Effect of Xiaoyu Zhixue Tablet (消瘀止血片) on Expression ofPlatelet Membrane Glycoproteins in Patients withHemorrhagic Thrombopathy

Objective: To observe the effect of Xiaoyu Zhixue tablet (消瘀止血片,XYZXT) on the expression of platelet membrane glycoproteins in patients with hemorrhagic thrombopathy, and to explore its possible mechanism. Methods: The total of 148 patients with hemorrhagic thrombopathy were randomly divided into two groups, the traditional Chinese medicicne (TCM) group (n=98) treated with XYZXT and the Western medicine (WM) group (n=50) treated with adrenosin, vitamins C, K and P, both for 6 months. The therapeutic effect and the recovery rate of platelet aggregation in the two groups were observed. And platelet membrane glycoprotein (GP) Ⅰb/Ⅸ, GPⅡb/Ⅲa complexes, GPⅠb, GPⅡb, GP Ⅲa and P-selectin were analyzed by flow cytometry in both groups before and after treatment and also in 34 normal healthy subjects. Results: The total effective rate of hemostasis was 89. 8% in TCM group and 54. 0% in the WM group (x2=45.83, P<0.01), and the recovery rate of platelet aggregation was 72.4% and 4.0% respectively (x2=62.06, P<0.01). The fluorescence intensity of GP Ⅰ b/Ⅸ, GPⅡb/Ⅲa complexes, GPⅠb, GPⅢa and P-selectin were lower in both groups before treatment than those in the healthy subjects. Expression of above-mentioned marks was elevated in TCM group after 6 months' therapy, which was insignificantly different as compared with the healthy subjects (P>0.05) and higher than those in the WM group (P<0.05). Conclusion: One of the mechanisms in treating hemorrhagic thrombopathy with XYZXT is that it could regulate the expression of GP Ⅰb/Ⅸ, GPⅡ b/Ⅲa complexes, GPⅠb, GPⅢa and P-selectin at the level of receptor protein.

Expression of Platelet Membrane Glycoprotein Ib/Ⅸ/Ⅴ Complex,a Receptor of Thrombin,in Patients with Hemorrhagic Thrombopathy

To investigate the role of platelet membrane glycoprotein （GP） Ib/Ⅸ/Ⅴ complex and its subunit GP Ibα in patients with hemorrhagic thrombopathy （HT）, the expressions of GP Ib/Ⅸ/Ⅴ complex and GP Ibα,defined as mean fluorescence intensity （MFI）, were assessed by flow cytometry. The maximum aggregation of platelet was determined by turbidity method. These indicators were compared among 68 HT patients with the presenting complaint of hemorrhage, 33 well-controlled HT patients and 32 normal healthy subjects. The results showed that the MFI of GP Ib/Ⅸ /Ⅴ complex and GP Ibα was markedly lower in HT patients with current hemorrhage than that in the healthy subjects, with difference being statistically significant （P〈0.05）. There was no significant difference in the expressions of GP Ib/ Ⅸ/ Ⅴ complex and GP Ibα between well-controlled HT patients and normal healthy subjects （P〉0.05）. It was concluded that the expression of GP Ib/Ⅸ /Ⅴ complex, the receptor of thrombin and von Willebrand factor, was down-regulated in HT patients with current hemorrhage, which might result in the dysfunction of platelet aggregation and recurrence of HT.

Association of the Platelet Membrane Glycoprotein Ⅰa C807T Gene Polymorphism with Aspirin Resistance

To explore the correlation between the C807T polymorphism of platelet membrane glycoprotein Ⅰa （GP Ⅰa） gene and aspirin resistance in Chinese people, 200 patients with high-risk of atherosclerosis took aspirin （100 mg/d） for 7 days. Platelet aggregation function was detected using adenosine diphosphate （ADP） and arachidonic acid （AA） before and after the administration of aspirin. Then the subjects were divided into three groups according to the results of platelet aggregation function： an aspirin resistant （AR） group, an aspirin semi-responder （ASR） group and an aspirin-sensitive （AS） group. Platelet GP Ⅰa gene 807CT polymorphism was examined by means of polymerase chain reaction-sequence specific primers （PCR-SSP）. The results showed that T allelic frequency in AR group and ASR group were higher that of AS group （P〈0.005）, and the prevalence of genotypes （TT＋TC） of these two groups was significantly higher than that in AS group （P〈0.05）. Platelet GP Ⅰa T allele was significantly associated with aspirin resistance as revealed by multiple logistic regression （OR=3.76, 95% CI： 2.87-9.58）. The results suggest that inherited platelet GP Ⅰa variations may have an important impact on aspirin resistance and the presence of GP Ⅰa T allele may be a marker of genetic susceptibility to aspirin resistance.

Association of the Platelet Glycoprotein Ia C807T Gene Polymorphism With Risk of Myocardial Infarction in Chinese

Objectives To investigate the relationship of the GPIa C807T dimorphism to the risk of myocardial infarction （MI） in Chinese. Methods We did a case-control study including 100 patients and 110 controls with same race. An allele-specific polymerase chain reaction （PCR） was used for genotyping of C807T polymorphism. Results An apparent association was found between the T807 allele and MI among individuals younger than the mean age of 60 years （odds ratio, 2. 49 ; 95 % confidence interval, 1.08 - 6.22 ）. The T807 allele remained an independent risk factor for MI when age, sex, smoking, hypertension, diabetes, bodymass index, LDL-cholesterol and HDL-cholesterol were adjusted by logistic regression. Conclusions GPIa T807 appears to be an independent risk factor for MI.

Redistribution of Platelet Membrane Glycoprotein IV and Release of Intracellular α-granule Thrombospondin in Patients with Chronic Myelogenous Leukemia

The redistribution of platelet membrane glycoprotein IV (GPIV) and the release of intracellular Q-granule thrombospondin (TSP) were examined and the inhibition of 5-thromboglobulin (&TG) and platelet factor 4 (PF4) in patients with chronic myelogenous leukemia (CML) was observed and quantitation of β-TG and PF4 in sera was conducted. GPIV in inactive platelet from CML was 36080±17010 molecules/platelet as compared with 13190±4810 from the controls (P<0,01), No abnormality was found in the distribution of platelet membrane GPIb and GPIIb/III.(P>0. 05). The GPIV redistribution on active platelet membrane induced thrombin (1U/ml) from CML and healthy donors was 44320132310 and 228001 12700 molecules/platelet respectively (P<0. 01 ). The difference in the release of intracellular Q-granule TSP between CML and the control group was not found (P>0.05). There was no direct correlation between GPIV expression and TSP binding after platelet activation. The high leveIs of β-TG and PF4 in sera inhibited release of intracellular a-granule TSP in vitro. These results indicate that the abnormality of platelet membrane GPIV is a common marker in CML, therefore the specific increase of platelet GPIV in patients with CML may be a useful tool for the diagnosis and monitoring of the platelet dysfunction. The release of interna1 TSP pools is hindered by either β-TG or PF4 in sera.

Facile Route to Synthesize Pore Expanded Platelet SBA-15 for Enhanced Amidoxime-Functionalization and Efficient Extraction of U(Ⅵ) from Aqueous Solution

Short channel platelet SBA-15 mesoporous material is one of the effective adsorbent for the recovery of U(Ⅵ) from aqueous solution. Nevertheless, the defect is that the mesoporous size limits the total stripping of attached U(Ⅵ) in recycling use and the increasing densities of organic groups after functionalization. Thus, a simple and controllable method was adopted to prepare SBA-15-type material with expanded pore channel by adding trimethylbenzene in synthesis procedure. The structure, morphology and functional groups were characterized by scanning electron microscope, powder X-ray diffraction, thermogravimetric analysis, transmission electron microscope, FTIR and N_2 adsorption-desorption isotherm analysis. Furthermore, the adsorption behavior of obtained product was test under various factors such as initial concentration, pH, elution rate and contact time. The pore expanded platelet SBA-15 exhibited higher U(Ⅵ) adsorption capacity, higher elution rate, and more bearing of amidoxime groups. Due to the higher amidoxime groups, the adsorption capacity of U(Ⅵ) on the amidoxime functionalized pore-expanded SBA-15 was 674 mg-Ug^-1. The results show that the simple and controllable pore-expanded method is an effective strategy to enhance the elution effect and increase grafting amount of organic groups on the mesoporous materials.

糖尿病足溃疡时血小板聚集、释放和膜糖蛋白Ⅵ变化的临床研究

目的研究糖尿病足溃疡患者血小板聚集、释放和膜糖蛋白Ⅵ(GPⅥ)的变化。方法 42例2型糖尿病患者按有无糖尿病足分为:非糖尿病足(DM)组(未患糖尿病足)17例和糖尿病足(DFU)组25例;同时选取15例健康志愿者为对照组。检测空腹血糖值、糖化血红蛋白、血小板聚集率、血小板P选择素释放和血小板GPⅥ阳性率。结果 DFU组空腹血糖值和糖化血红蛋白(Hb A1c)两项指标均高于对照组(P<0.05);DFU组血小板聚集率显著高于对照组与DM组(P<0.05);DFU组血小板P选择素释放高于对照组与DM组(P<0.05);DFU组的GPⅥ阳性率高于对照组和DM组,差异均具有统计学意义(P<0.05)。结论血小板功能的变化可能与糖尿病足的发病有关。

缺血性脑卒中发病早期血小板膜糖蛋白Ⅵ和血清白介素-6水平变化

目的:探讨血小板膜糖蛋白Ⅵ(GPVI)和白介素-6(IL-6)在急性缺血性脑卒中早期诊断中的意义。方法:分别采用流式细胞术和ELISA检测缺血性脑卒中患者和健康对照人群GPVI和IL-6水平。通过受试者工作曲线评估GPVI和IL-6的灵敏度、特异度及界值。结果:缺血性脑卒中病人血小板GPVI和血清IL-6水平显著高于对照组,差异有非常显著性(P<0.01)。缺血性脑卒中病人GPVI与IL-6水平呈正相关(P<0.01)。缺血性脑卒中病人GPVI的ROC曲线下面积为0.984,在最适诊断参考值17.76荧光强度(FI)时,诊断的灵敏度为90.00%,特异度为93.33%。IL-6的ROC曲线下面积为0.918,在最适诊断参考值0.55ng/L时,诊断的灵敏度为66.67%,特异度为86.67%。结论:血小板GPVI含量和血清IL-6水平升高与缺血性脑卒中有关。GPVI对缺血性脑卒中具有较高的诊断价值和准确度。

蛇毒血小板抑制因子对心肌缺血再灌注损伤大鼠血小板膜糖蛋白Ⅵ表达以及血液流变的影响及意义

目的:探讨皖南蝮蛇毒血小板抑制因子(agkistrodon halys venom platelet inhibitor,AHV-PI)对心肌缺血再灌注损伤(myocardial ischemia reperfusion injury,MIRI)、大鼠血小板膜糖蛋白VI(GPVI)表达以及血液流变的影响及意义。方法:SD雄性大鼠30只,随机分为假手术组(6只)、心肌缺血再灌注损伤模型组(6只)和AHV-PI实验组(18只),实验采用结扎大鼠左冠状动脉前降支方法制备大鼠MIRI模型。AHV-PI实验组根据大鼠舌下静脉注射AHV-PI的剂量(0.05,0.1,0.2 mg/kg)再依次分为低、中、高三组,每组6只,RM6240生物信号采集处理系统监测心电变化。蛋白质免疫印迹法(Western blot)监测AHV-PI干预下,大鼠GPVI的表达水平。血栓弹力仪(TEG■5000)描记凝血时间(R)、血凝块形成时间(K)、Alpha角度(A)和凝血最大幅度(MA)。采用比浊法检测血小板聚集率。结果:与MIRI模型组相比,AHV-PI中剂量实验组和高剂量实验组GPVI表达水平明显降低(P<0.05);R值和K值明显延长,A值和MA值减小(P<0.05);血小板聚集时间、聚集幅度和聚集率均明显降低(P<0.05)。结论:AHV-PI可显著抑制MIRI大鼠GPVI的表达并可改善大鼠心肌损伤相关的血液流变学特性,进而弱化其损伤过程。

血小板糖蛋白Ⅵ对缺血性脑卒中患者预后的影响

目的研究缺血性脑卒中患者血小板糖蛋白Ⅵ(GPⅥ)水平与缺血性脑卒中预后的关系。方法采用流式细胞术测定50例缺血性脑卒中患者发病后24h内的血小板GPⅥ水平,分析其与神经功能缺损程度评分、预后的关系。结果缺血性脑卒中患者血小板GPⅥ含量与病情轻重呈正相关(P<0.01);与病情恢复程度呈负相关(P<0.01)。结论缺血性脑卒中患者血小板GPⅥ含量对患者的近期预后有预测作用。

Tyro 3受体酪氨酸激酶调控糖蛋白Ⅵ介导的血小板活化

目的研究Tyro 3受体酪氨酸激酶在糖蛋白Ⅵ(glycoprotein VI,GPVI)介导的血小板活化中的调控作用。方法以Tyro 3基因敲除小鼠的血小板为研究对象,应用GPVI的特异性刺激剂,在体外检测血小板的聚集和铺展能力,并应用流式细胞术分析血小板的颗粒释放及整合素αIIbβ3的活化情况。结果与野生型小鼠相比,Tyro 3基因敲除小鼠血小板的聚集和铺展能力减弱,颗粒释放标记物CD 62P的数量减少,整合素αIIbβ3的活化也受到明显抑制。结论 Tyro 3受体酪氨酸激酶在糖蛋白Ⅵ介导的血小板活化中具有重要的调控作用。

血小板糖蛋白Ⅵ及其拮抗药物研究进展

胶原和血小板相互作用机制为进一步阐明血栓形成提供了依据;胶原与血小板糖蛋白受体(GPR)及其拮抗药的研究,为预防和早期治疗血栓性疾病开辟新领域。血小板糖蛋白Ⅵ(GPⅥ)是与胶原密切连接的血小板受体。本文综述了血小板糖蛋白Ⅵ的结构、生理功能及其与胶原的相互作用,并介绍其拮抗药研究的一些新进展。

血小板胶原受体糖蛋白Ⅵ体外表达及功能研究

为了深入研究血小板胶原受体糖蛋白Ⅵ(glycoprotein Ⅵ,GPⅥ)功能及筛选特异性抑制剂,利用基因重 组技术体外表达GPⅥ胞外区片段。采用PCR方法扩增GPⅥ胞外区片段cDNA,构建表达载体pET-20b(+)-GP Ⅵ,转化大肠杆茵BL21(DE3)pLysS,经IPTG诱导表达。表达产物经Ni-NTA Resin纯化、复性;使用Western blot方 法鉴定重组蛋白性质;采用胶原结合试验测定重组蛋白的胶原结合能力。结果表明,经测序证明PCR扩增产物与 GPⅥ胞外区cDNA序列完全一致;酶切分析证明成功构建了表达载体pET-20b(+)-GPⅥ;原核细胞经诱导表达后 出现新的相对分子量32 kD蛋白条带,诱导产物以包涵体形式存在;Western blot分析表明重组蛋白可与抗Penta- His抗体和抗GPⅥ多抗特异性结合;胶原结合试验表明重组蛋白拥有较好的生物学功能。结论:正确构建了GPⅥ 表达载体并成功表达重组蛋白,纯化、复性后的重组蛋白具有良好的抗原性和生物学活性。

冠心病患者血RDW、PLR及GPⅥ的测定及临床研究

目的探讨红细胞分布宽度(RDW)、血小板-淋巴细胞比值(PLR)及血小板胶原受体蛋白Ⅵ(GPⅥ)在冠心病中的水平及临床意义。方法选取2017年1—12月在我院治疗的冠心病患者104例,其中不稳定心绞痛37例(UAP组),心肌梗死32例(AMI组)和稳定型心绞痛35例(SAP组),同时选取健康自愿者40名作为对照组,检测各组RDW、PLR、GPⅥ等指标水平,同时采用Gensini评分评估各组病情。结果 UAP组和AMI组RDW、PLR、GPⅥ分别为(15.11±1.60)%和(15.03±1.89)%、(140.41±32.24)和(137.55±30.15)、(62.16±14.46) pg/mL和(60.70±15.51) pg/mL,明显高于对照组和SAP组;UAP组和AMI组肌酸激酶同工酶MB(CK-MB)、心肌肌钙蛋白T(cTnT)、心肌肌钙蛋白I(cTnI)分别为(132.44±24.44)IU/L 和(140.58±30.22)IU/L、(0.94±0.10) g/L和(0.98±0.09) g/L、(6.22±1.24) g/L和(6.48±1.31) g/L,明显高于对照组和SAP组;AMI组Gensini评分为(70.24±9.87)分,明显高于UAP组和SAP组;UAP组Gensini评分为(48.44±10.46)分,明显高于SAP组,差异均有统计学意义( P <0.05);RDW、PLR与cTnI呈正相关( r =0.322和0.311, P <0.05);GPⅥ与cTnI、CK-MB、Gensini评分呈正相关( r =0.307、0.322和0.297, P <0.05)。结论冠心病患者RDW、PLR及GPⅥ明显升高,与心肌损伤标记物存在相关性,其中GPⅥ与冠状动脉病变程度有一定关系。

血小板膜糖蛋白Ⅵ:一种新的急性冠状动脉综合征生物学指标

目前研究认为,血小板膜糖蛋白Ⅵ在动脉血栓形成方面发挥关键作用。用流式细胞技术测定血小板活性标志蛋白如血小板选择素(P-selectin)、血小板膜GPIbα(CD42b)和血小板膜糖蛋白Ⅵ的表达,发现患有急性冠状动脉综合征的患者,其血小板膜糖蛋白Ⅵ表达比稳定型心绞痛患者和健康人有明显的提高,且其表达量与P-selectin正相关。血小板膜糖蛋白Ⅵ高表达水平往往与急性冠状动脉综合征的心肌坏死因子如肌钙蛋白和肌酸激酶相关。同时发现,在急性冠状动脉综合征的患者中,血小板膜糖蛋白Ⅵ的表达比肌钙蛋白和肌酸激酶这些心肌受损的指标提早数小时。因此认为,血小板膜糖蛋白Ⅵ可作为心肌梗死患者的潜在性危险程度指标。

抗血小板治疗新靶点:糖蛋白Ⅵ

抗血小板治疗在心血管疾病的治疗中占重要地位,目前临床上可应用的药物有多种,但其疗效并不令人满意,主要存在出血等并发症,所以迫切需要找到既高效又安全的新型药物。糖蛋白Ⅵ(GPⅥ)是血小板膜上众多受体之一,也是目前寻找抗血栓药物的新方向。该文就GPⅥ相关内容作一综述。

Pharmacological actions of miltirone in the modulation of platelet function

OBJECTIVE Salvia miltiorrhiza bunge contains various active constituents,some of which have been developed as commercially available medicine.Moreover,some other ingredients in Salvia miltiorrhiza play great roles in anti-platelet activity.The aim of the present study was to investigate the effects and the underlying mechanism of miltirone,a lipophilic compound of Salvia miltiorrhiza Bunge.METHODS The ability of miltirone to modulate platelet function was investigated by a variety of in vitro and in vivo experiments.Platelet aggregation and dense granule secretion induced by various agonists were measured with platelet aggregometer.Clot retraction and spreading were imaged by digital camera and fl uorescence microscope.Ferric chloride-induced carotid injury model and pulmonary thromboembolism model were used to check miltirone effect in vivo.To elucidate the mechanisms of anti-platelet activity of miltirone,flow cytometry and Western blotting were performed.RESULTS Miltirone(2,4,8 μmol·L^(-1)) was shown to suppress platelet aggregation,dense granule and α granule secretion in a dose-dependent manner.Meanwhile,miltirone inhibited the clot retraction and spreading of washed platelets.It reduced the phosphorylation of PLCγ2,PKC,Akt,GSK3β and ERK1/2 in the downstream signal pathway of collagen receptor.It also reduced the phosphorylation of Src and FAK in the integrin αⅡbβ3 mediated "outside-in" signaling,while it did not suppress the phosphorylation of β3.In addition,miltirone prolonged the occlusion time and reduced collagen/epinephrine induced pulmonary thrombi.CONCLUSION Miltirone suppresses platelet "inside-out" and "outside-in" signaling by affecting PLCγ2/PKC/ERK1/2,PI3K/Akt and Src/FAK signaling.Therefore,miltirone might represent a potential anti-platelet candidate for the prevention of thrombotic disorders.

Platelet activation and the protective effect of aprotinin in hepatolithiasis patients

OBJECTIVE: To explore platelet activation and the protective effect of aprotinin in patients with hepatolithiasis. METHODS: The count of plaletets and levels of CD_(62P) and CD_(63) were measured by flow cytometry in 38 patients with hepatolithiasis. Several measurements were carried out after treatment with aprotinin. RESULTS: The levels of CD_(62P), CD_(63) in patients with hepalolithiasis were higher than those in patients with cholecystolithiasis (P<0.05), but the count of platelets was lower (P<0.05). After operation, the levels of CD_(62P), CD_(63) were significantly increased in patients with hepatolithiasis, but the count of platelets was lower (P<0.05). Postoperative levels of CD_(62P), CD_(63) were significantly lower in patients treated with aprotinin than in normal controls (P<0.05); but there was no significant change in the count of platelets in the two groups. CONCLUSION: Platelet activation occurs in patients with hepatolithiasis, and may be inhibited by aprotinin.

Diagnosis of Disorders of Platelet Function by Flow Cytometry

The platelet membrane glycoprotein (GP)Ⅱ b/Ⅲ a, GPIX were detected by immunogold assay and flow cytometry, respectively, in two cases of Glannzmann's thrombasthenia (GT). The immunogold assay showed that the GPⅡ b/Ⅲ a gold granules in GT were decreased obviously, compared with that in normal controls. Flow cytometry results showed that GPⅡ b/Ⅲ a in two cases of GT was 0.1 % and 0.5 % of normal control, respectively. While GPIX showed no difference between the GT and normal control. The patients' father showed no bleeding symptoms, whose GPⅡ b/Ⅲ a accounted for 36.99 % of normal control. The experiment results suggested that flow cytometry is a quick, simple and sensitive method for the diagnosis of GP disorders.