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Novel Proteasome Activators for the Study of Proteasome Population Dynamics and MHC-I Peptide Generation
Proteasome;MHC-I Peptide presentation;protein degradation
Nolasco-Sanchez, Jonathan
University:Havard University
Department:Biology
关键词: Proteasome;    MHC-I Peptide presentation;    protein degradation;   
Others  :  https://dash.harvard.edu/bitstream/handle/1/37365059/NOLASCO-SANCHEZ-DOCUMENT-2020.pdf?sequence=1&isAllowed=y
美国|英语
来源: Digital Access to Scholarship at Harvard
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【 摘 要 】

The 26S proteasome is the major protease found in eukaryotic cells. It is responsible for the degradation of most proteins into a mixture of heterogeneous small peptides. Proteasomes are tightly regulated, relying on ubiquitin tagging for substrate loading and ATP hydrolysis for protein degradation. A number of proteasome activators have been previously described. Here, I show that the UBL domain of Rad23a is a potent activator of the double-capped and single-capped 26S proteasome but an inhibitor of the 20S. Additionally, peptide presentation by MHC-I increases with heat shock, which also activates proteasomes.

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