吉林省杨树蛀干害虫的三种姬小蜂天敌(膜翅目:小蜂总科, 姬小蜂科)

1986年,原吉林省林业生防中心站(现为吉林省林业科学研究所)同中国科学院动物研究所合作,对吉林省杨树蛀千害虫的寄生蜂资源进行了开发利用研究。本文是该项研究成果的第一篇报道,记述了三种姬小蜂天敌,包括寄生白杨透翅蛾的透翅蛾黑姬小蜂Elachertus nigritulus(Zett.)和寄生杨窄吉丁的一新种丽凹面姬小蜂 Eniedon epicharisHuang及一新记录种 Eniedon zanara Walker。其它研究成果将陆续报道。     

Comparative biodistribution and antibody-dependent cellular cytotoxicity of native and heavy chain chimeric antibody.

We have recently chimerized the heavy chain of the pan-carcinoma monoclonal antibody (mAb) B72.3. Studies were undertaken to compare the IgG1 chimeric antibody, B72.3-1-3 with native murine B72.3 (nB72.3). Using fluorescence-activated cell sorting analysis, B72.3-1-3 demonstrated specific binding to fresh LS174T tumor cells. Biodistribution of 131I B72.3-1-3 was similar to 131I nB72.3 in nude mice bearing LS174T xenografts. Peak radiolocalization indices were noted on day 6 for B72.3-1-3 and day 8 for nB72.3. Both antibodies were capable of imaging LS174T tumors by radioimmunoscintigraphy. Antibody-dependent cellular cytotoxicity of LS174T by human peripheral blood lymphocytes was tested in 8h 51Cr release assays. With either no antibody or nB72.3, lymphocytes were not capable of killing LS174T cells. However, B72.3-1-3 at a concentration of 5 and 50 micrograms/ml mediated significant lysis of tumor cells by human lymphocytes. These results suggest that chimeric antibodies retain their binding properties to tumor cells and display biodistribution patterns similar to their unmodified counterparts. Such modifications may reduce the deleterious human antimouse antibody response to murine mAbs as well as augment antibody-dependent cellular cytotoxicity of tumor cells by human effectors.     

上海生态平衡学术讨论会

中国生态学会“生态平衡”学术讨论会于1981年11月7日至13日在上海召开,来自全国22个省市区的90余名代表出席了会议。大会针对当前国内外广泛重视和关心的“生态平衡”问题展开了热烈地讨论。代表们认为:生态学是社会主义建设蓝图的“底色”,这个“底色”搞不好,社会主义建设也难以搞好,为此,全国人民都要关心生态学的问题。目前污染严重,生态平衡失调,已引起人们的警觉和关注,“生态平衡”问题已提到了议事日程,不允许人们再忽视了。     

大鼠尾壳核衰老变化定量分析：Ⅱ.多巴胺（DA）系统

本实验结果表明:衰老大鼠(26—27月龄)尾壳核多巴胺(DA)神经末梢膨体较成年组(3—4月龄)明显减少,而单个膨体内DA含量较成年组显著增多,提示纹状体DA系统在衰老过程中可能具有一定的代偿机制。本文对其意义进行了讨论。     

A 3-hydroxy-3-methylglutaryl-CoA synthase-based probe for the discovery of the acyltransferase-less type I polyketide synthases

Acyltransferase (AT)-less type I polyketide synthases (PKSs) produce complex natural products due to the presence of many unique tailoring enzymes. The 3-hydroxy-3-methylglutaryl coenzyme A synthases (HCSs) are responsible for β-alkylation of the growing polyketide intermediates in AT-less type I PKSs. In this study, we discovered a large group of HCSs, closely associated with the characterized and orphan AT-less type I PKSs through in silico genome mining, sequence and genome neighbourhood network analyses. Using HCS-based probes, the survey of 1207 in-house strains and 18 soil samples from different geographic locations revealed the vast diversity of HCS-containing AT-less type I PKSs. The presence of HCSs in many AT-less type I PKSs suggests their co-evolutionary relationship. This study provides a new probe to study the abundance and diversity of AT-less type I PKSs in the environment and microbial strain collections. Our study should inspire future efforts to discover new polyketide natural products from AT-less type I PKSs.     

FXR在胃粘膜肠化生及胃癌中的表达及其意义研究

目的:研究FXR在胃炎,胃粘膜肠化生及胃癌组织中的表达,分析其在胃癌发生中的意义。方法:采用免疫组化方法检测FXR在55例胃炎组织,61例胃黏膜肠化生组织及61例胃癌组织中的表达,利用统计学方法 SPSS17.0软件分析其在三种组织中的表达变化,结合文献回顾,分析FXR在胃癌发生中的意义。结果:FXR在胃黏膜肠化生中的表达明显高于胃炎组织(P0.05),而在胃癌组织中,FXR的表达显著低于胃粘膜肠化生组织(P0.05)。结论:FXR是一个潜在的胃癌发生生物标记物,其具体机制有待于进一步探索。