Author
Listed:
- Jieqing Fan
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm)
Zhejiang Yao Yuan Biotechnology Ltd)
- Danyang Liu
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm)
Zhejiang Yao Yuan Biotechnology Ltd)
- Zhu Ming
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm))
- Chunyu Yan
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm))
- Huaixin Dang
(Zhejiang Yao Yuan Biotechnology Ltd)
- Yanfang Pan
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm))
- Xiong Wei
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm))
- Zhengle Zhao
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm))
- Wenzhi Wang
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm))
- Shuai Zhang
(Zhejiang Yao Yuan Biotechnology Ltd)
- Linlin Chen
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm))
- Shuo Cai
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm))
- Jiangbin Ke
(Vision and Brain Health))
- Yaru Luo
(Vision and Brain Health))
- Linjie Rao
(Vision and Brain Health))
- Jingjing Chen
(Zhejiang Yao Yuan Biotechnology Ltd)
- Zhenjie Chen
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm))
- Junlin Zhou
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm))
- Feixiang Chen
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm))
- Xiaodi Duan
(Zhejiang Yao Yuan Biotechnology Ltd)
- Boyue Ren
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm))
- Tong-Ruei R. Li
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm))
- Lawrence Melvin
(Drug Farm USA LLC)
- Jeysen Yogaratnam
(Drug Farm USA LLC)
- Vinit B. Mahajan
(Stanford University)
- Hongmei Song
(Chinese Academy of Medical Sciences and Peking Union Medical College)
- Henri Lichenstein
(Drug Farm USA LLC)
- Tian Xu
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm))
- Cong Xu
(Shanghai Yao Yuan Biotechnology Ltd (Drug Farm)
Zhejiang Yao Yuan Biotechnology Ltd)
Abstract
ROSAH (retinal dystrophy, optic nerve edema, splenomegaly, anhidrosis, and headache) syndrome is a rare genetic disease caused by variants in alpha-kinase 1 (ALPK1) resulting in downstream pro-inflammatory signaling mediated by the TIFA/TRAF6/NF-κB pathway. Here, we report the design of an ALPK1 inhibitor, DF-003, with pharmacokinetic properties suitable for daily oral dosing. In biochemical assays, DF-003 potently inhibits human ALPK1 (IC50 = 1.5 nM) and the ROSAH disease-causing mutant ALPK1[T237M] (IC50 = 16 nM). When tested against a panel of 394 human kinases, DF-003 exhibits ≥860-fold selectivity over the closest kinase. In cell-based assays, DF-003 suppresses inflammatory cytokine signaling mediated both by wild-type ALPK1 and the disease-causing ALPK1[T237M] mutant. Using mice heterozygous for wild-type human ALPK1 and ALPK1T237M established to model ROSAH syndrome that exhibit retinal microglial infiltration, astrocyte activation, and inflammatory cytokine upregulation in the retina, optic nerve, and cortex, we show that orally administered DF-003 is sufficient to inhibit these inflammatory phenotypes.
Suggested Citation
Jieqing Fan & Danyang Liu & Zhu Ming & Chunyu Yan & Huaixin Dang & Yanfang Pan & Xiong Wei & Zhengle Zhao & Wenzhi Wang & Shuai Zhang & Linlin Chen & Shuo Cai & Jiangbin Ke & Yaru Luo & Linjie Rao & J, 2025.
"Discovery of a selective alpha-kinase 1 inhibitor for the rare genetic disease ROSAH syndrome,"
Nature Communications, Nature, vol. 16(1), pages 1-15, December.
Handle:
RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-63731-5
DOI: 10.1038/s41467-025-63731-5
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