PLoS Pathogens (Jul 2024)

c-FLIP facilitates ZIKV infection by mediating caspase-8/3-dependent apoptosis.

  • Shengze Zhang,
  • Nina Li,
  • Shu Wu,
  • Ting Xie,
  • Qiqi Chen,
  • Jiani Wu,
  • Shike Zeng,
  • Lin Zhu,
  • Shaohui Bai,
  • Haolu Zha,
  • Weijian Tian,
  • Nan Wu,
  • Xuan Zou,
  • Shisong Fang,
  • Chuming Luo,
  • Mang Shi,
  • Caijun Sun,
  • Yuelong Shu,
  • Huanle Luo

DOI
https://doi.org/10.1371/journal.ppat.1012408
Journal volume & issue
Vol. 20, no. 7
p. e1012408

Abstract

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c-FLIP functions as a dual regulator of apoptosis and inflammation, yet its implications in Zika virus (ZIKV) infection remain partially understood, especially in the context of ZIKV-induced congenital Zika syndrome (CZS) where both apoptosis and inflammation play pivotal roles. Our findings demonstrate that c-FLIP promotes ZIKV infection in placental cells and myeloid-derived macrophages, involving inflammation and caspase-8/3-mediated apoptosis. Moreover, our observations reveal that c-FLIP augments ZIKV infection in multiple tissues, including blood cell, spleen, uterus, testis, and the brain of mice. Notably, the partial deficiency of c-FLIP provides protection to embryos against ZIKV-induced CZS, accompanied by a reduction in caspase-3-mediated apoptosis. Additionally, we have found a distinctive parental effect of c-FLIP influencing ZIKV replication in fetal heads. In summary, our study reveals the critical role of c-FLIP as a positive regulator in caspase-8/3-mediated apoptosis during ZIKV infection, significantly contributing to the development of CZS.