血清LRG1、TGF-β1水平与急性脑梗死颈动脉内膜中层厚度及近期预后不良的关系

目的探讨血清富亮氨酸α-2糖蛋白-1(LRG1)、转化生长因子-β1(TGF-β1)水平与急性脑梗死(ACI)颈动脉内膜中层厚度(IMT)及近期预后不良的关系。方法选取2020年1月至2023年1月在苏州市广济医院诊治的123例ACI患者,根据IMT将患者分为正常组(23例)、增厚组(30例)和斑块组(70例),另选取同期苏州市广济医院35例体检健康者作为健康对照组,比较4组血清LRG1、TGF-β1水平及IMT。随访3个月,根据预后情况将患者分为预后良好组(75例)和预后不良组(48例),采用Pearson法分析血清LRG1、TGF-β1与IMT的相关性;采用单因素和多因素Logistic回归分析ACI患者近期预后不良的危险因素;采用受试者工作特征(ROC)曲线分析血清LRG1、TGF-β1水平对ACI患者近期预后不良的预测价值。结果健康对照组、正常组、增厚组、斑块组血清LRG1水平依次升高,TGF-β1水平则依次降低(P<0.05)。Pearson相关性分析显示,血清LRG1与IMT呈正相关,TGF-β1则与IMT呈负相关(P<0.05)。预后不良组年龄、合并糖尿病患者占比、入院美国国立卫生研究院卒中量表(NIHSS)评分、低密度脂蛋白胆固醇(LDL-C)、空腹血糖(FPG)、白细胞计数(WBC)、C-反应蛋白(CRP)及血清LRG1水平均高于预后良好组(P<0.05),发病至溶栓时间长于预后良好组(P<0.05),血清TGF-β1水平则低于预后良好组(P<0.05)。多因素Logistic回归分析显示,NIHSS评分高、发病至溶栓时间长、血清LRG1水平升高及TGF-β1水平降低均是影响ACI患者近期近期预后不良的危险因素(P<0.05)。ROC曲线结果显示,血清LRG1、TGF-β1单独及联合预测ACI患者近期预后不良的曲线下面积分别为0.824、0.708、0.902。结论ACI患者存在血清LRG1水平升高、TGF-β1水平降低的情况,血清LRG1、TGF-β1水平与IMT及ACI患者近期预后密切相关,联合检测血清LRG1、TGF-β1水平对预测ACI患者近期预后不良有较高的参考价值。

康复新液联合标准化疗方案治疗肺结核的效果及对患者血清α1酸性糖蛋白和触珠蛋白水平的影响

目的探讨康复新液联合标准化疗方案(2HRZE/4HR方案)治疗肺结核的效果及对患者血清α1酸性糖蛋白和触珠蛋白水平的影响。方法选取河北省胸科医院2019年1月至2021年4月收治的188例肺结核患者。根据随机数字表法分为对照组和观察组,各94例。对照组给予2HRZE/4HR标准化疗方案及西药抗感染、止血、止咳化痰治疗,观察组在对照组基础上联合康复新液口服治疗,2组均连续治疗6个月。比较2组患者痰菌阴转率和CT病灶吸收、空洞变化、咯血症状缓解、不良反应发生情况,比较2组肺功能和炎症因子、T淋巴细胞亚群、血清α1酸性糖蛋白和触珠蛋白水平的变化。结果治疗2、5、6个月后观察组患者痰菌阴转率均高于对照组[83.0%(78/94)比69.2%(65/94)、93.6%(88/94)比83.0%(78/94)、97.9%(92/94)比88.3%(83/94)],差异均有统计学意义(均P<0.05)。治疗2及6个月后观察组的病灶吸收总有效率、空洞改善总有效率及治疗2个月后咯血症状缓解总有效率均高于对照组,治疗期间观察组不良反应总发生率低于对照组,治疗后观察组肺功能指标及炎症因子、T淋巴细胞亚群改善情况优于对照组,差异均有统计学意义(均P<0.05)。治疗后2组血清α1酸性糖蛋白和触珠蛋白水平均高于治疗前、且观察组高于对照组[(786±105)mg/L比(713±105)mg/L、(0.91±0.22)g/L比(0.78±0.21)g/L],差异均有统计学意义(均P<0.05)。结论康复新液联合标准化疗方案(2HRZE/4HR方案)治疗肺结核效果较好,不良反应发生率较低,同时可提高血清α1酸性糖蛋白和触珠蛋白水平。

血清LRG1、SDF-1联合检测对早期胃癌内镜黏膜下剥离术后复发的预测价值

目的探讨血清富亮氨酸α-2糖蛋白-1(LRG1)、基质细胞衍生因子-1(SDF-1)联合检测对早期胃癌患者内镜黏膜下剥离术(ESD)术后复发的预测价值。方法选取2018年1月至2021年10月在该院行ESD的317例早期胃癌患者作为研究对象,根据术后复查情况,分为复发组(32例)和未复发组(285例)。采用酶联免疫吸附试验检测血清LRG1和SDF-1水平,Pearson法分析ESD术后复发患者血清LRG1、SDF-1水平的相关性;采用Logistic回归分析影响早期胃癌患者ESD术后复发的因素;绘制受试者工作特征(ROC)曲线评估血清LRG1和SDF-1水平对早期胃癌患者ESD术后复发的预测价值。结果与未复发组相比,复发组血清LRG1和SDF-1水平均显著升高(P<0.05);复发组发生淋巴结转移的患者比例高于未复发组(P<0.05);ESD术后复发患者血清LRG1和SDF-1水平呈正相关(r=0.962,P<0.05);淋巴结转移、LRG1和SDF-1均为早期胃癌患者ESD术后复发的影响因素(P<0.05);血清LRG1和SDF-1联合预测早期胃癌患者ESD术后复发的曲线下面积(AUC)为0.936,优于血清LRG1和SDF-1各自单独预测(P<0.05)。结论血清LRG1和SDF-1水平与早期胃癌患者ESD术后复发密切相关,二者联合检测对早期胃癌患者ESD术后复发具有较好的预测价值。

脑梗死患者血清抗β2-糖蛋白1抗体水平变化与颈动脉粥样硬化的相关性

目的探讨脑梗死患者血清抗β2-糖蛋白1(β2-GP1)抗体水平与颈动脉粥样硬化(CAS)斑块及其危险因素的相关性。方法选取303例前循环脑梗死患者,应用血管多普勒超声仪进行颈部血管超声检测,根据有无CAS斑块及狭窄程度将患者分为三组,其中无斑块无狭窄组79例,有斑块无狭窄组98例,有斑块有狭窄组126例,有斑块有狭窄组中1级狭窄41例,2级狭窄34例,3级狭窄30例,4级狭窄21例。采用ELISA检测患者血清抗β2-GP1抗体水平,用酶法测量血糖、甘油三酯及总胆固醇水平,用直接法测量血清低密度脂蛋白胆固醇(LDLC)及高密度脂蛋白胆固醇(HDLC)水平。结果无斑块无狭窄组、有斑块无狭窄组、有斑块有狭窄组患者血清抗β2-GP1抗体水平分别为16.02±16.23 kRU/L、21.43±16.15 kRU/L、34.89±19.15 kRU/L;有斑块无狭窄组、有斑块有狭窄组患者血清抗β2-GP1抗体水平明显高于无斑块无狭窄组(P<0.05或P<0.01),有斑块有狭窄组患者血清抗β2-GP1抗体水平明显高于有斑块无狭窄组(P<0.01);血清抗β2-GP1抗体水平随CAS狭窄程度的增加而增高。Logistic回归分析显示,抗β2-GP1抗体水平与LDLC水平密切相关。结论血清抗β2-GP1抗体参与动脉粥样硬化的形成、发展,LDLC是血清抗β2-GP1抗体增高的独立危险因素,血清抗β2-GP1抗体可作为CAS的血清生化指标之一。

抗α-1酸性糖蛋白血清的制备

作者用分离纯化的α-1酸性糖蛋白免疫新西兰兔,制备抗α-1酸性糖蛋白血清。鉴定结果表明,制备的抗血清与进口商品抗α-1酸性糖蛋白血清特异性相同;与人血清其他蛋白无交叉反应。琼脂双向扩散法测得抗血清效价为128,检出α-1酸性糖蛋白的最低浓度为204μg/ml。

川崎病患儿血清总IgE、富亮氨酸α-2糖蛋白升高与冠状动脉病变的发生率、预后的相关性及影响因素分析

目的探究川崎病患儿血清总免疫球蛋白IgE(Immunoglobulin,IgE)、富亮氨酸α-2糖蛋白1(Leucine-richα-2 Glycoprotein-1,LRG1)升高与冠状动脉病变的发生率及预后相关性,并就川崎病患儿出现冠状动脉病变的危险因素开展分析。方法选择2020年1月—2022年12月本院儿童医院确诊为川崎病的127例患儿为研究对象,根据切面超声心动图对冠状动脉检测结果分为冠脉病变组(n=60)和无冠脉病变组(n=67)两组。比较两组患儿IgE、LRG1水平差异,对入组患者开展积极的治疗后,比较治疗前后入组患儿IgE、LRG1水平变化,最后分析导致川崎病患儿出现冠状动脉病变的危险因素。结果冠脉病变组患儿血清IgE、LRG1水平均明显高于无冠脉病变组患儿,差异具有统计学意义(P<0.05);治疗后入组川崎病患儿的血清IgE、LRG1水平均出现了明显的降低,差异具有统计学意义(P<0.05);通过非条件多因素Logistic回归分析显示,发热持续时间、CRP水平过高、IgE水平过高和LRG1水平过高是导致川崎病患儿出现冠状动脉损伤的独立危险因素,差异具有统计学意义(P<0.05)。结论川崎病患儿出现冠状动脉损伤几率较高,患儿血清IgE、LRG1水平会出现异常升高;发热持续时间、CRP水平过高、IgE水平过高和LRG1水平过高是导致川崎病患儿出现冠状动脉损伤的独立危险因素,对出现上述危险因素的川崎病患儿,建议加强干预,以改善其预后。

Orosomucoid in liver diseases

In this editorial,the roles of orosomucoid(ORM)in the diagnoses and follow-up assessments of both nonneoplastic diseases and liver tumors are discussed with respect to the publication by Zhu et al presented in the previous issue of World Journal of Gastroenterology(2020;26(8):840-817).ORM,or alpha-1 acid glycoprotein(AGP),is an acute-phase protein that constitutes 1%to 3%of plasma proteins in humans and is mainly synthesized in the liver.ORM exists in serum as two variants:ORM1 and ORM2.Although the variants share 89.6%sequence identity and have similar biological properties,ORM1 constitutes the main component of serum ORM.An interesting feature of ORM is that its biological effects differ according to variations in glycosylation patterns.This variable feature makes ORM an attractive target for diagnosing and monitoring many diseases,including those of the liver.Recent findings suggest that a sharp decrease in ORM level is an important marker for HBV-associated acute liver failure(ALF),and ORM1 plays an important role in liver regeneration.In viral hepatitis,increases in both ORM and its fucosylated forms and the correlation of these increases with fibrosis progression suggest that this glycoprotein can be used with other markers as a noninvasive method in the follow-up assessment of diseases.In addition,similar findings regarding the level of the asialylated form of ORM,called asialo-AGP(AsAGP),have been reported in a follow-up assessment of fibrosis in chronic liver disease.An increase in ORM in serum has also been shown to improve hepatocellular carcinoma(HCC)diagnosis performance when combined with other markers.In addition,determination of the ORM level has been useful in the diagnosis of HCC with AFP concentrations less than 500 ng/mL.For monitoring patients with AFP-negative HCC,a unique trifucosylated tetra-antennary glycan of ORM may also be used as a new potential marker.The fact that there are very few studies investigating the expression of this glycoprotein and its variants in liver tissues constitutes a potential limitation,especially in terms of revealing all the effects of ORM on carcinogenesis and tumor behavior.Current findings indicate that ORM2 expression is decreased in tumors,and this is related to the aggressive course of the disease.Parallel to this finding,in HCC cell lines,ORM2 decreases HCC cell migration and invasion,supporting reports of its tumor suppressor role.In conclusion,the levels of ORM and its different glycosylated variants are promising additional biomarkers for identifying ALF,for monitoring fibrosis in viral hepatitis,and for diagnosing early HCC.Although there is evidence that the loss of ORM2 expression in HCC is associated with poor prognosis,further studies are needed to support these findings.Additionally,investigations of ORM expression in borderline dysplastic nodules and hepatocellular adenomas,which pose diagnostic problems in the differential diagnosis of HCC,especially in biopsy samples,may shed light on whether ORM can be used in histopathological differential diagnosis.