Literature DB >> 24329799

Rapamycin-resistant effector T-cell therapy.

Daniel H Fowler1.   

Abstract

Pharmacologic inhibition of the mechanistic target of rapamycin (mTOR) represents a stress test for tumor cells and T cells. Mechanisms exist that allow cells to survive this stress, including suboptimal target block, alternative signaling pathways, and autophagy. Rapamycin-resistant effector T (T-Rapa) cells have an altered phenotype that associates with increased function. Ex vivo rapamycin, when used in combination with polarizing cytokines and antigen-presenting-cell free costimulation, is a flexible therapeutic approach as polarization to T-helper 1 (Th1)- or Th2-type effectors is possible. Murine T-Rapa cells skewed toward a Th2-type prevented graft rejection and graft-versus-host disease (GVHD) more potently than control Th2 cells and effectively balanced GVHD and graft-versus-tumor (GVT) effects. A phase II clinical trial using low-intensity allogeneic hematopoietic cell transplantation demonstrated that interleukin-4 polarized human T-Rapa cells had a mixed Th2/Th1 phenotype; T-Rapa cell recipients had a balanced Th2/Th1 cytokine profile, conversion of mixed chimerism toward full donor chimerism, and a potentially favorable balance between GVHD and GVT effects. In addition, a phase I clinical trial evaluating autologous T-Rapa cells skewed toward a Th1- and Tc1-type is underway. Use of ex vivo rapamycin to modulate effector T-cell function represents a promising new approach to transplantation therapy. Published 2013. This article is a U.S. Government work and is in the public domain in the USA.

Entities:  

Keywords:  Th1/Th2/Th17; apoptosis/autophagy; cytokines; graft versus host disease; transplantation

Mesh:

Substances:

Year:  2014        PMID: 24329799      PMCID: PMC6948844          DOI: 10.1111/imr.12127

Source DB:  PubMed          Journal:  Immunol Rev        ISSN: 0105-2896            Impact factor:   12.988


  147 in total

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Authors:  Shoba Amarnath; Courtney W Mangus; James C M Wang; Fang Wei; Alice He; Veena Kapoor; Jason E Foley; Paul R Massey; Tania C Felizardo; James L Riley; Bruce L Levine; Carl H June; Jeffrey A Medin; Daniel H Fowler
Journal:  Sci Transl Med       Date:  2011-11-30       Impact factor: 17.956

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Authors:  Luca Gattinoni; Christopher A Klebanoff; Douglas C Palmer; Claudia Wrzesinski; Keith Kerstann; Zhiya Yu; Steven E Finkelstein; Marc R Theoret; Steven A Rosenberg; Nicholas P Restifo
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5.  Combining mTor inhibitors with rapamycin-resistant T cells: a two-pronged approach to tumor elimination.

Authors:  Leslie E Huye; Yozo Nakazawa; Mayuri P Patel; Eric Yvon; Jiali Sun; Barbara Savoldo; Matthew H Wilson; Gianpietro Dotti; Cliona M Rooney
Journal:  Mol Ther       Date:  2011-08-30       Impact factor: 11.454

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Authors:  Brian R Rosborough; Dàlia Raïch-Regué; Benjamin M Matta; Keunwook Lee; Boyi Gan; Ronald A DePinho; Holger Hackstein; Mark Boothby; Hēth R Turnquist; Angus W Thomson
Journal:  Blood       Date:  2013-02-26       Impact factor: 22.113

7.  Cutting edge: Foxp3-mediated induction of pim 2 allows human T regulatory cells to preferentially expand in rapamycin.

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9.  A unifying model for mTORC1-mediated regulation of mRNA translation.

Authors:  Carson C Thoreen; Lynne Chantranupong; Heather R Keys; Tim Wang; Nathanael S Gray; David M Sabatini
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Authors:  Linda V Sinclair; David Finlay; Carmen Feijoo; Georgina H Cornish; Alex Gray; Ann Ager; Klaus Okkenhaug; Thijs J Hagenbeek; Hergen Spits; Doreen A Cantrell
Journal:  Nat Immunol       Date:  2008-04-06       Impact factor: 25.606

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2.  Engineering T cells for cancer: our synthetic future.

Authors:  Robert H Vonderheide; Carl H June
Journal:  Immunol Rev       Date:  2014-01       Impact factor: 12.988

3.  A Comparison of Automated Perfusion- and Manual Diffusion-Based Human Regulatory T Cell Expansion and Functionality Using a Soluble Activator Complex.

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Journal:  Cell Transplant       Date:  2020 Jan-Dec       Impact factor: 4.064

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