CYCLOSPORINE AND CREMAPHOR MODULATE VON-WILLEBRAND-FACTOR RELEASE FROM CULTURED HUMAN ENDOTHELIAL-CELLS

被引：36

作者：

COLLINS, P

WILKIE, M

RAZAK, K

ABBOT, S

HARLEY, S

BAX, C

ZAIDI, M

BLAKE, D

CUNNINGHAM, J

NEWLAND, A

机构：

[1] ROYAL LONDON HOSP & MED SCH, DEPT HAEMATOL, LONDON, ENGLAND

[2] ROYAL LONDON HOSP & MED SCH, DEPT NEPHROL, LONDON, ENGLAND

[3] ROYAL LONDON HOSP & MED SCH, BONE & JOINT RES GRP, LONDON, ENGLAND

[4] ST GEORGE HOSP, SCH MED, DIV BIOCHEM, BONE & MINERAL RES UNIT, LONDON, ENGLAND

来源：

TRANSPLANTATION | 1993年 / 56卷 / 05期

关键词：

D O I：

10.1097/00007890-199311000-00032

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Cyclosporine has been associated with microangiopathic hemolysis (MAHA) and other thrombotic complications of bone marrow and renal transplantation. MAHA is characterized by intravascular platelet aggregation, which, in some situations, is thought to be mediated by hyperactive high molecular weight von Willebrand factor (vWF). We have hypothesized that transplant-related MAHA may be caused by CsA-mediated release of von Willebrand factor from endothelial cells. This hypothesis was tested by studying vWF release from human umbilical vein endothelial cells primed with either CsA or cremophor EL. CsA and cremophor alone did not increase vWF release until toxic concentrations were reached (50-100 mu g/ml). However, at therapeutic concentrations (0.1-5 mu g/ml) vWF release by cells stimulated with thrombin, histamine, PMA, and the calcium ionophore A23187 was enhanced by both CsA and cremophor in a concentration-dependent manner. In single isolated endothelial cells, the thrombin-induced increase in cytosolic free calcium was enhanced by both CsA and cremophor. Preincubation for 24 hr with CsA but not cremophor suppressed vWF release after thrombin stimulation. These observations were mirrored by a concentration-dependent suppression of [H-3]thymidine uptake by CsA. We conclude that CsA vehicle, cremophor, enhances stimulated vWF release in vitro, probably by processes dependent upon increased cytosolic free calcium. This suggests a possible mechanism for thrombotic transplant complications.

引用

页码：1218 / 1223

页数：6

共 41 条

[1] THE INFLUENCE OF THE CYCLOSPORINE VEHICLE, CREMOPHOR EL, ON RENAL MICROVASCULAR BLOOD-FLOW IN THE RAT
ABRAHAM, JS
BENTLEY, FR
GARRISON, RN
CRYER, HM
[J]. TRANSPLANTATION, 1991, 52 (01) : 101 - 105
[2] INCREASED FACTOR-VIII AS AN INDEX OF VASCULAR INJURY IN CYCLOSPORINE NEPHROTOXICITY
BROWN, Z
NEILD, GH
WILLOUGHBY, JJ
SOMIA, NV
CAMERON, SJ
[J]. TRANSPLANTATION, 1986, 42 (02) : 150 - 153
[3] BROWN Z, 1989, CYCLOSPORIN THERAPEU, P654
[4] CYTOKINE-INDUCED PROCOAGULANT ACTIVITY IN MONOCYTES AND ENDOTHELIAL-CELLS - FURTHER ENHANCEMENT BY CYCLOSPORINE
CARLSEN, E
FLATMARK, A
PRYDZ, H
[J]. TRANSPLANTATION, 1988, 46 (04) : 575 - 580
[5] COLLINS PW, 1992, BONE MARROW TRANSPL, V10, P499
[6] DEGROOT PG, 1984, J BIOL CHEM, V259, P3329
[7] VENOCCLUSIVE DISEASE OF THE LIVER AFTER CHEMORADIOTHERAPY AND AUTOLOGOUS BONE-MARROW TRANSPLANTATION
DULLEY, FL
KANFER, EJ
APPELBAUM, FR
AMOS, D
HILL, RS
BUCKNER, CD
SHULMAN, HM
MCDONALD, GB
THOMAS, ED
[J]. TRANSPLANTATION, 1987, 43 (06) : 870 - 873
[8] COMPARISON OF THE HISTAMINE-RELEASING ACTIVITY OF CREMOPHOR EL AND SOME OF ITS DERIVATIVES IN 2 EXPERIMENTAL-MODELS - THE INVIVO ANESTHETIZED DOG AND INVITRO RAT PERITONEAL MAST-CELLS
ENNIS, M
LORENZ, W
KAPP, B
LUBEN, L
SCHMAL, A
[J]. AGENTS AND ACTIONS, 1985, 16 (3-4): : 265 - 268
[9] DECREASE IN ENDOTHELIAL CELL-DEPENDENT PROTEIN-C ACTIVATION INDUCED BY THROMBOMODULIN BY TREATMENT WITH CYCLOSPORINE
GARCIAMALDONADO, M
KAUFMAN, CE
COMP, PC
[J]. TRANSPLANTATION, 1991, 51 (03) : 701 - 705
[10] CHANGES IN CYTOSOLIC CA-2+ASSOCIATED WITH VONWILLEBRAND-FACTOR RELEASE IN HUMAN-ENDOTHELIAL CELLS EXPOSED TO HISTAMINE - STUDY OF MICROCARRIER CELL MONOLAYERS USING THE FLUORESCENT-PROBE INDO-1
HAMILTON, KK
SIMS, PJ
[J]. JOURNAL OF CLINICAL INVESTIGATION, 1987, 79 (02) : 600 - 608

← 1 2 3 4 5 →