Zhang Yang-De, Zhou Jian, Zhao Jin-Feng, Peng Jian, Liu Xiao-Dong, Liu Xin-Sheng, Jia Ze-Ming
National Hepatobiliary and Enteric Surgery Research Center, Ministry of Health, 141 Xiangya Road, Changsha 410008, Hunan Province, China.
World J Gastroenterol. 2006 Jul 21;12(27):4401-5. doi: 10.3748/wjg.v12.i27.4401.
To construct the expression vectors for prokaryotic and eukaryotic human augmenter of liver regeneration (hALR) and to study their biological activity.
hALRcDNA clone was obtained from plasmid pGEM-T-hALR, and cDNA was subcloned into the prokatyotic expression vector pGEX-4T-2. The recombinant vector and pGEX-4T-2hALR were identified by enzyme digestion and DNA sequencing and transformed into E coli JM109. The positively selected clone was induced by the expression of GST-hALR fusion protein with IPTG, then the fusion protein was purified by glutathine s-transferase (GST) sepharose 4B affinity chromatography, cleaved by thrombin and the hALR monomer was obtained and detected by measuring H thymidine incorporation.
The product of PCR from plasmid pGEM-T-hALR was examined by 1.5% sepharose electrophoresis. The specific strap was coincident with the theoretical one. The sequence was accurate and pGEX-4T-hALP digested by enzymes was coincident with the theoretical one. The sequence was accurate and the fragment was inserted in the positive direction. The recombinant vector was transformed into E coli JM109. SDS-PAGE proved that the induced expressive fusion protein showed a single band with a molecular weight of 41 kDa. The product was purified and cleaved. The molecular weights of GST and hALR were 26 kDa, 15 kDa respectively. The recombinant fusion protein accounted for 31% of the total soluble protein of bacterial lysate. HALR added to the culture medium of adult rat hepatocytes in primary culture and HepG2 cell line could significantly enhance the rate of DNA synthesis compared to the relevant control groups (P < 0.01).
Purified hALR has the ability to stimulate DNA synthesis of adult rat hepatocytes in primary culture and HepG2 cells in vitro, and can provide evidence for its clinical application.
构建原核和真核人肝再生增强因子(hALR)表达载体并研究其生物学活性。
从质粒pGEM-T-hALR中获得hALR cDNA克隆,将cDNA亚克隆至原核表达载体pGEX-4T-2。通过酶切和DNA测序鉴定重组载体和pGEX-4T-2hALR,并转化至大肠杆菌JM109。用异丙基-β-D-硫代半乳糖苷(IPTG)诱导阳性选择克隆表达GST-hALR融合蛋白,然后通过谷胱甘肽S-转移酶(GST)琼脂糖4B亲和层析纯化融合蛋白,用凝血酶切割获得hALR单体,并通过测量H-胸腺嘧啶核苷掺入进行检测。
用1.5%琼脂糖凝胶电泳检测质粒pGEM-T-hALR的PCR产物。特异性条带与理论条带一致。序列准确,酶切后的pGEX-4T-hALP与理论一致。序列准确且片段正向插入。重组载体转化至大肠杆菌JM109。十二烷基硫酸钠-聚丙烯酰胺凝胶电泳(SDS-PAGE)证明诱导表达的融合蛋白呈现一条分子量为41 kDa的单带。产物经纯化和切割。GST和hALR的分子量分别为26 kDa、15 kDa。重组融合蛋白占细菌裂解物总可溶性蛋白的31%。与相关对照组相比,添加到原代培养的成年大鼠肝细胞和HepG2细胞系培养基中的hALR可显著提高DNA合成速率(P<0.01)。
纯化的hALR具有刺激原代培养的成年大鼠肝细胞和体外HepG2细胞DNA合成的能力,可为其临床应用提供依据。