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Intraperitoneal injection of genetically modified, human mesothelial cells for systemic gene therapy

被引:32
作者
Murphy, JE [1 ]
Rheinwald, JG [1 ]
机构
[1] HARVARD UNIV, BRIGHAM & WOMENS HOSP,SCH MED,DEPT MED, DIV DERMATOL, BOSTON, MA 02115 USA
来源
HUMAN GENE THERAPY | 1997年 / 8卷 / 16期
关键词
D O I
10.1089/hum.1997.8.16-1867
中图分类号
Q81 [生物工程学(生物技术)]; Q93 [微生物学];
学科分类号
071005 ; 0836 ; 090102 ; 100705 ;
摘要
An ideal cell type for ex vivo gene therapy should be easy to biopsy, propagate, and genetically engineer in culture, should be transplantable using simple procedures, and should express therapeutic proteins at useful levels, The mesothelial cell appears to satisfy these criteria, Several thousand proliferative mesothelial cells were present in typical specimens of nonpathologic human peritoneal fluid obtained by needle aspiration, These divided rapidly in a specialized medium to yield pure cultures of similar to 10(7) cells within 2 weeks, The replicative lifespan of mesothelial cells cultured from adults was similar to 42-52 population doublings, permitting expansion and cryopreservation of a lifetime supply of autologous cells from one fluid sample. Cells transduced with a human growth hormone (hGH) adenoviral vector secreted 100-300 mu g of hGH/10(6) cells per day for at least 6 weeks in culture when maintained at quiescence. Intraperitoneal injection of transduced cells into athymic mice resulted in rapid systemic delivery of hGH, with peak plasma levels of 0.1-1 mu g/ml declining over 3 weeks to <1 ng/ml, Mice receiving a second injection of engineered cells displayed the same plasma hGH levers and duration as naive mice, Cells labeled with a beta-galactosidase vector were identifiable by in situ enzymatic staining as clusters attached to peritoneal surfaces at multiple sites for at least 19 days after injection, Cells serially passaged through about three-quarters of their lifespan before transduction and injection mere as effective at hGH delivery as earlier-passage cells, These results indicate the clinical potential for ex vivo gene therapy using mesothelial cells.
引用
收藏
页码:1867 / 1879
页数:13
相关论文
共 66 条
[1]  
ABUHIJLEH MF, 1995, J ANAT, V186, P453
[2]   INTRAARTICULAR EXPRESSION OF BIOLOGICALLY-ACTIVE INTERLEUKIN-1 RECEPTOR-ANTAGONIST PROTEIN BY EX-VIVO GENE-TRANSFER [J].
BANDARA, G ;
MUELLER, GM ;
GALEALAURI, J ;
TINDAL, MH ;
GEORGESCU, HI ;
SUCHANEK, MK ;
HUNG, GL ;
GLORIOSO, JC ;
ROBBINS, PD ;
EVANS, CH .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (22) :10764-10768
[3]   TRANSPLANTATION OF TRANSDUCED CHONDROCYTES PROTECTS ARTICULAR-CARTILAGE FROM INTERLEUKIN 1-INDUCED EXTRACELLULAR-MATRIX DEGRADATION [J].
BARAGI, VM ;
RENKIEWICZ, RR ;
JORDAN, H ;
BONADIO, J ;
HARTMAN, JW ;
ROESSLER, BJ .
JOURNAL OF CLINICAL INVESTIGATION, 1995, 96 (05) :2454-2460
[4]   SYSTEMIC DELIVERY OF RECOMBINANT PROTEINS BY GENETICALLY MODIFIED MYOBLASTS [J].
BARR, E ;
LEIDEN, JM .
SCIENCE, 1991, 254 (5037) :1507-1509
[5]  
BECKER TC, 1994, METHOD CELL BIOL, V43, P161
[6]   INTRATHYMIC IMPLANTS OF GENETICALLY MODIFIED FIBROBLASTS [J].
BEHARA, AMP ;
WESTCOTT, AJ ;
CHANG, PL .
FASEB JOURNAL, 1992, 6 (10) :2853-2858
[7]   T-LYMPHOCYTE-DIRECTED GENE-THERAPY FOR ADA(-) SCID - INITIAL TRIAL RESULTS AFTER 4 YEARS [J].
BLAESE, RM ;
CULVER, KW ;
MILLER, AD ;
CARTER, CS ;
FLEISHER, T ;
CLERICI, M ;
SHEARER, G ;
CHANG, L ;
CHIANG, YW ;
TOLSTOSHEV, P ;
GREENBLATT, JJ ;
ROSENBERG, SA ;
KLEIN, H ;
BERGER, M ;
MULLEN, CA ;
RAMSEY, WJ ;
MUUL, L ;
MORGAN, RA ;
ANDERSON, WF .
SCIENCE, 1995, 270 (5235) :475-480
[8]   GENE-THERAPY - A NOVEL FORM OF DRUG-DELIVERY [J].
BLAU, HM ;
SPRINGER, ML .
NEW ENGLAND JOURNAL OF MEDICINE, 1995, 333 (18) :1204-1207
[9]   GENE-THERAPY IN PERIPHERAL-BLOOD LYMPHOCYTES AND BONE-MARROW FOR ADA(-) IMMUNODEFICIENT PATIENTS [J].
BORDIGNON, C ;
NOTARANGELO, LD ;
NOBILI, N ;
FERRARI, G ;
CASORATI, G ;
PANINA, P ;
MAZZOLARI, E ;
MAGGIONI, D ;
ROSSI, C ;
SERVIDA, P ;
UGAZIO, AG ;
MAVILIO, F .
SCIENCE, 1995, 270 (5235) :470-475
[10]   MULTIPLE MODIFICATIONS IN CIS-ELEMENTS OF THE LONG TERMINAL REPEAT OF RETROVIRAL VECTORS LEAD TO INCREASED EXPRESSION AND DECREASED DNA METHYLATION IN EMBRYONIC CARCINOMA-CELLS [J].
CHALLITA, PM ;
SKELTON, D ;
ELKHOUEIRY, A ;
YU, XJ ;
WEINBERG, K ;
KOHN, DB .
JOURNAL OF VIROLOGY, 1995, 69 (02) :748-755
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