Frontiers in Immunology (May 2018)

NKp44-Derived Peptide Binds Proliferating Cell Nuclear Antigen and Mediates Tumor Cell Death

  • Avishai Shemesh,
  • Avishai Shemesh,
  • Kiran Kundu,
  • Kiran Kundu,
  • Refael Peleg,
  • Rami Yossef,
  • Irena Kaplanov,
  • Susmita Ghosh,
  • Yana Khrapunsky,
  • Orly Gershoni-Yahalom,
  • Orly Gershoni-Yahalom,
  • Tatiana Rabinski,
  • Adelheid Cerwenka,
  • Roee Atlas,
  • Angel Porgador,
  • Angel Porgador

DOI
https://doi.org/10.3389/fimmu.2018.01114
Journal volume & issue
Vol. 9

Abstract

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Proliferating cell nuclear antigen (PCNA) is considered as a hub protein and is a key regulator of DNA replication, repair, cell cycle control, and apoptosis. PCNA is overexpressed in many cancer types, and PCNA overexpression is correlated with cancer virulence. Membrane-associated PCNA is a ligand for the NKp44 (NCR2) innate immune receptor. The purpose of this study was to characterize the PCNA-binding site within NKp44. We have identified NKp44-derived linear peptide (pep8), which can specifically interact with PCNA and partly block the NKp44–PCNA interaction. We then tested whether NKp44-derived pep8 (NKp44-pep8) fused to cell-penetrating peptides (CPPs) can be employed for targeting the intracellular PCNA for the purpose of anticancer therapy. Treatment of tumor cells with NKp44-pep8, fused to R11-NLS cell-penetrating peptide (R11-NLS-pep8), reduced cell viability and promoted cell death, in various murine and human cancer cell lines. Administration of R11-NLS-pep8 to tumor-bearing mice suppressed tumor growth in the 4T1 breast cancer and the B16 melanoma in vivo models. We therefore identified the NKp44 binding site to PCNA and further developed an NKp44-peptide-based agent that can inhibit tumor growth through interfering with the function of intracellular PCNA in the tumor cell.

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