Prediction of quaternary structure from primary structure

MOTIVATION: The 'sequence implies conformation' principle has been the motivation for the construction of numerous systems of secondary and tertiary structure prediction. Computational experiments have shown that this principle can now be extended to quaternary structure prediction. This work appears to be the first effort to predict quaternary structure properties from sequence. RESULTS: The software developed to conduct these experiments was the Quaternary Structure Explorer (QSE). Successful rule-based classifiers have been found that can discriminate between the primary sequences of homodimers and non-homodimers.     

Serpin crystal structure and serpin polymer structure

Serpins are a family of structurally homologous proteins having metastable native structures. As a result, a serpin variant destabilized by mutation(s) has a tendency to undergo conformational changes leading to inactive forms, e.g., the latent form and polymer. Serpin polymers are involved in a number of conformational diseases. Although several models for polymer structure have been proposed, the actual structure remains unknown. Here, we provide a comprehensive list of serpins, both free and in complexes, deposited in the Protein Data Bank. Our discussion focuses on structures that potentially can contribute to a better understanding of polymer structure.     

Protein structure search and local structure characterization

Background  

Structural similarities among proteins can provide valuable insight into their functional mechanisms and relationships. As the number of available three-dimensional (3D) protein structures increases, a greater variety of studies can be conducted with increasing efficiency, among which is the design of protein structural alphabets. Structural alphabets allow us to characterize local structures of proteins and describe the global folding structure of a protein using a one-dimensional (1D) sequence. Thus, 1D sequences can be used to identify structural similarities among proteins using standard sequence alignment tools such as BLAST or FASTA.     

Population structure of stream-dwelling darters: correspondence with habitat structure

Synopsis Patterns of ecotopic variation in the population structure of two common and relatedPercina species were examined among seven central Gulf-Coast stream sites by Kendall's concordance tests, revealing four complexes of variables with significant covariation from a total of 18 population and habitat variables. The first complex comprised three interrelated habitat variables, implying that mid-stream surface current varied inversely with both instream cover and substrate heterogeneity. The second complex of five interrelated variables revealed (1) that darter abundance was better correlated with the area of instream cover than with total area, and (2) that site density [number m^-2] varied inversely with site area. Along with three other variables, cover density (number per square meter of instream cover) formed a third complex, demonstrating resource complementarity between instream cover and macroinvertebrate abundance. Variables within the fourth complex all increased concomitantly with the key variable of mean darter size, including body-size diversity, biomass, relative abundance of the two darter species and mid-stream depth. Within the study region, local ecological factors largely regulate distributions, abundances and size-structures ofPercina populations, apparently even outweighing the effects of stochastic and historical factors     

Three-dimensional structure of acylphosphatase. Refinement and structure analysis.

We report here the complete determination of the solution structure of acylphosphatase, a small enzyme that catalyses the hydrolysis of organic acylphosphates, as determined by distance geometry methods based on nuclear magnetic resonance information. A non-standard strategy for the distance geometry calculations was used and is described here some detail. The five best structures were then refined by restrained energy minimization and molecular dynamics in order to explore the conformational space consistent with the experimental data. We address the question of whether the solution structure of acylphosphatase follows the general principles of protein structure, i.e. those learned from analysing crystal structures. Static and dynamic features are discussed in detail. An uncommon beta-alpha-beta motif, so far found only in procarboxypeptidase B and in an RNA-binding protein, is present in acylphosphatase.     

Protein structure comparison by probability-based matching of secondary structure elements

MOTIVATION: Protein structure comparison (PSC) has been used widely in studies of structural and functional genomics. However, PSC is computationally expensive and as a result almost all of the PSC methods currently in use look only for the optimal alignment and ignore many alternative alignments that are statistically significant and that may provide insight into protein evolution or folding. RESULTS: We have developed a new PSC method with efficiency to detect potentially viable alternative alignments in all-against-all database comparisons. The efficiency of the new PSC method derives from the ability to directly home in on a limited number of viable and ranked alignment solutions based on intuitively derived SSE (secondary structure element)-matching probabilities.     

The structure of protein evolution and the evolution of protein structure

The observed distribution of protein structures can give us important clues about the underlying evolutionary process, imposing important constraints on possible models. The availability of results from an increasing number of genome projects has made the development of these models an active area of research. Models explaining the observed distribution of structures have focused on the inherent functional capabilities and structural properties of different folds and on the evolutionary dynamics. Increasingly, these elements are being combined.     

Biogenesis and revised structure of rosellisin; structure of rosellisin aldehyde

On the basis of new data from biogenetic studies on rosellisin, the positions of the 3-OMe and the 4-CH₂OH have been interchanged, resulting in a revised structure. A new metabolite has been identified as rosellisin aldehyde.     

Effect of superhelical structure on the secondary structure of DNA rings

A quantity, called the linking number, is defined, which specifies the total number of twists in a circular helix. The linking number is invariant under continuous deformations of the ring and therefore enables one to calculate the influence of superhelical structures on the secondary helix of a circular molecule. The linking number can be determined by projecting the helix into a plane and counting strand crosses in the projection as described. For example, it has been shown that for each 180° twist in a left-handed superhelix, a right-handed 360° twist is removed from the secondary helix, thus allowing local unwinding.     

Integrin structure

The integrins are a family of alpha,beta heterodimeric receptors that mediate dynamic linkages between extracellular adhesion molecules and the intracellular actin cytoskeleton. Integrins are expressed by all multicellular animals, but their diversity varies widely among species; for example, in mammals, 19 alpha and 8 beta subunit genes encode polypeptides that combine to form 25 different receptors, whereas the Drosophila and Caenorhabditis genomes encode only five and two integrin alpha subunits respectively. Thousands of studies over the last two decades have investigated the molecular, cellular and organismal basis of integrin function. Gene deletion has demonstrated essential roles for almost all integrins, with the defects suggesting widespread contributions to both the maintenance of tissue integrity and the promotion of cellular migration. Integrin-ligand interactions are now considered to provide physical support for cells in order to maintain cohesion, to permit the generation of traction forces to enable movement, and to organize signalling complexes to modulate differentiation and cell fate. Animal-model studies have also shown that integrins contribute to the progression of many common diseases, and have implicated them as potential therapeutic targets. The use of anti-integrin monoclonal antibodies and ligand-mimetic peptides has validated this suggestion for inflammatory, neoplastic, traumatic and infectious conditions. Thus, to understand more about the mechanisms underlying tissue organization and cellular trafficking, and to identify approaches for regulating these processes in disease, there is intense interest in determining the molecular basis of integrin function. It is important to state at the outset that the tertiary structure of the integrin dimer is unknown. Our current understanding of the molecular basis of integrin function is therefore compiled from the results of a large number of studies that have employed a wide range of complementary technologies.     

Electroencephalogram structure

The representation of an electroencephalogram as a convolution of harmonic functions having negative decrements with discrete (evenly discontinuous) white Gaussian noise was considered. A substantiation of this representation is given. It was numerically shown that the convolution of the decrement damping alpha-rhythm of one frequency with discrete white noise is a narrow-band chaos, an irregular spindle-shaped activity, which results in the appearance of close spectral components in the spectrum of power. The estimation of the autocorrelation function represented a damping cosinusoid shifted in phase depending of the factor of fading. The absolute value of convolution described an envelope of the output signal. The average duration of spindles decreased as the module of the decrement increased.