Is Platelet Aggregation a Useful Investigation in Assessing the Risk of Thrombosis in Patients With JAK-Positive Chronic Myeloproliferative Disorders? Brief Report: A Study on 14 Patients

V.M. Popov , A.M. Vladareanu , H. Bumbea , D. Casleanu , A. Ilea , M. Onisai , A. Nicolescu , C. Marinescu , C. Ciufu , I. Voican , M. Begu , A.M. Vintilescu , C. Dobrea , E. Kovacs , T. Savopol
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As stimuli, we used ADP, collagen, epinephrine, and ristocetin.</p></div><div><h3>Results and Discussion</h3><p>We studied 14 JAK2-positive patients (5 patients, ET; 6, PV; 1, IMF; and 2, unclassifiable CMPD), 9 men and 5 women, with a median age of 58.35 years; and 6 JAK2-negative patients (1 patient, ET; 2, PV; 3, IMF), 4 men and 2 women, with a median age of 67.16 years. Thrombosis was present in 69.12% of the JAK2-positive patients. Of these, 3 patients presented with portal vein thrombosis as the first clinical manifestation; all 3 patients were young (median age, 33 years). Ischemic stroke was presented in 5 patients (median age, 74.75 years), arterial or venal thrombosis in 2 patients. Patients who were JAK negative rarely presented with thrombosis (1 patient in our study). Platelet aggregation studies showed decreased response to ADP (49.75 vs. 50.92), epinephrine (23.05 vs. 11.53), and collagen (42.93 vs. 66.51). For ristocetin, we obtained normal value for JAK2-positive patients (60.67 vs. 44). We also obtained higher duration of collagen lag phase for JAK2-positive patients (153.97 vs. 61.57) and no differences for amplitude or duration of ADP lag phase (4.27 vs. 5.1; 8.14 vs. 9.46) or amplitude of collagen lag phase (6.21 vs. 7.61). Deaggregation is more frequent for JAK2-positive patients: 6 cases (42.85%) versus 5 cases (83.33%) for ADP; 4 cases (28.57%) versus 2 cases (33.33%) for collagen.</p></div><div><h3>Conclusion</h3><p>Patients with CMPD frequently present with venal thrombosis (portal/suprahepatic veins) or ischemic strokes. In patients with JAK2-positive CMPD, platelet aggregation is diminished for ADP, epinephrine, and collagen; also, the lag phase was longer for collagen in JAK2-positive patients. Platelet aggregation is not enough of a technique for the investigation of platelet function in order to correctly establish the risk of thrombosis. 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引用次数: 0

Abstract

Patients with chronic myeloproliferative disorders have frequently thrombosis, especially for JAK2-positive patients. The aim of this study is to identify and correlate abnormalities of platelet aggregation for 14 JAK-positive patients, with thrombosis incidence. Thromboses were present more frequently in the JAK-positive group than the JAK-negative group. Patients with JAK2 genotype have more diminished platelet response for ADP, epinephrine, and collagen than the JAK-negative group and normal response for ristocetin, but these results do not have statistical significance to correlate with a higher risk of thrombosis

Full Abstract

Background

Patients with chronic myeloproliferative disorders (CMPD) have a variety of structural and functional abnormalities of platelets. JAK2, which is constitutively activated in most patients with CMPD, might be involved in signal transduction for thrombopoietin-induced aggregation of platelets in these disorders. The patients with JAK2-positive CMPD have a higher incidence of venous thrombosis compared with noncarriers; these are more frequent in patients with the wild-type JAK2 genotype.

Aim

We aim to identify abnormalities of platelet aggregation for CMPD patients with JAK present and to correlate these findings with increased risk of thrombosis.

Materials and Methods

We present a retrospective study on 14 cases with JAK2-positive CMPD compared with 6 cases with JAK2-negative CMPD admitted in University Emergency Hospital Bucharest. We analyzed the clinical and laboratory parameters for both groups. Platelet function was investigated by platelet aggregation on Chrono-log aggregometer. As stimuli, we used ADP, collagen, epinephrine, and ristocetin.

Results and Discussion

We studied 14 JAK2-positive patients (5 patients, ET; 6, PV; 1, IMF; and 2, unclassifiable CMPD), 9 men and 5 women, with a median age of 58.35 years; and 6 JAK2-negative patients (1 patient, ET; 2, PV; 3, IMF), 4 men and 2 women, with a median age of 67.16 years. Thrombosis was present in 69.12% of the JAK2-positive patients. Of these, 3 patients presented with portal vein thrombosis as the first clinical manifestation; all 3 patients were young (median age, 33 years). Ischemic stroke was presented in 5 patients (median age, 74.75 years), arterial or venal thrombosis in 2 patients. Patients who were JAK negative rarely presented with thrombosis (1 patient in our study). Platelet aggregation studies showed decreased response to ADP (49.75 vs. 50.92), epinephrine (23.05 vs. 11.53), and collagen (42.93 vs. 66.51). For ristocetin, we obtained normal value for JAK2-positive patients (60.67 vs. 44). We also obtained higher duration of collagen lag phase for JAK2-positive patients (153.97 vs. 61.57) and no differences for amplitude or duration of ADP lag phase (4.27 vs. 5.1; 8.14 vs. 9.46) or amplitude of collagen lag phase (6.21 vs. 7.61). Deaggregation is more frequent for JAK2-positive patients: 6 cases (42.85%) versus 5 cases (83.33%) for ADP; 4 cases (28.57%) versus 2 cases (33.33%) for collagen.

Conclusion

Patients with CMPD frequently present with venal thrombosis (portal/suprahepatic veins) or ischemic strokes. In patients with JAK2-positive CMPD, platelet aggregation is diminished for ADP, epinephrine, and collagen; also, the lag phase was longer for collagen in JAK2-positive patients. Platelet aggregation is not enough of a technique for the investigation of platelet function in order to correctly establish the risk of thrombosis. In our study, the low number of cases does not allow obtaining statistically significant results.

血小板聚集是评估jak阳性慢性骨髓增殖性疾病患者血栓形成风险的有用调查吗?摘要报告:对14例患者的研究
慢性骨髓增生性疾病患者常发生血栓形成,尤其是jak2阳性患者。本研究的目的是确定14例jak阳性患者血小板聚集异常与血栓形成的相关性。与jak -阴性组相比,jak -阳性组血栓发生率更高。与JAK2基因型患者相比,JAK2基因型患者血小板对ADP、肾上腺素和胶原蛋白的反应更低,而对瑞索他汀的反应正常,但这些结果与血栓形成的高风险没有统计学意义。背景:慢性骨髓增生性疾病(CMPD)患者有多种血小板结构和功能异常。JAK2在大多数CMPD患者中被组成性激活,可能参与了这些疾病中血小板生成素诱导的血小板聚集的信号转导。jak2阳性CMPD患者静脉血栓的发生率高于非携带者;这些在野生型JAK2基因型患者中更为常见。我们的目的是确定存在JAK的CMPD患者的血小板聚集异常,并将这些发现与血栓形成风险增加联系起来。材料与方法对布加勒斯特大学急救医院收治的14例jak2阳性CMPD与6例jak2阴性CMPD进行回顾性分析。我们分析了两组患者的临床和实验室参数。采用Chrono-log聚集仪检测血小板聚集功能。我们使用ADP、胶原蛋白、肾上腺素和瑞斯托司汀作为刺激。结果与讨论我们研究了14例jak2阳性患者(5例ET;6,光伏;1、国际货币基金组织(IMF);2例未分类CMPD),男9例,女5例,中位年龄58.35岁;jak2阴性患者6例(ET 1例;2、光伏;3人(IMF),男性4人,女性2人,平均年龄67.16岁。69.12%的jak2阳性患者存在血栓形成。其中3例以门静脉血栓形成为首发临床表现;3例患者均为年轻(中位年龄33岁)。缺血性脑卒中5例(中位年龄74.75岁),动脉或静脉血栓2例。JAK阴性的患者很少出现血栓形成(本研究中1例)。血小板聚集研究显示ADP (49.75 vs. 50.92)、肾上腺素(23.05 vs. 11.53)和胶原蛋白(42.93 vs. 66.51)的反应降低。对于瑞斯托司汀,我们在jak2阳性患者中获得正常值(60.67 vs. 44)。我们还发现jak2阳性患者的胶原滞后期持续时间更长(153.97比61.57),ADP滞后期的幅度和持续时间没有差异(4.27比5.1;8.14 vs. 9.46)或胶原滞后期幅度(6.21 vs. 7.61)。jak2阳性患者脱聚集更频繁:6例(42.85%)对ADP患者5例(83.33%);胶原蛋白4例(28.57%),2例(33.33%)。结论CMPD患者多以静脉血栓形成(门静脉/肝上静脉)或缺血性脑卒中为主。在jak2阳性CMPD患者中,ADP、肾上腺素和胶原蛋白的血小板聚集减少;此外,jak2阳性患者胶原蛋白的滞后期更长。血小板聚集不足以用于血小板功能的调查,以正确确定血栓形成的风险。在我们的研究中,病例数少,不允许获得统计上显著的结果。
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