Bone marrow stromal cells dictate lanosterol biosynthesis and ferroptosis of multiple myeloma

Author:

Jiang Hongmei,Wang Lijuan,Zhang Qiguo,Wang Sheng,Jia Linchuang,Cheng Hao,Wang Jingya,Li Xin,Xie Ying,Wang Yixuan,Hu Meilin,Guo Jing,Li Qian,Peng Ziyi,Wang Mengqi,Xie Yangyang,Li Tiantian,Wang Yafei,Geng Bill D.,Swaminathan Sundararaman,Bergsagel P. LeifORCID,Liu Zhiqiang

Abstract

AbstractFerroptosis has been demonstrated a promising way to counteract chemoresistance of multiple myeloma (MM), however, roles and mechanism of bone marrow stromal cells (BMSCs) in regulating ferroptosis of MM cells remain elusive. Here, we uncovered that MM cells were more susceptible to ferroptotic induction under the interaction of BMSCs using in vitro and in vivo models. Mechanistically, BMSCs elevated the iron level in MM cells, thereby activating the steroid biosynthesis pathway, especially the production of lanosterol, a major source of reactive oxygen species (ROS) in MM cells. We discovered that direct coupling of CD40 ligand and CD40 receptor constituted the key signaling pathway governing lanosterol biosynthesis, and disruption of CD40/CD40L interaction using an anti-CD40 neutralizing antibody or conditional depletion of Cd40l in BMSCs successfully eliminated the iron level and lanosterol production of MM cells localized in the Vk*MYC Vk12653 or NSG mouse models. Our study deciphers the mechanism of BMSCs dictating ferroptosis of MM cells and highlights the therapeutic potential of non-apoptosis strategies for managing refractory or relapsed MM patients.

Funder

Natural Science Foundation of Beijing Municipality

National Natural Science Foundation of China

Publisher

Springer Science and Business Media LLC

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