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Literature DB >> 9415889

A cell surface tethered enzyme improves efficiency in gene-directed enzyme prodrug therapy.

R Marais¹, R A Spooner, S M Stribbling, Y Light, J Martin, C J Springer.

Abstract

The potential for expressing the bacterial enzyme carboxypeptidase G2 (CPG2) tethered to the outer surface of mammalian cells was examined for use in gene-directed enzyme prodrug therapy. The affinity of CPG2 for the substrate methotrexate was unaffected by three mutations required to prevent N-linked glycosylation. Breast carcinoma MDA MB 361 cells expressing CPG2 internally showed only a very modest increase in sensitivity to the prodrug CMDA because the prodrug did not enter the cells. Cells expressing surface-tethered CPG2, however, became 16-24-fold more sensitive to CMDA and could mount a good bystander effect. Systemic administration of CMDA to mice bearing established xenografts of the transfected cells led to sustained tumor regressions or cures.

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Year: 1997 PMID： 9415889 DOI： 10.1038/nbt1297-1373

Source DB: PubMed Journal: Nat Biotechnol ISSN： 1087-0156 Impact factor: 54.908

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Cited

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A cell surface tethered enzyme improves efficiency in gene-directed enzyme prodrug therapy.

Review 1. Prodrug-activating systems in suicide gene therapy.

Review 2. Introduction to the background, principles, and state of the art in suicide gene therapy.

3. A functional assay for gap junctional examination; electroporation of adherent cells on indium-tin oxide.

4. Engineering CAR-T cells to activate small-molecule drugs in situ.

Review 5. Recent trends in targeted anticancer prodrug and conjugate design.

6. Detection of the prodrug-activating enzyme carboxypeptidase G2 activity with chemical exchange saturation transfer magnetic resonance.

7. Strategies in gene therapy for glioblastoma.

Review 8. Advancement and prospects of tumor gene therapy.

9. A novel vascular endothelial growth factor-directed therapy that selectively activates cytotoxic prodrugs.

10. Effect of Cellular Location of Human Carboxylesterase 2 on CPT-11 Hydrolysis and Anticancer Activity.