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Cell-autonomous innate immunity by proteasome-derived defence peptides

Nature. 2025-03; 
Karin Goldberg, Arseniy Lobov, Paola Antonello, Merav D Shmueli, Idan Yakir, Tal Weizman, Adi Ulman, Daoud Sheban, Einav Laser, Matthias P Kramer, Ronen Shteinvil, Guoyun Chen, Angham Ibraheem, Vera Sysoeva, Vered Fishbain-Yoskovitz, Gayatree Mohapatra, Anat Abramov, Sandy Shimshi, Kseniia Ogneva, Madhurima Nandy, Sivan Amidror, Hadar Bootz-Maoz, Shanny H Kuo, Nili Dezorella, Assaf Kacen, Aaron Javitt, Gee W Lau, Nissan Yissachar, Zvi Hayouka, Yifat Merbl Weizmann Institute of Science
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Peptide Synthesis To assess the antibacterial activity of selected MAPP-derived peptides, which were predicted to have antibacterial activity, we used chemically synthesized peptides with the same amino acid sequences (GenScript). The plasmids were cut by restriction enzymes ClaI and AgeI followed by ligation with a T4 ligation enzyme (NEB). PSMG2 cloning into pLEX_305-N-dTAG was ordered from GenScript. Get A Quote

摘要

For decades, antigen presentation on major histocompatibility complex class I for T cell-mediated immunity has been considered the primary function of proteasome-derived peptides1,2. However, whether the products of proteasomal degradation play additional parts in mounting immune responses remains unknown. Antimicrobial peptides serve as a first line of defence against invading pathogens before the adaptive immune system responds. Although the protective function of antimicrobial peptides across numerous tissues is well established, the cellular mechanisms underlying their generation are not fully understood. Here we uncover a role for proteasomes in the constitutive and bacterial-induced generation of defence ... More

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