东亚钳蝎抑制型神经毒素基因在昆虫细胞中的表达及活性鉴定

基因BmKIT3R 是根据东亚钳蝎 (ButhusmartensiiKarsch)抑制型神经毒素基因BmKIT3 优化而得的 .将优化过的蝎毒素基因BmKIT3R 通过Bac to Bac操作技术 ,使重组杆状病毒基因组DNA转染到草地粘虫sf2 1细胞中对IT3R 基因进行表达 ,经SDS PAGE检测在 8.7× 10 3 处有一表达条带 .表达产物经生物鉴定 ,证明具有很高的活性 ,它对昆虫具有非常明显的致死作用 .图 3参 5     

混合酶强化剩余污泥微生物燃料电池性能

为了提高剩余污泥为燃料的微生物燃料电池(SMFC)产电性能以及污泥减量化效果,在不同的温度(40、45和50℃)研究单室无膜微生物燃料电池中酶对SMFC产电特性的强化效果.加入单一酶(蛋白酶或α-淀粉酶)的结果表明,随着温度的上升,SMFC功率密度均上升,但40℃时强化效果最明显,与加入失活酶的对照组相比分别增加198％和130％.在40℃下,混合酶比(蛋白酶浓度:淀粉酶浓度)为2∶3时,SMFC最大功率密度为776 mW/m2.随着混合酶中淀粉酶的比例提高,SMFC库伦效率逐渐增加,当混合酶比为4∶1时,CE(库伦效率)可达18.3％,同时TCOD、TSS和VSS去除率分别为70.3％、66.7％和80.4％.因此,温度相对较低时,外加酶强化效果更明显;与单种酶相比,混合酶对SMFC产电性能和污泥减量化的强化效果更显著.     

BPA暴露对本体和子代胰岛β细胞转录组差异对比分析

双酚A(BPA)作为一种典型的环境内分泌干扰物,与二型糖尿病和肥胖症等代谢类疾病密切相关.在这项研究中,旨在探讨BPA直接暴露以及围产期暴露对本体和子代胰岛β细胞影响的差异,从而实现对不同易感人群的精准预防与治疗.通过对GEO数据库中GSE126297和GSE82175两个数据集进行分析,共筛选出108个共有的差异基因...     

3种兽药及饲料添加剂对鱼类的毒理效应

采用斑马鱼、鲤鱼作为生物材料,通过斑马鱼急性毒性试验、胚胎发育试验和鲤鱼肾细胞单细胞凝胶电泳试验,分别从生物个体水平、细胞水平和分子水平,对兽药及饲料添加剂喹乙醇、阿散酸和土霉素进行了生态毒理学效应研究。急性毒性试验结果表明,3种兽药及饲料添加剂在有生态学意义的浓度范围内对斑马鱼的急性毒性均不大;胚胎发育试验结果表明,喹乙醇和阿散酸对斑马鱼胚胎发育72 h的EC50值分别为221.20和239.54 mg.L-1,具有明显的致畸效应;单细胞凝胶电泳试验结果表明,喹乙醇和土霉素均具有一定的遗传毒性,能引起鲤鱼肾细胞DNA的明显损伤,并呈现出一定的剂量-效应关系。     

Selective effects of fenitrothion on murine splenic T-lymphocyte populations and cytokine/granzyme production

The aim of this study was to investigate in vitro effects of fenitrothion (FNT) on mouse splenic lymphocytes. Here, naïve mice had their spleens harvested and splenocytes isolated. After exposure to FNT for 48 hr: splenocyte viability was measured using a tetrazolium dye assay; cell phenotypes, i.e., B-cells (CD19⁺), T-cells (CD3⁺), and T-cell subsets (CD4⁺ and CD8⁺), were quantified by flow cytometry; and, production of cytokines/granzyme-B was assessed via enzyme-linked immunosorbent assay. The ability for FNT to induce oxidative stress in the cells was evaluated by measuring hydroxyl radical (·OH) and malondialdehyde (MDA) production and changes in glutathione peroxidase (GSH-Px) and superoxide dismutase (SOD) activity. The results showed that FNT significantly inhibited splenocyte proliferation, and decreased production of interleukin (IL)-2, interferon gamma, IL-4, and granzyme B, but had no impact on IL-6 production. FNT also selectively decreased splenic T-cell levels but did not induce changes in CD19⁺ B-cells. Further, within the T-cell populations, percentages of CD3⁺, CD4⁺, and CD8⁺ T-cells (particularly CD8⁺ T-cells) were reduced. Lastly, FNT selectively increased MDA and ·OH production and inhibited SOD and GSH-Px activities in the splenic lymphocytes. These findings suggest that, due to oxidative damage, FNT selectively inhibits splenic T-lymphocyte survival and cytokine/granzyme production in vitro.     

A possible prenatal evaluation of renal function by amino acid analysis on fetal urine

Intrauterine treatment of 4 fetuses with urethral obstruction was attempted in the third trimester of pregnancy. The fetuses displayed varying sonographic findings including pyelectasis, caliectasis, hydroureter, bladder dilatation, ascites, hydrops, missing kidneys and oligohydramnios. Ultrasonically guided aspiration from the dilated structures was carried out to relieve pressure on the kidney parenchyme and to collect fluid samples for diagnostic purposes. Amino acid concentrations in the fetal urine showed a pattern similar to plasma in 2 fetuses, a pattern almost like urine in 1 fetus and an intermediate pattern in the 4th fetus. Only the fetus with normal amino acid concentrations in the urine survived: the other 3 died in uremia shortly after birth. In 3 cases cells from the aspirated urine were cultured and used for chromosome analysis. The cell cultures grew fast and karyotyping was possible within 1 week. In 2 fetuses an intrauterine catheter was inserted to drain the kidney permanently into the amniotic cavity. In the first case the catheter was displaced to the fetal abdomen after some days of successful drainage. In the second case the catheter tore the placenta, and the child had to be delivered immediately.     

固定化细胞技术及应用于废水处理的最新进展

本文简要介绍了用于废水处理的固定化细胞技术及应用此技术进行废水处理的七个领域的最新成就。     

Detection of fetal cells in maternal blood

We report the detection of fetal cells in the maternal circulation by enzymatic amplification of a single copy gene sequence that was fetal-specific. Fetal HLA-A2-positive cells were sorted from maternal HLA-A2-negative cells by flow cytometry and confirmed by demonstration of a fetal-specific HLA-DR4 sequence. However, this sequence could not be detected in unenriched maternal DNA prepared at 28 and 32 weeks' gestation. The sensitivity of detection was 1 HLA-DR4-positive cell in 10⁵ HLA-DR4-negative cells. We conclude that prenatal diagnosis of paternally inherited autosomal-dominant genetic defects may be possible by selective gene amplification of maternal peripheral blood. However, preliminary enrichment for fetal cells may be necessary.     

The time of appearance and disappearance of fetal DNA from the maternal circulation

A single copy Y-chromosome DNA sequence was amplified using the polymerase chain reaction (PCR) from the peripheral blood of 30 women who had achieved a pregnancy through an in vitro fertilization (IVF) programme. The time of conception was known precisely and was confirmed by serial ultrasound scans. Conceptions were dated as the number of weeks after fertilization plus 2, to give a time equivalent to the obstetric menstrual dating of the pregnancy (LMP). Y-chromosome-specific DNA was detected in all pregnancies with a male fetus (18/30). The earliest detection was at 4 weeks and 5 days, and the latest at 7 weeks and 1 day. Y-chromosome-specific sequences were no longer detected in any of the male pregnancies 8 weeks after delivery. No Y-chromosome sequences were detected in any of the pregnancies where only female babies were delivered. This demonstrates that fetal DNA appears in the maternal circulation early in the first trimester, that it can be identified in all pregnancies tested by 7 weeks, that it continues to be present throughout pregnancy, and that it has been cleared from the maternal circulation 2 months after parturition. Early non-invasive prenatal diagnosis for aneuploidies and inherited disorders will be possible in all pregnancies if fetal cells can be isolated free from maternal contamination (or identified accurately in the presence of maternal cells) without problems of contamination from previous pregnancies.     

裂变产物170Tm的体内蓄积特性诱发骨髓细胞突变效应研究

对裂变产物~(170)Tm的体内蓄积特性和诱发细胞突变效应的监测结果表明,当机体摄入~(170)Tm后,在短时间内即能迅速进入并滞留于骨组织中,其滞留量占体内各器官组织中的首位呈现高度选择性亲骨特征,在机体摄入~(170)Tm后的不同阶段,骨组织中的累积吸收剂量随着观察时间的延长而增升,其诱发骨髓细胞的染色体畸变率亦相应增高。由~(170)Tm内污染所诱发的染色体结构异常为染色单体型畸变,其中主要为染色单体断裂。随着骨组织中累积吸收剂量的增升,可观察到在一个细胞中同时有两个畸变发生,也诱发个别的染色体易位。