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Systematic identification of minor histocompatibility antigens predicts outcomes of allogeneic hematopoietic cell transplantation

Nat Biotechnol. 2024-08; 
Nicoletta Cieri 1 2 3, Nidhi Hookeri 1 2 4, Kari Stromhaug 1 2, Liang Li 2, Julia Keating 4, Paula Díaz-Fernández 5, Valle Gómez-García de Soria 6, Jonathan Stevens 7, Raphael Kfuri-Rubens 1 2, Yiren Shao 1 2 4, Kameron A Kooshesh 3, Kaila Powell 1, Helen Ji 1, Gabrielle M Hernandez 2, Jennifer Abelin 2, Susan Klaeger 2 8, Cleo Forman 1 4, Karl R Clauser 2, Siranush Sarkizova 2, David A Braun 1 2 3 9 10, Livius Penter 1 2 3 11, Haesook T Kim 4, William J Lane 3 7, Giacomo Oliveira 1 2 3, Leslie S Kean 3 12, Shuqiang Li 1 13, Kenneth J Livak 1 13, Steven A Carr 2, Derin B Keskin 1 2 3 13 14 15, Cecilia Muñoz-Calleja 5 16, Vincent T Ho 1 3 9, Jerome Ritz 1 3 9, Robert J Soiffer 1 3 9, Donna Neuberg 4, Chip Stewart 2, Gad Getz 2 3 17 18, Catherine J Wu 19 20 21 22
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Peptides and Peptide Library . All synthetic 8–11 mers peptides used throughout the study were purchased as microscale libraries with purity >70% (median purity: 93.8%, range: 70.1–99.8%) from GenScript and dissolved in ultrapure DMSO (Sigma-Aldrich) to a stock concentration of 10 mM. Get A Quote

摘要

T cell alloreactivity against minor histocompatibility antigens (mHAgs)-polymorphic peptides resulting from donor-recipient (D-R) disparity at sites of genetic polymorphisms-is at the core of the therapeutic effect of allogeneic hematopoietic cell transplantation (allo-HCT). Despite the crucial role of mHAgs in graft-versus-leukemia (GvL) and graft-versus-host disease (GvHD) reactions, it remains challenging to consistently link patient-specific mHAg repertoires to clinical outcomes. Here we devise an analytic framework to systematically identify mHAgs, including their detection on HLA class I ligandomes and functional verification of their immunogenicity. The method relies on the integration of polymorphism de... More

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