喉癌患者PAC-1、CD62P表达与临床病理特征和复发的关系

目的探讨喉癌患者血小板表面血小板膜糖蛋白Ⅱb/Ⅲa纤维蛋白原受体(PAC-1)、血小板P-选择素(CD62P)阳性表达率以及与患者临床病理特征和复发的关系。方法选取2014年1月~2015年12月间在我院耳鼻喉科手术治疗的116例喉癌患者,随访≥2年,并选取同期在我院体检的健康人群60例为对照组,采用流式细胞仪检测法检测外周血PAC-1和CD62P阳性率,并分析与临床病理特征、复发的关系。结果喉癌患者PAC-1和CD62P阳性表达率分别为(17.82±1.76)%和(22.87±3.13)%,明显高于健康人群(P<0.05);而且在喉癌患者PAC-1表达和CD62P表达呈正相关性(r=0.238,P<0.05)。T3-T4分期或N2-N3分期患者PAC-1和CD62P阳性表达率高于T1-T2分期或N0-N1分期患者(P<0.05)。另外远处转移组PAC-1和CD62P阳性表达率高于未发生转移组(P<0.05);随访期间有24例患者复发,复发率为20.69%。复发喉癌患者PAC-1、CD62P阳性表达率分别为(17.02±0.85)%和(21.84±1.17)%,明显高于未复发的喉癌患者(P<0.05)。经Logistics回归分析,PAC-1和CD62P是喉癌患者复发的独立危险因素(P<0.05)。结论PAC-1和CD62P阳性表达率与喉癌患者T分期、淋巴结转移和远处转移密切相关,同时可作为喉癌局部复发、区域淋巴结转移、远处转移的预测指标。     

安氏Ⅲ类错畸形病因的logistic分析

目的研究引起安氏Ⅲ类错牙合畸形的病因。方法对50例安氏Ⅲ类错牙合患者和50例正常牙合人作病因问卷调查,将结果用logistic法分析,提取有效病因。结果共有慢性扁桃体炎、遗传因素、咬上唇3项病因进入方程。结论按贡献大小,长期慢性扁桃体炎、经常咬上唇和遗传因素是导致安氏Ⅲ类错牙合畸形的危险因素。     

活化血小板葡萄糖摄取及血小板膜整合素对其的影响

目的 :了解活化血小板葡萄糖摄取过程及血小板膜整合素对其影响 ,探讨整合素与血小板能量代谢的关系 ,旨在研究血小板能量代谢涉及的信号传导 ,并为目前临床应用血小板膜糖蛋白Ⅱb/Ⅲa(GPⅡb/Ⅲa)单抗抗血小板活化提供新的理论依据。方法 :用液态闪烁计数方法检测在血小板膜糖蛋白Ⅱb/Ⅲa单抗 10E5及血小板整合素αυβ3 单抗 6 0 9干预与否情况下凝血酶激活后血小板摄取氚标 2 脱氧葡萄糖 ([3 H]2 DG)率。结果 :在生理浓度范围内活化血小板 [3 H]2 DG摄取率较静息时明显升高 ,单抗 10E5可充分阻断活化血小板葡萄糖摄取 ,单抗 6 0 9可部分阻断。结论 :整合素家族单抗可抑制血小板激活后葡萄糖摄取 ,提示其可能参与血小板能量代谢信号传导过程 ,并可能以GPⅡb/Ⅲa为主     

尿激酶治疗以偏瘫为主的急性脑梗塞160例疗效观察

本文报告急性脑梗塞260例,其中160例急性脑梗塞应用尿激酶10万~U+N·S100ml,静脉滴注,q12h×10天;100例应用Svate-Ⅲ 2~U+N·S100ml,静脉滴注一次/日×15天,两组同时应用Ca~(++)拮抗剂,稀释疗法及脑细胞赋形剂治疗。结果尿激酶组基愈率为65%,显效率90.63%,总有效率达96.26%,非常显著优于Svate-Ⅲ的51%、75%及89%。结果提示尿激酶治疗急性脑梗塞在注意出血倾向发生时是安全、有效的。     

p38MAPK参与高糖刺激大鼠肾小管上皮细胞产生细胞外基质胶原Ⅲ

目的：探讨p38MAPK信号通路在高糖刺激大鼠肾小管上皮细胞产生细胞外基质胶原Ⅲ中的作用。 方法： 采用体外培养和Western blotting等方法，以不同浓度D-葡萄糖、p38MAPK信号通路特异性阻断剂SB203580以及用不同时间刺激正常大鼠肾小管上皮细胞NRK52E，分别检NRK52E细胞p38MAPK磷酸化水平和细胞外基质胶原Ⅲ的表达。 结果： 随D-葡萄糖浓度增加，p38MAPK磷酸化水平、胶原Ⅲ的产生也增加，SB203580可有效阻断高糖引起p38MAPK磷酸化水平的升高和细胞外基质胶原Ⅲ的表达的增高。 结论： 高糖引起p38MAPK磷酸化水平的升高可能在糖尿病肾病的肾间质纤维化中发挥重要作用。SB203580有潜在的糖尿病肾病防治的临床应用价值。     

(ATT) trinucleotide repeats in the antithrombin gene and their use in determining the origin of repeated mutations

Two (ATT) trinucleotide repeat polymorphisms have been identified in the tails of Alu repeat elements in intron 5 of the antithrombin gene. The frequency and distribution of allele sizes for the Alu 5 and Alu 8 tail polymorphisms have been defined in a sample Caucasian population. The Alu 5 polymorphism has two alleles while that of Alu 8 has 10 alleles with a heterozygosity of 0.83. These polymorphisms have been used in combination with four previously described polymorphisms within the antithrombin gene to construct antithrombin gene haplotypes in the sample Caucasian population. Twenty-two different haplotypes were observed, with the Alu 8 polymorphism being particularly useful in subdividing the core haplotype based on the previously identified polymorphisms. The haplotype data were used to investigate the origin of repeat mutations within the antithrombin locus. We compared the haplotypes associated the mutant antithrombin genes in five families with the mutation 2759C→T (L99F) and five families with the mutation 5381C→T (R129Stop). The mutation 2759C→T (L99F), which occurs within a non-CpG dinucleotide, was carried on a gene associated with an identical haplotype in each of the five families. The mutation 5381C→T (R129Stop), a single base substitution within a CpG dinucleotide, was associated with at least two different haplotypes. The findings suggest a founder effect in the five families sharing the 2759C→T (L99F) and at least two independent origins for the CpG dinucleotide mutation 5381C→T (Rl29Stop). © 1994 Wiley-Liss, Inc.     

Modulation of hemostatic balance with antithrombin III replacement therapy in a case of liver cirrhosis associated with recurrent venous thrombosis

Patients with liver failure can present both thrombotic and hemorragic complications because of the deficiency in coagulation factors and inhibitors (protein C and S, antithrombin III) and impairment of fibrinolytic balance. Here we report the case of a 63-year-old man with liver cirrhosis, recurrent thrombosis, and features of low-grade consumption coagulopathy, showing severe antithrombin III deficiency (about 30% of normal values). Treatment with antithrombin III (2000 U/day) and low doses of heparin (5000 U b.i.d.) was successful in modulating the coagulation system toward an antithrombotic effect. After discharge from hospital the ambulatory treatment with antithrombin III concentrates (2000 U twice a week) allowed the attainment of antithrombin III activity of about 60% and prevented the patient from recurrence of venous thrombosis.Abbreviations AT-III Antithrombin III - DIC Disseminated intravascular coagulation - TAT complexes Thrombin-antithrombin III complexes - PAI-1 Plasminogen activator inhibitor-1     

血栓性脑血管疾病患者治疗前后血小板活化膜表面糖蛋白检测及临床意义

目的 :探讨血栓性脑血管疾病患者治疗前后血小板活化标记物CD62 P,GPⅡb/Ⅲa的表达及其临床应用价值。方法 :采用流式细胞仪 (FCM )检测治疗前后血小板活化标记物CD62 P、GPⅡb/Ⅲa的表达。结果 :血栓性脑血管疾病患者治疗前血小板活化标志物CD62 P、GPⅡb/Ⅲa分别为CD62 P5 2 .19± 12 .3 7% ,GPⅡb/Ⅲa 77.98± 14 .2 2 % ,较正常对照组有显著性升高 (P <0 .0 1) ;治疗后CD62 P3 1.16± 17.43 % ,GPⅡb/Ⅲa 40 .71± 11.64 %较治疗前有显著性下降 (P<0 .0 1) ,但仍高于正常对照组 (P <0 .0 1)。结论 :血小板活化标志物CD62 P、GPⅡb/Ⅲa对血栓性脑血管疾病的诊断具有重要价值 ,为临床症状缓解后患者长期药物预防提供理论依据     

慢性丙型肝炎患者血清IGF-Ⅰ水平与血清HA、PⅢP关系的探讨

目的：探讨了慢性丙型肝炎患者血清IGF-Ⅰ水平及其与血清HA、PⅢP的关系。方法：采用放射免疫分析对39例慢性丙型肝炎患者进行了血清IGF-Ⅰ和HA、PⅢP含量测定，并与35名正常健康人作比较。结果：慢性丙型肝炎患者血清IGF-Ⅰ水平与HA、PⅢP水平呈明显正相关（r=0．8018、0．7126，P〈0．01）。结论：检测慢性丙型肝炎患者血清IGF-Ⅰ和HA、PⅢP水平的变化对疾病的诊断、治疗是一个十分有用的临床检测指标。