Cell Death and Disease (May 2021)

MYCN mediates TFRC-dependent ferroptosis and reveals vulnerabilities in neuroblastoma

  • Yuxiong Lu,
  • Qing Yang,
  • Yubin Su,
  • Yin Ji,
  • Guobang Li,
  • Xianzhi Yang,
  • Liyan Xu,
  • Zhaoliang Lu,
  • Jiajun Dong,
  • Yi Wu,
  • Jin-Xin Bei,
  • Chaoyun Pan,
  • Xiaoqiong Gu,
  • Bo Li

DOI
https://doi.org/10.1038/s41419-021-03790-w
Journal volume & issue
Vol. 12, no. 6
pp. 1 – 14

Abstract

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Abstract MYCN amplification is tightly associated with the poor prognosis of pediatric neuroblastoma (NB). The regulation of NB cell death by MYCN represents an important aspect, as it directly contributes to tumor progression and therapeutic resistance. However, the relationship between MYCN and cell death remains elusive. Ferroptosis is a newly identified cell death mode featured by lipid peroxide accumulation that can be attenuated by GPX4, yet whether and how MYCN regulates ferroptosis are not fully understood. Here, we report that MYCN-amplified NB cells are sensitive to GPX4-targeting ferroptosis inducers. Mechanically, MYCN expression reprograms the cellular iron metabolism by upregulating the expression of TFRC, which encodes transferrin receptor 1 as a key iron transporter on the cell membrane. Further, the increased iron uptake promotes the accumulation of labile iron pool, leading to enhanced lipid peroxide production. Consistently, TFRC overexpression in NB cells also induces selective sensitivity to GPX4 inhibition and ferroptosis. Moreover, we found that MYCN fails to alter the general lipid metabolism and the amount of cystine imported by System Xc(−) for glutathione synthesis, both of which contribute to ferroptosis in alternative contexts. In conclusion, NB cells harboring MYCN amplification are prone to undergo ferroptosis conferred by TFRC upregulation, suggesting that GPX4-targeting ferroptosis inducers or TFRC agonists can be potential strategies in treating MYCN-amplified NB.