Frontiers in Immunology (Feb 2022)

A Paradoxical Effect of Interleukin-32 Isoforms on Cancer

  • Saerok Shim,
  • Siyoung Lee,
  • Siyoung Lee,
  • Yasmin Hisham,
  • Sinae Kim,
  • Sinae Kim,
  • Tam T. Nguyen,
  • Tam T. Nguyen,
  • Afeisha S. Taitt,
  • Jihyeong Hwang,
  • Hyunjhung Jhun,
  • Ho-Young Park,
  • Youngmin Lee,
  • Su Cheong Yeom,
  • Sang-Yeob Kim,
  • Yong-Gil Kim,
  • Soohyun Kim,
  • Soohyun Kim

DOI
https://doi.org/10.3389/fimmu.2022.837590
Journal volume & issue
Vol. 13

Abstract

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IL-32 plays a contradictory role such as tumor proliferation or suppressor in cancer development depending on the cancer type. In most cancers, it was found that the high expression of IL-32 was associated with more proliferative and progression of cancer. However, studying the isoforms of IL-32 cytokine has placed its paradoxical role into a wide range of functions based on its dominant isoform and surrounding environment. IL-32β, for example, was found mostly in different types of cancer and associated with cancer expansion. This observation is legitimate since cancer exhibits some hypoxic environment and IL-32β was known to be induced under hypoxic conditions. However, IL-32θ interacts directly with protein kinase C-δ reducing NF-κB and STAT3 levels to inhibit epithelial-mesenchymal transition (EMT). This effect could explain the different functions of IL-32 isoforms in cancer. However, pro- or antitumor activity which is dependant on obesity, gender, and age as it relates to IL-32 has yet to be studied. Obesity-related IL-32 regulation indicated the role of IL-32 in cancer metabolism and inflammation. IL-32-specific direction in cancer therapy is difficult to conclude. In this review, we address that the paradoxical effect of IL-32 on cancer is attributed to the dominant isoform, cancer type, tumor microenvironment, and genetic background. IL-32 seems to have a contradictory role in cancer. However, investigating multiple IL-32 isoforms could explain this doubt and bring us closer to using them in therapy.

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