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Literature DB >> 18289015

Overcoming immune evasion in T cell therapy of cancer: lessons from animal models.

Abstract

Cancer antigen-specific cytotoxic T lymphocytes (CTL) are the major effectors against cancer cells. However, large established tumors are usually not fully controlled by CTL for at least two reasons. First, large established tumors have immune suppressive networks that not only suppress CTL effector function but also permit tumor progression. Second, the genetic instability of cancer cells often results in the selection of antigenic variants by CTL, which allow cancer cells to escape destruction. Simply enhancing T cell capacity may not fully control large established tumors. Other measures, such as enhancing local costimulation, inhibiting angiogenesis and down-regulating functions of tumor associated myeloid cells should also be considered. In this paper we will review some of the progress from animal studies.

Entities: Disease

Mesh：

Year: 2008 PMID： 18289015 DOI： 10.2174/156652408783565531

Source DB: PubMed Journal: Curr Mol Med ISSN： 1566-5240 Impact factor: 2.222

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Cited

7 in total

1. IL-10 contributes to the suppressive function of tumour-associated myeloid cells and enhances myeloid cell accumulation in tumours.

Authors: L-X Wang; F Talebian; J-Q Liu; M Khattabi; L Yu; X-F Bai
Journal: Scand J Immunol Date: 2012-03 Impact factor: 3.487

2. IL-10 enhances CTL-mediated tumor rejection by inhibiting highly suppressive CD4⁺ T cells and promoting CTL persistence in a murine model of plasmacytoma.

Authors: Lixin Wang; Jin-Qing Liu; Fatemeh Talebian; Zhenzhen Liu; Li Yu; Xue-Feng Bai
Journal: Oncoimmunology Date: 2015-05-13 Impact factor: 8.110

3. Oncogene-targeting T cells reject large tumors while oncogene inactivation selects escape variants in mouse models of cancer.

Authors: Kathleen Anders; Christian Buschow; Andreas Herrmann; Ana Milojkovic; Christoph Loddenkemper; Thomas Kammertoens; Peter Daniel; Hua Yu; Jehad Charo; Thomas Blankenstein
Journal: Cancer Cell Date: 2011-12-13 Impact factor: 31.743

4. IL-27 enhances the survival of tumor antigen-specific CD8+ T cells and programs them into IL-10-producing, memory precursor-like effector cells.

Authors: Zhenzhen Liu; Jin-Qing Liu; Fatemeh Talebian; Lai-Chu Wu; Shulin Li; Xue-Feng Bai
Journal: Eur J Immunol Date: 2013-01-15 Impact factor: 5.532

Overcoming immune evasion in T cell therapy of cancer: lessons from animal models.

1. IL-10 contributes to the suppressive function of tumour-associated myeloid cells and enhances myeloid cell accumulation in tumours.

2. IL-10 enhances CTL-mediated tumor rejection by inhibiting highly suppressive CD4⁺ T cells and promoting CTL persistence in a murine model of plasmacytoma.

3. Oncogene-targeting T cells reject large tumors while oncogene inactivation selects escape variants in mouse models of cancer.

4. IL-27 enhances the survival of tumor antigen-specific CD8+ T cells and programs them into IL-10-producing, memory precursor-like effector cells.

5. The role of IL-27 in the induction of anti-tumor cytotoxic T lymphocyte response.

6. Immune parameters to consider when choosing T-cell receptors for therapy.

Review 7. Adoptive cell therapies for glioblastoma.

Overcoming immune evasion in T cell therapy of cancer: lessons from animal models.

1. IL-10 contributes to the suppressive function of tumour-associated myeloid cells and enhances myeloid cell accumulation in tumours.

2. IL-10 enhances CTL-mediated tumor rejection by inhibiting highly suppressive CD4+ T cells and promoting CTL persistence in a murine model of plasmacytoma.

3. Oncogene-targeting T cells reject large tumors while oncogene inactivation selects escape variants in mouse models of cancer.

4. IL-27 enhances the survival of tumor antigen-specific CD8+ T cells and programs them into IL-10-producing, memory precursor-like effector cells.

5. The role of IL-27 in the induction of anti-tumor cytotoxic T lymphocyte response.

6. Immune parameters to consider when choosing T-cell receptors for therapy.

Review 7. Adoptive cell therapies for glioblastoma.

2. IL-10 enhances CTL-mediated tumor rejection by inhibiting highly suppressive CD4⁺ T cells and promoting CTL persistence in a murine model of plasmacytoma.