抗衰老药物对线虫生存曲线影响的荟萃分析

随着世界人口老龄化步伐的加快,衰老机制及抗衰老药物的研究日益成为生物医学领域的热点前沿之一.国内外已有大量研究报道抗衰老药物能够延长多种模式生物包括线虫、果蝇、小鼠、大鼠及灵长类等的寿命,然而,这些药物延缓衰老方式的差异仍缺乏系统研究.因此,本研究以衰老研究的热点模式生物线虫为对象,搜集1990年以来国内外刊物上正式发表的有关抗衰老药物寿命试验的研究文献及其涉及的生存曲线,利用荟萃分析比较了不同抗衰老药物与生存曲线变化类型间的关系,并结合药物的药理作用探讨其延寿机制.生存曲线特征聚类结果与药物生物学分类交叉分析结果表明,药理作用类型与增益类型具有很强相关性,提示这2种分类方法的结果是匹配的.抗氧化剂类药物和控制血糖类药物对生存曲线的改善总体增益虽然不是最高,但相对于正常组生存曲线其增益部分呈平移形,表明该类药物可以通过改善年龄结构对整个群体产生显著增益,且其衰老曲线的特征与自然衰老相似.抗癫痫药物及胃肠道菌群相关药物总体增益较大,其曲线增益形状呈梯形,提示该类药物(尤其是胃肠道菌群相关药物)尽管显著延长了少数个体的最大寿命,但是从整个群体来看,大多数个体寿命延长程度并不明显,受益的少数个体可能需要较长的外界资源支持方能保持较长时间的存活状态,这种模式既不大众化也不经济.综上所述,清除自由基和控制血糖类药物对健康老年有着更为积极合理的作用与效应.     

长白山林区核桃楸种群数量动态变化的研究

运用种群年龄结构、存活曲线统计和Leslie模型对长白山核桃楸种群在水胡林、针阔混交林、核桃楸占优杂木林和杂木林4种不同群落类型中种群数量动态变化进行了研究和预测。结果表明,核桃楸种群表现出衰退型的年龄结构特点,幼苗和幼树比例较小,种群在幼年期死亡率较高,反映出核桃楸种群15~20龄在个体经历了比较强烈的环境筛作用;Leslie模型预测显示,核桃楸幼苗数量和种群总数量在今后35年基本呈下降趋势,除在核桃楸占优的林分中种群维持增长外,在其它3中森林类型都表现出衰退趋势。因此,促进核桃楸的天然更新、加强幼苗幼树的抚育工作对长白山地区核桃楸种群的发展至关重要。     

模拟水流条件下初级生产力及光动力学参数

为探讨水动力作用及其他物理因子改变对湖泊初级生产力的影响 ,1999年 5月 8日～ 6月 2 4日在中国科学院太湖湖泊生态系统研究站大型生态实验槽内进行模拟水动力实验 ,分 3种水流状态 2种光强测定初级生产力及其他相关参数。分析了初级生产力、光合速率的垂直分布 ,光合速率随光强的变化 ,并借助光动力学模型拟合得到光动力学参数。结果表明 ,在静止状态下 ,当水表面光强大于 5 0 0μmol/ (m2 · s)时 ,0～ 0 .4 m处存在光抑制现象 ,最大初级生产力出现在 0 .4～ 0 .6 m,此后由于动力作用使水体悬浮物增加 ,改变了水下光照条件 ,致使最大初级生产力呈向上移动的趋势 ,出现在 0～ 0 .2 m间 ;光合速率在静止状态下随深度递减缓慢 ,而到大水流状态则递减极为迅速 ,大水流状态下的平均光合速率明显低于静止状态和小水流状态 ;基于 2种类型的光动力学模型进行非线性拟合得到的 P- I曲线相关性很好 ,2种模型模拟的结果比较接近 ,基本上能够反映太湖光合速率随光强变化的实际情况 ;在太湖这种大型浅水湖泊 ,水动力的作用使得水体中悬浮物增加 ,造成光强的迅速衰减 ,这可能会大大降低湖泊的初级生产过程     

北京东灵山地区辽东栎(Quercus liaotungensis)种群生活史特征与空间分布

种群生活史特征和空间分布格局对于分析种群演替动态规律、判定种群分布规律和预测种群演化过程及变化趋势均具有重要的理论和现实意义.本文从静态生命表、年龄结构、存活曲线三个方面分析了东灵山地区辽东栎种群的生活史特征.结果表明:物种生物学因素是影响辽东栎种群生存力最主要因素,辽东栎种群静态生命表中生命期望值逐渐降低反映出种群生存力下降的趋势.空间分布格局分析表明辽东栎种群各个径级的个体都属于聚集分布.辽东栎实生苗和萌生苗共存是辽东栎种群适应环境压力和与环境协同进化的结果,表明自然状态下辽东栎种群具有较高的稳定性.由于辽东栎种群的这种较强的稳定性和适应能力,随着辽东栎种群发育整个群落将趋于进展演替,最终形成稳定和充分利用环境资源的顶极群落结构.     

阔叶树的叶形曲线方程：—适于叶面积计算的数学模型

树木的叶形可以看作一个平面几何图形。这种几何图形可用解析方程给予表达,我们把这种解析方程称为叶形曲线方程。由于叶形是一个左右对称,而上下不对称的图形,也就是说叶的最宽处绝大多数不在叶的中部,少数在     

山西霍山油松林的物种多度分布格局

物种多度格局分析对理解群落结构具有重要的意义。该文首次选用描述种-多度关系的生态位模型(生态位优先模型NPM、分割线段模型BSM、生态位重叠模型ONM)、生物统计模型(对数级数分布模型LSD、对数正态分布模型LN)以及中性理论模型NT, 对山西霍山油松(Pinus tabulaeformis)林的物种数量关系进行了拟合研究, 并采用卡方(χ²)检验、Likelihood-ratios (L-R)检验、Kolmogorov-Smirnov (K-S)检验和赤池信息量准则(AIC)选择最适合模型, 结果表明: (1)描述乔木层物种多度格局的最优生态位模型为NPM (3种检验方法均接受该模型, p > 0.05, 且该模型具有最小的 AIC值), ONM的拟合效果次之, 不服从BSM; 三种生态位模型均可较好地拟合灌木层物种多度格局; ONM是草本层最佳生态位模型, BSM、NPM拟合效果较差; LSD可以描述油松林各层物种多度结构; LN可以很好地解释灌草层物种数量关系; NT不能解释油松林任何层次的物种多度结构。(2)霍山油松林乔木层和灌木层的物种丰富度和物种多样性均明显小于草本层; 该群落物种富集种少而稀疏种多, 且群落的均匀度相对较小。(3)从该区油松林种-多度分布来看, 同一个模型可以拟合不同的物种多度数据, 相同的数据可以由不同的模型来解释。因此, 研究森林群落物种分布时, 应采用多个模型进行拟合, 同时选用多种方法筛选最优模型。     

Community-wide assessment of protein-interface modeling suggests improvements to design methodology

The CAPRI (Critical Assessment of Predicted Interactions) and CASP (Critical Assessment of protein Structure Prediction) experiments have demonstrated the power of community-wide tests of methodology in assessing the current state of the art and spurring progress in the very challenging areas of protein docking and structure prediction. We sought to bring the power of community-wide experiments to bear on a very challenging protein design problem that provides a complementary but equally fundamental test of current understanding of protein-binding thermodynamics. We have generated a number of designed protein-protein interfaces with very favorable computed binding energies but which do not appear to be formed in experiments, suggesting that there may be important physical chemistry missing in the energy calculations. A total of 28 research groups took up the challenge of determining what is missing: we provided structures of 87 designed complexes and 120 naturally occurring complexes and asked participants to identify energetic contributions and/or structural features that distinguish between the two sets. The community found that electrostatics and solvation terms partially distinguish the designs from the natural complexes, largely due to the nonpolar character of the designed interactions. Beyond this polarity difference, the community found that the designed binding surfaces were, on average, structurally less embedded in the designed monomers, suggesting that backbone conformational rigidity at the designed surface is important for realization of the designed function. These results can be used to improve computational design strategies, but there is still much to be learned; for example, one designed complex, which does form in experiments, was classified by all metrics as a nonbinder.     

PV技术的计算机处理及其在树木水分关系研究中的应用

ＰＶ技术的计算机处理及其在树木水分关系研究中的应用刘建伟,刘雅荣,王世绩（中国林业科学研究院林业研究所,北京１０００９１）ＣｏｍｐｕｔｅｒＰｒｏｃｅｓｓｉｎｇｏｆＰＶＣｕｒｖｅＡｎａｌｙｓｉｓａｎｄＩｔｓＡｐｐｌｉｃａｔｉｏｎｉｎｔｈｅＲｅｓｅａｒｃ...     

A strategy for modelling dynamic responses in metabolic samples characterized by GC/MS

A multivariate strategy for studying the metabolic response over time in urinary GC/MS data is presented and exemplified by a study of drug-induced liver toxicity in the rat. The strategy includes the generation of representative data through hierarchical multivariate curve resolution (H-MCR), highlighting the importance of obtaining resolved metabolite profiles for quantification and identification of exogenous (drug related) and endogenous compounds (potential biomarkers) and for allowing reliable comparisons of multiple samples through multivariate projections. Batch modelling was used to monitor and characterize the normal (control) metabolic variation over time as well as to map the dynamic response of the drug treated animals in relation to the control. In this way treatment related metabolic responses over time could be detected and classified as being drug related or being potential biomarkers. In summary the proposed strategy uses the relatively high sensitivity and reproducibility of GC/MS in combination with efficient multivariate curve resolution and data analysis to discover individual markers of drug metabolism and drug toxicity. The presented results imply that the strategy can be of great value in drug toxicity studies for classifying metabolic markers in relation to their dynamic responses as well as for biomarker identification.     

Evaluation of antifungal pharmacodynamic characteristics of AmBisome against Candida albicans

A liposomal formulation of Amphotericin B (AmBisome), with small unilamellar vesicles containing amphotericin B, shows characteristic pharmacokinetics as liposomes, and in consequence, has different pharmacological activity and toxicity from amphotericin B deoxycholate (Fungizone). In this study, we evaluated the antifungal pharmacodynamic characteristics of AmBisome against Candida albicans using the in vitro time-kill method and murine systemic infection model. A time-kill study indicated that the in vitro fungicidal activities of AmBisome and Fungizone against C. albicans ATCC 90029 increased with increasing drug concentration. For in vivo experiments, leucopenic mice were infected intravenously with the isolate 4 hr prior to the start of therapy. The infected mice were treated for 24 hr with twelve dosing regimens of AmBisome administered at 8-, 12-, 24-hr dosing intervals. Correlation analysis between the fungal burden in the kidney after 24 hr of therapy and each pharmacokinetic/pharmacodynamic parameter showed that the peak level/MIC ratio was the best predictive parameter of the in vivo outcome of AmBisome. These results suggest that AmBisome, as well as Fungizone, has concentration-dependent antifungal activity. Furthermore, since AmBisome can safely achieve higher concentrations in serum than Fungizone, AmBisome is thought to have superior potency to Fungizone against fungal infections.