Construction and Analysis of Three-dimensional Graphic Model of Single-chain Fv Derived from an Anti-human Placental Acidic Isoferritin Monoclonal Antibody by Computer

Summary: A three-dimensional (3D) graphic model of a single-chain Fv (scFv) which was derived from an anti-human placental acidic isoferritin (PAF) monoclonal antibody (MAb) was construct- ed by a homologous protein-predicting computer algorithm on Silicon graphic computer station. The structure, surface static electricity and hydrophobicity of scFv were investigated. Computer graphic modelling indicated that all regions of scFv including the linker, variable regions of the heavy (VH) and light (VL) chains were suitable. The VH region and the VL region were involved in composing the 'hydrophobic pocket'. The linker was drifted away VH and VL regions. The complementarity determining regions (CDRs) of VH and VL regions surrounded the 'hydrophobic pocket'. This study provides a theory basis for improving antibody affinity, investigating antibody structure and analyzing the functions of VH and VL regions in antibody activity.

Placental Isoferritin Action in Pathogenesis of Pre-eclampsia and/or Intrauterine Growth Retardation and Its Earlier Predictive Value

In order to investigate the role of placental isoferritin (PLF) in pathogenesis of pre-eclampsia and/or intrauterine growth retardation (IUGR) and its earlier predictive value, a prospective double-blinded study was performed. In 120 initial normal pregnant women at earlier third trimester (from 24 to 34 weeks), plasma placental isoferritin and nitric oxide (NO) metabolites (nitrite/nitrate) (NO 2 -/NO 3 -) were examined by using ELISA and Criess assay respectively. The outcome of pregnancies and birth weight of their infants were followed up. The receiver operating characteristic curves (ROC) and predictive values of PLF predicting the outcome of pregnancy with IUGR, pre-eclampsia were analyzed. Results showed that in 120 initial normal pregnant women, IUGR occurred in 15 pregnant women (IUGR group) and pre-eclampsia in 19 (pre-eclampsia group), and the remaining 86 had normal pregnancy (normal group). The levels of plasma placental isoferritin were significantly decreased in IUGR group (260.01±58.95) μg/ml and pre-eclampsia group (285.31±53.73) μg/ml as compared with those in normal group (775.62±89.32) μg/ml at earlier third trimester (both P<0.01). The levels of plasma NO were significantly increased in IUGR group (61.57±46.22) μmol/L and pre-eclampsia group (58.37±30.52) μmol/L as compared with those in the normal group (35.29±24.46) μmol/L (both P<0.01). There was no significant difference in plasma placental isoferritin and NO levels between IUGR group and pre-eclampsic group (both P>0 05). The plasma placental isoferritin was negatively correlated with NO levels (r=0.329,P<0 01). The areas under ROC of PLF predicting IUGR and pre-eclampsia were 0.977 and 0.905 respectively. At the cut point of 400 μg/ml PLF level, the sensitivity, specificity, positive predictive value, negative predictive value and Kappa index of PLF levels predicting the outcome of pregnancy with pre-eclampsia were 100 %, 85.15 %, 55.88 %, 100 % and 0.645 respectively. At the cut point of 390 μg/ml PLF level, the sensitivity, specificity, positive predictive value, negative predictive value and Kappa index of PLF levels predicting the outcome of pregnancy with IUGR were 100 %, 81.9 %, 44.12 %, 100 % and 0.663 respectively. It was concluded that the decrease of plasma placental isoferritin levels at earlier third trimester was associated with IUGR and/or pre-eclampsia, and the endothelial cell damage may be one of its mechanisms. The plasma PLF level can be used as an earlier predictor for screening of IUGR and/or pre-eclampsia.

Effects of Placental Isoferritin on the Mouse Embryo Development in vitro

To investigate the effect of placental isoferritin （PLF） on mouse embryo development in vitro, mice 2-cell embryos were co-cultured with human first trimester decidual cells at different concentrations of PLF in vitro. The following changes of the above system were observed under an invert microscope and the number of embryos were recorded and the embryos were classified. The results showed there was no significant difference in the percentage of embryos development to 4-cell 8-cell and morula （P〉0.05）. PLF at the doses of 10 and 100 U/mL significantly enhanced more embryos development to the blastocyst and hatching blastocyst （P〈0.05）. PLF at the dose of 1000 U/mL depressed more embryos development from 2-cell to hatching blastocyst, meanwhile such phenomena as cell degeneration and irregular cleavage were observed in part of embryos, but there was no significant difference in statistics （P〉0.05）. It was concluded that PLF at the concentration of 10-- 100 U/mL had no significant effects on the early development of mice embryos, however, PLF could promote the growth, differentiation, and hatching of preimplantion blastocysts.

人酸性铁蛋白H亚基固相免疫放射分析

从人心肌组织纯化酸性铁蛋白（ＡＩＦ），免疫家兔产生的ＡＩＦ血清用ＡＩＦ偶联的亲和层析柱纯化，将抗ＡＩＦ免疫球蛋白制成固相。１２５Ⅰ－抗ＡＩＦ－Ｈ亚基单克隆抗体用氯胺－Ｔ法制备；采用顺序法建立ＡＩＦ－Ｈ亚基因相免疫放射分析，数据用自动拟合样条函数处理，批内和批间ＣＶ分别为２．４４３％和１０．１６０％，灵敏度为０．７３６μｇ／Ｌ，回收率为９２．２９３％，可测范围为１．４７２－３２０μｇ／Ｌ，ＥＤ５０为２３．０５μｇ／Ｌ。与ＡＦＰ、ＣＥＡ和乳铁蛋白（ＬＦ）无交叉反应，与铁蛋白有３．１２５％的交叉反应。健全性试验证明血清基质对本方法无干扰。４０例男女血清ＡＩＦ－Ｈ亚基含量分别为３．７５±１．８５和２．９２±０．９６μｇ／Ｌ（Ｓ±２Ｓ），１０例肝癌患者血清ＡＩＦ—Ｈ亚基含量为８．３９±３．８７μｇ／Ｌ（Ｓ±２Ｓ），显著高于正常参考值。本方法可为肿瘤，尤其是肝癌的基础和临床研究提供一种有效的手段。

血清同工铁蛋白酶联免疫吸附测定及其临床观察

用酶联免疫吸附测定法(ELISA)观察了96例正常人,11例原发性肝细胞肝癌(HCC)、28例乳癌(BC)、31例肺癌(LC)、26例乳腺纤维瘤(BF)、11例肺炎(LF)及11例肺结核(TB)患者的血清同工铁蛋白(Serum isoferritin,SIF)水平。结果显示:正常人与HCC、BC、LC、BF及LF患者之间的SIF水平存在非常显著差异(P<0.01或P<0.001),在上述各类疾病中恶性肿瘤与相应组织的非癌性疾病患者之间的SIF水平也呈现非常显著的差异(BC与BF间、LC与LF间的P<0.01,LC与TB间的P<0.001)。SIF对检测HCC、LC及BC有较高的灵敏度,对鉴别这些恶性肿瘤具有重要价值。

抗人肝癌铁蛋白抗体对原发性肝癌患者的放射免疫显像

用^(131)Ⅰ标记抗人肝癌铁蛋白抗体对16例原发性肝癌患者作放射免疫显像分析。结果:显像阳性率为81.3％,其中经肝动脉插管和经外周静脉注射者各8例,前者阳性率为100％,注射后当天用单光子发射计算机处理断层摄影即可获得阳性显像,以第4～6天显像最为清晰,有3例追踪到第20天仍可获阳性显像。后者阳性率为62.5％,以第5～7天显像最为清晰。第3、5和8天肝癌与周围肝组织的中位放射强度比值前者分别为1.4,1.6和1.8,最高可达2.9;后者分别为1.2、1.3和1.4最高达1.8。

肝脏同工铁蛋白性质的研究

本文研究了Wistar大鼠、正常人及肝细胞肝癌(HCC)病人的肝脏同工铁蛋白的性质。HCC病人的肝脏同工铁蛋白的铁与蛋白质比值为0.021,约为正常人的1/12。正常人及HCC病人的肝脏同工铁蛋白的分子量分别为20.5及21.5kd。鼠肝及HCC病人的肝脏同工铁蛋白的PAGE呈现一条区带,正常人肝为两条区带。正常人及Wistar大鼠肝脏及马脾同工铁蛋白的双向免疫扩散存在交叉反应。电镜观察到HCC病人肝脏同工铁蛋白颗粒疏松,大小不均。

酸性铁蛋白放免分析中抗体纯化的可行性

用改进的工艺自人心肌组织中提取的高纯度酸性铁蛋白（ＡＩＦ），与经溴化氰（ＢｒＣＮ）活化的ＳｅｐｈａｒｏｓｅＣＬ－６Ｂ偶联，制得ＡＩＦ－ＳｅｐｈａｒｏｓｅＣＬ－６Ｂ亲和层析柱。用经该柱纯化的兔抗ＡＩＦ抗血清来组建酸性铁蛋白放免分析法（ＡＩＦＲＩＡ）用四参数Ｌｏｇｉｓｔｉｃ数据处理程序处理数据。批内、批间ＣＶ分别为１．６５％和９．７１％，灵敏度为１．８９μｇ／ｌ，回收率为１０２％，可测范围为７．０—３６９．６μｇ／ｌ，ＥＤ５０为２７．５０μｇ／ｌ，与ＡＦＰ、ＣＥＡ、ＬＦ无交叉反应，同常规铁蛋白的交叉反应率为１．７４％。对照组男、女性各３０例，血清ＡＩＦ含量（ｘ±２ｓ）分别为１６．７６±６．９８μｇ／ｌ和１３．３２±６．２５μｇ／１，差异不显著（Ｐ＜０．０５）。１０例肝癌患者血清ＡＩＦ含量为３６．０９±１５．８４μｇ／ｌ，较对照组有非常显著的增高（Ｐ＜０．００１）。上述结果提示，用亲和层析技术纯化ＡＩＦ抗血清是可行的，有利于提高ＲＩＡ的灵敏度、特异性、准确性及临床有效性。

血浆胎盘异铁蛋白与妊娠高血压综合征和胎儿生长迟缓的关系

目的 探讨血浆胎盘异铁蛋白 (PLF)在妊娠高血压综合征和胎儿生长迟缓发病机制中的作用及其早期预测价值。方法 采用前瞻性研究方法 ,在妊娠 2 4～ 34周对 12 0例最初正常的孕妇 ,分别用ELISA法和Griess法测定血浆PLF和NO代谢产物亚硝酸基 /硝酸基 (NO2 -/NO3 -)水平 ,观测孕妇孕期血压的变化并随访妊娠结局。结果① 12 0例正常孕妇妊娠结局随访结果 ,发生胎儿生长迟缓 15例 (IUGR组 )、妊娠高血压综合征 19例 (妊高征组 ) ,86例妊娠结局正常 (正常组 )。②IUGR组和妊高征组PLF水平明显低于正常组 (P <0 0 1) ;NO水平明显高于正常组 (P <0 0 1) ;IUGR组与妊高征组血浆PLF和NO水平差异均无显著性 (均为P >0 0 5 ) ;血浆PLF水平与NO水平呈负相关(r=- 0 32 9,P <0 0 1)。③PLF预测IUGR、妊高征 ,其ROC曲线下面积分别为 0 977、 0 90 5。以PLF等于 4 0 0 μg/ml预测妊高征、以PLF等于 390 μg/ml预测IUGR时的Kappa指数分别为 0 6 4 5和 0 6 6 3,预测值与实际情况有良好的一致性。结论 血浆胎盘异铁蛋白水平的降低与胎儿生长迟缓和妊高征的发生有密切关系 ,血管内皮细胞损伤可能是其作用机制之一。

薄层聚丙烯酰胺等电聚焦电泳鉴定肝脏同工铁蛋白的研究

作者应用高分辨率的蛋白质分析技术——薄层等电聚焦电泳对肝脏同工铁蛋白进行了鉴定和分析研究。结果表明:Wistar大鼠、正常人及肝细胞性肝癌病人的肝脏同工铁蛋白电泳区带分别为7、6、3三条;等电点分别为5.76～4.75、5.80～4.85、4.50～4.43,肝细胞性肝癌病人肝脏同工铁蛋白的等电点明显偏酸。

酸性同工铁蛋白和AFP联检对原发性肝癌诊断价值的研究

目的:探讨酸性同工铁蛋白(ＡＩＦ)与甲胎蛋白(ＡＦＰ)联合检测对原发性肝癌诊断的价值。方法:采用放射免疫测定法测定原发性肝癌 ７８例、转移性肝癌 ２２例、肝炎和肝硬化病人 ８４例,正常对照 ８０例血清 ＡＩＦ和 ＡＦＰ含量。结果:原发性肝癌、转移性肝癌、肝炎和肝硬化病人ＡＩＦ的阳性率分别为６０．３%、４０．０%和２３．８%,对原发性肝癌诊断的阳性率显著高于其它组(Ｐ＜０．０１)。ＡＩＦ和ＡＦＰ联合检测对原发性肝癌诊断的阳性率分别由６０．３%和６８．０%提高至 ９０．９%;诊断的特异性由 ７６．８%和 ８４．５%提高至 ９７．３%。结论:ＡＩＦ与 ＡＦＰ联合检测明显提高对原发性肝癌诊断的灵敏度和特异性。

酸性同功铁蛋白单克隆抗体免疫学特性的研究

目的：探讨抗不同组织酸性同功铁蛋白（ＡＩＦ）单克隆抗体（ＭｃＡｂ）的免疫学特性。方法：应用聚焦层析技术分别从人胎盘和原发性肝癌组织中分离出低ｐＩ值的ＡＩＦ，常规制备ＭｃＡｂ和进行免疫组织化学测定。结果：共筛选到５株抗人胎盘ＡＩＦ和２株抗人原发性肝癌（ＰＨＣ）ＡＩＦ的ＭｃＡｂ，即２ｆ８、４ｇ７、４ｇ８、５ｃ３、７ａ９和４ｃ９、４ｅ２。抗ＡＩＦＭｃＡｂｓ均与各自ＡＩＦ分子上不同抗原决定簇结合，其中针对不同组织ＡＩＦ的ＭｃＡb５ｃ３和４ｅ２作用于同一抗原决定簇。使用ＭｃＡｂ２ｆ８和４ｃ９，对正常肝组织、慢性肝炎与肝硬化和ＰＨＣ肝组织进行了免疫组织化学检查，其阳性率分别为２ｆ８：０、１０．０％、７６．３％；４ｃ９：０．６．７％、８１．６％。结论：人胎盘和ＰＨＣ组织ＡＩＦ中存在着共同的抗原决定簇，抗ＰＨＣＡＩＦＭｃＡｂ在免疫诊断中优于抗人胎盘ＡＩＦＭｃＡｂ。

AFP、SF、AIF联合检测对原发性肝癌诊断的价值

用放射免疫分析法（ＲＩＡ）对４６例原发性肝癌（ＰＨＣ）患者及１４５例正常人进行血清甲胎蛋白（ＡＦＰ）、铁蛋白（ＳＦ）、酸性铁蛋白（ＡＩＦ）测定，结果ＰＨＣ组血清ＡＦＰ、ＳＦ、ＡＩＦ测定值显著高于对照组及其他肝病组（Ｐ＜０．００１），肝癌组ＡＦＰ阳性中为７８．２６％，联合测定ＳＦ、ＡＩＦＩａ性检出中可达１００％，提示血清八ＦＰ、ＳＦ、ＡＩＦ测定在ＰＨＣ诊断中有重要的价值，尤其联合测定ＡＦＰ，ＳＦ、ＡＩＦ３项可提高原发性肝癌的早期诊断率，降低了漏诊率。

原发性肝癌患者血清酸性铁蛋白RIA结果分析

对１２８例原发性肝癌、３７例肝硬化、６０例健康人作血清酸性铁蛋白（ＡＦＦ）检测。正常组６０例，其中男（３０例）测得ＡＩＦ值为１１２±４０．０３ｍｇ／Ｌ（Ｘ±ＳＤ），女（３０例）测得ＡＩＦ值为６２±２８．７２ｍｇ／Ｌ（Ｘ±ＳＤ）。原发性肝癌组，男（１１１例），测得ＡＩＦ值为４８１±２８１．５６ｍｇ／Ｌ（Ｘ±ＳＤ），女（１７例）测得ＡＩＦ值为３３４±１５０．０２ｍｇ／Ｌ（Ｘ±ＳＤ），与正常组比较，差异有显著性意义（Ｐ＜０．０１）。肝硬化组，男（３１例）测得ＡＩＦ值为１３６±６３．３６ｍｇ／Ｌ（Ｘ±ＳＤ），女（６例）ＡＩＦ测得值为９０．７±５９．６３ｍｇ／ｌ（Ｘ±ＳＤ）；与正常组比较无统计学意义（Ｐ＞０．０５）。ＡＦＰ＜２０μｇ／Ｌ的７７例原发性肝癌中，ＡＩＦ阳性率８０．５％（６２／７７）。ＡＦＰ阳性与ＡＦＰ阴性的原发性肝癌ＡＩＦ测定值之间差异无显著性意义（Ｐ＞０．０５）。

胎盘异铁蛋白对小鼠胚胎生长发育影响的研究

目的:探讨胎盘异铁蛋白对小鼠胚胎生长发育的影响。方法:将人早孕蜕膜细胞和小鼠2-细胞期胚胎置于含不同浓度胎盘异铁蛋白的培养液中共培养,倒置显微镜下观察记录胚胎数目并分级。结果:①发育至4-细胞期、8-细胞期及桑葚胚阶段鼠胚数的百分率比较,差异无显著性(P>0.05)。②在10 U/mL和100 U/mL浓度的胎盘异铁蛋白作用下,发育至囊胚期和孵出期鼠胚数的百分率明显提高(P<0.05)。③在1 000 U/mL浓度的胎盘异铁蛋白作用下,从2-细胞期发育至孵出期鼠胚数的百分率有所下降,部分细胞发生变性、退化和不规则分裂等现象,但无统计学意义(P>0.05)。结论:10～100 U/mL浓度的的胎盘异铁蛋白对鼠胚的早期发育没有显著影响,但能促进晚期鼠胚的生长、分化和孵出。

抗AIF单链抗体在大肠杆菌中的可溶性表达和鉴定

目的:获得具有生物活性的抗酸性同功铁蛋白(AIF)单链抗体(scFv)。方法:将AIF4c9scFv基因亚克隆于原核表达载体pPOW3,构建重组表达质粒pPOW4c9,电转化大肠杆菌DH5α,以温度诱导重组抗AIFscFv表达,经镍螯合层析柱纯化后,用ELISA和Westernblot检测表达蛋白与AIF的结合特性。结果:抗AIFscFv抗体在大肠杆菌中获得可溶性表达,亲和力常数KD为3.18×10-8mol/L;纯化后的可溶性AIFscFv含量约为1.6mg/L。重组蛋白能特异识别AIF,并且具有良好的抗体生物学活性。结论:在大肠杆菌中表达并纯化了特异性可溶性抗AIFscFv抗体。

AFP、SF、AIF联合检测对原发性肝癌诊断的价值

用放射免疫分析法（RIA）对46例原发性肝癌（P＜C）患者及145例正常人进行血清甲胎蛋白（AFP）、铁蛋白（SF）、酸住铁蛋白（AIF）测定，结果P＜C组血清AFP、SF、AIF测定值显著高于对照组及其它肝病组（P＜0．001），肝癌组AFP阳性率为78.26％，联合测定SF、AIF阳性检出率可达100％，提示血清AFP、SF、AIF测定在P＜C诊断中有重要的价值，尤其联合测定AFP、SF、AIF三项可提高原发性肝癌的早期诊断率，减少漏诊率．

人心肌酸性铁蛋白的分离纯化及临床应用

人心肌匀浆经热变性、酸化、硫酸铵盐析、超离心、ＳｅｐｈａｒｏｓｅＣＬ－４Ｂ柱层析和制备等电聚焦分离，得到酸性铁蛋白。经鉴定，所得酸性铁蛋白ｐＩ为５．０，Ｈ亚基分子量为２１ｋＤ，Ｌ亚基为１９ｋＤ，ＰＡＧＥ分析呈单一区带。制备了兔抗人酸性铁蛋白抗血清，用该抗血清建立的人酸性铁蛋白放射免疫分析可检测出８０％甲胎蛋白阴性肝癌病人。

胎盘异铁蛋白与妊娠

由妊娠滋养细胞分泌的一种生理性储铁蛋白的异构体 ,即胎盘异铁蛋白 (placental isoferritin,PL F) ,具有免疫抑制作用 ,对维持正常妊娠有着重要意义 ,如果产生和分泌不足 ,易导致流产、早产及新生儿低出生体重。 PL F与妊娠高血压综合征。

血清同工铁蛋白RIA测定对AFP阴性肝占位性病变的鉴别诊断

46例病理诊断的AFP阴性肝占位性病变病人的血清铁蛋白(SF)和酸性铁蛋白(SAF)放射免疫测定结果。结果表明,在这些病人中,原发性肝癌病人约占一半;SF和SAF的放免测定对AFP阴性肝占位性病变的性质具有一定的鉴别诊断价值、有助于对AFP阴性原发性肝癌(HCC)的诊断。SF和SAF放免测定诊断HCC的敏感性分別为57.1%和76.2%,特异性分別为96.0%和100%,诊断准确性分别为78.3%和89.1%。结果提示,对AFP阴性HCC的诊断价值,SAF优于SF。