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dc.contributor.authorThistlethwaite, Fiona C
dc.contributor.authorElkord, Eyad
dc.contributor.authorGriffiths, Richard W
dc.contributor.authorBurt, Deborah J
dc.contributor.authorShablak, Alaaeldin
dc.contributor.authorCampbell, John D M
dc.contributor.authorGilham, David E
dc.contributor.authorAustin, Eric B
dc.contributor.authorStern, Peter L
dc.contributor.authorHawkins, Robert E
dc.date.accessioned2009-03-12T17:15:40Z
dc.date.available2009-03-12T17:15:40Z
dc.date.issued2008-05
dc.identifier.citationAdoptive transfer of T(reg) depleted autologous T cells in advanced renal cell carcinoma. 2008, 57 (5):623-34 Cancer Immunol. Immunother.en
dc.identifier.issn0340-7004
dc.identifier.pmid17899077
dc.identifier.doi10.1007/s00262-007-0400-6
dc.identifier.urihttp://hdl.handle.net/10541/55038
dc.description.abstractPURPOSE: CD4(+)CD25(+) regulatory T (T(reg)) cells are present in increased numbers in patients with advanced cancer and CD25(+) T cell depletion potentiates tumour immunity in animal models. The aim of this study was to assess the feasibility and safety of adoptive transfer of CD25(+) depleted autologous T cells in patients with advanced renal cell carcinoma and to examine resulting changes in lymphocyte subsets. PATIENTS AND METHODS: Six patients with advanced renal cell carcinoma underwent leukapheresis followed by conditioning chemotherapy with cyclophosphamide and fludarabine. The autologous leukapheresis product was depleted of CD25(+) cells using CliniMACS System then re-infused into the patient. RESULTS: Efficient CD25(+) depletion from all leukapheresis products was achieved and 0.55-5.87 x 10(7)/kg CD3(+) cells were re-infused. Chemotherapy related haematological toxicity was observed, but blood counts recovered in all patients allowing discharge after a mean inpatient stay of 21 days. One patient subsequently developed a rapidly progressive neurological syndrome. A transient reduction in CD25(+) subset was noted in the peripheral blood of 5 out of 6 patients with evidence of increased T cell responses to PHA in 4 out of 6 patients. One patient showed increased specific proliferative responses to the tumour associated antigen h5T4 coinciding with the nadir of T(reg) cells. CONCLUSIONS: Given the transient nature of the reduction in CD25(+) subset and the observed toxicity there is a need to explore further strategies to improve the safety and efficacy of this approach. Nevertheless, the results provide proof of concept in potentiation of tumour antigen T cell responses when T(reg) cell levels are depleted.
dc.language.isoenen
dc.subjectRegulatory T Cellsen
dc.subjectCD25en
dc.subjectFOXP3en
dc.subjectAdoptive Cell Therapyen
dc.subjectConditioning Chemotherapyen
dc.subject.meshAdult
dc.subject.meshAged
dc.subject.meshAntigens, CD3
dc.subject.meshCarcinoma, Renal Cell
dc.subject.meshFemale
dc.subject.meshFlow Cytometry
dc.subject.meshHumans
dc.subject.meshImmunotherapy, Adoptive
dc.subject.meshKidney Neoplasms
dc.subject.meshLeukapheresis
dc.subject.meshLymphocyte Depletion
dc.subject.meshMale
dc.subject.meshMiddle Aged
dc.subject.meshT-Lymphocytes
dc.subject.meshT-Lymphocytes, Regulatory
dc.subject.meshTransplantation, Autologous
dc.titleAdoptive transfer of T(reg) depleted autologous T cells in advanced renal cell carcinoma.en
dc.typeArticleen
dc.contributor.departmentCancer Research UK Department of Medical Oncology, University of Manchester and Christie Hospital NHS Foundation Trust, Manchester, UK. fthistlethwaite@PICR.man.ac.uken
dc.identifier.journalCancer Immunology, Immunotherapyen
html.description.abstractPURPOSE: CD4(+)CD25(+) regulatory T (T(reg)) cells are present in increased numbers in patients with advanced cancer and CD25(+) T cell depletion potentiates tumour immunity in animal models. The aim of this study was to assess the feasibility and safety of adoptive transfer of CD25(+) depleted autologous T cells in patients with advanced renal cell carcinoma and to examine resulting changes in lymphocyte subsets. PATIENTS AND METHODS: Six patients with advanced renal cell carcinoma underwent leukapheresis followed by conditioning chemotherapy with cyclophosphamide and fludarabine. The autologous leukapheresis product was depleted of CD25(+) cells using CliniMACS System then re-infused into the patient. RESULTS: Efficient CD25(+) depletion from all leukapheresis products was achieved and 0.55-5.87 x 10(7)/kg CD3(+) cells were re-infused. Chemotherapy related haematological toxicity was observed, but blood counts recovered in all patients allowing discharge after a mean inpatient stay of 21 days. One patient subsequently developed a rapidly progressive neurological syndrome. A transient reduction in CD25(+) subset was noted in the peripheral blood of 5 out of 6 patients with evidence of increased T cell responses to PHA in 4 out of 6 patients. One patient showed increased specific proliferative responses to the tumour associated antigen h5T4 coinciding with the nadir of T(reg) cells. CONCLUSIONS: Given the transient nature of the reduction in CD25(+) subset and the observed toxicity there is a need to explore further strategies to improve the safety and efficacy of this approach. Nevertheless, the results provide proof of concept in potentiation of tumour antigen T cell responses when T(reg) cell levels are depleted.


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