AI Article Synopsis
- The RZZ complex, made up of Rough-Deal (Rod), Zw10, and Zwilch, is crucial for the spindle assembly checkpoint (SAC), which ensures proper separation of sister chromatids during mitosis.
- Researchers studied the Rod_C domain to see its role in RZZ function by introducing mutations and observed that some mutations hindered RZZ's ability to recruit to kinetochores, even though they could still form a complex with Zw10 and Zwilch.
- The findings indicate that the Rod_C domain is important for the interactions that allow RZZ to operate effectively at kinetochores.
Article Abstract
Background: The RZZ complex, composed of the proteins Rough-Deal (Rod), Zw10 and Zwilch, plays a central role in the spindle assembly checkpoint (SAC), which assures proper sister chromatid segregation during mitosis. RZZ contributes to the regulation of the spindle assembly checkpoint by helping to recruit Mad1-Mad2 and the microtubule motor dynein to unattached kinetochores. It is an important component of the outer kinetochore and specifically the fibrous corona whose expansion is believed to facilitate microtubule capture. How RZZ carries out its diverse activities is only poorly understood. The C-terminal region of the Rod subunit is relatively well-conserved across metazoan phylogeny, but no function has been attributed to it.
Results: To explore the importance of the Rod_C domain in RZZ function in Drosophila, we generated a series of point mutations in a stretch of 200 residues within this domain and we report here their phenotypes. Several of the mutations profoundly disrupt recruitment of RZZ to kinetochores, including one in a temperature-sensitive manner, while still retaining the capacity to assemble into a complex with Zw10 and Zwilch. Others affect aspects of dynein activity or recruitment at the kinetochore.
Conclusions And Significance: These results suggest that the Rod_C domain participates in the protein interactions necessary for RZZ recruitment and functionality at kinetochores.
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| http://dx.doi.org/10.1111/boc.201900105 | DOI Listing |
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