Department of Biochemistry, Maastricht University P.O. Box 616, 6200 Maastricht, The Netherlands.
Haematologica. 2010 Sep;95(9):1563-71. doi: 10.3324/haematol.2010.021923. Epub 2010 Apr 26.
Protein S, which circulates in plasma in both free and bound forms, is an anticoagulant protein that stimulates activated protein C and tissue factor pathway inhibitor. Hereditary type I protein S deficiency (low total and low free protein S) is a well-established risk factor for venous thrombosis, whereas the thrombosis risk associated with type III deficiency (normal total and low free protein S) has been questioned.
Kaplan-Meier analysis was performed on 242 individuals from 30 families with protein S deficiency. Subjects were classified as normal, or having type I or type III deficiency according to their total and free protein S levels. Genetic and functional studies were performed in 23 families (132 individuals).
Thrombosis-free survival was not different between type I and type III protein S-deficient individuals. Type III deficient individuals were older and had higher protein S, tissue factor pathway inhibitor and prothrombin levels than type I deficient individuals. Thrombin generation assays sensitive to the activated protein C- and tissue factor pathway inhibitor-cofactor activities of protein S revealed similar hypercoagulable states in type I and type III protein S-deficient plasma. Twelve PROS1 mutations and two large deletions were identified in the genetically characterized families.
Not only type I, but also type III protein S deficiency is associated with a hypercoagulable state and increased risk of thrombosis. These findings may, however, be restricted to type III deficient individuals from families with mixed type I/III protein S deficiency, as these represented 80% of type III deficient individuals in our cohort.
蛋白 S 以游离和结合两种形式循环于血浆中,是一种抗凝蛋白,可激活蛋白 C 和组织因子途径抑制物。遗传性 I 型蛋白 S 缺乏症(总蛋白 S 和游离蛋白 S 均降低)是静脉血栓形成的明确危险因素,而 III 型缺乏症(总蛋白 S 正常而游离蛋白 S 降低)与血栓形成的相关性一直存在争议。
对 30 个蛋白 S 缺乏症家系的 242 名个体进行 Kaplan-Meier 分析。根据总蛋白 S 和游离蛋白 S 水平,将受试者分为正常、I 型或 III 型缺乏。对 23 个家系(132 名个体)进行了遗传和功能研究。
I 型和 III 型蛋白 S 缺乏个体的无血栓生存无差异。III 型蛋白 S 缺乏个体年龄较大,且蛋白 S、组织因子途径抑制物和凝血酶原水平高于 I 型蛋白 S 缺乏个体。对蛋白 S 的激活蛋白 C 和组织因子途径抑制物辅因子活性敏感的凝血酶生成试验显示,I 型和 III 型蛋白 S 缺乏血浆均存在类似的高凝状态。在遗传特征明确的家系中发现了 12 个 PROS1 突变和 2 个大片段缺失。
不仅 I 型,III 型蛋白 S 缺乏也与高凝状态和血栓形成风险增加相关。然而,这些发现可能仅限于伴有 I/III 型蛋白 S 混合缺乏症的家系中的 III 型蛋白 S 缺乏个体,因为这些个体占我们队列中 III 型蛋白 S 缺乏个体的 80%。