Vascular dysmorphogenesis caused by an activating mutation in the receptor tyrosine kinase TIE2

被引:578
作者
Vikkula, M
Boon, LM
Carraway, KL
Calvert, JT
Diamonti, AJ
Goumnerov, B
Pasyk, KA
Marchuk, DA
Warman, ML
Cantley, LC
Mulliken, JB
Olsen, BR
机构
[1] HARVARD UNIV,SCH DENT MED,HARVARD FORSYTH DEPT ORAL BIOL,BOSTON,MA 02115
[2] HARVARD UNIV,CHILDRENS HOSP,SCH MED,DIV PLAST SURG,BOSTON,MA 02115
[3] DUKE UNIV,MED CTR,DEPT GENET,DURHAM,NC 27710
[4] HARVARD UNIV,CHILDRENS HOSP,SCH MED,DEPT PATHOL,BOSTON,MA 02115
[5] UNIV MICHIGAN,INST GERONTOL,ANN ARBOR,MI 48109
[6] HARVARD UNIV,BETH ISRAEL DEACONESS HOSP,SCH MED,DEPT CELL BIOL,DIV SIGNAL TRANSDUCT,BOSTON,MA 02115
来源
CELL | 1996年 / 87卷 / 07期
关键词
D O I
10.1016/S0092-8674(00)81814-0
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Venous malformations (VMs), the most common errors of vascular morphogenesis in humans, are composed of dilated, serpiginous channels. The walls of the channels have a variable thickness of smooth muscle; some mural regions lack smooth muscle altogether. A missense mutation resulting in an arginine-to-tryptophan substitution at position 849 in the kinase domain of the receptor tyrosine kinase TIE2 segregates with dominantly inherited VM in two unrelated families. Using proteins expressed in insect cells, we demonstrate that the mutation results in increased activity of TIE2. We conclude that an activating mutation in TlE2 causes inherited VMs in the two families and that the TIE2 signaling pathway is critical for endothelial cell-smooth muscle cell communication in venous morphogenesis.
引用
收藏
页码:1181 / 1190
页数:10
相关论文
共 45 条
[1]   HUMAN VENOUS ENDOTHELIUM CAN PROMOTE INTIMAL HYPERPLASIA IN A PARACRINE MANNER [J].
ALLEN, KE ;
VARTY, K ;
JONES, L ;
SAYERS, RD ;
BELL, PRF ;
LONDON, NJM .
JOURNAL OF VASCULAR SURGERY, 1994, 19 (04) :577-584
[2]   AN ACTIVATED FORM OF TRANSFORMING GROWTH FACTOR-BETA IS PRODUCED BY COCULTURES OF ENDOTHELIAL-CELLS AND PERICYTES [J].
ANTONELLIORLIDGE, A ;
SAUNDERS, KB ;
SMITH, SR ;
DAMORE, PA .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (12) :4544-4548
[3]  
BELLUS GA, 1995, AM J HUM GENET, V56, P368
[4]  
BETSHOLTZ C, 1993, BIOL PLATELET DERIVE, P11
[5]   VASCULAR CELL-INTERACTIONS MODULATE THE EXPRESSION OF ENDOTHELIN-1 AND PLATELET-DERIVED GROWTH-FACTOR BB [J].
BONIN, LR ;
DAMON, DH .
AMERICAN JOURNAL OF PHYSIOLOGY-HEART AND CIRCULATORY PHYSIOLOGY, 1994, 267 (05) :H1698-H1706
[6]   ASSIGNMENT OF A LOCUS FOR DOMINANTLY INHERITED VENOUS MALFORMATIONS TO CHROMOSOME 9P [J].
BOON, LM ;
MULLIKEN, JB ;
VIKKULA, M ;
WATKINS, H ;
SEIDMAN, J ;
OLSEN, BR ;
WARMAN, ML .
HUMAN MOLECULAR GENETICS, 1994, 3 (09) :1583-1587
[7]   SINGLE-STEP METHOD OF RNA ISOLATION BY ACID GUANIDINIUM THIOCYANATE PHENOL CHLOROFORM EXTRACTION [J].
CHOMCZYNSKI, P ;
SACCHI, N .
ANALYTICAL BIOCHEMISTRY, 1987, 162 (01) :156-159
[8]   GROWTH-FACTOR EFFECTS ON CELLS OF THE VASCULAR WALL - A SURVEY [J].
DAMORE, PA ;
SMITH, SR .
GROWTH FACTORS, 1993, 8 (01) :61-75
[9]   TRANSFORMING GROWTH-FACTOR-BETA-1 INDUCES ALPHA-SMOOTH MUSCLE ACTIN EXPRESSION IN GRANULATION-TISSUE MYOFIBROBLASTS AND IN QUIESCENT AND GROWING CULTURED FIBROBLASTS [J].
DESMOULIERE, A ;
GEINOZ, A ;
GABBIANI, F ;
GABBIANI, G .
JOURNAL OF CELL BIOLOGY, 1993, 122 (01) :103-111
[10]   VASCULARIZATION OF THE MOUSE EMBRYO - A STUDY OF FLK-1, TEK, TIE, AND VASCULAR ENDOTHELIAL GROWTH-FACTOR EXPRESSION DURING DEVELOPMENT [J].
DUMONT, DJ ;
FONG, GH ;
PURI, MC ;
GRADWOHL, G ;
ALITALO, K ;
BREITMAN, ML .
DEVELOPMENTAL DYNAMICS, 1995, 203 (01) :80-92
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