Scientific Reports (May 2022)

Translational development of a tumor junction opening technology

  • Jiho Kim,
  • Chang Li,
  • Hongjie Wang,
  • Swarnendu Kaviraj,
  • Sanjay Singh,
  • Laxman Savergave,
  • Arjun Raghuwanshi,
  • Sucheol Gil,
  • Audrey Germond,
  • Audrey Baldessari,
  • Bingmae Chen,
  • Steve Roffler,
  • Pascal Fender,
  • Charles Drescher,
  • Darrick Carter,
  • André Lieber

DOI
https://doi.org/10.1038/s41598-022-11843-z
Journal volume & issue
Vol. 12, no. 1
pp. 1 – 14

Abstract

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Abstract Our goal is to overcome treatment resistance in ovarian cancer patients which occurs in most cases after an initial positive response to chemotherapy. A central resistance mechanism is the maintenance of desmoglein-2 (DSG2) positive tight junctions between malignant cells that prevents drug penetration into the tumor. We have generated JO4, a recombinant protein that binds to DSG2 resulting in the transient opening of junctions in epithelial tumors. Here we present studies toward the clinical translation of c-JO4 in combination with PEGylated liposomal doxorubicin/Doxil for ovarian cancer therapy. A manufacturing process for cGMP compliant production of JO4 was developed resulting in c-JO4. GLP toxicology studies using material from this process in DSG2 transgenic mice and cynomolgus macaques showed no treatment-related toxicities after intravenous injection at doses reaching 24 mg/kg. Multiple cycles of intravenous c-JO4 plus Doxil (four cycles, 4 weeks apart, simulating the treatment regimen in the clinical trial) elicited antibodies against c-JO4 that increased with each cycle and were accompanied by elevation of pro-inflammatory cytokines IL-6 and TNFα. Pretreatment with steroids and cyclophosphamide reduced anti-c-JO4 antibody response and blunted cytokine release. Our data indicate acceptable safety of our new treatment approach if immune reactions are monitored and counteracted with appropriate immune suppression.