TOWARD GENE-THERAPY FOR HEMOPHILIA-A - LONG-TERM PERSISTENCE OF FACTOR VIII-SECRETING FIBROBLASTS AFTER TRANSPLANTATION INTO IMMUNODEFICIENT MICE

被引：64

作者：

HOEBEN, RC ^{[1
]}

FALLAUX, FJ ^{[1
]}

VANTILBURG, NH ^{[1
]}

CRAMER, SJ ^{[1
]}

VANORMONDT, H ^{[1
]}

BRIET, E ^{[1
]}

VANDEREB, AJ ^{[1
]}

机构：

[1] UNIV HOSP LEIDEN, DEPT HAEMATOL, 2300 RC LEIDEN, NETHERLANDS

来源：

HUMAN GENE THERAPY | 1993年 / 4卷 / 02期

关键词：

D O I：

10.1089/hum.1993.4.2-179

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：

Hemophilia A is caused by the lack of functional blood-clotting factor VIII. We have used retrovirus-mediated gene transfer to generate various cell lines, rodent as well as human, that secrete the human factor VIII protein. To study whether transplantation of genetically modified fibroblasts is a feasible approach for gene therapy of hemophilia A, we implanted the factor VIII-secreting cells into immune-deficient mice. Implantation of factor VIII-secreting primary human skin fibroblasts resulted in long-term persistence of the transplanted cells; cells recovered from the implants up to 2 months post-implantation still had the capacity to secrete factor VIII when regrown in tissue culture. However, we were unable to detect any human factor VIII in plasma samples of the recipient mice. The absence of human factor VIII in the recipients' plasma is shown to be due neither to (epigenetic) inactivation of the retroviral vector in vivo, nor to inability of the stationary cells to secrete factor VIII protein. However, we did note a rapid clearing of the human factor VIII : CAg from plasma upon intravenous injection of plasma-derived human factor VIII in mice (t1/2 < 60 min vs. 10 hr in humans). This phenomenon can fully explain the apparent absence of human factor VIII in the recipients' plasma.

引用

页码：179 / 186

页数：8

共 45 条

[31] GENETICALLY MODIFIED SKIN FIBROBLASTS PERSIST LONG AFTER TRANSPLANTATION BUT GRADUALLY INACTIVATE INTRODUCED GENES
PALMER, TD
ROSMAN, GJ
OSBORNE, WRA
MILLER, AD
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1991, 88 (04) : 1330 - 1334
[32] 2 INDEPENDENT DOMAINS OF FACTOR-VIII COEXPRESSED USING RECOMBINANT VACCINIA VIRUSES HAVE PROCOAGULANT ACTIVITY
PAVIRANI, A
MEULIEN, P
HARRER, H
DOTT, K
MISCHLER, F
WIESEL, ML
MAZURIER, C
CAZENAVE, JP
LECOCQ, JP
[J]. BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1987, 145 (01) : 234 - 240
[33] PIJNAPPELS MIM, 1986, THROMB HAEMOSTASIS, V55, P70
[34] DERIVATIVES OF MOLONEY MURINE SARCOMA-VIRUS CAPABLE OF BEING TRANSCRIBED IN EMBRYONAL CARCINOMA STEM-CELLS HAVE GAINED A FUNCTIONAL-SP1 BINDING-SITE
PRINCE, VE
RIGBY, PWJ
[J]. JOURNAL OF VIROLOGY, 1991, 65 (04) : 1803 - 1811
[35] LONG-TERM INVIVO EXPRESSION OF RETROVIRUS-MEDIATED GENE-TRANSFER IN MOUSE FIBROBLAST IMPLANTS
SCHARFMANN, R
AXELROD, JH
VERMA, IM
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1991, 88 (11) : 4626 - 4630
[36] HUMAN RECOMBINANT DNA-DERIVED ANTIHEMOPHILIC-FACTOR (FACTOR-VIII) IN THE TREATMENT OF HEMOPHILIA-A
SCHWARTZ, RS
ABILDGAARD, CF
ALEDORT, LM
ARKIN, S
BLOOM, AL
BRACKMANN, HH
BRETTLER, DB
FUKUI, H
HILGARTNER, MW
INWOOD, MJ
KASPER, CK
KERNOFF, PBA
LEVINE, PH
LUSHER, JM
MANNUCCI, PM
SCHARRER, I
MACKENZIE, MA
PANCHAM, N
KUO, HS
ALLRED, RU
[J]. NEW ENGLAND JOURNAL OF MEDICINE, 1990, 323 (26) : 1800 - 1805
[37] IMPLANTATION OF GENETICALLY ENGINEERED FIBROBLASTS INTO MICE - IMPLICATIONS FOR GENE-THERAPY
SELDEN, RF
SKOSKIEWICZ, MJ
HOWIE, KB
RUSSELL, PS
GOODMAN, HM
[J]. SCIENCE, 1987, 236 (4802) : 714 - 718
[38] PHYSICAL CONDITION, LONGEVITY, AND SOCIAL PERFORMANCE OF DUTCH HEMOPHILIACS, 1972-85
SMIT, C
ROSENDAAL, FR
VAREKAMP, I
BROCKERVRIENDS, A
VANDIJCK, H
SUURMEIJER, TPBM
BRIET, E
[J]. BRITISH MEDICAL JOURNAL, 1989, 298 (6668) : 235 - 238
[39] STLOUIS D, 1988, P NATL ACAD SCI USA, V85, P3150
[40] TANI K, 1989, BLOOD, V74, P1274

← 1 2 3 4 5 →