INHIBITION OF MELANOMA GROWTH BY ADENOVIRAL-MEDIATED HSV THYMIDINE KINASE GENE-TRANSFER IN-VIVO

被引：60

作者：

BONNEKOH, B

GREENHALGH, DA

BUNDMAN, DS

ECKHARDT, JN

LONGLEY, MA

CHEN, SH

WOO, SLC

ROOP, DR

机构：

[1] BAYLOR COLL MED,DEPT CELL BIOL,HOUSTON,TX 77030

[2] BAYLOR COLL MED,DEPT DERMATOL,HOUSTON,TX 77030

[3] BAYLOR COLL MED,HOWARD HUGHES MED INST,HOUSTON,TX 77030

来源：

JOURNAL OF INVESTIGATIVE DERMATOLOGY | 1995年 / 104卷 / 03期

关键词：

GENE THERAPY; GANCICLOVIR; ADENOVIRUS;

D O I：

10.1111/1523-1747.ep12664614

中图分类号：

R75 [皮肤病学与性病学];

学科分类号：

100206 ;

摘要：

To assess the potential of an in vivo, adenovirus-mediated gene therapy approach for the treatment of malignant melanoma, the efficacy of adenovirus-mediated herpes simplex virus thymidine kinase gene (HSV-Ek) transfer and administration of ganciclovir (GCV) was investigated using a nude mouse model. Initially, B16 murine melanoma cells were efficiently transduced in vitro by a recombinant replication-defective adenovirus containing the HSV-tk gene (ADV/RSVtk), and rendered sensitive to cell killing by 10 mu g/ml GCV, A significant ''bystander effect'' was observed at low multiplicity of infection in comparison of cell killing to control B16 transduction by adenovirus containing the beta-galactosidase gene (ADV/RSV-beta-gal), In vivo, melanomas established from subcutaneous injection of 4 x 10(5) B16 cells were injected after 14 d with 1 x 10(10) ADV/RSV-tk viral particles, Subsequent treatment for 6 d with GCV resulted in an inhibition of melanoma growth, with an approximately 40-50% reduction in melanoma volume in comparison to controls in repeated experiments, These data demonstrate that adenovirus-mediated gene transfer can function as an efficient delivery system to reduce established tumor burden in vivo. This result map hold significant promise for the development of effective in situ gene therapy for melanoma in humans.

引用

页码：313 / 317

页数：5

共 25 条

[1] GENE-THERAPY FOR BRAIN-TUMORS - REGRESSION OF EXPERIMENTAL GLIOMAS BY ADENOVIRUS-MEDIATED GENE-TRANSFER IN-VIVO
CHEN, SH
SHINE, HD
GOODMAN, JC
GROSSMAN, RG
WOO, SLC
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1994, 91 (08) : 3054 - 3057
[2] INVIVO GENE-TRANSFER WITH RETROVIRAL VECTOR PRODUCER CELLS FOR TREATMENT OF EXPERIMENTAL BRAIN-TUMORS
CULVER, KW
RAM, Z
WALLBRIDGE, S
ISHII, H
OLDFIELD, EH
BLAESE, RM
[J]. SCIENCE, 1992, 256 (5063) : 1550 - 1552
[3] VACCINATION WITH IRRADIATED TUMOR-CELLS ENGINEERED TO SECRETE MURINE GRANULOCYTE-MACROPHAGE COLONY-STIMULATING FACTOR STIMULATES POTENT, SPECIFIC, AND LONG-LASTING ANTITUMOR IMMUNITY
DRANOFF, G
JAFFEE, E
LAZENBY, A
GOLUMBEK, P
LEVITSKY, H
BROSE, K
JACKSON, V
HAMADA, H
PARDOLL, D
MULLIGAN, RC
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (08) : 3539 - 3543
[4] INTERLEUKIN-2 PRODUCTION BY TUMOR-CELLS BYPASSES T-HELPER FUNCTION IN THE GENERATION OF AN ANTITUMOR RESPONSE
FEARON, ER
PARDOLL, DM
ITAYA, T
GOLUMBEK, P
LEVITSKY, HI
SIMONS, JW
KARASUYAMA, H
VOGELSTEIN, B
FROST, P
[J]. CELL, 1990, 60 (03) : 397 - 403
[5] FIDLER IJ, 1975, CANCER RES, V35, P218
[6] FREEMAN SM, 1993, CANCER RES, V53, P5274
[7] THE EMERGING EPIDEMIC OF MELANOMA AND SQUAMOUS-CELL SKIN-CANCER
GLASS, AG
HOOVER, RN
[J]. JAMA-JOURNAL OF THE AMERICAN MEDICAL ASSOCIATION, 1989, 262 (15): : 2097 - 2100
[8] RECORD LOW GLOBAL OZONE IN 1992
GLEASON, JF
BHARTIA, PK
HERMAN, JR
MCPETERS, R
NEWMAN, P
STOLARSKI, RS
FLYNN, L
LABOW, G
LARKO, D
SEFTOR, C
WELLEMEYER, C
KOMHYR, WD
MILLER, AJ
PLANET, W
[J]. SCIENCE, 1993, 260 (5107) : 523 - 526
[9] A CHEMILUMINESCENT ASSAY FOR QUANTITATION OF BETA-GALACTOSIDASE IN THE FEMTOGRAM RANGE - APPLICATION TO QUANTITATION OF BETA-GALACTOSIDASE IN IACZ-TRANSFECTED CELLS
JAIN, VK
MAGRATH, IT
[J]. ANALYTICAL BIOCHEMISTRY, 1991, 199 (01) : 119 - 124
[10] JIMBOW K, 1984, CLINICAL ONCOLOGY MONOGRAPHS, V3, P477

← 1 2 3 →