Characterising the geometric diversity of functional groups in chemical databases

Summary We have developed a program, HookSpace, which provides a simplistic approach to assessing the diversity of molecular databases. The spatial relationship between pairs of intramolecular functional groups can be analysed in a variety of ways to provide both qualitative and quantitative measures of diversity. Results are described and contrasted for two commercially available databases and a combinatorial library of benzodiazepam derivatives. HookSpace highlights the main differences in molecular content of these data sets.     

大花无柱兰遗传多样性的SRAP标记分析

大花无柱兰是一种珍稀兰科植物,具有一定的观赏和药用价值,但数量十分稀少,该物种亟待保护。本研究采用SRAP分子标记技术,对10个居群的115份DNA样品进行PCR扩增,并开展遗传多样性分析。从81对引物中筛选出9个条带清晰、多态性好、重复性高的引物组合,共扩增得到305条谱带。在物种水平上,多态性比率（PPB）为100%,Nei’s基因多样性指数（H）为0.209 8,Shannon’s指数（I）为0.340 2;在居群水平上,PPB为24.59%～52.13%,H为0.079 6～0.165 5,I为0.120 9～0.252 3。居群水平上,基因分化度（Gst）为0.520 9,基因流（Nm）为0.459 9,遗传距离为0.091 9～0.198 4。UPGMA聚类结果表明,10个居群可分为3大类,地理距离相近的居群优先聚集。大花无柱兰的遗传多样性较为丰富,居群间存在一定的遗传分化和基因交流,可采用就地保护和人工栽培等方式加以保护。     

Molecular and functional diversity of vascular endothelial growth factors

Summary Members of the vascular endothelial growth factor (VEGF) family are crucial regulators of neovascularization and are classified as cystine knot growth factors that specifically bind cellular receptor tyrosine kinases VEGFR-1, VEGFR-2, and VEGFR-3 with high but variable affinity and selectivity. The VEGF family has recently been expanded and currently comprises seven members: VEGF-A, VEGF-B, placenta growth factor (PlGF), VEGF-C, VEGF-D, viral VEGF (also known as VEGF-E), and snake venom VEGF (also known as VEGF-F). Although all members are structurally homologous, there is molecular diversity among the subtypes, and several isoforms, such as VEGF-A, VEGF-B, and PlGF, are generated by alternative exon splicing. These splicing isoforms exhibit differing properties, particularly in binding to co-receptor neuropilins and heparin. VEGF family proteins play multiple physiological roles, such as angiogenesis and lymphangiogenesis, while exogenous members (viral and snake venom VEGFs) display activities that are unique in physiology and function. This review will highlight the molecular and functional diversity of VEGF family proteins.     

Acquisition Time for Ground-to-Satellite Optical Communication System in Weak Atmospheric Turbulence with Spatial Diversity

Abstract

In this article, various issues involved in a ground-to-satellite optical communication link (i.e., acquisition time, uncertainty area, and channel noise) are discussed. Acquisition time of a free-space optical link is evaluated for coherent (sub-carrier BPSK and QPSK) and non-coherent (OOK and -PPM) modulation schemes over weak turbulent channel with transmit diversity. In the analysis, both uncorrelated and correlated beams are considered. It is seen that an increase in transmit diversity order helps to improve the acquisition time, irrespective of turbulence strength in the atmosphere. At high correlation, a marginal change in acquisition time is observed with the increase in diversity order.     

A hybrid metaheuristic method for the Maximum Diversity Problem

The Maximum Diversity Problem (MDP) consists in selecting a subset of m$m$ elements from a given set of n$n$ elements (n>m$n>m$) in such a way that the sum of the pairwise distances between the m$m$ chosen elements is maximized. We present a hybrid metaheuristic algorithm (denoted by MAMDP) for MDP. The algorithm uses a dedicated crossover operator to generate new solutions and a constrained neighborhood tabu search procedure for local optimization. MAMDP applies also a distance-and-quality based replacement strategy to maintain population diversity. Extensive evaluations on a large set of 120 benchmark instances show that the proposed approach competes very favorably with the current state-of-art methods for MDP. In particular, it consistently and easily attains all the best known lower bounds and yields improved lower bounds for 6 large MDP instances. The key components of MAMDP are analyzed to shed light on their influence on the performance of the algorithm.     

Activity-Directed Synthesis of Inhibitors of the p53/hDM2 Protein–Protein Interaction

Protein–protein interactions (PPIs) provide a rich source of potential targets for drug discovery and biomedical science research. However, the identification of structural-diverse starting points for discovery of PPI inhibitors remains a significant challenge. Activity-directed synthesis (ADS), a function-driven discovery approach, was harnessed in the discovery of the p53/hDM2 PPI. Over two rounds of ADS, 346 microscale reactions were performed, with prioritisation on the basis of the activity of the resulting product mixtures. Four distinct and novel series of PPI inhibitors were discovered that, through biophysical characterisation, were shown to have promising ligand efficiencies. It was thus shown that ADS can facilitate ligand discovery for a target that does not have a defined small-molecule binding site, and can provide distinctive starting points for the discovery of PPI inhibitors.     

Use and Abuse of Entropy in Biology: A Case for Caliber

Here, I discuss entropy and its use as a tool in fields of biology such as bioenergetics, ecology, and evolutionary biology. Statistical entropy concepts including Shannon’s diversity, configurational entropy, and informational entropy are discussed in connection to their use in describing the diversity, heterogeneity, and spatial patterning of biological systems. The use of entropy as a measure of biological complexity is also discussed, and I explore the extension of thermodynamic entropy principles to open, nonequilibrium systems operating in finite time. I conclude with suggestions for use of caliber, a metric similar to entropy but for time-dependent trajectories rather than static distributions, and propose the complementary notion of path information.     

Total Synthesis,Stereochemical Assignment,and Field‐Testing of the Sex Pheromone of the Strepsipteran Xenos peckii

The sex pheromone of the endoparasitoid insect Xenos peckii (Strepsiptera: Xenidae) was recently identified as (7E,11E)‐3,5,9,11‐tetramethyl‐7,11‐tridecadienal. Herein we report the asymmetric synthesis of three candidate stereostructures for this pheromone using a synthetic strategy that relies on an sp³–sp² Suzuki–Miyaura coupling to construct the correctly configured C7‐alkene function. Comparison of ¹H NMR spectra derived from the candidate stereostructures to that of the natural sex pheromone indicated a relative configuration of (3R*,5S*,9R*). Chiral gas chromatographic (GC) analyses of these compounds supported an assignment of (3R,5S,9R) for the natural product. Furthermore, in a 16‐replicate field experiment, traps baited with the synthetic (3R,5S,9R)‐enantiomer alone or in combination with the (3S,5R,9S)‐enantiomer captured 23 and 18 X. peckii males, respectively (mean±SE: 1.4±0.33 and 1.1±0.39), whereas traps baited with the synthetic (3S,5R,9S)‐enantiomer or a solvent control yielded no captures of males. These strong field trapping data, in combination with spectroscopic and chiral GC data, unambiguously demonstrate that (3R,5S,9R,7E,11E)‐3,5,9,11‐tetramethyl‐7,11‐tridecadienal is the X. peckii sex pheromone.