Antibodies Against Annexin V and Prothrombin,Their Correlation with Other Anti-phospholipid Antibodies in Recurrent Pregnancy Loss

Objective To study the findings of serum antibodies against annexin V, prothrombin, ph-inositol, ph-acid, ph-ethanolamine, ph-serine, ph-glycerol, cardiolipin, and beta2-glycoprotein I and analyze the trophoblast annexin V receptors Methods Sera from 156patients aged 26-41 years with recurrent pregnancy loss （3-7 times） were investigated. Eighty-four fertile healthy women aged 24-38 years were included in a control group. ELISA methods were used for detecting a panel of sera anti-phospholipid antibodies. Immunolocalization of annexin V receptors in 143 trophoblast specimens of 156 patients was investigated by the immunofluorescence technique using Annexin V-FITC, Apoptosis and Annexin V-CY3 commercial kits. Results Positivity for anti-phospholipid antibodies mainly against ph-serine, ph- ethanolamine, and ph-inositol was found together in 80. 8%（126 out of 156 patients）, anti-prothrombin antibodies in 12% （18）, and anti-annexin V antibodies in 13. 5% （21） women. No significant levels of anti-phospholipid antibodies were found in 6 controls. Placenta immunohistopathology also exhibited some changes manifested by the presence of apoptotic and necrotic cells in trophoblast, and very few microthrombotization in some intervillous spaces. Conclusion Our detailed study demonstrated the prevalence of majority of antiphospholipid antibodies as a high risk factor for repeated reproductive failure. Very low microthrombosis in placentas could be explained by the changes of haemocoagulation properties out of uterus.

Prevalence, significance and predictive value of antiphospholipid antibodies in Crohn's disease

AIM: To assess the prevalence and stability of different antiphospholipid antibodies(APLAs) and their association with disease phenotype and progression in inflammatory bowel diseases(IBD) patients.METHODS: About 458 consecutive patients [Crohn's disease(CD): 271 and ulcerative colitis(UC): 187] were enrolled into a follow-up cohort study in a tertiary IBD referral center in Hungary. Detailed clinical phenotypes were determined at enrollment by reviewing the patients' medical charts. Disease activity, medical treatment and data about evolvement of complications or surgical interventions were determined prospectively during the follow-up. Disease course(development f complicated disease phenotype and need for surgery),occurrence of thrombotic events, actual state of diseaseactivity according to clinical, laboratory and endoscopic scores and accurate treatment regime were recorded during the follow-up,(median, 57.4 and 61.6 mo for CD and UC). Sera of IBD patients and 103 healthy controls(HC) were tested on individual anti-β2-Glycoprotein-I(anti-β2-GPI IgA/M/G), anti-cardiolipin(ACA IgA/M/G)and anti-phosphatidylserine/prothrombin(anti-PS/PT IgA/M/G) antibodies and also anti-Saccharomyces cerevisiae antibodies(ASCA IgA/G) by enzyme-linked immunosorbent assay(ELISA). In a subgroup of CD(n = 198) and UC patients(n = 103), obtaining consecutive samples over various arbitrary timepoints during the disease course, we evaluated the intraindividual stability of the APLA status. Additionally,we provide an overview of studies, performed so far, in which significance of APLAs in IBD were assessed.RESULTS: Patients with CD had significantly higher prevalence of both ACA(23.4%) and anti-PS/PT(20.4%) antibodies than UC(4.8%, p < 0.0001 and10.2%, p = 0.004) and HC(2.9%, p < 0.0001 and15.5%, p = NS). No difference was found for the prevalence of anti-β2-GPI between different groups(7.2%-9.7%). In CD, no association was found between APLA and ASCA status of the patients.Occurrence of anti-β2-GPI, ACA and anti-PS/PT was not different between the group of patients with active vs inactive disease state according to appropriate clinical, laboratory and endoscopic scores in CD as well as in UC patients. All subtypes of anti-β2-GPI and ACA IgM status were found to be very stable over time, in contrast ACA IgG and even more ACA IgA status showed significant intraindividual changes.Changes in antibody status were more remarkable in CD than UC(ACA IgA: 49.9% vs 23.3% and ACA IgG:21.2% vs 5.8%). Interestingly, 59.1% and 30.1% of CD patients who received anti-TNF therapy showed significant negative to positive changes in ACA IgA and IgG antibody status respectively. APLA status was not associated with the clinical phenotype at diagnosis or during follow-up, medical therapy, or thrombotic events and it was not associated with the probability of developing complicated disease phenotype or surgery in a Kaplan-Meier analysis.CONCLUSION: The present study demonstrated enhanced formation of APLAs in CD patients. However,presence of different APLAs were not associated with the clinical phenotype or disease course.

B1-cell-produced anti-phosphatidylserine antibodies contribute to lupus nephritis development via TLR-mediated Syk activation

Autoantibodies produced by B cells play a pivotal role in the pathogenesis of systemic lupus erythematosus (SLE). However, both the cellular source of antiphospholipid antibodies and their contributions to the development of lupus nephritis (LN) remain largely unclear. Here, we report a pathogenic role of anti-phosphatidylserine (PS) autoantibodies in the development of LN. Elevated serum PS-specific IgG levels were measured in model mice and SLE patients, especially in those with LN. PS-specific IgG accumulation was found in the kidney biopsies of LN patients. Both transfer of SLE PS-specific IgG and PS immunization triggered lupus-like glomerular immune complex deposition in recipient mice. ELISPOT analysis identified B1a cells as the main cell type that secretes PS-specific IgG in both lupus model mice and patients. Adoptive transfer of PS-specific B1a cells accelerated the PS-specific autoimmune response and renal damage in recipient lupus model mice, whereas depletion of B1a cells attenuated lupus progression. In culture, PS-specific B1a cells were significantly expanded upon treatment with chromatin components, while blockade of TLR signal cascades by DNase I digestion and inhibitory ODN 2088 or R406 treatment profoundly abrogated chromatin-induced PS-specific IgG secretion by lupus B1a cells. Thus, our study has demonstrated that the anti-PS autoantibodies produced by B1 cells contribute to lupus nephritis development. Our findings that blockade of the TLR/Syk signaling cascade inhibits PS-specific B1-cell expansion provide new insights into lupus pathogenesis and may facilitate the development of novel therapeutic targets for the treatment of LN in SLE.

抗磷脂酰丝氨酸/凝血酶原抗体与不明原因复发性流产的相关性分析

目的:探讨抗磷脂酰丝氨酸/凝血酶原抗体及其IgG或IgM亚型是否与不明原因复发性流产相关。方法:选择2021年1月至2023年8月在北京大学第三医院就诊的年龄18~40岁且检测过抗磷脂酰丝氨酸/凝血酶原抗体的283例至少一次不明原因流产患者的病例资料进行回顾性分析,使用卡方检验和Logistic回归分析抗磷脂酰丝氨酸/凝血酶原抗体及其IgG或IgM亚型与不明原因复发性流产的相关性,使用四格表法计算抗磷脂酰丝氨酸/凝血酶原抗体及其IgG或IgM亚型在不明原因复发性流产中的灵敏度、特异度、阳性预测值和阴性预测值。结果:卡方检验表明,复发性流产组抗磷脂酰丝氨酸/凝血酶原抗体及其IgM亚型阳性率高于非复发性流产组(P均<0.05),而抗PS/PT抗体IgG亚型阳性率在两组间的差异无统计学意义(P>0.05)。以抗心磷脂抗体、抗β2糖蛋白抗体、狼疮抗凝物、抗核抗体以及年龄校正后,Logistic回归分析发现抗磷脂酰丝氨酸/凝血酶原抗体阳性与复发性流产相关(OR=2.084,95%CI 1.045~4.155,P<0.05),抗磷脂酰丝氨酸/凝血酶原抗体IgM亚型与复发性流产相关(OR=2.368,95%CI 1.187~4.722,P<0.05)。抗磷脂酰丝氨酸/凝血酶原抗体诊断复发性流产的灵敏度为65.43%,特异度为48.51%,阳性预测值为33.76%,阴性预测值为77.78%。在经典抗磷脂抗体阴性的复发性流产患者中,抗磷脂酰丝氨酸/凝血酶原抗体的灵敏度为59.09%,特异度为63.23%,阳性预测值为40.63%,阴性预测值为78.40%。抗磷脂酰丝氨酸/凝血酶原抗体IgM亚型诊断复发性流产的灵敏度为65.43%,特异度为50.99%,阳性预测值为34.87%,阴性预测值为78.63%。结论:抗磷脂酰丝氨酸/凝血酶原抗体及IgM亚型阳性与至少一次不明原因流产患者的复发性流产相关,其在不明原因复发性流产诊断中是否有预测价值尚需要未来前瞻性研究确定。

抗磷脂综合征中非标准抗磷脂抗体的诊断价值和风险预测

目的分析非标准抗磷脂抗体(aPLs)与抗磷脂综合征(APS)患者临床症状的相关性,探讨抗磷脂酰丝氨酸/凝血酶原抗体(aPS/PT)、抗磷脂酰肌醇抗体(aPI)、抗磷脂酸抗体(aPA)和抗磷脂酰乙醇胺抗体(aPE)检测在APS的诊断价值和风险评估能力。方法收集2018年1月至2021年12月在北京协和医院门诊就诊的146例APS患者,包括98例原发性APS(PAPS组),41例继发性APS(SAPS组),7例血清阴性APS(SNAPS组),以及同期SLE患者138例(SLE组),健康对照者55例(HC组)。采用化学发光免疫试验(CLIA)检测血清抗心磷脂抗体(aCL)、抗β_(2)糖蛋白I抗体(aβ_(2)GPI);酶联免疫吸附试验(ELISA)检测aPS/PT、aPI、aPA和aPE。分析比较各指标在不同组间的差异以及与临床事件的相关性。结果APS组间比较结果显示,SAPS组IgG型aPS/PT(37.80 U/mL)、aPE(6.64 U/mL)和IgA型aPE(7.23 U/mL)水平均高于PAPS组(5.10、2.89、5.07 U/mL),差异有统计学意义(P=0.000、0.016、0.023);SAPS组IgG型aPS/PT(37.80 U/mL)、aPI(13.66 U/mL)和aPA(4.48 U/mL)水平均高于SNAPS组(5.10、2.09、0.95 U/mL),差异有统计学意义(P=0.002、0.025、0.009)。与SLE组比较结果显示,PAPS组IgM型aPS/PT(26.61 U/mL)、aPI(5.93 U/mL)、aPA(3.21 U/mL)和aPE(20.08 U/mL)均高于SLE组(5.10、1.94、1.30、8.79 U/mL),而IgA型aPE(5.07 U/mL)低于SLE组(7.53 U/mL),差异均有统计学意义(P=0);SAPS组IgG型aPS/PT(37.80 U/mL)、aPI(13.66 U/mL)、aPA(4.48 U/mL),aPE(6.64 U/mL)以及IgM型aPS/PT(48.67 U/mL)和aPI(5.55 U/mL)均高于SLE组(5.10、3.86、1.75、3.65、5.10、1.94 U/mL),差异有统计学意义(P=0、0、0、0.004、0.022、0)。与HC组比较结果显示,PAPS组的aPI(IgG 5.68 U/mL,IgM 5.93 U/mL)、aPA(IgG 2.44 U/mL,IgM 3.21 U/mL)、aPE(IgG 2.89 U/mL,IgM 20.08 U/mL)和IgG型aPS/PT(5.10 U/mL)均高于HC组(1.13、0.79、1.22、0.51、1.73、8.60、5.10 U/mL),差异有统计学意义(P值分别为0、0、0、0、0、0.006、0.002);SAPS组的aPS/PT(IgG 37.80 U/mL,IgM 48.67 U/mL)、aPI(IgG 13.66 U/mL,IgM 5.55 U/mL)、aPA(IgG 4.48 U/mL,IgM 2.14 U/mL)以及aPE(IgG 6.64 U/mL,IgA 7.23 U/mL)水平高于HC组(5.10、21.12、1.13、0.79、1.22、0.51、1.73、3.62 U/mL),差异有统计学意义(P值分别为0、0.022、0、0、0、0、0、0)。aPS/PT IgG/M、aPI IgG/M、aPA IgG/M和aPE IgG/M/A在APS患者的阳性率为56.20%、43.80%、29.50%和58.90%。IgG型和IgM型aPS/PT是血栓事件(P=0.046和P=0.04)、血小板减少(P=0.016和P=0.004)的危险因素;IgM型aPS/PT是中风(P=0.018)、子痫前期早产(P=0.023)的危险因素;IgG型aPS/PT是非中风神经系统症状(P=0.029)的危险因素。IgG型aPI和aPA是APS相关肾病(P=0.035和P=0.02)和子痫前期早产(P=0.046和P=0.09)的危险因素,IgM型aPI和aPA是溶血性贫血(P=0.006和P=0.024)和大血管狭窄/闭塞(P=0.038和P=0.027)的危险因素;IgA型aPE是静脉事件(P=0.032)的危险因素。结论将非标准抗磷脂抗体aPS/PT IgG/M、aPI IgG/M、aPA IgG/M和aPE IgG/M/A作为APS的生物学标志物,不仅有助于提高诊断APS的能力,还有助于评估APS的发展,预测不良事件。

抗磷脂抗体综合征的临床表现及抗体研究进展

抗磷脂抗体综合征临床表现复杂多样,主要有血管血栓事件和习惯性流产,但其他的相关临床表现在诊断中也越来越被重视。除了已有的3种实验诊断标志物,抗凝血酶原抗体、抗β_2糖蛋白I新的结构域抗体、抗磷脂酰乙醇胺抗体、抗负电荷磷脂抗体、抗波形蛋白抗体、抗膜联蛋白抗体都具有一定的敏感性和特异性。其中该抗β_2糖蛋白Ⅰ结构域Ⅰ抗体和抗凝血酶原抗体可能是将来临床诊断应用的新标志物。

抗磷脂酰丝氨酸/凝血酶原复合物抗体对血清学阴性抗磷脂综合征的诊断价值研究

目的·研究抗磷脂酰丝氨酸/凝血酶原复合物抗体(anti-phosphatidylserine/prothrombin antibody,aPS/PT)、IgA型抗心磷脂抗体(anti-cardiolipin antibody,aCL)及IgA型抗β2糖蛋白1抗体(anti-β2-glycoproteinⅠantibody,aβ2-GPI)对血清阴性抗磷脂综合征(seronegative antiphospholipid,SNAPS)的诊断价值。方法·选取86例抗磷脂综合征(antiphospholipid,APS)患者(APS组)、48例SNAPS患者(SNAPS组)、79例系统性红斑狼疮(systemic lupus erythematosus,SLE)患者(SLE组)和85例健康者(健康对照组),应用ELISA法测定IgG型和IgM型aPS/PT、IgA型aCL和IgA型aβ2-GPI 4种抗磷脂抗体。计算这4种抗体用于诊断SNAPS的敏感度及特异度,并做受试者工作特征(ROC)曲线,以及分析4种抗体与SNAPS临床表现的相关性。结果·SNAPS组aPS/PT总检出率为52.1%,其中IgG型a PS/PT检出率为29.2%,IgM型aPS/PT检出率为35.4%,IgA型aβ2-GPI检出率为16.7%,IgA型aCL未检出;SNAPS组IgG型和IgM型aPS/PT,以及IgA型aβ2-GPI检出率显著高于健康对照组(均P=0.000)。IgG型aPS/PT用于诊断SNAPS的ROC曲线下面积最大,其次为IgA型aβ2-GPI,分别为0.753和0.725。IgG型aPS/PT(OR=5.54,95%CI1.67～17.33,P=0.003)和IgA型aβ2-GPI(OR=3.43,95%CI 0.86～11.53,P=0.041)与静脉血栓风险均呈正相关,IgM型aPS/PT与妊娠丢失风险正相关(OR=5.11,95%CI 1.31～21.29,P=0.004)。结论·IgG/IgM型aPS/PT和IgA型aβ2-GPI可作为SNAPS实验室诊断潜在的补充指标,IgG/IgM型aPS/PT对于临床评估SNAPS患者血栓形成和妊娠丢失的风险也有一定的应用价值。

冠心病患者血清抗凝血酶原抗体的检测

目的检测冠心病(CHD)患者血清中抗凝血酶原抗体(aPT)的含量,以探求其与该病的临床相关性。方法应用间接ELISA法检测HCD患者血中的aPT(IgG及IgM型)及总抗磷脂抗体(aPL)(IgG及IgM型),同时计算其阳性率和优势比(OR,95%置信区间)。结果49例CHD病人IgG,IgM,IgG/IgM-aPL的阳性率分别为22.4%,14.3%和28.6%,而对照组分别为5%,5%和10%,说明aPL在CHD病人中有明显的升高(除了IgM外,P<0.05)。CHD病人的IgG,IgM,IgG/IgM-aPT的阳性率分别为12.2%,10.2%和18.4%,对照组为2.5%,2.5%和5%,虽aPT有高于对照组的趋势,但无统计学意义(均P>0.05)。尽管如此,在AMI病人中aPL和aPT均比OMI和AP病人高,aPT更为明显。结论aPT可能是AMI的危险因素之一。aPL和aPT在一些CHD病人血清中有较高的水平,检测这些患者血中的aPL及aPT,将有助于进一步完善抗磷脂抗体综合征(APS)的临床研究及这些疾病的预防、诊断及治疗。

抗凝血酶原抗体与系统性红斑狼疮的临床相关性

目的检测抗凝血酶原抗体（aPT）在系统性红斑狼疮（SLE）患者血清中的含量，以进一步辅助SLE的诊断及治疗。方法应用间接ELISA法检测系统性红斑狼疮患者血中的aPT（IgG及IgM型），应用商品抗磷脂抗体筛查试剂盒检测患者的总抗磷脂抗体（IgG及IgM型），同时计算其阳性率和优势比（OR，95％置信区间）。结果30例SLE患者的IgG、IgM、IgG＋IgM-aPL阳性率分别为36．7％、26．7％和46．7％，对照组分别为2．5％、5．0％和7．5％，P〈O．05，两者差异有统计学意义。IgG、IgM、IgG＋IgM-aPT的阳性率分别为20．0％、16．7％和26．7％；健康对照组分别2．5％、2．5％和5．O％，P值均〈O．05，差异有统计学意义，不论抗磷脂抗体（aPL）或aPT在SLE患者中均高于正常人。结论aPL和aPT在SLE患者血清中有较高的水平，检测这些患者血中的aPT及aPL，将有助于进一步完善抗磷脂综合征的临床研究及这些疾病的预防、诊断及治疗。

凝血酶原片段PF1+2单克隆抗体的制备及其应用

目的:自制凝血酶原片段F1+2单克隆抗体,探讨其在血栓性疾病中的诊断作用。方法:常规方法制备F1+2单克隆抗体,用ELISA法检测血浆F1+2片段。结果:血栓患者、短暂性脑缺血发作(TIA)患者、脑梗塞患者与正常对照组比较,F1+2水平明显升高,具有显著性差异。结论:F1+2片段是血栓性疾病的特异指标,自制的F1+2片段单抗可以用于检测F1+2片段水平。

异常凝血酶DCP基因克隆表达、纯化及单克隆抗体制备与鉴定

目的:通过克隆、表达一种有前景的肝癌肿瘤标志物人去羟基凝血素(Des--carboxy prothrombin,DCP),制备抗DCP单克隆抗体并初步鉴定其特性.方法:依据DCP基因序列,合成DCP全长基因,构建原核表达载体pColdⅡ-DCP,转化至Escherichia coli BL21(DE3),IPTG诱导表达,以Ni2+亲和层析柱纯化带有His标签的DCP蛋白.纯化的蛋白免疫Balb/c小鼠,制备抗DCP单克隆抗体.以ELISA法检测抗体效价与亚型;Western blot和免疫组织化学染色鉴定抗体特异性.结果:成功表达并获得DCP蛋白,其相对分子量约为23000;获得1株稳定分泌抗人DCP单克隆抗体杂交瘤细胞株3B5;Western blot和免疫组织化学结果显示抗人DCP单克隆抗体能与DCP发生特异性结合,且ELISA检测抗体的效价为1∶2.43×105,其亚类为IgG2a.结论:成功制备了抗人DCP单克隆抗体,为进一步将该抗体应用于肝癌的早期诊断提供了重要工具.

抗磷脂酰丝氨酸-凝血酶原复合物抗体在狼疮抗凝物阳性患者中的危险预测价值

目的研究抗磷脂酰丝氨酸-凝血酶原复合物抗体(a PS/PT)在狼疮抗凝物(LA)阳性患者中的临床事件危险预测价值。方法连续入选2018年1月至2019年9月在北京大学第三医院2次及2次以上LA检测阳性的患者,且每次检测间隔12周及以上,共167例。将研究对象分为发生临床事件组(n=115)和未发生临床事件组(即LA携带者组,n=52),发生临床事件组中又分为发生血栓栓塞事件(TE)组(n=18)、不良妊娠结局(APO)组(n=91)及TE+APO组(n=6)。通过化学免疫分析方法检测研究对象的抗心磷脂抗体(a CL)、抗β2糖蛋白Ⅰ抗体(aβ2GPⅠ)和a PS/PT并进行统计学分析。结果与LA携带者组相比,临床事件组a PS/PT Ig G阳性率(37.4%vs 9.6%,P<0.001)以及a PS/PT Ig G和Ig M同时阳性率(31.3%vs 5.8%,P<0.001)升高;且临床事件组a PS/PT Ig G浓度也升高[(49.2±5.2) units vs(20.1±3.4) units,P<0.01)]。a PS/PT Ig G阳性率在TE+APO组(100.0%)、TE组(55.6%)以及APO组(29.7%)高于LA携带者组(9.6%),P<0.05;a PS/PT Ig G浓度在TE+APO组[(125.7±40.3) units]、TE组[(76.3±61.4) units]和APO组[(40.9±50.2) units]也高于LA携带者组[(38.6±22.1) units],P<0.05。a PS/PT Ig M阳性率只在TE+APO组(100.0%)高于LA携带者组(38.5%),P<0.05,浓度也升高[(116.3±40.0) units vs(46.5±52.1) units,P<0.05)]。而a PS/PT Ig G和Ig M同时阳性率在TE+APO组(100.0%)、TE组(44.4%)以及APO组(24.2%)高于LA携带者组(5.8%),P<0.05。a PS/PT阳性与抗磷脂抗体谱(a CL、aβ2GPⅠ和LA) 3种抗体全阳组具有一致性(Kappa=0.114,P=0.012),且a PS/PT Ig G与Ig M浓度在3种抗体全阳组[(64.6±62.8) units,(84.3±51.8) units)]都高于LA单阳组[(19.7±16.7) units,(29.3±40.8) units,P<0.05]。结论 LA阳性患者在a PS/PT阳性情况下发生临床事件的危险增高,且Ig G与发生临床事件相关度优于Ig M;抗磷脂抗体谱中3种抗体全阳组与a PS/PT阳性具有一致性且发生临床事件危险度最高。

抗磷脂酰丝氨酸/凝血酶原复合物抗体与标准抗磷脂抗体在狼疮性肾炎中的应用

目的:探讨抗磷脂酰丝氨酸/凝血酶原复合物抗体(aPS/PT)与“标准”抗磷脂抗体(aPL)在狼疮性肾炎中的应用。方法:选取2020年12月至2021年4月在国家肾脏疾病临床医学研究中心就诊的82例LN患者,检测“标准”aPL狼疮抗凝物(LA)、抗心磷脂抗体(aCL)、抗β2糖蛋白1抗体(aβ2GP1)和“非标准”aPL aPS/PT。根据“标准”aPL检测结果,将患者分为“标准”阳性组和“标准”阴性组;再根据aPS/PT检测结果分为“标准和(或)aPS/PT”阳性组和“标准和aPS/PT”阴性组,比较各组的临床、实验室资料以及肾组织病理。结果:LA、aCL和aβ2GP1检出率分别为22.0%、13.4%和39.0%;aPS/PT检出率为48.8%,其中aPS/PT IgG检出率为25.6%,aPS/PT IgM检出率为35.4%。LA阳性患者中,aPS/PT IgG/IgM阳性率高达94.4%。aPS/PT IgG与LA一致性最强,Cohen’s kappa系数0.429(P<0.01)。aPS/PT IgG阳性与血栓形成风险和神经精神狼疮发生呈正相关。“标准和(或)aPS/PT”阳性组C3、C4显著低于“标准和aPS/PT”阴性组(P<0.05),SLE疾病活动性指数显著高于“标准和aPS/PT”阴性组(P<0.05)。结论:aPS/PT与LA具有较好的一致性,补充检测aPS/PT有助于识别LN患者中血栓事件、神经精神狼疮、狼疮活动等风险。

子痫前期患者血清aPS/PT效价与血小板参数及凝血指标的相关性

目的分析子痫前期(preeclampsia,PE)患者血清中抗磷脂酰丝氨酸/凝血酶原抗体(aPS/PT)效价与其血小板参数及凝血指标的相关性。方法选取从2020年10月~2021年6月于徐州医科大学附属医院住院的PE及重度PE患者各50例,同时选取正常孕妇50例作为对照。检测各组血小板参数[血小板计数(PLT)、血小板平均体积(MPV)、血小板分布宽度(PDW)、血小板压积(PCT)]及凝血指标[凝血酶原时间(PT)、活化部分凝血活酶时间(APTT)、凝血酶时间(TT)、纤维蛋白原(FIB)、D-二聚体(D-D)],同时用ELISA法检测各组aPS/PT-IgG、aPS/PT-IgM的效价,分析aPS/PT效价与血小板参数及凝血指标的相关性。结果重度PE组aPS/PT-IgG及aPS/PT-IgM效价、MPV、PDW、PCT、FIB、D-D均较PE组及对照组升高(P<0.05),而PLT、PT、APTT、TT低于其他两组(P<0.05);PE组MPV、PDW、PCT、FIB、D-D高于对照组(P<0.05),但PLT、PT、APTT、TT低于对照组(P<0.05);PE组aPS/PT-IgG及aPS/PT-IgM效价虽较对照组高,但差异无统计学意义(P>0.05)。相关性分析结果显示,PE患者血清aPS/PT-IgG效价与MPV、PDW呈正相关(P<0.05),与PLT、PT、TT呈负相关(P<0.05);而aPS/PT-IgM效价与MPV、PDW、PCT、FIB、D-D呈正相关(P<0.05),与PLT、PT、APTT、TT呈负相关(P<0.05)。对影响重度PE的指标进行单因素分析,结果显示aPS/PT-IgG及aPS/PT-IgM效价、PLT、MPV、PDW、PCT、APTT、FIB、D-D等指标比较,差异有统计学意义(P<0.05)。二元Logistic回归分析结果显示,aPS/PT-IgG及aPS/PT-IgM效价、PLT、MPV、PDW、PCT、APPT为重度PE的独立影响因素。结论PE患者血清aPS/PT效价与血小板参数及凝血指标密切相关,其共同参与了PE的发生、发展,在重度PE的病情进展中起到重要作用。

抗组织因子途径抑制物单克隆抗体对血浆凝固时间的影响

观察自制抗组织因子途径抑制物单克隆抗体（ＭｃＡｂ４Ｆ８）对血浆凝血酶原时间（ＰＴ）及活化的部分凝血活酶时间（ＡＰＴＴ）的影响。结果发现：外源性的组织因子途径抑制物（ＴＦＰＩ）可使ＰＴ及ＡＰＴＴ延长。ＭｃＡｂ４Ｆ８则使稀释的ＰＴ缩短，且呈量效关系。低分子量肝素（ＬＭＷＨ）使ＰＴ及ＡＴＰＰ均明显延长，加入兔抗人抗凝血酶Ⅲ抗体则可以减弱ＬＭＷＨ的这种作用。ＭｃＡｂ４Ｆ８还可使乏因子Ⅸ血浆稀释的ＰＴ明显缩短。提示组织因子途径在正常生理条件和血友病人的血凝过程中均起重要作用。

抗磷脂酰丝氨酸-凝血酶原复合物抗体在抗磷脂综合征患者中的诊断价值

目的研究抗磷脂酰丝氨酸-凝血酶原复合物抗体(aPS/PT)在血清阴性抗磷脂综合征(SN-APS)患者中的诊断价值。方法入选2023年4月至2023年9月来河南省人民医院就诊患者,将研究对象分为健康对照组、抗磷脂综合征(APS)组和SN-APS组,采用磁微粒化学发光法检测标准抗磷脂抗体和aPS/PT,计算各抗磷脂抗体百分位值并评估aPS/PT诊断价值。结果aCL和aβ2GP I-IgA/IgM/IgG的P99分别为5.52、19.81、20.22 IU/mL和21.16、25.38、19.30 IU/mL,P97.5分别为4.77、18.89、16.35 IU/mL和20.20、16.90、18.18 IU/mL,P95分别为3.22、14.99、8.61 IU/mL和7.49、5.04、6.95 IU/mL。aPS/PT-IgM/IgG的P99分别为19.72、20.96 IU/mL,aPS/PT-IgM/IgG的P97.5分别为18.84、20.7 IU/mL,aPS/PT-IgM/IgG的P95分别为18.36、17.24 IU/mL。SN-APS组的aPS/PT-IgM水平高于健康对照组,以17.26 IU/mL为截断值时,诊断敏感性为29.73%,特异性为93.33%。结论本研究建立了实验室内部标准抗磷脂抗体和aPS/PT的参考区间,并发现aPS/PT-IgM对SN-APS患者有一定的诊断价值。