Genetic, colocalization, and biochemical studies suggest that the ankyrin repeat-containing proteins Inversin (INVS) and ANKS6 function with the NEK8 kinase to control tissue patterning and maintain organ physiology. It is unknown whether these three proteins assemble into a static "Inversin complex" or one that adopts multiple bioactive forms. Through the characterization of hyperactive alleles in C. elegans, we discovered that the Inversin complex is activated by dimerization. Genome engineering of an RFP tag onto the nematode homologues of INVS (MLT-4) and NEK8 (NEKL-2) induced a gain-of-function, cyst-like phenotype that was suppressed by monomerization of the fluorescent tag. Stimulated dimerization of MLT-4 or NEKL-2 using optogenetics was sufficient to recapitulate the phenotype of a constitutively active Inversin complex. Further, dimerization of NEKL-2 bypassed a lethal MLT-4 mutant, demonstrating that the dimeric form is required for function. We propose that dynamic switching between at least two functionally distinct states - an active dimer and an inactive monomer - gates the output of the Inversin complex.
Dimerization activates the Inversin complex in C. elegans.
二聚化激活秀丽隐杆线虫中的 Inversin 复合物
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作者:Beyrent Erika, Wei Derek T, Beacham Gwendolyn M, Park Sangwoo, Zheng Jian, Paszek Matthew J, Hollopeter Gunther
| 期刊: | Molecular Biology of the Cell | 影响因子: | 2.700 |
| 时间: | 2024 | 起止号: | 2024 Oct 1; 35(10):ar127 |
| doi: | 10.1091/mbc.E24-05-0218 | 研究方向: | 其它 |
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