Downregulation of orosomucoid 2 acts as a prognostic factor associated with cancer-promoting pathways in liver cancer

BACKGROUND Liver cancer has a high mortality and morbidity rate throughout the world.In clinical practice,the prognosis of liver cancer patients is poor,and the complex reasons contribute to treatment failures,including fibrosis,hepatitis viral infection,drug resistance and metastasis.Thus,screening novel prognostic biomarkers is of great importance for guiding liver cancer therapy.Orosomucoid genes(ORMs)encode acute phase plasma proteins,including orosomucoid 1(ORM1)and ORM2.Previous studies showed their upregulation upon inflammation,but the specific function of ORMs has not yet been determined,especially in the development of liver cancer.AIM To determine the expression of ORMs and their potential function in liver cancer.METHODS Analysis of the expression of ORMs in different human tissues was performed on data from the HPA RNA-seq normal tissues project.The expression ratio of ORMs was determined using the HCCDB database,including the ratio between liver cancer and other cancers,normal liver and other normal tissues,liver cancer and adjacent normal liver tissues.Analysis of ORM expression in different cancer types was performed using The Cancer Genome Atlas and TIMER database.The expression of ORMs in liver tumor tissues and adjacent normal tissues were further confirmed using Gene Expression Omnibus data,including GSE36376 and GSE14520.The 10-year overall survival(OS),progression-free survival(PFS)and relapse-free survival(RFS)rates between high and low ORM expression groups in liver cancer patients were determined using the Kaplan-Meier plotter tool.Gene Set Enrichment Analysis(GSEA)was employed to explore the ORM2-associated signaling network.Correlations between ORM2 expression and tumor purity or the infiltration level of macrophages in liver tumor tissues were determined using the TIMER database.The correlation between ORM2 gene levels,tumor-associated macrophage(TAM)markers(including CD68 and TGFβ1)and T cell immunosuppression(including CTLA4 and PD-1)in liver tumor tissues and liver GTEx was determined using the GEPIA database.RESULTS ORM1 and ORM2 were highly expressed in normal liver and liver tumor tissues.ORM1 and ORM2 expression was significantly decreased in liver tumor tissues compared with adjacent normal tissues,and similar results were also noted in cholangiocarcinoma,esophageal carcinoma,and lung squamous cell carcinoma.Further analysis of the Gene Expression Omnibus Database also confirmed the downregulation of ORM1 and ORM2 in liver tumors.Survival analysis showed that the high ORM2 group had better survival rates in OS,PFS and RFS.ORM1 only represented better performance in PFS,but not in OS or RFS.GSEA analysis of ORM2 from The Cancer Genome Atlas liver cancer data identified that ORM2 positively associated with the G2/M checkpoint,E2F target signaling,as well as Wnt/β-catenin and Hedgehog signaling.Moreover,apoptosis,IFN-αresponses,IFN-γresponses and humoral immune responses were upregulated in the ORM2 high group.ORM2 expression was negatively correlated with the macrophage infiltration level,CD68,TGFβ1,CTLA4 and PD-1 levels.CONCLUSION The results showed that ORM1 and ORM2 were highly expressed specifically in liver tissues,whereas ORM1 and ORM2 were downregulated in liver tumor tissues.ORM2 is a better prognostic factor for liver cancer.Furthermore,ORM2 is closely associated with cancer-promoting pathways.

Estrogen weakens muscle endurance via estrogen receptor-MAPK mediated orosomucoid suppression

Gender differences in fatigue,manifesting as female more prone to feel exhausted with lower muscle endurance,still remains unclear mechanism.Here,we investigated whether orosomucoid,an endogenous anti-fatigue protein which can enhance muscle endurance,is involved in this regulation.Female rats showed lower muscle endurance,and this gender difference was disappeared in orosomucoid 1-deficient mice.Female rats also displayed weaker orosomucoid induction in serum,liver and muscle in response to fatigue when compared to male ones.Ovariectomy in female rats results in elevated orosomucoid level and increased swimming time which was reversed by estrogen replenishment,while exogenous estrogen treatment both in male or female mice produced opposite effects.In vitro C2C12 muscle and Chang liver cells,estrogen decreased orosomucoid expression and its promoter activity,and this effect was abolished when estrogen receptor or MAPK was blocked.Thus,estrogen negatively regulates orosomucoid expression,which is responsible for the weaker muscle endurance in females.

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.

Regulation of cytokine gene expression by orosomucoid in neonatal swine adipose tissue

Background： Porcine adipose tissue expresses orosomucoid（ORM1） mRNA, a protein with anti-inflammatory and immunomodulatory properties. Previous research has demonstrated that porcine ORM1 can reduce insulin stimulated glucose metabolism in porcine adipose tissue in vitro. The present study was designed to examine the preweaning ontogeny of ORM1 m RNA abundance in porcine subcutaneous adipose and to determine if ORM1 can regulate m RNA abundance of inflammatory cytokines that contribute to insulin resistance in primary cultures derived from neonatal porcine subcutaneous adipose tissue. Cultures were differentiated in vitro and subsequently the adipocyte containing cultures were incubated for 24 h with 0–5000 ng porcine ORM1/m L medium. Cultures were then harvested, total RNA extracted for use in reverse transcription and the m RNA abundance of cytokine m RNA quantified by real-time PCR.Results： ORM1 m RNA abundance within neonatal adipose tissue does not change from d 1 to d 21 of age and is a very small fraction relative to liver m RNA abundance. The ORM1 m RNA level in porcine adipocytes and stromalvascular cells are similar（P 〉 0.05）. Treatment with ORM1 did not affect TNFα（tumor necrosis factor α） m RNA level（P 〉 0.05）, while interleukin 6（IL6） m RNA abundance was reduced 32 % at 1,000 ng ORM1/m L（P 〈 0.01）. However,TNFα protein content in the cell culture media was reduced by ORM1 treatment（5,000 ng/m L, P 〈 0.05）, whereas ORM1 had no detectable effect on the media content of IL6（P 〉 0.05）. The reduction of macrophage migration inhibitory factor（MIF） m RNA abundance by ORM1 was dose dependent（P 〈 0.01）. Monocyte chemotactic protein（MCP） m RNA level was reduced 27 % by 1,000 ng ORM1/m L（P 〈 0.05）.Conclusions： The data suggest that ORM1 has limited effects TNFα, IL6, MIF or MCP expression at the concentrations tested. Secondly, these cytokines do not appear to contribute to the reported insulin resistance induced by ORM1 in porcine adipose tissue in vitro as an increase in the abundance of these inflammatory cytokines would be predicted during an insulin resistant state.

血清ORMDL3结合FeNO对哮喘稳定期急性发作的预测分析

目的 分析血清类黏蛋白1样蛋白3(ORMDL3)结合呼出气一氧化氮(FeNO)对哮喘稳定期急性发作的预测价值。方法 选择2018年7月—2023年8月在本院门诊随访的120例哮喘稳定期患者作为疾病组,另同期选取120名健康体检者作为对照组,检测两组ORMDL3 mRNA表达量和FeNO浓度。依据疾病组3个月内是否出现哮喘急性发作将其分为急性发作组和非急性发作组,比较两组患者ORMDL3 mRNA表达量和FeNO浓度,采用多因素Logistic回归分析哮喘稳定期急性发作的影响因素,采用受试者工作特征(ROC)曲线分析ORMDL3 mRNA、FeNO单项及联合对哮喘稳定期急性发作的预测价值。结果 疾病组ORMDL3 mRNA表达量、FeNO浓度均高于对照组(P<0.05);急性发作组ORMDL3 mRNA表达量、FeNO浓度、体质量指数(BMI)以及吸烟史占比均高于非急性发作组(P<0.05),淋巴细胞计数、用力肺活量占预计值百分比(FVC%)、第一秒用力呼气末容积占预计值百分比(FEV1%)低于非急性发作组(P<0.05);经多因素Logistic回归分析显示,高ORMDL3 mRNA、高FeNO、高BMI均为哮喘稳定期患者急性发作的危险因素(P<0.05),高FVC%、高FEVI%为其保护因素(P<0.05)。ORMDL3 mRNA、FeNO联合预测哮喘稳定期患者急性发作的灵敏度高于单独预测,联合预测的AUC高于单独预测(P<0.05),联合预测的特异度与单独预测相近。结论 ORMDL3、FeNO均在哮喘稳定期急性发作患者中存在异常高表达,均是哮喘稳定期急性发作的影响因素,且两者联合对哮喘稳定期急性发作具有较好的预测价值。

99例哮喘儿童ORMDL3基因多态性及其与血清IgE水平的关联性

目的探讨血清类黏蛋白1样蛋白3(ORMDL3)基因多态性与儿童哮喘易感性及与血清免疫球蛋白E(IgE)水平的关系。方法选取首诊哮喘的患儿99例为哮喘组,另选取同期健康儿童51例为对照组;采用PCR-Sanger测序对ORMDL3基因rs7216389位点进行基因分型,散射比浊法测定血清IgE水平,比较rs7216389基因型在两组间的分布差异,采用共显性、显性和隐性3种遗传模型分析血清IgE水平。结果rs7216389位点哮喘组TC、TT基因型频率高于对照组(P<0.05),相比CC基因型,TT、TC基因型儿童患哮喘的风险分别增加7.500倍、8.094倍(P<0.05);哮喘组共显性遗传模型TT基因型的IgE水平高于TC基因型(P<0.05);隐性遗传模型TT基因型的IgE水平高于CC+TC基因型(P<0.05);哮喘组显性遗传模型、对照组3种遗传模型IgE比较,差异均无统计学意义(P>0.05)。结论ORMDL3 rs7216389多态性可能与儿童哮喘患病风险有关,TC、TT基因型可能是儿童哮喘患病的风险因子;哮喘儿童rs7216389位点的基因型与血清IgE水平有关。

PCT、CRP、AAG与老年COPD患者下呼吸道感染的相关性分析

【目的】探讨C反应蛋白(c-reaetive protein,CRP)、降钙素原(Procalcitonin,PCT)、α1-酸性糖蛋白(αl acid glycoprotein,AAG)与老年COPD患者下呼吸道感染的相关性。【方法】回顾性分析本院2018年1月至2021年12月收治的84例老年COPD患者的临床资料,分析患者下呼吸道感染情况,统计患者年龄、性别、体重指数(BMI)、合并疾病、血脂指标、慢性阻塞性肺病防治(GOLD)分级、凝血指标及PCT、CRP、AAG水平等一般资料;采用多因素Logistic回归分析影响老年COPD患者下呼吸道感染的独立危险因素;采用Spearman检验分析PCT、CRP、AAG与老年COPD患者下呼吸道感染的相关性。【结果】84例老年COPD患者中,有50例(59.52%)患者无下呼吸道感染,纳为未感染组;有34例(40.48%)患者伴下呼吸道感染,纳为感染组。两组年龄、性别、合并疾病、血脂指标、BMI、凝血指标、GOLD分级、吸烟史、病程比较,差异无统计学意义(P>0.05);感染组PCT、CRP、AAG水平均高于未感染组(P<0.05)。多因素Logistic回归分析显示:CRP、PCT、AAG是影响老年COPD患者下呼吸道感染的独立危险因素(P<0.05)。Spearman检验结果显示:血清PCT、CRP、AAG水平与老年COPD患者下呼吸道感染呈正相关(P<0.05)。【结论】PCT、CRP、AAG是影响老年COPD患者下呼吸道感染的危险因素,随着PCT、CRP、AAG水平升高,老年COPD患者发生下呼吸道感染的风险也相应增加。

类粘蛋白的遗传多态性对奎尼丁游离药物浓度与蛋白结合率的影响

目的：探讨类粘蛋白（ｏｒｏｓｏｍｕｃｏｉｄ，ＯＲＭ）表型对弱碱性药物奎尼丁血清游离浓度和蛋白结合率的影响。方法：对健康受试者的去唾液酸血清ＯＲＭ用等电聚焦电泳、免疫印迹法进行表型分型。ＯＲＭ１的３种表型分别为纯合子ＯＲＭ１Ｆ１（ｎ＝１０）， ＯＲＭ１Ｓ（ｎ＝８），和杂合子ＯＲＭ１ Ｆ１Ｓ（ｎ＝１０）。受试者口服单剂量的硫酸奎尼丁片２００ｍｇ，测定服药后不同时间血清奎尼丁总浓度（ＲＰ－ＨＰＬＣ）和游离浓度（微超滤离心／ＲＰ－ＨＰＬＣ）。结果：给药后２４ｈ内，３组不同ＯＲＭ１表型者奎尼丁血清总浓度的经时过程、血浆 ｔ１／２、 Ｃｍａｘ和ｔｍａｘ值相似。但ＯＲＭＩ Ｆ１表型组的奎尼丁游离浓度高于ＯＲＭ１Ｓ和ＯＲＭ１ Ｆ１Ｓ表型组，而其蛋自结合率（８０．２１±６．１３Ｔ）却明显低于ＯＲＭ１Ｓ（８９．３１±４．８３％）（Ｐ＜０．０１）和ＯＲＭ１ Ｆ１Ｓ（８７．２６±３．４２％）（Ｐ＜０．０１）表型者；奎尼丁游离药物分数则分别为 ＯＲＭ１ Ｆ１：１９．７９％，ＯＲＭ１ Ｓ １０．６９％和ＯＲＭ１ Ｆ１Ｓ １２．７４％（Ｐ＜０．０１）。结论：不同ＯＲＭ１表型明显影响弱碱性药物奎尼丁的血清游离药物浓度和蛋白结合率； ＯＲＭ１ Ｆ１表?

<3岁反复喘息患儿外周血血清ORMDL3基因在不同临床表型中的表达及其与IL-17和ECP的关系

目的探讨<3岁反复喘息患儿外周血血清类黏蛋白1样蛋白3(ORMDL3)基因在不同临床表型中的表达及其与血清白介素-17(IL-17)和嗜酸性细胞阳离子蛋白(ECP)的关系。方法选取该院儿科就诊<3岁反复哮喘的患儿87例,根据患儿是否存在高危因素分成特应性哮喘组(64例)和非特应性哮喘组(23例),再选取同期在儿科体检的健康儿童30例。分析3组研究对象ORMDL3基因表达水平、血清IL-17和ECP含量和ORMDL3基因频率分布的差异,并对3组研究对象ORMDL3基因表达水平和血清IL-17和ECP含量的相关性进行分析。结果特应性哮喘组ORMDL3基因表达水平(11.57±1.96)%,血清IL-17(1 354.46±873.48)pg/ml和血清ECP(45.65±12.76)μg/L均高于非特应性哮喘组和对照组(P=0.000);3组的ORMDL3基因AA、AG和GG 3种基因型的频率分布差异有统计学意义(χ~2=12.84,P=0.012)。特应性哮喘组的ORMDL3基因表达水平与血清IL-17(r=0.318,P=0.000)、血清ECP(r=0.540,P=0.000)均呈正相关。结论不同临床类型的哮喘患儿血清中的ORMDL3基因表达水平、IL-17和ECP含量不同。特应性哮喘患儿的血清ORMDL3基因表达水平与血清IL-17、ECP含量存在正相关性。

类粘蛋白的遗传表型对阿米替林血浆游离型药物浓度和蛋白结合率的影响

目的：探讨类粘蛋白(orosomucoid, ORM)表型对弱碱性药物阿米替林血浆游离浓度和蛋白结合率的影响. 方法：对28名健康受试者的去唾液酸血清ORM用等电聚焦电泳、免疫印迹法进行表型分型.ORM1的三种表型分别为纯合子ORM1 F1 (n=10)、ORM1 S (n=8)和杂合子ORM1 F1S(n=10).受试者口服单剂量的硫酸阿米替林片50 mg,测定服药后不同时间血浆阿米替林总浓度(RP-HPLC)和游离浓度(微超滤离心/RP-HPLC). 结果：给药后12和24 h,三组不同ORM1表型者阿米替林血浆总浓度的经时过程、血浆t1/2、Cmax和tmax值相似.与ORM1 S表型组比较,ORM1 F1表型组的阿米替林游离浓度较高；而蛋白结合率较低,12 h为(82.77±4.05)%,24 h为(79.99±4.39)% (P<0.01).杂合子ORM1 F1S表型组的游离药物浓度和蛋白结合率介于两组纯合子表型之间. 结论：不同ORM1表型,将明显影响弱碱性药物阿米替林的血清游离药物浓度和蛋白结合率；ORM1 F1表型者药物的血浆蛋白结合率最低,而游离型药物浓度最高.临床用药中应予以注意,并适当调整给药剂量.

血清类黏蛋白1样蛋白3表达与5岁以下儿童喘息的相关性分析

目的探讨血清类黏蛋白1样蛋白3(ORMDL3)基因表达量与5岁以下儿童喘息的相关性。方法选取2013年8月—2014年12月在上海交通大学医学院附属仁济医院南院儿科就诊的89例5岁以下喘息患儿,依据哮喘预测指数(API)严格标准分为API^+(过去1年内喘息次数≥4)组(n=42)和API-(过去1年内喘息次数1~3次)组(n=47);另设API0(5岁以下健康儿童)对照组(n=51)。检测3组血清ORMDL3基因表达量,分析血清ORMDL3表达水平与API、喘息、鼻炎、总免疫球蛋白E(TIg E)、家族史、湿疹、年龄、尘螨等吸入性过敏原及牛奶等摄入性过敏原的相关性。结果 API^+组患者血清ORMDL3表达水平显著高于API-和API0组。ORMDL3表达水平与API(r=0.405,P=0.000)、喘息(r=0.492,P=0.000)、湿疹(r=0.454,P=0.000)、户尘螨(r=0.298,P=0.000)、狗毛皮屑(r=0.251,P=0.000)和TIg E(r=0.170,P=0.002)存在正相关;与性别、家族史、鼻炎、年龄、屋尘螨、猫毛皮屑、树木、点青/分枝/烟曲/黑曲/交链霉及饮食因素(牛奶、鸡蛋白、牛肉、腰果、蟹、虾)不存在相关性(P>0.05)。结论 ORMDL3基因表达量与儿童API之间呈正相关,提示ORMDL3表达量与API相结合可作为诊断5岁以下儿童哮喘的诊断依据之一。

血清类黏蛋白的功能和临床意义

类黏蛋白(ORM)属于急性时相反应蛋白,机体许多组织和细胞均能合成,但主要的合成器官是肝脏。ORM能够调节参与天然免疫和获得性免疫的多种细胞,平衡机体的能量代谢,并具有抗疲劳作用。许多组织损伤均可诱导细胞及血中的ORM升高。在感染和创伤的过程中,血中ORM水平在炎症的多个阶段均持续升高。因此,监测血中ORM水平能够与C反应蛋白(CRP)互补,反映炎症性疾病的持续、进展和消退情况,从而为精准治疗提供新的线索。文章从ORM的结构特征、生物功能以及检测ORM的临床意义等方面对ORM进行综合性的阐述。

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。

川芎嗪对支气管上皮细胞ORMDL3表达影响

目的探讨川芎嗪对哮喘易感基因血清类黏蛋白1样蛋白3(ORMDL3)表达的影响。方法应用IL-4+IL-13刺激人支气管上皮(HBE)细胞ORMDL3过表达,以不同浓度的川芎嗪(200、300、400、500、600、700、800μg/L)干预72 h,选取干预作用最明显的川芎嗪浓度。以IL-4+IL-13培养的HBE细胞作为模型组,以干预作用最明显的川芎嗪浓度干预IL-4+IL-13培养HBE细胞作为治疗组,PBS培养HBE细胞作为空白组。应用RT-PCR方法分别检测3组ORMDL3 mRNA表达,Western blot方法、免疫组化法检测ORMDL3蛋白表达。结果400μg/L浓度的川芎嗪干预作用最明显。治疗组、空白组、模型组ORMDL3 mRNA表达比较差异有显著性(F=176.45,P<0.01),治疗组表达最低。模型组、治疗组ORMDL3蛋白表达较空白组升高,治疗组较模型组降低,差异有统计学意义(F=23.48、91.56,P<0.01)。结论川芎嗪可通过下调HBE细胞ORMDL3基因表达,改善哮喘病人气道重塑。

Evaluation of IFIT3 and ORM1 as Biomarkers for Discriminating Active Tuberculosis from Latent Infection

Objective Current commercially available immunological tests cannot be used for discriminating active tuberculosis(TB)from latent TB infection.To evaluate the value of biomarker candidates in the diagnosis of active TB,this study aimed to identify differentially expressed genes in peripheral blood mononuclear cells(PBMCs)between patients with active TB and individuals with latent TB infection by transcriptome sequencing.Methods The differentially expressed genes in unstimulated PBMCs and in Mycobacterium tuberculosis(Mtb)antigen-stimulated PBMCs from patients with active TB and individuals with latent TB infection were identified by transcriptome sequencing.Selected candidate genes were evaluated in cohorts consisting of 110 patients with TB,30 individuals with latent TB infections,and 50 healthy controls by quantitative real-time RT-PCR.Receiver operating characteristic(ROC)curve analysis was performed to calculate the diagnostic value of the biomarker candidates.Results Among the differentially expressed genes in PBMCs without Mtb antigen stimulation,interferon-induced protein with tetratricopeptide repeats 3(IFIT3)had the highest area under curve(AUC)value(0.918,95%CI:0.852-0.984,P<0.0001)in discriminating patients with active TB from individuals with latent TB infection,with a sensitivity of 91.86%and a specificity of 84.00%.In Mtb antigen-stimulated PBMCs,orosomucoid 1(ORM1)had a high AUC value(0.833,95%CI:0.752-0.915,P<0.0001),with a sensitivity of 81.94%and a specificity of 70.00%.Conclusion IFIT3 and ORM1 might be potential biomarkers for discriminating active TB from latent TB infection.

甘露聚糖、壳聚糖、α-酸性糖蛋白和姜黄素对脂蛋白(a)和去唾液酸脂蛋白(a)代谢影响的对比分析

分析多糖和姜黄素对脂蛋白 (a)和去唾液酸脂蛋白 (a)代谢的影响 ,从刺猬腋下静脉注入甘露聚糖、壳聚糖、α -酸性糖蛋白和姜黄素 ,2min后注射12 5I-脂蛋白 (a)或12 5I-去唾液酸脂蛋白 (a) ,1h后处死动物 ,测定血、肝、肾、脾、胆汁和肾上腺的同位素含量。结果发现 ,脂蛋白 (a)去唾液酸后能大量进入肝脏 ,加速在体内的分解代谢 ,使血中浓度迅速降低。α -酸性糖蛋白抑制组织对脂蛋白 (a)和去唾液酸脂蛋白 (a)的摄入 ,使血中脂蛋白 (a)和去唾液酸脂蛋白 (a)含量显著增高。壳聚糖和姜黄素增加肝脏和肾上腺对脂蛋白 (a)的摄取 ,使血中脂蛋白 (a)含量略降低 ,但对去唾液酸脂蛋白 (a)代谢无明显影响。甘露聚糖增加脾脏对脂蛋白 (a)的摄取 ,减少胆囊中脂蛋白 (a)含量 ,但增加肾脏和胆囊对去唾液酸脂蛋白 (a)的摄取 ,降低肾上腺对去唾液酸脂蛋白 (a)的摄取。结果提示 ,脂蛋白 (a)去唾液酸后能使脂蛋白 (a)分解代谢加快 ,脂蛋白 (a)分子中的唾液酸在结构稳定中起重要的作用。α -酸性糖蛋白抑制脂蛋白 (a)和去唾液酸脂蛋白 (a)代谢 ,而壳聚糖和姜黄素则促进脂蛋白 (a)

辽宁汉族人血清类粘蛋白(ORM)型的分布及其在血痕精液(斑)及脑脊液中的检出

本文作者采用PAGIEF结合免疫固定法,调查了辽宁汉族群体(431人)ORM的分布,检出了ORM1型和ORM2型各8种表现型;对不同条件下的血痕标本进行检测,成功地检出了37℃保存2年血痕的ORM1型;首次由脑脊髓液中检出了ORM1型。ORM型的总鉴别机率为0.7043,是进行个人识别和亲子鉴定的良好遗传标记。

α-1酸性糖蛋白的分离纯化

本文报道α-1酸性糖蛋白的分离纯化。人血清经DEAE-Sephadex-A50和ReactiveBlue 2-Sepharose CL-6B两次柱层析即可获得纯化的α-1酸性糖蛋白。纯化产物经聚丙烯酰胺凝胶电泳、SDS-聚丙烯酰胺梯度凝胶电泳、免疫电泳和琼脂双向扩散等证明,其纯度和特异性均符合要求。

血液病患者血、尿酸溶性蛋白检测的临床意义

用过氯酸—考马氏亮蓝比色法对114例血液病患者的血清及尿液酸溶性蛋白含量进行检测.白血病、多发性骨髓瘤、淋巴瘤病人血清及尿液酸溶性蛋白含量明显高于非肿瘤性血液病患者及正常对照组(P<0.01);血清酸溶性蛋白含量与白血病患者外周血幼稚细胞绝对值呈显著正相关(r=0.5571,P<0.01);各类白血病患者血清和尿液酸溶性蛋白含量以急性淋巴细胞性白血病最高,慢性粒细胞性白血病最低(t=4.150,P<0.01).提示血清和尿液酸溶性蛋白测定对鉴别肿瘤与非肿瘤性血液病、白血病的类型有着重要的参考意义.

糖尿病患者血清酸性糖蛋白测定的意义

本文报告36例糖尿病患者血清α_1-酸性糖蛋白的测定结果,糖尿病患者明显增高,且以糖尿病并酮症及糖尿病性肾病者更为明显。其α_1酸性糖蛋白含量与血糖值和血胆固醇浓度无相关性。提示检测α_1酸性糖蛋白对糖尿病有诊断意义,并对糖尿病是否并酮症、肾功能损害有鉴别诊断意义。