Literature DB >> 30728302

Breaking tolerance with engineered class I antigen-presenting molecules.

Christopher A Parks1,2, Kalli R Henning1, Kevin D Pavelko1, Michael J Hansen1, Virginia P Van Keulen1, Brendan K Reed1,2, Jennifer D Stone3, Adam G Schrum4,5,6, Diana Gil4,5,6, David M Kranz7, Andrew J Bordner8, Michael A Barry9, Larry R Pease10.   

Abstract

Successful efforts to activate T cells capable of recognizing weak cancer-associated self-antigens have employed altered peptide antigens to activate T cell responses capable of cross-reacting on native tumor-associated self. A limitation of this approach is the requirement for detailed knowledge about the altered self-peptide ligands used in these vaccines. In the current study we considered allorecognition as an approach for activating CTL capable of recognizing weak or self-antigens in the context of self-MHC. Nonself antigen-presenting molecules typically contain polymorphisms that influence interactions with the bound peptide and TCR interface. Recognition of these nonself structures results in peptide-dependent alloimmunity. Alloreactive T cells target their inducing alloantigens as well as third-party alloantigens but generally fail to target self-antigens. Certain residues located on the alpha-1/2 domains of class I antigen-presenting molecules primarily interface with TCR. These residues are more conserved within and across species than are residues that determine peptide antigen binding properties. Class I variants designed with amino acid substitutions at key positions within the conserved helical structures are shown to provide strong activating signals to alloreactive CD8 T cells while avoiding changes in naturally bound peptide ligands. Importantly, CTL activated in this manner can break self-tolerance by reacting to self-peptides presented by native MHC. The ability to activate self-tolerant T cells capable of cross-reacting on self-peptide-MHC in vivo represents an approach for inducing autoimmunity, with possible application in cancer vaccines.

Entities:  

Keywords:  MHC; T cells; adenovirus; cancer immunotherapy; tolerance

Mesh:

Substances:

Year:  2019        PMID: 30728302      PMCID: PMC6386718          DOI: 10.1073/pnas.1807465116

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  89 in total

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Review 2.  Natural selection of tumor variants in the generation of "tumor escape" phenotypes.

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Journal:  Nat Immunol       Date:  2002-11       Impact factor: 25.606

3.  Structure of the complex between human T-cell receptor, viral peptide and HLA-A2.

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Journal:  Immunogenetics       Date:  1981       Impact factor: 2.846

5.  The frequency of neoantigens per somatic mutation rather than overall mutational load or number of predicted neoantigens per se is a prognostic factor in ovarian clear cell carcinoma.

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Journal:  Virology       Date:  2011-01-20       Impact factor: 3.616

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Authors:  M D Tallquist; T J Yun; L R Pease
Journal:  J Exp Med       Date:  1996-09-01       Impact factor: 14.307

Review 8.  Specificity in cancer immunotherapy.

Authors:  Andrea Schietinger; Mary Philip; Hans Schreiber
Journal:  Semin Immunol       Date:  2008-08-05       Impact factor: 11.130

9.  An immunogenic personal neoantigen vaccine for patients with melanoma.

Authors:  Patrick A Ott; Zhuting Hu; Derin B Keskin; Sachet A Shukla; Jing Sun; David J Bozym; Wandi Zhang; Adrienne Luoma; Anita Giobbie-Hurder; Lauren Peter; Christina Chen; Oriol Olive; Todd A Carter; Shuqiang Li; David J Lieb; Thomas Eisenhaure; Evisa Gjini; Jonathan Stevens; William J Lane; Indu Javeri; Kaliappanadar Nellaiappan; Andres M Salazar; Heather Daley; Michael Seaman; Elizabeth I Buchbinder; Charles H Yoon; Maegan Harden; Niall Lennon; Stacey Gabriel; Scott J Rodig; Dan H Barouch; Jon C Aster; Gad Getz; Kai Wucherpfennig; Donna Neuberg; Jerome Ritz; Eric S Lander; Edward F Fritsch; Nir Hacohen; Catherine J Wu
Journal:  Nature       Date:  2017-07-05       Impact factor: 49.962

10.  Induced sensitization of tumor stroma leads to eradication of established cancer by T cells.

Authors:  Bin Zhang; Natalie A Bowerman; Joseph K Salama; Hank Schmidt; Michael T Spiotto; Andrea Schietinger; Ping Yu; Yang-Xin Fu; Ralph R Weichselbaum; Donald A Rowley; David M Kranz; Hans Schreiber
Journal:  J Exp Med       Date:  2007-01-08       Impact factor: 14.307

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Authors:  Laura R E Becher; Wendy K Nevala; Shari Lee Sutor; Megan Abergel; Michele M Hoffmann; Christopher A Parks; Larry R Pease; Adam G Schrum; Svetomir N Markovic; Diana Gil
Journal:  Blood Adv       Date:  2020-11-10

2.  Phase I Clinical Trial of an Autologous Dendritic Cell Vaccine Against HER2 Shows Safety and Preliminary Clinical Efficacy.

Authors:  Hoyoung M Maeng; Brittni N Moore; Hadi Bagheri; Seth M Steinberg; Jon Inglefield; Kim Dunham; Wei-Zen Wei; John C Morris; Masaki Terabe; Lee C England; Brenda Roberson; Douglas Rosing; Vandana Sachdev; Svetlana D Pack; Markku M Miettinen; Frederic G Barr; Louis M Weiner; Sandhya Panch; David F Stroncek; Lauren V Wood; Jay A Berzofsky
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