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Literature DB >> 23891987

Nanoscale artificial antigen presenting cells for T cell immunotherapy.

Karlo Perica¹, Andrés De León Medero², Malarvizhi Durai², Yen Ling Chiu², Joan Glick Bieler², Leah Sibener², Michaela Niemöller³, Mario Assenmacher³, Anne Richter³, Michael Edidin⁴, Mathias Oelke², Jonathan Schneck⁵.

Abstract

Artificial antigen presenting cells (aAPC), which deliver stimulatory signals to cytotoxic lymphocytes, are a powerful tool for both adoptive and active immunotherapy. Thus far, aAPC have been synthesized by coupling T cell activating proteins such as CD3 or MHC-peptide to micron-sized beads. Nanoscale platforms have different trafficking and biophysical interaction properties and may allow development of new immunotherapeutic strategies. We therefore manufactured aAPC based on two types of nanoscale particle platforms: biocompatible iron-dextran paramagnetic particles (50-100 nm in diameter) and avidin-coated quantum dot nanocrystals (~30 nm). Nanoscale aAPC induced antigen-specific T cell proliferation from mouse splenocytes and human peripheral blood T cells. When injected in vivo, both iron-dextran particles and quantum dot nanocrystals enhanced tumor rejection in a subcutaneous mouse melanoma model. This is the first description of nanoscale aAPC that induce antigen-specific T cell proliferation in vitro and lead to effective T cell stimulation and inhibition of tumor growth in vivo. FROM THE CLINICAL EDITOR: Artifical antigen presenting cells could revolutionize the field of cancer-directed immunotherapy. This team of investigators have manufactured two types of nanoscale particle platform-based aAPCs and demonstrates that both iron-dextran particles and quantum dot nanocrystals enhance tumor rejection in a melanoma model, providing the first description of nanoscale aAPCs that lead to effective T cell stimulation and inhibition of tumor growth.

Entities: Chemical

Keywords: Artificial antigen presenting cell; Immunotherapy; Nanoparticle; T cell

Mesh：

Substances：

Year: 2013 PMID： 23891987 PMCID： PMC4114774 DOI： 10.1016/j.nano.2013.06.015

Source DB: PubMed Journal: Nanomedicine ISSN： 1549-9634 Impact factor: 5.307

50 in total

1. Exploiting lymphatic transport and complement activation in nanoparticle vaccines.

Authors: Sai T Reddy; André J van der Vlies; Eleonora Simeoni; Veronique Angeli; Gwendalyn J Randolph; Conlin P O'Neil; Leslie K Lee; Melody A Swartz; Jeffrey A Hubbell
Journal: Nat Biotechnol Date: 2007-09-16 Impact factor: 54.908

2. In vitro induction of naive cytotoxic T lymphocytes with complexes of peptide and recombinant MHC class I molecules coated onto beads: role of TCR/ligand density.

Authors: I Motta; Y C Lone; P Kourilsky
Journal: Eur J Immunol Date: 1998-11 Impact factor: 5.532

3. T cell receptor binding kinetics required for T cell activation depend on the density of cognate ligand on the antigen-presenting cell.

Authors: Pablo A González; Leandro J Carreño; Daniel Coombs; Jorge E Mora; Edith Palmieri; Byron Goldstein; Stanley G Nathenson; Alexis M Kalergis
Journal: Proc Natl Acad Sci U S A Date: 2005-03-16 Impact factor: 11.205

4. Increased sensitivity of antigen-experienced T cells through the enrichment of oligomeric T cell receptor complexes.

Authors: Rashmi Kumar; María Ferez; Mahima Swamy; Ignacio Arechaga; María Teresa Rejas; Jose M Valpuesta; Wolfgang W A Schamel; Balbino Alarcon; Hisse M van Santen
Journal: Immunity Date: 2011-09-08 Impact factor: 31.745

Review 5. Engineering nano- and microparticles to tune immunity.

Authors: James J Moon; Bonnie Huang; Darrell J Irvine
Journal: Adv Mater Date: 2012-05-29 Impact factor: 30.849

6. In vivo functional efficacy of tumor-specific T cells expanded using HLA-Ig based artificial antigen presenting cells (aAPC).

Authors: Malarvizhi Durai; Christine Krueger; Zhaohui Ye; Linzhao Cheng; Andreas Mackensen; Mathias Oelke; Jonathan P Schneck
Journal: Cancer Immunol Immunother Date: 2008-06-18 Impact factor: 6.968

7. Increased intensity lymphodepletion enhances tumor treatment efficacy of adoptively transferred tumor-specific T cells.

Authors: Claudia Wrzesinski; Chrystal M Paulos; Andrew Kaiser; Pawel Muranski; Douglas C Palmer; Luca Gattinoni; Zhiya Yu; Steven A Rosenberg; Nicholas P Restifo
Journal: J Immunother Date: 2010-01 Impact factor: 4.456

Review 8. Overview of a HLA-Ig based "Lego-like system" for T cell monitoring, modulation and expansion.

Authors: Mathias Oelke; Jonathan P Schneck
Journal: Immunol Res Date: 2010-07 Impact factor: 2.829

Review 9. T cell activation.

Authors: Jennifer E Smith-Garvin; Gary A Koretzky; Martha S Jordan
Journal: Annu Rev Immunol Date: 2009 Impact factor: 28.527

10. TCR and Lat are expressed on separate protein islands on T cell membranes and concatenate during activation.

Authors: Björn F Lillemeier; Manuel A Mörtelmaier; Martin B Forstner; Johannes B Huppa; Jay T Groves; Mark M Davis
Journal: Nat Immunol Date: 2009-12-13 Impact factor: 25.606

43 in total

1. Enrichment and Expansion with Nanoscale Artificial Antigen Presenting Cells for Adoptive Immunotherapy.

Authors: Karlo Perica; Joan Glick Bieler; Christian Schütz; Juan Carlos Varela; Jacqueline Douglass; Andrew Skora; Yen Ling Chiu; Mathias Oelke; Kenneth Kinzler; Shibin Zhou; Bert Vogelstein; Jonathan P Schneck
Journal: ACS Nano Date: 2015-07-14 Impact factor: 15.881

Nanoscale artificial antigen presenting cells for T cell immunotherapy.

1. Exploiting lymphatic transport and complement activation in nanoparticle vaccines.

2. In vitro induction of naive cytotoxic T lymphocytes with complexes of peptide and recombinant MHC class I molecules coated onto beads: role of TCR/ligand density.

3. T cell receptor binding kinetics required for T cell activation depend on the density of cognate ligand on the antigen-presenting cell.

4. Increased sensitivity of antigen-experienced T cells through the enrichment of oligomeric T cell receptor complexes.

Review 5. Engineering nano- and microparticles to tune immunity.

6. In vivo functional efficacy of tumor-specific T cells expanded using HLA-Ig based artificial antigen presenting cells (aAPC).

7. Increased intensity lymphodepletion enhances tumor treatment efficacy of adoptively transferred tumor-specific T cells.

Review 8. Overview of a HLA-Ig based "Lego-like system" for T cell monitoring, modulation and expansion.

Review 9. T cell activation.

10. TCR and Lat are expressed on separate protein islands on T cell membranes and concatenate during activation.

1. Enrichment and Expansion with Nanoscale Artificial Antigen Presenting Cells for Adoptive Immunotherapy.

Review 2. Biomimetic and synthetic interfaces to tune immune responses.

3. Antigen-Presenting Cells: Potential of Proven und New Players in Immune Therapies.

4. Nanoparticle Design Strategies for Effective Cancer Immunotherapy.

Review 5. Surface engineering for lymphocyte programming.

Review 6. Biomaterials for nanoparticle vaccine delivery systems.

Review 7. Biomimetic Nanotechnology toward Personalized Vaccines.

Review 8. Modulating the immune system through nanotechnology.

Review 9. Advances in immunotherapy delivery from implantable and injectable biomaterials.

Review 10. Nanoscale artificial antigen presenting cells for cancer immunotherapy.