Frontiers in Microbiology (Apr 2022)

The Plasma Level of Interleukin-1β Can Be a Biomarker of Angiopathy in Systemic Chronic Active Epstein–Barr Virus Infection

  • Ayaka Ohashi,
  • Ayaka Ohashi,
  • Ayaka Ohashi,
  • Yu Uemura,
  • Mayumi Yoshimori,
  • Naomi Wada,
  • Ken-Ichi Imadome,
  • Kazuo Yudo,
  • Takatoshi Koyama,
  • Takatoshi Koyama,
  • Norio Shimizu,
  • Miwako Nishio,
  • Ayako Arai,
  • Ayako Arai

DOI
https://doi.org/10.3389/fmicb.2022.874998
Journal volume & issue
Vol. 13

Abstract

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Systemic chronic active Epstein–Barr virus infection (sCAEBV) is an EBV-positive T- or NK-cell neoplasm revealing persistent systemic inflammation. Twenty-five percent of sCAEBV patients accompany angiopathy. It is crucial to clarify the mechanisms of angiopathy development in sCAEBV because angiopathy is one of the main causes of death. Interleukin-1β (IL-1β) is reported to be involved in angiopathy onset. We investigated if IL-1β plays a role as the inducer of angiopathy of sCAEBV. We detected elevated IL-1β levels in four out of 17 sCAEBV patient’s plasma. Interestingly, three out of the four had clinically associated angiopathy. None of the other patients with undetectable level of IL-1β had angiopathy. In all patients with high plasma levels of IL-1β and vascular lesions, EBV-infected cells were CD4-positive T cells. In one patient with high plasma IL-1β, the level of IL-1β mRNA of the monocytes was 17.2 times higher than the level of the same patient’s EBV-infected cells in peripheral blood. In Ea.hy926 cells, which are the models of vascular endothelial cells, IL-1β inhibited the proliferation and induced the surface coagulation activity. IL-1β is a potent biomarker and a potent therapeutic target to treat sCAEBV accompanying angiopathy.

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