化学免疫疗法
癌症研究
化学
调节器
背景(考古学)
胞浆
免疫系统
作用机理
磷酸化
肿瘤微环境
干扰素
药理学
激酶
下调和上调
酪氨酸激酶
癌症
生物
免疫疗法
吞噬作用
作者
Sushil Dhakal,Muntequa I. Siraji,Sturla Magnus Grøndal,Gard N. Skarsten,Emmanuel E. Moutoussamy,Gro Gausdal,James B. Lorens,Sébastien Bougnaud
标识
DOI:10.1158/1535-7163.mct-24-0440
摘要
AXL is an important negative regulator of type I IFN responses during viral infections. In the context of tumors, AXL is associated with driving tumor progression, spread, immune evasion, and therapy resistance. AXL regulation of tumor cell-intrinsic IFN responses remains unexplored. We show that AXL suppresses tumor cell-intrinsic IFN responses by inhibiting the cytosolic DNA sensor cGAS via an AKT-dependent pathway. AXL inhibition in combination with chemoimmunotherapy demonstrated potent antitumor effects in poorly immunogenic tumors that are refractory to immunotherapy. The inhibition of AXL correlated with increased cGAMP levels, activation of IFN, and enhanced infiltration of T cells and NK cells into the tumor microenvironment. These findings reveal a novel role for AXL in suppressing IFN within tumors and support AXL targeting as a promising strategy in conjunction with chemoimmunotherapy for treating therapy-resistant tumors.
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