Cancers (Aug 2020)

Therapeutic Zfra4-10 or WWOX7-21 Peptide Induces Complex Formation of WWOX with Selective Protein Targets in Organs that Leads to Cancer Suppression and Spleen Cytotoxic Memory Z Cell Activation In Vivo

  • Wan-Pei Su,
  • Wan-Jen Wang,
  • Jean-Yun Chang,
  • Pei-Chuan Ho,
  • Tsung-Yun Liu,
  • Kuang-Yu Wen,
  • Hsiang-Ling Kuo,
  • Yu-Jie Chen,
  • Shenq-Shyang Huang,
  • Dudekula Subhan,
  • Yu-An Chen,
  • Chen-Yu Lu,
  • Chia-Yun Wu,
  • Sing-Ru Lin,
  • Ming-Hui Lee,
  • Ming-Fu Chiang,
  • Chun-I Sze,
  • Nan-Shan Chang

DOI
https://doi.org/10.3390/cancers12082189
Journal volume & issue
Vol. 12, no. 8
p. 2189

Abstract

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Synthetic Zfra4-10 and WWOX7-21 peptides strongly suppress cancer growth in vivo. Hypothetically, Zfra4-10 binds to the membrane Hyal-2 of spleen Z cells and activates the Hyal-2/WWOX/SMAD4 signaling for cytotoxic Z cell activation to kill cancer cells. Stimulation of membrane WWOX in the signaling complex by a WWOX epitope peptide, WWOX7-21, is likely to activate the signaling. Here, mice receiving Zfra4-10 or WWOX7-21 peptide alone exhibited an increased binding of endogenous tumor suppressor WWOX with ERK, C1qBP, NF-κB, Iba1, p21, CD133, JNK1, COX2, Oct4, and GFAP in the spleen, brain, and/or lung which led to cancer suppression. However, when in combination, Zfra4-10 and WWOX7-21 reduced the binding of WWOX with target proteins and allowed tumor growth in vivo. In addition to Zfra4-10 and WWOX7-21 peptides, stimulating the membrane Hyal-2/WWOX complex with Hyal-2 antibody and sonicated hyaluronan (HAson) induced Z cell activation for killing cancer cells in vivo and in vitro. Mechanistically, Zfra4-10 binds to membrane Hyal-2, induces dephosphorylation of WWOX at pY33 and pY61, and drives Z cell activation for the anticancer response. Thus, Zfra4-10 and WWOX7-21 peptides, HAson, and the Hyal-2 antibody are of therapeutic potential for cancer suppression.

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