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排序方式: 共有498条查询结果,搜索用时 169 毫秒
1.
促渗剂对水合胼胝类脂热转变影响的差示扫描热分析研究   总被引:8,自引:0,他引:8  
从人胼胝组织提取出类脂经水合后代替人皮肤角质层用作差示扫描热分析研究促渗剂作用的简单模型。研究了1,8-桉油精,月桂氮酮和丙二醇等促渗剂对水合胼胝类脂热转变特征的影响。三种促渗剂均不同程度地降低水合胼胝类脂的热变温度,作用强弱依次为1,8-桉油精>月桂氮酮>丙二醇。丙二醇与1,8-桉油精或月桂氮酮混合应用时对热转变的影响具有协同作用。结果提示促渗剂可能改变脂质分子的排列和增加其流动性。同时,水的存在对脂质分子物理结构的形成具有重要作用。  相似文献   
2.
Summary: Linear unsaturated nylons 6 u18 and 18 u18 have been made containing a double bond in the center of the diacid segment with potential for additional functionalization. Solution state NMR showed the presence of a small portion of cis amide units. Solid state NMR verified the presence of the double bond in the bulk, and that the polyamides were present in the α‐crystalline form. Thermal stability was comparable to linear saturated nylons, and the melting and crystallization temperatures of the unsaturated nylons were lower compared to the saturated analogs.

DSC heating and cooling thermograms for nylons 6 u18 and 18 u18.  相似文献   

3.
Drawn gelatin films with improved mechanical properties   总被引:4,自引:0,他引:4  
Chain anisotropic distribution in gelatin films has been obtained by uniaxial stretching at constant relative humidity, followed by air drying and successive cross-linking with glutaraldehyde. The drawn samples have been characterized by mechanical tests, differential scanning calorimetry and scanning electron microscopy. The Young’s modulus, E, and the stress at break, σb, increase linearly with the draw ratio and reach values which are about five times those characteristic of undrawn samples. Furthermore, on stretching the alignment of the gelatin strands along the direction of deformation increases while the thickness of the layers decreases significantly. The renaturation level, that is the fraction of gelatin in a collagen-like structure, has been calculated as the ratio between the melting enthalpy of gelatin samples and that of tendon collagen. The results indicate that the improvement of mechanical properties achieved by drawn gelatin is closely related to the renaturation level. The experimental approach utilized to induce segmental orientation in gelatin films, allows to obtain anisotropic materials with improved mechanical properties in the direction of deformation, and can be usefully applied in the preparation of biomaterials.  相似文献   
4.
The in situ thermal protein denaturation and its correlation with direct hyperthermic cell injury in Dunning AT-1 prostate tumor cells were investigated in this study. The in situ thermal protein denaturation was studied using both Fourier transform infrared spectroscopy (FTIR) and differential scanning calorimetry (DSC). The FTIR spectra at different temperatures show changes in protein secondary structure (from alpha helix to extended beta sheet) during in situ thermal protein denaturation within AT-1 cells. Calorimetric studies using DSC show that endothermic heat release is associated with the in situ thermal protein denaturation. Furthermore, both the secondary structure changes detected by FTIR and the calorimetric changes detected by DSC were quantified and the kinetics of the overall in situ thermal protein denaturation was derived under different heating conditions. The onset temperature where the overall in situ thermal protein denaturation is first detectable was found to be scanning rate dependent (approximately 41 degrees C at 2 degrees C min(-1) and approximately 44 degrees C at 5 degrees C min(-1)). The kinetics of the overall in situ thermal protein denaturation was derived from both DSC and FTIR measurements and was fit using kinetic and statistical models. The kinetic data determined by FTIR and DSC under the same heating conditions match well with each other. The activation energy of the overall in situ thermal protein denaturation is found to be strongly dependent on the temperature range considered (the activation energy ranges from approximately 110 kJ mol(-1) between 44 and 90 degrees C to approximately 750 kJ mol(-1) between 44 and 50 degrees C). However, its dependence on heating rate is negligible. Several denaturation peaks, including a dominant one between approximately 62 and 65 degrees C, are identifiable from both the DSC and the FTIR results. To investigate directly the relationship between thermally induced cell injury and the in situ thermal protein denaturation, both acute (propidium iodide dye exclusion, assessed 3-h postthermal treatment) and chronic (clonogenics, assessed 7-day postthermal treatment) cell injury were quantified using AT-1 cells prepared under the same conditions as for the DSC protein studies. Comparisons of the results from the cell injury studies and the DSC protein denaturation studies show that the overall in situ thermal protein denaturation correlates well with both the acute and the chronic cell injury, which suggests that overall in situ thermal protein denaturation is an important mechanism of direct hyperthermic cell injury in AT-1 cells at the macromolecular level.  相似文献   
5.
Several syndiotactic polystyrene (sPS) samples have been synthesized by using different catalytic systems. Their stereochemistry has been determined by 13C NMR spectra in both the aliphatic CH2 and aromatic C1 resonance regions. The observed peaks have been unambiguously assigned to specific hexads and heptads, respectively, and their intensities have been used to draw the percent of defects (meso dyads) in the polymer chains. On the hypothesis that chain defects are at the origin of chain folding and thus determine the thickness of crystalline lamellae, we performed differential scanning calorimetry (DSC) analysis on the same samples, and their thermal parameters were measured. A model was developed to determine the amount of steric defects from the DSC melting‐peak profiles, and the results obtained were compared with the NMR results. A satisfactory agreement was found (correlation factor 0.96) in the explored range of defect concentrations (up to 2.5% of meso dyads). The possible influence of the extraction procedure of the amorphous fraction was found to be negligible. Thus, information on stereochemistry can be obtained from DSC experiments starting from as‐prepared (not extracted) samples.

  相似文献   

6.
目的分析人早孕期蜕膜基质细胞趋化因子配基受体对CXCL16/CXCR6的表达及免疫活性细胞趋化因子受体CXCR6的表达,以探讨CXCL16/CXCR6在蜕膜免疫活性细胞募集中的可能规律.方法收集早孕期蜕膜组织,分离蜕膜基质细胞和免疫细胞,分别采用半定量RT-PCR、免疫细胞化学、流式细胞术分析蜕膜基质细胞CXCL16和CXCR6的表达;流式细胞术分析蜕膜CD56^+CD16^-NK细胞、CD56^+CD16^+NK细胞、NKT细胞、T细胞、γδT细胞、单核细胞CXCR6的表达.结果人早孕蜕膜基质细胞高水平转录趋化因子受体CXCR6,低水平转录其配体CXCL16,但CXCL16和CXCR6在蛋白水平的表达偏低.早孕蜕膜γδT细胞CXCR6阳性率为87.29%;CD14^+单核细胞CXCR6阳性率为47.71%;NKT细胞CXCR6阳性率为44.14%;T细胞CXCR6表达率为32.91%;而蜕膜两种NK细胞(CD56^+CD16^-、CD56^+CD16^+)几乎不表达CXCR6.结论人γδT细胞、单核细胞、NKT细胞、T细胞可能通过表达趋化因子受体CXCR6被募集到蜕膜局部并驻留,从而参与早孕期母胎界面的免疫调节.  相似文献   
7.
CORDIC算法在B超数字扫描变换器中的应用   总被引:1,自引:0,他引:1  
数字扫描变换器在B型超声诊断仪的应用,能使现代实时B型超声诊断仪实现一些新的诸如图像冻结、多帧贮存、数据测量计算和TV显示等功能。在设计B型超声诊断仪中数字扫描变化器的过程中,直角坐标到极坐标变换是一个关键的技术,本研究论述了应用在数字扫描变化器中的一种新的算法——CORDIC算法,对该算法的原理进行了简介,将CORDIC算法应用到直角——极坐标变换中,并进行了算法修正和公式计算。根据其具体的应用对该算法进行了优化,并给出了算法的硬件实现结构。最后,对算法进行了软件仿真,并给出了结果分析。  相似文献   
8.
马鞭草提取液对体外培养人早孕蜕膜细胞的影响   总被引:10,自引:0,他引:10  
目的:探讨马鞭草及米非司酮抗早孕的细胞学作用机理,初步确定马鞭草抗生育的有效部位。方法:实验选用早孕人工流产蜕膜组织进行体外培养,观察马鞭草提取液A、B、C、D及米非司酮对蜕膜细胞形态,增殖,细胞凋亡及细胞周期动力学的影响。结果:高于12.5mg/na的A、B、C及80ug/na的米非司同酮均可明显改变蜕膜基质细胞(DSC)的形态,并对其增殖产生显著的抑制作用。25mg/ml的A、B、C及米非司酮(80μg/na)均促进细胞凋亡,对细胞周期无明显影响。D均无明显作用。结论:马鞭草、米非司酮均有抗早孕作用。抑制蜕膜细胞生长,促进凋亡为其抗早孕机制之一。  相似文献   
9.
目的用差示扫描量热(DSC)法测定药物纯度及探讨影响测定结果的因素。方法用DSC法测定吲哚美辛等7种不同类别药物的纯度,并与《中国药典》规定方法结果进行对照。结果DSC法测定药物纯度的准确性好;试药的用量、纯度、升温速度对测定结果产生影响。结论本法测定高纯度药物简便、结果准确。  相似文献   
10.
Differential scanning calorimetry and Fourier transform infrared spectroscopy were applied as screening analytical methods to assess the solid-state compatibility of indapamide (4-chloro-N-(2-methyl-2,3-dihydroindol-1-yl)-3-sulfamoyl-benzamide) with several polymers aimed for development of 24?h sustained release solid-dosage formulation. After the initial research phase which was directed towards selection of suitable polymer matrices, based on their solid-state compatibility with the studied pharmaceutical active ingredient, the second phase of evaluation was intended for compatibility selection of other excipients required to complete a sustained release formulation. The preformulation studies have shown that polyvinylpyrrolydone/polyvinyl acetate might be considered incompatible with indapamide, and the implementation of this polymer career should be avoided in the case of the entitled development. The experimental data additionally have revealed that sorbitol is incompatible with indapamide. The obtained results afforded deeper insight in to the solid-state stability of the studied binary systems and pointed out directions for further development of indapamide sustained release solid-dosage formulation.  相似文献   
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