PRL3-zumab, a first-in-class humanized antibody for cancer therapy.

نویسندگان

  • Min Thura
  • Abdul Qader Omer Al-Aidaroos
  • Wei Peng Yong
  • Koji Kono
  • Abhishek Gupta
  • You Bin Lin
  • Kousaku Mimura
  • Jean Paul Thiery
  • Boon Cher Goh
  • Patrick Tan
  • Ross Soo
  • Cheng William Hong
  • Lingzhi Wang
  • Suling Joyce Lin
  • Elya Chen
  • Sun Young Rha
  • Hyun Cheol Chung
  • Jie Li
  • Sayantani Nandi
  • Hiu Fung Yuen
  • Shu-Dong Zhang
  • Yeoh Khay Guan
  • Jimmy So
  • Qi Zeng
چکیده

Novel, tumor-specific drugs are urgently needed for a breakthrough in cancer therapy. Herein, we generated a first-in-class humanized antibody (PRL3-zumab) against PRL-3, an intracellular tumor-associated phosphatase upregulated in multiple human cancers, for unconventional cancer immunotherapies. We focused on gastric cancer (GC), wherein elevated PRL-3 mRNA levels significantly correlated with shortened overall survival of GC patients. PRL-3 protein was overexpressed in 85% of fresh-frozen clinical gastric tumor samples examined but not in patient-matched normal gastric tissues. Using human GC cell lines, we demonstrated that PRL3-zumab specifically blocked PRL-3+, but not PRL-3-, orthotopic gastric tumors. In this setting, PRL3-zumab had better therapeutic efficacy as a monotherapy, rather than simultaneous combination with 5-fluorouracil or 5-fluorouracil alone. PRL3-zumab could also prevent PRL-3+ tumor recurrence. Mechanistically, we found that intracellular PRL-3 antigens could be externalized to become "extracellular oncotargets" that serve as bait for PRL3-zumab binding to potentially bridge and recruit immunocytes into tumor microenvironments for killing effects on cancer cells. In summary, our results document a comprehensive cancer therapeutic approach to specific antibody-targeted therapy against the PRL-3 oncotarget as a case study for developing antibodies against other intracellular targets in drug discovery.

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عنوان ژورنال:
  • JCI insight

دوره 1 9  شماره 

صفحات  -

تاریخ انتشار 2016