SUPPRESSION OF ERYTHRO-MEGAKARYOCYTOPOIESIS AND THE INDUCTION OF REVERSIBLE THROMBOCYTOPENIA IN MICE TRANSGENIC FOR THE THYMIDINE KINASE GENE TARGETED BY THE PLATELET GLYCOPROTEIN ALPHA-IIB PROMOTER

被引:58
作者
TRONIKLEROUX, D
ROULLOT, V
SCHWEITZER, A
BERTHIER, R
MARGUERIE, G
机构
[1] CEN GRENOBLE, DEPT BIOL MOLEC & STRUCT, TRANSGENESE & DIFFERENCIAT CELLULAIRE LAB, CEA, F-38054 GRENOBLE 9, FRANCE
[2] CEN GRENOBLE, DEPT BIOL MOLEC & STRUCT,INSERM,U217,HEMATOL LAB, CEA, F-38054 GRENOBLE 9, FRANCE
来源
JOURNAL OF EXPERIMENTAL MEDICINE | 1995年 / 181卷 / 06期
关键词
D O I
10.1084/jem.181.6.2141
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
The mechanisms that regulate the commitment of a totipotent stem cell to the megakaryocytic lineage are largely unknown. Using a molecular approach to the study of megakaryocytopoiesis and platelet production, mice in which thrombocytopoiesis could be controlled were produced by targeting the expression of the herpes simplex virus thymidine kinase toxigene to megakaryocytes using the regulatory region of the gene encoding the or subunit of the platelet integrin alpha IIb beta 3. The programmed eradication of the megakaryocytic lineage was induced by treating transgenic mice bearing the hybrid construct (alpha IIbtk) with the antiherpetic drug ganciclovir (GCV). After 10 d of treatment, the platelet number was reduced by >94.6%. After discontinuing GCV, the bone marrow was repopulated with megakaryocytes and the platelet count was restored within 7 d. Prolonged GCV treatment induced erythropenia in the transgenic mice. Assays of myeloid progenitor cells in vitro demonstrated that the transgene was expressed in early erythro-megakaryocytic progenitor cells. The reversibility and facility of this system provides a powerful model to determine both the critical events in megakaryocytic and erythroid lineage development and for evaluating the precise role that platelets play in the pathogenesis of a number of vascular occlusive disorders.
引用
收藏
页码:2141 / 2151
页数:11
相关论文
共 57 条
[1]   THE HERPES-SIMPLEX VIRUS TYPE-1 THYMIDINE KINASE IS EXPRESSED IN THE TESTES OF TRANSGENIC MICE UNDER THE CONTROL OF A CRYPTIC PROMOTER [J].
ALSHAWI, R ;
BURKE, J ;
WALLACE, H ;
JONES, C ;
HARRISON, S ;
BUXTON, D ;
MALEY, S ;
CHANDLEY, A ;
BISHOP, JO .
MOLECULAR AND CELLULAR BIOLOGY, 1991, 11 (08) :4207-4216
[2]  
BERRIDGE MV, 1985, BLOOD, V66, P76
[3]   SERUM-FREE MEDIUM ALLOWS THE OPTIMAL-GROWTH OF HUMAN MEGAKARYOCYTE PROGENITORS COMPARED WITH HUMAN PLASMA SUPPLEMENTED CULTURES - ROLE OF TGF-BETA [J].
BERTHIER, R ;
VALIRON, O ;
SCHWEITZER, A ;
MARGUERIE, G .
STEM CELLS, 1993, 11 (02) :120-129
[4]   TARGETING OF AN INDUCIBLE TOXIC PHENOTYPE IN ANIMAL-CELLS [J].
BORRELLI, E ;
HEYMAN, R ;
HSI, M ;
EVANS, RM .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1988, 85 (20) :7572-7576
[5]   MODELS OF HEMATOPOIESIS [J].
BROWN, G ;
BUNCE, CM ;
LORD, JM .
LEUKEMIA RESEARCH, 1990, 14 (06) :495-499
[6]   PITUITARY HYPERPLASIA AND GIGANTISM IN MICE CAUSED BY A CHOLERA-TOXIN TRANSGENE [J].
BURTON, FH ;
HASEL, KW ;
BLOOM, FE ;
SUTCLIFFE, JG .
NATURE, 1991, 350 (6313) :74-77
[7]   INVIVO GENE-TRANSFER WITH RETROVIRAL VECTOR PRODUCER CELLS FOR TREATMENT OF EXPERIMENTAL BRAIN-TUMORS [J].
CULVER, KW ;
RAM, Z ;
WALLBRIDGE, S ;
ISHII, H ;
OLDFIELD, EH ;
BLAESE, RM .
SCIENCE, 1992, 256 (5063) :1550-1552
[8]  
DEBILI N, 1989, LEUKEMIA, V3, P669
[9]   STIMULATION OF MEGAKARYOCYTOPOIESIS AND THROMBOPOIESIS BY THE C-MPL LIGAND [J].
DESAUVAGE, FJ ;
HASS, PE ;
SPENCER, SD ;
MALLOY, BE ;
GURNEY, AL ;
SPENCER, SA ;
DARBONNE, WC ;
HENZEL, WJ ;
WONG, SC ;
KUANG, WJ ;
OLES, KJ ;
HULTGREN, B ;
SOLBERG, LA ;
GOEDDEL, DV ;
EATON, DL .
NATURE, 1994, 369 (6481) :533-538
[10]  
DUPERRAY A, 1991, BLOOD CELL BIOCH, V2, P37
123456