Methodology for Anti-Gene Anti-IGF-I Therapy of Malignant Tumours
Author(s) -
Jerzy Trojan,
Yuexin Pan,
Ming Wei,
Adama Ly,
Alexander Shevelev,
Maciej Bierwagen,
Maryvonne Ardourel,
L. Trojan,
Álvaro Pérez Álvarez,
Christian Andrés,
Maria Claudia Noguera,
Ignacio Briceño,
Beatriz Bernal,
Heliodor Kasprzak,
Huynh Thien Duc,
Donald D. Anthony
Publication year - 2012
Publication title -
chemotherapy research and practice
Language(s) - English
Resource type - Journals
eISSN - 2090-2115
pISSN - 2090-2107
DOI - 10.1155/2012/721873
Subject(s) - cd8 , medicine , radiation therapy , glioblastoma , chemotherapy , cancer , major histocompatibility complex , immunotherapy , cancer research , immunology , immune system
The aim of this study was to establish the criteria for methodology of cellular “anti-IGF-I” therapy of malignant tumours and particularly for glioblastoma multiforme. The treatment of primary glioblastoma patients using surgery, radiotherapy, and chemotherapy was followed by subcutaneous injection of autologous cancer cells transfected by IGF-I antisense/triple helix expression vectors. The prepared cell “vaccines” should it be in the case of glioblastomas or other tumours, have shown a change of phenotype, the absence of IGF-I protein, and expression of MHC-I and B7. The peripheral blood lymphocytes, PBL cells, removed after each of two successive vaccinations, have demonstrated for all the types of tumour tested an increasing level of CD8 + and CD8 + 28 + molecules and a switch from CD8 + 11b + to CD8 + 11. All cancer patients were supervised for up to 19 months, the period corresponding to minimum survival of glioblastoma patients. The obtained results have permitted to specify the common criteria for “anti-IGF-I” strategy: characteristics sine qua non of injected “vaccines” (cloned cells IGF-I(−) and MHC-I(+)) and of PBL cells (CD8 + increased level).
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