Literature DB >> 23879717

Cytosine arabinoside promotes cytotoxic effect of T cells on leukemia cells mediated by bispecific antibody.

Wei Li1, DongMei Fan, Ming Yang, Yan Yan, RuiZan Shi, JunPing Cheng, ZhenZhen Li, MengNan Zhang, JianXiang Wang, Dongsheng Xiong.   

Abstract

Chemotherapeutic drugs can enhance an immune response of the host against the tumor in addition to killing cancer cells by direct cytotoxicity. Therefore, the combination of chemotherapy and immunotherapy is a promising approach for eliminating tumors, particularly in advanced stages. A strategic medication is to use a bispecific antibody format that is capable of recruiting polyclonal T cells around antibody-target-expressing tumor cells. Recently, we have constructed a bispecific antibody, anti-CD3×anti-CD19, in a diabody configuration. In this study, we measured B7 family members B7.1 (CD80) and B7.2 (CD86) expressed on a CD19(+) human leukemia cell line, Nalm-6, stimulated by cytosine arabinoside (Ara-C). We found that a low concentration of Ara-C could upregulate CD80 expressed on CD19(+) Nalm-6 cells. The cytotoxicity of T lymphocytes against Nalm-6 cells in vitro and in vivo mediated by the anti-CD3×anti-CD19 diabody with or without a low dose of Ara-C was compared. The combination of the anti-CD3×anti-CD19 diabody and Ara-C showed the greatest effectiveness in enhancing the cytotoxicity of T cells against the tumor cells in vitro and in vivo. Activated T cells expressed higher levels of CD25 and CD69 and released more interleukin 2. Both perforin/granzyme B system and Fas/FasL pathway were involved in the diabody-induced T-cell cytotoxicity. Moreover, the activated T cells could upregulate ICAM-3 expression on Nalm-6 cells, and inhibition of LFA-1-ICAM-3 interaction impaired cytotoxicity of T cells. It was noted that Ara-C could upregulate CD80 expressed on two of five specimens of acute B lymphoblastic leukemia patient-derived cells. Cytotoxicity of T cells against these two patient-derived cells was enhanced in the presence of the anti-CD3×anti-CD19 diabody. These findings indicate that treatment strategy using both cytotoxic lymphocyte-based immunotherapy and chemotherapy may have synergistic effects.

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Year:  2013        PMID: 23879717      PMCID: PMC3746281          DOI: 10.1089/hum.2013.051

Source DB:  PubMed          Journal:  Hum Gene Ther        ISSN: 1043-0342            Impact factor:   5.695


  38 in total

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9.  Improvement of tumor targeting and antitumor activity by a disulphide bond stabilized diabody expressed in Escherichia coli.

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10.  BCL6 controls the expression of the B7-1/CD80 costimulatory receptor in germinal center B cells.

Authors:  Huifeng Niu; Giorgio Cattoretti; Riccardo Dalla-Favera
Journal:  J Exp Med       Date:  2003-07-14       Impact factor: 14.307

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  4 in total

1.  Immunological Mechanisms of Low and Ultra-Low Dose Cancer Chemotherapy.

Authors:  Joshua P Landreneau; Michael R Shurin; Marianna V Agassandian; Anton A Keskinov; Yang Ma; Galina V Shurin
Journal:  Cancer Microenviron       Date:  2013-11-29

2.  4-1BB costimulation promotes CAR T cell survival through noncanonical NF-κB signaling.

Authors:  Benjamin I Philipson; Roddy S O'Connor; Michael J May; Carl H June; Steven M Albelda; Michael C Milone
Journal:  Sci Signal       Date:  2020-03-31       Impact factor: 8.192

3.  T-cell ligands modulate the cytolytic activity of the CD33/CD3 BiTE antibody construct, AMG 330.

Authors:  G S Laszlo; C J Gudgeon; K H Harrington; R B Walter
Journal:  Blood Cancer J       Date:  2015-08-21       Impact factor: 11.037

4.  Redirection of CD4+ and CD8+ T lymphocytes via an anti-CD3 × anti-CD19 bi-specific antibody combined with cytosine arabinoside and the efficient lysis of patient-derived B-ALL cells.

Authors:  Dongmei Fan; Wei Li; Yuqi Yang; Xiaolong Zhang; Qing Zhang; Yan Yan; Ming Yang; Jianxiang Wang; Dongsheng Xiong
Journal:  J Hematol Oncol       Date:  2015-10-06       Impact factor: 17.388

  4 in total

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