| Literature DB >> 33555115 |
Hsiang-I Tsai1, Xiaobin Zeng2,3, Longshan Liu4, Shengchang Xin5, Yingyi Wu1, Zhanxue Xu1, Huanxi Zhang4, Gan Liu1, Zirong Bi4, Dandan Su1, Min Yang1, Yijing Tao1, Changxi Wang4, Jing Zhao5, John E Eriksson6,7, Wenbin Deng1, Fang Cheng1, Hongbo Chen1.
Abstract
Herein, we demonstrate that NFAT, a key regulator of the immune response, translocates from cytoplasm to nucleolus and interacts with NF45/NF90 complex to collaboratively promote rDNA transcription via triggering the directly binding of NF45/NF90 to the ARRE2-like sequences in rDNA promoter upon T-cell activation in vitro. The elevated pre-rRNA level of T cells is also observed in both mouse heart or skin transplantation models and in kidney transplanted patients. Importantly, T-cell activation can be significantly suppressed by inhibiting NF45/NF90-dependent rDNA transcription. Amazingly, CX5461, a rDNA transcription-specific inhibitor, outperformed FK506, the most commonly used immunosuppressant, both in terms of potency and off-target activity (i.e., toxicity), as demonstrated by a series of skin and heart allograft models. Collectively, this reveals NF45/NF90-mediated rDNA transcription as a novel signaling pathway essential for T-cell activation and as a new target for the development of safe and effective immunosuppressants.Entities:
Keywords: CX5461; NF45/NF90; NFAT; nucleolus; organ transplantation
Year: 2021 PMID: 33555115 PMCID: PMC7933818 DOI: 10.15252/emmm.202012834
Source DB: PubMed Journal: EMBO Mol Med ISSN: 1757-4676 Impact factor: 12.137