Literature DB >> 18261838

Peripheral blood progenitor cell product contains Th1-biased noninvariant CD1d-reactive natural killer T cells: implications for posttransplant survival.

Angela Shaulov1, Simon Yue, Ruojie Wang, Robin M Joyce, Steven P Balk, Haesook T Kim, David E Avigan, Lynne Uhl, Robert Sackstein, Mark A Exley.   

Abstract

OBJECTIVE: Bone marrow (BM) Th1 populations can contribute to graft-vs-leukemia responses. Granulocyte/granulocyte macrophage colony-stimulating factor (CSF)-mobilized peripheral blood progenitor cells (PBPC) have become widely accepted alternatives to BM transplantation. T cells coexpressing natural killer cell proteins (NKT) include a CD1d-reactive subset that influences immunity by rapidly producing large amounts of Th1 and/or Th2 cytokines dependent upon microenvironment and disease. There are two types of CD1d-reactive NKT. iNKT express a semi-invariant T-cell receptor-alpha. Other noninvariant CD1d-reactive NKT from BM and liver produce large amounts of interleukin-4 or interferon-gamma, respectively, and within the intestine can be biased in either direction. Recent data suggests that NKT might contribute to clinical benefits of PBPC.
MATERIALS AND METHODS: To address these issues, we phenotypically and functionally studied PBPC NKT.
RESULTS: Similarly to BM, NKT-like cells were common in allogeneic and autologous PBPC, there were relatively few classical iNKT, but high CD1d-reactivity concentrated in NKT fractions. Significantly, PBPC CD1d-reactive cells were relatively Th1-biased and their presence was associated with better prognosis. Granulocyte CSF treatment of BM to yield PBPC in vivo as well as in vitro Th2-polarizes conventional T cells and iNKT. However, granulocyte CSF treatment of BM in vitro produced Th1-biased NKT, providing a mechanism for opposite polarization of NKT from BM vs PBPC.
CONCLUSIONS: These results suggest distinct Th1 CD1d-reactive NKT cells could stimulate anti-tumor responses from those previously described, which can suppress graft-vs-host disease.

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Year:  2008        PMID: 18261838      PMCID: PMC2390922          DOI: 10.1016/j.exphem.2007.12.010

Source DB:  PubMed          Journal:  Exp Hematol        ISSN: 0301-472X            Impact factor:   3.084


  32 in total

1.  T-cell subsets and suppressor cells in human bone marrow.

Authors:  I G Schmidt-Wolf; S Dejbakhsh-Jones; N Ginzton; P Greenberg; S Strober
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Authors:  Dale I Godfrey; Mitchell Kronenberg
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3.  Stimulation of host NKT cells by synthetic glycolipid regulates acute graft-versus-host disease by inducing Th2 polarization of donor T cells.

Authors:  Daigo Hashimoto; Shoji Asakura; Sachiko Miyake; Takashi Yamamura; Luc Van Kaer; Chen Liu; Mitsune Tanimoto; Takanori Teshima
Journal:  J Immunol       Date:  2005-01-01       Impact factor: 5.422

4.  Granulocyte colony-stimulating factor-induced comobilization of CD4- CD8- T cells and hematopoietic progenitor cells (CD34+) in the blood of normal donors.

Authors:  C R Kusnierz-Glaz; B J Still; M Amano; J D Zukor; R S Negrin; K G Blume; S Strober
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5.  In vitro and in vivo analysis of bone marrow-derived CD3+, CD4-, CD8-, NK1.1+ cell lines.

Authors:  M Sykes; K A Hoyles; M L Romick; D H Sachs
Journal:  Cell Immunol       Date:  1990-09       Impact factor: 4.868

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Authors:  Mark A Exley; Margaret James Koziel
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7.  Effect of granulocyte colony-stimulating factor treatment on ex vivo blood cytokine response in human volunteers.

Authors:  T Hartung; W D Döcke; F Gantner; G Krieger; A Sauer; P Stevens; H D Volk; A Wendel
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8.  CD161 (NKR-P1A) costimulation of CD1d-dependent activation of human T cells expressing invariant V alpha 24 J alpha Q T cell receptor alpha chains.

Authors:  M Exley; S Porcelli; M Furman; J Garcia; S Balk
Journal:  J Exp Med       Date:  1998-09-07       Impact factor: 14.307

9.  Requirements for CD1d recognition by human invariant Valpha24+ CD4-CD8- T cells.

Authors:  M Exley; J Garcia; S P Balk; S Porcelli
Journal:  J Exp Med       Date:  1997-07-07       Impact factor: 14.307

10.  Bone marrow NK1.1(-) and NK1.1(+) T cells reciprocally regulate acute graft versus host disease.

Authors:  D Zeng; D Lewis; S Dejbakhsh-Jones; F Lan; M García-Ojeda; R Sibley; S Strober
Journal:  J Exp Med       Date:  1999-04-05       Impact factor: 14.307

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2.  Adoptive Transfer of Invariant NKT Cells as Immunotherapy for Advanced Melanoma: A Phase I Clinical Trial.

Authors:  Mark A Exley; Phillip Friedlander; Nadia Alatrakchi; Lianne Vriend; Simon Yue; Tetsuro Sasada; Wanyong Zeng; Yo Mizukami; Justice Clark; David Nemer; Kenneth LeClair; Christine Canning; Heather Daley; Glenn Dranoff; Anita Giobbie-Hurder; F Stephen Hodi; Jerome Ritz; Steven P Balk
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Review 3.  Developing understanding of the roles of CD1d-restricted T cell subsets in cancer: reversing tumor-induced defects.

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4.  Emergency granulopoiesis promotes neutrophil-dendritic cell encounters that prevent mouse lung allograft acceptance.

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Review 5.  Tissue-Resident Innate Immune Cell-Based Therapy: A Cornerstone of Immunotherapy Strategies for Cancer Treatment.

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8.  Differential Activation of Unconventional T Cells, Including iNKT Cells, in Alcohol-Related Liver Disease.

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9.  Circulating myeloid dendritic cells of advanced cancer patients result in reduced activation and a biased cytokine profile in invariant NKT cells.

Authors:  Hans J J van der Vliet; Ruojie Wang; Simon C Yue; Henry B Koon; Steven P Balk; Mark A Exley
Journal:  J Immunol       Date:  2008-06-01       Impact factor: 5.422

Review 10.  The regulatory role of invariant NKT cells in tumor immunity.

Authors:  Rosanna M McEwen-Smith; Mariolina Salio; Vincenzo Cerundolo
Journal:  Cancer Immunol Res       Date:  2015-05       Impact factor: 11.151

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