BFAR coordinates TGFβ signaling to modulate Th9-mediated cancer immunotherapy

Pei, S; Huang, M; Huang, J; Zhu, X; Wang, H; Romano, S; Deng, X; Wang, Y; Luo, Y; Hao, S; J, Xu; T, Yu; Zhu, Q; Yuan, J; Shen, K; Liu, Z; G, Hu; Peng, C; Luo, Q; Wen, Z; Dai, D; Xiao, Y.

doi:10.1084/jem.20202144

TGFβ is essential for the generation of anti-tumor Th9 cells; on the other hand, it causes resistance against anti-tumor immunity. Despite recent progress, the underlying mechanism reconciling the double-edged effect of TGFβ signaling in Th9- mediated cancer immunotherapy remains elusive. Here, we find that TGFβ-induced down-regulation of bifunctional apoptosis regulator (BFAR) represents the key mechanism preventing the sustained activation of TGFβ signaling and thus impairing Th9 inducibility. Mechanistically, BFAR mediates K63-linked ubiquitination of TGFβR1 at K268, which is critical to activate TGFβ signaling. Thus, BFAR deficiency or K268R knock-in mutation suppresses TGFβR1 ubiquitination and Th9 differentiation, thereby inhibiting Th9-mediated cancer immunotherapy. More interestingly, BFAR-overexpressed Th9 cells exhibit promising therapeutic efficacy to curtail tumor growth and metastasis and promote the sensitivity of anti–PD-1–mediated checkpoint immunotherapy. Thus, our findings establish BFAR as a key TGFβ-regulated gene to fine-tune TGFβ signaling that causes Th9 induction insensitivity, and they highlight the translational potential of BFAR in promoting Th9-mediated cancer immunotherapy.

BFAR coordinates TGFβ signaling to modulate Th9-mediated cancer immunotherapy / Pei, S; Huang, M; Huang, J; Zhu, X; Wang, H; Romano, S; Deng, X; Wang, Y; Luo, Y; Hao, S; Xu, J; Yu, T; Zhu, Q; Yuan, J; Shen, K; Liu, Z; Hu, G; Peng, C; Luo, Q; Wen, Z; Dai, D; Xiao, Y.. - In: JOURNAL OF EXPERIMENTAL MEDICINE. - ISSN 0022-1007. - 218:7 e20202144(2021), pp. 1-20. [10.1084/jem.20202144]