A novel targeting therapy of malignant mesothelioma using anti-podoplanin antibody.

نویسندگان

  • Shinji Abe
  • Yuki Morita
  • Mika Kato Kaneko
  • Masaki Hanibuchi
  • Yuta Tsujimoto
  • Hisatsugu Goto
  • Soji Kakiuchi
  • Yoshinori Aono
  • Jun Huang
  • Seidai Sato
  • Masatoshi Kishuku
  • Yuki Taniguchi
  • Mami Azuma
  • Kazuyoshi Kawazoe
  • Yoshitaka Sekido
  • Seiji Yano
  • Shin-ichi Akiyama
  • Saburo Sone
  • Kazuo Minakuchi
  • Yukinari Kato
  • Yasuhiko Nishioka
چکیده

Podoplanin (Aggrus), which is a type I transmembrane sialomucin-like glycoprotein, is highly expressed in malignant pleural mesothelioma (MPM). We previously reported the generation of a rat anti-human podoplanin Ab, NZ-1, which inhibited podoplanin-induced platelet aggregation and hematogenous metastasis. In this study, we examined the antitumor effector functions of NZ-1 and NZ-8, a novel rat-human chimeric Ab generated from NZ-1 including Ab-dependent cellular cytotoxicity (ADCC) and complement-dependent cytotoxicity against MPM in vitro and in vivo. Immunostaining with NZ-1 showed the expression of podoplanin in 73% (11 out of 15) of MPM cell lines and 92% (33 out of 36) of malignant mesothelioma tissues. NZ-1 could induce potent ADCC against podoplanin-positive MPM cells mediated by rat NK (CD161a(+)) cells, but not murine splenocytes or human mononuclear cells. Treatment with NZ-1 significantly reduced the growth of s.c. established tumors of MPM cells (ACC-MESO-4 or podoplanin-transfected MSTO-211H) in SCID mice, only when NZ-1 was administered with rat NK cells. In in vivo imaging, NZ-1 efficiently accumulated to xenograft of MPM, and its accumulation continued for 3 wk after systemic administration. Furthermore, NZ-8 preferentially recognized podoplanin expressing in MPM, but not in normal tissues. NZ-8 could induce higher ADCC mediated by human NK cells and complement-dependent cytotoxicity as compared with NZ-1. Treatment with NZ-8 and human NK cells significantly inhibited the growth of MPM cells in vivo. These results strongly suggest that targeting therapy to podoplanin with therapeutic Abs (i.e., NZ-8) derived from NZ-1 might be useful as a novel immunotherapy against MPM.

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عنوان ژورنال:
  • Journal of immunology

دوره 190 12  شماره 

صفحات  -

تاریخ انتشار 2013