Selective perturbation of protein interactions with chemical compounds enables dissection and control of developmental processes. Differentiation of stomata, cellular valves vital for plant growth and survival, is specified by the basic-helix-loop-helix (bHLH) heterodimers. Harnessing a new amination reaction, we here report a synthesis, derivatization, target identification, and mode of action of an atypical doubly-sulfonylated imidazolone, Stomidazolone, which triggers stomatal stem cell arrest. Our forward chemical genetics followed by biophysical analyses elucidates that Stomidazolone directly binds to the C-terminal ACT-Like (ACTL) domain of MUTE, a master regulator of stomatal differentiation, and perturbs its heterodimerization with a partner bHLH, SCREAM in vitro and in plant cells. On the other hand, Stomidazolone analogs that are biologically inactive do not bind to MUTE or disrupt the SCREAM-MUTE heterodimers. Guided by structural docking modeling, we rationally design MUTE with reduced Stomidazolone binding. These engineered MUTE proteins are fully functional and confer Stomidazolone resistance in vivo. Our study identifies doubly-sulfonylated imidazolone as a direct inhibitor of the stomatal master regulator, further expanding the chemical space for perturbing bHLH-ACTL proteins to manipulate plant development.
Chemical inhibition of stomatal differentiation by perturbation of the master-regulatory bHLH heterodimer via an ACT-Like domain.
通过 ACT 样结构域扰乱主调控 bHLH 异二聚体,从而化学抑制气孔分化
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作者:Nakagawa Ayami, Sepuru Krishna Mohan, Yip Shu Jan, Seo Hyemin, Coffin Calvin M, Hashimoto Kota, Li Zixuan, Segawa Yasutomo, Iwasaki Rie, Kato Hiroe, Kurihara Daisuke, Aihara Yusuke, Kim Stephanie, Kinoshita Toshinori, Itami Kenichiro, Han Soon-Ki, Murakami Kei, Torii Keiko U
| 期刊: | Nature Communications | 影响因子: | 15.700 |
| 时间: | 2024 | 起止号: | 2024 Oct 23; 15(1):8996 |
| doi: | 10.1038/s41467-024-53214-4 | 研究方向: | 其它 |
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