and interleukin 2 enzyme-linked immunosorbent assay and a chromium-51 release assay were used to evaluate the antitumor immune response of CAR T cells in coculture with tumor cells . Furthermore , SKBR 3 tumor -bearing nonobese diabetic /severe combined immunodeficiency (NOD /SCID ) mice were treated with HER 2 CAR T cells to evaluate antitumor activity . Human CD 3 + T cell accumulation in tumor xenograft was detected by immunohistochemistry .chA 21 -28 z CAR was successfully constructed , and both CD 4 + and CD 8 + T cells were transduced . The expanded HER 2 CAR T cells expressed a central memory phenotype and specifically reacted against HER 2 + tumor cell lines . Furthermore , the SKBR 3 tumor xenograft model revealed that HER 2 CAR T cells significantly inhibited tumor growth in vivo . Immunohistochemical analysis showed robust accumulation of human CD 3 + T cells in regressing SKBR 3 lesions .The results of this study show that novel chA 21 scFv-based , HER 2 -specific CAR T cells not only recognized and killed HER 2 + breast and ovarian cancer cells ex vivo but also induced regression of experimental breast cancer in vivo . Our data support further exploration of the HER 2 CAR T -cell therapy for HER 2 -expressing cancers .