RETROVIRAL-MEDIATED GENE-TRANSFER INTO HUMAN MYELOMA CELLS

被引：16

作者：

BJORKSTRAND, B

DILBER, MS

SMITH, CIE

GAHRTON, G

XANTHOPOULOS, KG

机构：

[1] HUDDINGE HOSP,KAROLINSKA INST,CTR BIOTECHNOL,S-14186 HUDDINGE,SWEDEN

[2] NOVUM,RES CTR,HUDDINGE,SWEDEN

来源：

BRITISH JOURNAL OF HAEMATOLOGY | 1994年 / 88卷 / 02期

关键词：

MYELOMA; RETROVIRUS; GENE TRANSFER; NEOR-GENE;

D O I：

10.1111/j.1365-2141.1994.tb05026.x

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

We have studied retroviral-mediated gene transfer into human myeloma cells. Bone marrow cells were obtained from four patients with advanced myeloma, where the marrow was heavily infiltrated with myelomatous plasma cells. Myeloma cells were isolated by immunomagnetic separation, using the high-affinity B-B4 monoclonal antibody. Following separation, cells were transduced with the LN retroviral vector, which carries the gene for neomycin phosphotransferase, by incubation in cell-free supernatant with or without a growth-factor combination of IL-3, IL-6 and SCF. After infection, the cells were cultured for 9 d in RPMI-1640 and 10% FCS, either in the presence or absence of the neomycin analogue G418. Transduction efficiency was 1.5-3.8%, when compared to the number of cells at initiation of the culture, and 5.0-50.0% when compared to the number of surviving infected cells cultured without G418. The gene transfer rate was similar whether or not growth factors were present during the retroviral infection. These preclinical data provide evidence that retroviral-mediated gene transfer into human myeloma cells is feasible, and form part of the basis for current clinical studies of gene marking of bone marrow or peripheral blood progenitor cells before autologous stem cell transplantation in multiple myeloma.

引用

页码：325 / 331

页数：7

共 23 条

[1] TREATMENT FOR MULTIPLE MYELOMA - COMBINATION CHEMOTHERAPY WITH DIFFERENT MELPHALAN DOSE REGIMENS [J].

ALEXANIAN, R ;

HAUT, A ;

KHAN, AU ;

LANE, M ;

MCKELVEY, EM ;

MIGLIORE, PJ ;

STUCKEY, WJ ;

WILSON, HE .

JOURNAL OF THE AMERICAN MEDICAL ASSOCIATION, 1969, 208 (09) :1680-+

[2] PROSPECTS FOR HUMAN-GENE THERAPY [J].

ANDERSON, WF .

SCIENCE, 1984, 226 (4673) :401-409

[3] GENE-THERAPY - CURRENT STATUS AND FUTURE-DIRECTIONS [J].

APPERLEY, JF ;

WILLIAMS, DA .

BRITISH JOURNAL OF HAEMATOLOGY, 1990, 75 (02) :148-155

[4]

BJORKSTRAND B, 1994, IN PRESS LEUKEMIA LY

[5]

BORINAGA AM, 1990, BRIT J HAEMATOL, V76, P476

[6]

BORSET M, 1993, BRIT J HAEMATOL, V85, P446

[7]

BRENNER M, 1991, HUM GENE THER, V2, P137

[8] GENE-MARKING TO TRACE ORIGIN OF RELAPSE AFTER AUTOLOGOUS BONE-MARROW TRANSPLANTATION [J].

BRENNER, MK ;

RILL, DR ;

MOEN, RC ;

KRANCE, RA ;

MIRRO, J ;

ANDERSON, WF ;

IHLE, JN .

LANCET, 1993, 341 (8837) :85-86

[9] IMPROVED SURVIVAL DURATION WITH COMBINATION CHEMOTHERAPY INDUCTION FOR MULTIPLE-MYELOMA - A SOUTHWEST ONCOLOGY GROUP-STUDY [J].

DURIE, BGM ;

DIXON, DO ;

CARTER, S ;

STEPHENS, R ;

RIVKIN, S ;

BONNET, J ;

SALMON, SE ;

DABICH, L ;

FILES, JC ;

COSTANZI, JJ .

JOURNAL OF CLINICAL ONCOLOGY, 1986, 4 (08) :1227-1237

[10] ALLOGENEIC BONE-MARROW TRANSPLANTATION IN MULTIPLE-MYELOMA [J].

GAHRTON, G ;

TURA, S ;

LJUNGMAN, P ;

BELANGER, C ;

BRANDT, L ;

CAVO, M ;

FACON, T ;

GRANENA, A ;

GORE, M ;

GRATWOHL, A ;

LOWENBERG, B ;

NIKOSKELAINEN, J ;

REIFFERS, JJ ;

SAMSON, D ;

VERDONCK, L ;

VOLIN, L .

NEW ENGLAND JOURNAL OF MEDICINE, 1991, 325 (18) :1267-1273

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