Preparation and activity of conjugate of monoclonal antibody HAb18 against hepatoma F( ab′ )_2 fragment and staphylococcal enterotoxin A

AIM To prepare the conjugate of staphylococcal enterotoxin A (SEA) protein which is a bacterial SAg and the F(ab')2 fragment of mAb HAbl8 against human hepatocellular carcinoma (HCC), and identify its activity in order to use SAg in the targeting therapy of HCC.METHODS MAb HAbl8 was extracted from the abdominal dropsy of Balb/ c mice, and was purified through chromatography column SP-40HR with Fast protein liquid chromatography (FPLC) system. The F(ab')2 fragment of mAb HAb18 was prepared by papainic digestion method. The conjugate of mAb HAb18 F(ab')2fragment and SEA was prepared with chemical conjugating reagent N-succinimidyl-3-( 2-pyridyldithio) propionate (SPDP) and purified through chromatography column Superose 12with FPLC system. The molecular mass and purity of each collected peak were identified with SDS-PAGE assay. The protein content was assayed by Lowry's method. The antibody activity of HAb18 F (ab')2 against HCC in the conjugate was identified by indirect immunocytochemical ABC method, and the activity of SEA in the conjugate to activate peripheral blood mononuclear cells (PBMC) was identified with MTT assay.RESULTS The lgG mAb HAb18 was extracted,and purified successfully. Immunocytochemical staining demonstrated that it reacted with most of HHCC cells of human HCC cell line. There were two peaks in the process of purification of the prepared HAb18 F(ab)2-SEA conjugate. SDS-PAGE assay demonstrated that the molecular mass of the first peak was about 130 ku, and the second peak was the mixture of about 45 ku and a little 100 ku proteins. The immunocytochemical staining was similar in HAb18 F (ab ')2-SEAconjugate and HAb18 F (ab ')2, i.e., thecytoplasm and/or cell membranes of most HHCC cells were positively stained. The MTT assay showed that the optical absorbance (A) value at 490 nm of HAb18 F (ab')2-SEA conjugate was 0.182 ± 0.012, that of negative control was 0.033± 0.009, and there was significant difference between them ( P < 0.05).CONCLUSION SPDP is a good proteinconjugating reagent and can be used in preparing protein conjugate. The conjugate of mAb HAb18F(ab')2 fragment and SEA protein was preparedsuccessfully in present study and can be used in the experimental study of HCC targeting therapy with the conjugate of SAg and anti-HCC mAbs or their fragments.

重组葡萄球菌B型肠毒素超抗原的制备及抗肿瘤活性分析

目的 采用基因工程技术制备葡萄球菌B型肠毒素 (SEB) ,并对其体内外抗肿瘤活性进行分析。方法 对SEB在大肠杆菌中进行高效表达和分离纯化 ,并对其超抗原活性和免疫学活性与天然SEB进行比较研究。观察重组SEB对人肝癌细胞的体外抑制作用 ,以及对小鼠肝癌和肉瘤的体内抑瘤效果。结果 SEB获得高效表达 ,并一步将其纯化至均质。与天然毒素相比较 ,重组SEB的免疫学活性与超抗原活性基本相似。首次证明 ,即使SEB的浓度为 10ng/L ,仍然对人肝癌细胞有显著地抑制作用 ,其对小鼠体内的肝癌和肉瘤有一定的抑制作用。结论 重组SEB在体内外均有一定肿瘤抑制作用 。

单克隆抗体导向的超抗原葡萄球菌肠毒素A抗肝癌实验研究

目的:制备超抗原(SAg)葡萄球菌汤毒素A(SEA)与搞人肝细胞癌单克隆抗体(McAb)F(ab’)_2段的结合物,并观察其介导外周皿单个核细胞(PBAMC)的抗人肝癌作用,方法:提取McAb HAbl8,用木瓜蛋日酶制取其F(ab’)_2段,再用N-琥珀酰亚氨基-3-(2二硫吡啶)丙酸酯(SPDP)制备HAb18 F(ab’)_2-SEA结合物;经凝胶色谱柱纯化后用SDS-PAGE鉴定各收集峰,免疫组化ABC法鉴定此结合物的抗体活性,MTT法观察HAb18 F(ab’)_2SEA介导PBMC的抗肝癌作用.结果:成功地制备了HAb18 F(ab’)_2-SEA结合物,并且此结合物具有明显的介导PBMC靶向杀伤肝癌细胞的作用,并与其剂量呈正相关.对照组无此作用结论:MCAb与SAg结合物导向治疗肝癌是一种有发表前景的肝癌免疫治疗模式.

肝癌单克隆抗体F(ab′)_2段与葡萄球菌肠毒素A结合物的制备及其活性

目的：制备超抗原（SAg）葡萄球菌肠毒素A（SEA）与抗人肝细胞癌单克隆抗体（McAb）HAb18F（ab′）2段的结合物，并对其活性进行鉴定．方法：提取MCAbHAb18并用木瓜蛋白酶切取其F（ab′）2段，用SPDP制备HAb18F（ab′）2－SEA结合物，凝胶色谱柱纯化后用SDS－PAGE鉴定各收集峰，免疫组化ABC法鉴定结合物中的HAb18F（ab′）2的抗体活性，MMT法鉴定结合物中的SEA活化T细胞的活性．结果：成功地制备了HAb18F（ab′）2－SEA结合物，并且制备的结合物具有肝癌抗体活性和活化外周血单个核细胞的功能．结论：SPDP是一种很好的蛋白质交联剂，本实验制备的HAb18F（ab′）2－SEA结合物可用于McAb与SAg结合物导向治疗肝癌的实验研究．

单抗靶向超抗原SEA体内抗膀胱肿瘤实验研究

背景与目的:超抗原葡萄球菌肠毒素A(staphylococcal enterotoxin A,SEA)在体内、外以及临床的膀胱灌注治疗试验中对膀胱癌均具有明显的抑瘤效应,本研究旨在探讨单抗靶向的超抗原SEA体内对人膀胱癌的抑瘤作用。方法:以腹腔注射人外周血单个核细胞、皮下注射人膀胱癌BIU87细胞建立人免疫重建荷人膀胱癌SCID小鼠复合模型,再将模型小鼠随机分为对照组、SEA组及单抗靶向SEA实验组,分别予以PBS、SEA及单抗靶向SEA瘤周注射,以SonoSite彩超在建模后6周内检测小鼠皮下移植瘤体积、瘤体血流。结果:单抗靶向SEA组瘤体体积、瘤体血流均小于对照组及SEA组,在建模后4、5、6周差异均有统计学意义(P<0.05)。结论:单抗靶向的超抗原SEA对膀胱癌皮下移植瘤生长的抑制作用更强,可能与其进一步减少瘤体血流有关。

SEA-McAb融合蛋白对SMMC-7221细胞的抑制作用及机制

目的研究葡萄球菌肠毒素A(SEA)与单克隆抗体(McAb)融合蛋白的抗肝癌细胞活性及其机制。方法制备健康人外周血单个核细胞(PBMC)作为效应细胞。MTT法测定SEA-McAb融合蛋白对人肝癌细胞SMMC-7221的体外抑制率;采用荧光抗体流式细胞术测定肿瘤细胞HLA-I和HLA-DR抗原分子的表达;酶联免疫吸附(ELISA)法检测上清液中细胞因子IL-2、IL-12、TNF-α和IFN-γ的水平。结果肿瘤细胞在上清液作用后,HLA-I和HLA-DR的表达均有明显上升(P<0.01)。分泌IL-2、IL-12、TNF-α和IFN-γ均较对照组显著增加(P<0.01)。SMMC-7221明显被抑制(P<0.01)。结论SEA-McAb通过激发PBMC的杀伤作用,对肝癌细胞株表现出较强的靶向抑制作用。

单克隆抗体与葡萄球菌肠毒素A结合物的制备及其抗肝癌作用

目的制备超抗原(SAg)葡萄球菌肠毒素A(SEA)与抗人原发性肝细胞癌(简称肝癌)单克隆抗体(McAb)HAb18F(ab')2段的结合物,探讨其介导外周血单个核细胞(PBMC)的抗人肝癌作用.方法制备McAbHAb18,并用木瓜蛋白酶消化法制备其F(ab')2段.再用化学连接剂N-琥珀酰亚氨基-3-(2-二硫吡啶)丙酸酯(SPDP)制备HAb18F(ab')2-SEA结合物.结合物经快速蛋白质液相层析系统用凝胶色谱柱纯化后,用SDS-PAGE鉴定各收集峰.免疫组化ABC法鉴定结合物的抗体活性.MTT法鉴定结合物活化PBMC的活性及其介导PBMC的杀伤肝癌细胞作用.结果制备的HAb18F(ab')2-SEA结合物具有肝癌抗体活性和活化PBMC的功能.此结合物具有明显的介导PBMC杀伤肝癌细胞的作用,并与其浓度呈正相关.结论 SPDP是一种很好的蛋白质交联剂.HAb18 F(ab')2-SEA结合物导向治疗肝癌具有一定的发展前景.

超抗原分子SEA在肝癌细胞的表达和HLA-Ⅰ分子递呈

目的 将超抗原葡萄球菌肠毒素A(staphylococcalenterotoxinA ,SEA)分子转入肝癌细胞以增强其免疫原性 ,开辟肝癌免疫排斥的新途径。方法 从产SEA标准菌株中获得SEA基因全长片段 ,构建SEA逆转录真核表达载体 ,通过病毒包装和滴度测定 ,最后转导肝癌细胞 ,并进行T细胞杀伤实验 ,同时利用抗体阻断的方法研究递呈途径。结果 成功的获得了表达SEA人肝癌细胞株HHCSEA。结果显示微量表达的SEA蛋白即可引发高效的免疫活性。将细胞表面的HLA I分子利用抗体阻断后 ,杀伤活性明显降低。结论 肝癌细胞表达的SEA分子具有较高的免疫激活能力 ,且有可能主要通过HLA Ⅰ分子递呈。