GENE-THERAPY FOR B-CELL LYMPHOMA IN A SCID MOUSE MODEL USING AN IMMUNOGLOBULIN-REGULATED DIPHTHERIA-TOXIN GENE DELIVERED BY A NOVEL ADENOVIRUS-POLYLYSINE CONJUGATE
Despite advances in conventional therapy, many lives continue to be lost to common forms of B-cell cancers, including leukemias, lymphomas and multiple myeloma. We propose a novel approach to therapy of such cancers using controlled expression of a diphtheria toxin gene (DT-A) to kill malignant cells. We have previously demonstrated selective killing of various cell types, in vitro and in vivo, by cell-specific, transcriptionally controlled expression of this gene. Organ-specific ablation in otherwise healthy transgenic mice has convincingly demonstrated the exquisite specificity achievable by this technique1-5. In the studies now described, DT-A was delivered in vitro and in vivo using a novel gene delivery system employing DNA physically attached to the exterior of adenovirus. After demonstrating the efficacy of gene delivery to Epstein-Barr virus transformed human B-cells in vitro, in vivo work was performed using a SCID mouse model for B-cell lymphoma, in which protection against tumor was observed. The concepts of tissue-regulated toxin gene therapy, and this novel adenovirus gene delivery system are discussed
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E BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLANDE BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLAND
ROWE, M
YOUNG, LS
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E BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLANDE BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLAND
YOUNG, LS
CROCKER, J
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E BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLANDE BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLAND
CROCKER, J
STOKES, H
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E BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLANDE BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLAND
STOKES, H
HENDERSON, S
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E BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLANDE BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLAND
HENDERSON, S
RICKINSON, AB
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E BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLANDE BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLAND
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E BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLANDE BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLAND
ROWE, M
YOUNG, LS
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E BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLANDE BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLAND
YOUNG, LS
CROCKER, J
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E BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLANDE BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLAND
CROCKER, J
STOKES, H
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E BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLANDE BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLAND
STOKES, H
HENDERSON, S
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E BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLANDE BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLAND
HENDERSON, S
RICKINSON, AB
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E BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLANDE BIRMINGHAM DIST GEN HOSP, DEPT HISTOPATHOL, BIRMINGHAM B9 5ST, W MIDLANDS, ENGLAND