Your search keyword '"Zainul Abedin"' showing total 4 results

1. CCR7

Author

Gray, Kueberuwa, Hannah, Gornall, Erik Marcelo, Alcantar-Orozco, Deborah, Bouvier, Zainul Abedin, Kapacee, Robert Edward, Hawkins, and David Edward, Gilham

Subjects

Receptors, CCR7, T-Lymphocytes, Central memory, Immunotherapy, Adoptive, Adoptive cell therapy, Mice, Transgenic TCR, Phenotype, DMF5, Animals, Humans, CD62L, Immunotherapy, Differentiation status, K562 Cells, Immunologic Memory, Research Article, CCR7

Abstract

Background Adoptive T cell immunotherapy (ATCT) for cancer entails infusing patients with T cells that recognise and destroy tumour cells. Efficient engraftment of T cells and persistence in the circulation correlate with favourable clinical outcomes. T cells of early differentiation possess an increased capacity for proliferation and therefore persistence, using these cells for ATCT could therefore lead to improved clinical outcomes. Method We describe a method to enrich T cells of early differentiation status using paramagnetic beads and antibodies targeting cells expressing C-C motif chemokine receptor 7 (CCR7). Results Selection of cells expressing CCR7 enriches T cells of bearing markers of early differentiation status. This was validated through analysis of an array of surface markers and an observed reduction in effector cell functions ex vivo. CCR7 selection resulted in dramatic 83.6 and 137 fold increases in circulating levels of CD4 and CD8 T cells respectively compared to non-sorted T cells 3 weeks after adoptive transfer to NSG mice. We observed no significant difference in the engraftment levels of CCR7 or CD62L selected cells in the NSG mouse model. Comparison of cells ex vivo, however, suggests CCR7 selection is superior to CD62L selection in enriching T cells of early differentiation status. Conclusions CCR7 selection offers a means to enrich T cells of early differentiation status for ACTC. Together our data suggests that these T cells are likely to display enhanced engraftment and persistence in patients in vivo and could therefore improve therapeutic efficacy of ACTC. Electronic supplementary material The online version of this article (doi:10.1186/s40425-017-0216-7) contains supplementary material, which is available to authorized users.

Published

2016

2. CCR7+ selected gene-modified T cells maintain a central memory phenotype and display enhanced persistence in peripheral blood in vivo

Author

Kueberuwa, Gray, primary, Gornall, Hannah, additional, Alcantar-Orozco, Erik Marcelo, additional, Bouvier, Deborah, additional, Kapacee, Zainul Abedin, additional, Hawkins, Robert Edward, additional, and Gilham, David Edward, additional

Published

2017

3. CCR7+ selected gene-modified T cells maintain a central memory phenotype and display enhanced persistence in peripheral blood in vivo.

Author

Kueberuwa, Gray, Gornall, Hannah, Alcantar-Orozco, Erik Marcelo, Bouvier, Deborah, Kapacee, Zainul Abedin, Hawkins, Robert Edward, and Gilham, David Edward

Subjects

GENE expression, T cell differentiation, CELLULAR therapy

Abstract

Background: Adoptive T cell immunotherapy (ATCT) for cancer entails infusing patients with T cells that recognise and destroy tumour cells. Efficient engraftment of T cells and persistence in the circulation correlate with favourable clinical outcomes. T cells of early differentiation possess an increased capacity for proliferation and therefore persistence, using these cells for ATCT could therefore lead to improved clinical outcomes. Method: We describe a method to enrich T cells of early differentiation status using paramagnetic beads and antibodies targeting cells expressing C-C motif chemokine receptor 7 (CCR7). Results: Selection of cells expressing CCR7 enriches T cells of bearing markers of early differentiation status. This was validated through analysis of an array of surface markers and an observed reduction in effector cell functions ex vivo. CCR7 selection resulted in dramatic 83.6 and 137 fold increases in circulating levels of CD4 and CD8 T cells respectively compared to non-sorted T cells 3 weeks after adoptive transfer to NSG mice. We observed no significant difference in the engraftment levels of CCR7 or CD62L selected cells in the NSG mouse model. Comparison of cells ex vivo, however, suggests CCR7 selection is superior to CD62L selection in enriching T cells of early differentiation status. Conclusions: CCR7 selection offers a means to enrich T cells of early differentiation status for ACTC. Together our data suggests that these T cells are likely to display enhanced engraftment and persistence in patients in vivo and could therefore improve therapeutic efficacy of ACTC. [ABSTRACT FROM AUTHOR]

Published

2017

4. CCR7 + selected gene-modified T cells maintain a central memory phenotype and display enhanced persistence in peripheral blood in vivo.

Author

Kueberuwa G, Gornall H, Alcantar-Orozco EM, Bouvier D, Kapacee ZA, Hawkins RE, and Gilham DE

Subjects

Animals, Humans, Immunologic Memory, K562 Cells, Mice, Phenotype, Immunotherapy, Adoptive, Receptors, CCR7 immunology, T-Lymphocytes immunology, T-Lymphocytes transplantation

Abstract

Background: Adoptive T cell immunotherapy (ATCT) for cancer entails infusing patients with T cells that recognise and destroy tumour cells. Efficient engraftment of T cells and persistence in the circulation correlate with favourable clinical outcomes. T cells of early differentiation possess an increased capacity for proliferation and therefore persistence, using these cells for ATCT could therefore lead to improved clinical outcomes., Method: We describe a method to enrich T cells of early differentiation status using paramagnetic beads and antibodies targeting cells expressing C-C motif chemokine receptor 7 (CCR7)., Results: Selection of cells expressing CCR7 enriches T cells of bearing markers of early differentiation status. This was validated through analysis of an array of surface markers and an observed reduction in effector cell functions ex vivo. CCR7 selection resulted in dramatic 83.6 and 137 fold increases in circulating levels of CD4 and CD8 T cells respectively compared to non-sorted T cells 3 weeks after adoptive transfer to NSG mice. We observed no significant difference in the engraftment levels of CCR7 or CD62L selected cells in the NSG mouse model. Comparison of cells ex vivo, however, suggests CCR7 selection is superior to CD62L selection in enriching T cells of early differentiation status., Conclusions: CCR7 selection offers a means to enrich T cells of early differentiation status for ACTC. Together our data suggests that these T cells are likely to display enhanced engraftment and persistence in patients in vivo and could therefore improve therapeutic efficacy of ACTC.

Published

2017