精巢间质细胞雄激素合成及其调节的研究进展

本文综述了近年来精巢间质细胞雄激素的合成及其分泌调节的研究进展。间质细胞内的雄激素合成的限速步骤是胆固醇转化为孕烯醇酮时的胆固醇跨线粒体膜转运。在此转运过程中，PBR可能是作为依赖于配体的通道蛋白，对胆固醇分子进行跨膜转移；StAR则通过解离线粒体膜与胆固醇分子的吸附作用，加速了胆固醇分子的转运。雄激素的合成还受垂体、支持细胞、巨噬细胞和其自身分泌激素和细胞因子的调控。同时对今后研究的方向做了总结和展望。     

RNA抑制技术在神经干细胞研究中的应用

神经干细胞是在神经系统中发现的一种可以再生的细胞，不仅具有自我复制能力，还可以分化为神经元、星状胶质细胞和少突胶质细胞，对研究神经退行性疾病和神经系统的发育过程产生很大的影响，因而在国际上形成了一个研究热点，但其增殖、分化乃至迁移的机制仍有待解决，RNA抑制技术是目前流行的基因沉默法，利用导入小片段核酸进入细胞，对特定基因表达的翻译阶段进行抑制，从而观察基因对细胞的影响，该文在已获得分化相关基因的基础上，利用RNA干扰(RNAi)和反义RNA(antisense RNA)法检测几个基因对神经干细胞的影响。     

刷轮式苗盘精播装置排种板型孔直径的设计

为使种子在活动型孔板移动过程中，能够依靠自重顺利排出。固定排种板必须具有台理的直径，利用活动型孔板回移复位的结构特点，理论分析了种子顺利排出而不被回位型孔板干涉所需最少时间的条件，在此基础上优化设计排种板型孔直径。     

遗传指纹图谱技术对微生物群落的分析

微生物培养技术无法获得自然生境中99％以上的微生物，而可培养的微生物也仅提供极少的形态学线索，鉴定和生理学特性经常是模糊的。分子生物学技术对不可培养微生物的研究，开启了探索微生物多样性和新资源的大门。DNA杂交、rRNA分子标记测序等已经成为研究分子微生物生态学的常规手段，可以鉴定和描述微生物群落的种群，但却不适于探索微生物复杂群落的动力学。遗传指纹图谱技术允许同时进行多样本的分析，可比较不同生境和随时间变化的微生物群落行为，是传统手段的有力补充。     

EUT对TEM传输室特性阻抗影响的边界元分析

采用边界元法分析了金属箱体的受试设备对横电磁波传输室特性阻抗的影响．计算结果表明，当受试设备不满足“三分之一准则”时，对特性阻抗的影响达5Ω以上，当满足“三分之一准则”时，对特性阻抗的影响小于2Ω．测量结果证实了计算方法的有效性，所得结论对TEM传输室的设计与测试具有重要意义。     

Inhibitory effect of the adenovirus type 5 E1A protein expressed in the yeast system

The human adenovirus type 5 E1A, a tumor- suppressor gene[1], codes for two major related proteins of 243 amino acids (12S) and 289 amino acids (13S) by al-ternative splicing in two exons[2]. Studies have been shown that E1A can regulate expression of many genes and cell cycle[3]. Both in vitro and in vivo experiments indicated that E1A could induce tumor cells differentia-tion, convert tumor cells into an epithelial phenotype, in-hibit tumor cell growth and metastasis and strongly en-ha…     

Mechanical Studies on Treatment of Malignant Tumour by Ultralow Frequency Pulsed-Gradient Magnetic Fields

Ultralow frequency (ULF) pulsed-gradient magnetic field (with the maximum intensity of 0.6-2.0 T, gradient of 10-100 T·m-1, pulse width of 20-200 ms and frequency of 0. 16-1. 34 Hz) treatment of mice can inhibit murine malignant tumour growth and can induce apoptosis of cancer cell. The apoptotic cancer cell contracted, became rounder and divorced from adjacent cells; the heterochromatin condensed and coagulated together along the inner side of the nuclear membrane; the endoplasmic reticulums expanded and fused with the cellular membrane; many apoptotic bodies which were packed by the cellular membrane appeared and were devoured by some lymphocytes and plasma. By Lorentz force the magnetic field keeps the moving ions within bounds of Larmor radius. Thus, penetrating capability of the positive and negative ions through the cell membrane was affected, even the role on the cell membrane formed.     

东营凹陷沙三段-沙二下亚段T-R层序特征及成因

将东营凹陷古近系沙三段沙二下亚段划分为 3个三级层序 ,即沙三下层序 (SSⅠ )、沙三中层序 (SSⅡ )和沙三上沙二下层序 (SSⅢ )。SSⅠ和SSⅡ层序由湖进体系域和湖退体系域组成T R旋回 ,其特征是代表层序边界的不整合分布局限 ,湖进体系域厚度小 ,主要为细粒沉积物 ,退积式叠加 ;湖退体系域较厚 ,由进积式叠加的砂岩、砾岩和泥岩组成。T R层序的形成主要是由于层序形成早期的构造沉降和气候起主导作用 ,其基底快速沉降 ,湖水供应充分 ,湖平面快速上升。在层序形成晚期 ,沉积物供给和气候起主导作用 ,沉积物供给多 ,快速向前推进 ,湖平面下降。构造沉降和沉积物供给因素对层序控制作用的转换促使其形成层序和体系域的边界。T R层序与三分层序之间的转换是由于层序形成的不同阶段的主控因素不同而引起的     

Effects of hyaluronic acid－chitosan－gelatin complex on the apoptosis and cell cycle of L929 cells

With the development in the field of tissue engineering, the interaction between biomaterials and cells has been deeply studied. Viewing the cells seeded on the surface of materials as an organic whole, cell cycle and apoptosis are analyzed to deepen the study of cell compatibility on biomaterials, while cell proliferation and differentiation are studied at the same time. In this paper, hyaluronic acid is incorporated into the chitosan-gelatin system. Propidium iodide (PI) was used in cell cycle analysis and the double-staining of cells with annexin-V and PI was applied in cell apoptosis analysis. The results show that incorporated hyaluronic acid shortens the adaptation period of cells on the material surface, and then cells enter the normal cell cycle quickly. In addition, added hyaluronic acid inhibits cell apoptosis triggered by the membranes. Therefore, hyaluronic acid improves the cell compatibility of chitosan-gelatin system and benefits the design of biomimetic materials.     

Inhibitory effect of the adenovirus type 5 E1A protein expressed in the yeast system of the human tumor cell growth

Adenovirus 5 type E1A as a tumor suppressor gene can inhibit tumor growth and enhance the censitivity of chemotherapy and radiotherapy.E1A have the ability to integrate into the host genome,resulting in long-time expres-sion that induces Rb gene inactivation and animal cells im-mortalization.This prompted us to select the E1A protein for treatment of cancer in order to overcome the limitations of E1A gene therapy.Thus,we firstly comstructed E1A eu-caryotic expression vector (pPIC9/E1A),transformated the pichia pastoris yeast cells(GS115) and screened the high-expressing recombinant strains.The positive yeast strains were cultured in the shake flask,and induced for 3d.The crude E1A protein was purified using two steps of col-umu chromatography on HiTrap Q and HiTrap SP.The pu-rified E1A protein was identified by SDS-PAGE and Western blot.E1A protein was mostly located at cellular unclear when Cheriot delivered E1A protein into cells.The analysis in vitro indicated that the E1A protein arrested LN686 cell cycle at G2/M phase,and significantly inhibited the growth of LN686 tumor cells.The current studies firstly provided an experimental basis to further develop E1A protein for tumor treatment.