ABSTRACT
The global decline of freshwater mussels and their crucial ecological services highlight the need to understand their phylogeny, phylogeography and patterns of genetic diversity to guide conservation efforts. Such knowledge is urgently needed for Unio crassus, a highly imperilled species originally widespread throughout Europe and southwest Asia. Recent studies have resurrected several species from synonymy based on mitochondrial data, revealing U. crassus to be a complex of cryptic species. To address long-standing taxonomic uncertainties hindering effective conservation, we integrate morphometric, phylogenetic, and phylogeographic analyses to examine species diversity within the U. crassus complex across its entire range. Phylogenetic analyses were performed using cytochrome c oxidase subunit I (815 specimens from 182 populations) and, for selected specimens, whole mitogenome sequences and Anchored Hybrid Enrichment (AHE) data on â¼ 600 nuclear loci. Mito-nuclear discordance was detected, consistent with mitochondrial DNA gene flow between some species during the Pliocene and Pleistocene. Fossil-calibrated phylogenies based on AHE data support a Mediterranean origin for the U. crassus complex in the Early Miocene. The results of our integrative approach support 12 species in the group: the previously recognised Unio bruguierianus, Unio carneus, Unio crassus, Unio damascensis, Unio ionicus, Unio sesirmensis, and Unio tumidiformis, and the reinstatement of five nominal taxa: Unio desectusstat. rev., Unio gontieriistat. rev., Unio mardinensisstat. rev., Unio nanusstat. rev., and Unio vicariusstat. rev. Morphometric analyses of shell contours reveal important morphospace overlaps among these species, highlighting cryptic, but geographically structured, diversity. The distribution, taxonomy, phylogeography, and conservation of each species are succinctly described.
Subject(s)
Unio , Animals , Phylogeny , Phylogeography , Unio/genetics , Europe , DNA, Mitochondrial/genetics , Genetic VariationABSTRACT
A single incompressible, inviscid, irrotational fluid medium bounded by a free surface and varying bottom is considered. The Hamiltonian of the system is expressed in terms of the so-called Dirichlet-Neumann operators. The equations for the surface waves are presented in Hamiltonian form. Specific scaling of the variables is selected which leads to approximations of Boussinesq and Korteweg-de Vries (KdV) types, taking into account the effect of the slowly varying bottom. The arising KdV equation with variable coefficients is studied numerically when the initial condition is in the form of the one-soliton solution for the initial depth.This article is part of the theme issue 'Nonlinear water waves'.
ABSTRACT
Animals and humans are exposed to a wide array of xenobiotics and have developed complex enzymatic mechanisms to detoxify these chemicals. Detoxification pathways involve a number of biotransformations, such as oxidation, reduction, hydrolysis and conjugation reactions. The intermediate substances created during the detoxification process can be extremely toxic compared with the original toxins, hence metabolism should be accounted for when hazard effects of chemicals are assessed. Alternatively, metabolic transformations could detoxify chemicals that are toxic as parents. The aim of the present paper is to describe specificity of eukaryotic metabolism and its simulation and incorporation in models for predicting skin sensitization, mutagenicity, chromosomal aberration, micronuclei formation and estrogen receptor binding affinity implemented in the TIMES software platform. The current progress in model refinement, data used to parameterize models, logic of simulating metabolism, applicability domain and interpretation of predictions are discussed. Examples illustrating the model predictions are also provided.
Subject(s)
Computer Simulation , Mammals/metabolism , Models, Biological , Risk Assessment , Xenobiotics/metabolism , Xenobiotics/toxicity , Animals , Biotransformation , Humans , Metabolic Networks and Pathways , Models, Statistical , Quantitative Structure-Activity RelationshipABSTRACT
The multiparameter formulation of the COmmon REactivity PAttern (COREPA) approach has been used to describe the structural requirements for eliciting rat androgen receptor (AR) binding affinity, accounting for molecular flexibility. Chemical affinity for AR binding was related to the distances between nucleophilic sites and structural features describing electronic and hydrophobic interactions between the receptor and ligands. Categorical models were derived for each binding affinity range in terms of specific distances, local (maximal donor delocalizability associated with the oxygen atom of the A ring), global nucleophilicity (partial positive surface areas and energy of the highest occupied molecular orbital) and hydrophobicity (log Kow) of the molecules. An integral screening tool for predicting binding affinity to AR was constructed as a battery of models, each associated with different activity bins. The quality of the screening battery of models was assessed using a high value (0.9) of the Pearson contingency coefficient. The predictability of the model was assessed by testing the model performance on external validation sets. A recently developed technique for selection of potential androgenically active chemicals was used to test the performance of the model in its applicability domain. Some of the selected chemicals were tested for AR transcriptional activation. The experimental results confirmed the theoretical predictions.
Subject(s)
Androgens/chemistry , Androgens/pharmacology , Quantitative Structure-Activity Relationship , Receptors, Androgen/metabolism , Androgens/metabolism , Animals , Drug Evaluation, Preclinical/methods , Models, Chemical , Models, Statistical , Protein Binding , RatsABSTRACT
Our previous work has investigated the utility of mutagenicity data in the development and application of Integrated Testing Strategies (ITS) for skin sensitization by focusing on the chemical mechanisms at play and substantiating these with experimental data where available. The hybrid expert system TIMES (Tissue Metabolism Simulator) was applied in the identification of the chemical mechanisms since it encodes a comprehensive set of established structure-activity relationships for both skin sensitization and mutagenicity. Based on the evaluation, the experimental determination of mutagenicity was thought to be potentially helpful in the evaluation of skin sensitization potential. This study has evaluated the dataset reported by Wolfreys and Basketter (Cutan. Ocul. Toxicol. 23 (2004), pp. 197-205). Upon an update of the experimental data, the original reported concordance of 68% was found to increase to 88%. There were several compounds that were 'outliers' in the two experimental evaluations which are discussed from a mechanistic basis. The discrepancies were found to be mainly associated with the differences between skin and liver metabolism. Mutagenicity information can play a significant role in evaluating sensitization potential as part of an ITS though careful attention needs to be made to ensure that any information is interpreted in the appropriate context.
Subject(s)
Mutagens/toxicity , Skin/drug effects , Mutagenicity Tests , Mutagens/chemistry , Quantitative Structure-Activity Relationship , Skin Tests/methodsABSTRACT
To develop quantitative structure-activity relationships (QSAR) models capable of predicting adverse effects for large chemical inventories and diverse structures, an interactive approach is presented that includes testing of strategically selected chemicals to expand the scope of a preliminary model to cover a target inventory. The goal of chemical selection in this context is to make the testing more effective in terms of adding maximal new structural information to the predictive model with minimal testing. The aim of this paper is to describe a set of algorithmic solutions and modelling techniques that can be used to efficiently select chemicals for testing to achieve a variety of goals. One purpose of chemical selection is to refine the model thus extending our knowledge about the modelled subject. Alternatively, the selection of chemicals for testing could be targeted at achieving a more adequate structural representation of a specific universe of untested chemicals to extend the model applicability domain on each subsequent step of model development. The chemical selection tools are collectively provided in a software package referred to as ChemPick. The system also allows the visualisation of chemical inventories and training sets in multidimensional (two and three dimensions) descriptor space. The software environment allows one or more datasets to be simultaneously loaded in a three-dimensional (or N-dimensional) chart where each point represents a combination of values for the descriptors for a given conformation of a chemical. The application of the chemical selection tools to select chemicals to expand a preliminary model of human oestrogen receptor (hER) ligand binding to more adequately cover a diverse chemical inventory is presented to demonstrate the application of these tools.
Subject(s)
Forecasting/methods , Organic Chemicals/adverse effects , Organic Chemicals/chemistry , Quantitative Structure-Activity Relationship , Algorithms , HumansABSTRACT
A multi-dimensional formulation of the COmmon REactivity PAttern (COREPA) modeling approach has been used to investigate chemical binding to the human estrogen receptor (hER). A training set of 645 chemicals included 497 steroid and environmental chemicals (database of the Chemical Evaluation and Research Institute, Japan - CERI) and 148 chemicals to further explore hER-structure interactions (selected J. Katzenellenbogen references). Upgrades of modeling approaches were introduced for multivariate COREPA analysis, optimal conformational generation and description of the local hydrophobicity of chemicals. Analysis of reactivity patterns based on the distance between nucleophilic sites resulted in identification of distinct interaction types: a steroid-like A-B type described by frontier orbital energies and distance between nucleophilic sites with specific charge requirements; an A-C type where local hydrophobic effects are combined with electronic interactions to modulate binding; and mixed A-B-C (AD) type. Chemicals were grouped by type, then COREPA models were developed for within specific relative binding affinity ranges of >10%, 10 > RBA > or = 0.1%, and 0.1 > RBA > 0.0%. The derived models for each interaction type and affinity range combined specific prefiltering requirements (interatomic distances) and a COREPA classification node using no more than 2 discriminating parameters. The interaction types are becoming less distinct in the lowest activity range for each chemicals of each type; here, the modeling was performed within chemical classes (phenols, phthalates, etc.). The ultimate model was organized as a battery of local models associated to interaction type and mechanism.
Subject(s)
Endocrine Disruptors/chemistry , Receptors, Estrogen/chemistry , Humans , Hydrophobic and Hydrophilic Interactions , Ligands , Models, Chemical , Molecular Structure , Multivariate Analysis , Quantitative Structure-Activity Relationship , Risk AssessmentABSTRACT
The tissue metabolic simulator (TIMES) modeling approach is a hybrid expert system that couples a metabolic simulator together with structure toxicity rules, underpinned by structural alerts, to predict interaction of chemicals or their metabolites with target macromolecules. Some of the structural alerts representing the reactivity pattern-causing effect could interact directly with the target whereas others necessitated a combination with two- or three-dimensional quantitative structure-activity relationship models describing the firing of the alerts from the rest of the molecules. Recently, TIMES has been used to model bacterial mutagenicity [Mekenyan, O., Dimitrov, S., Serafimova, R., Thompson, E., Kotov, S., Dimitrova, N., and Walker, J. (2004) Identification of the structural requirements for mutagenicity by incorporating molecular flexibility and metabolic activation of chemicals I: TA100 model. Chem. Res. Toxicol. 17 (6), 753-766]. The original model was derived for a single tester strain, Salmonella typhimurium (TA100), using the Ames test by the National Toxicology Program (NTP). The model correctly identified 82% of the primary acting mutagens, 94% of the nonmutagens, and 77% of the metabolically activated chemicals in a training set. The identified high correlation between activities across different strains changed the initial strategic direction to look at the other strains in the next modeling developments. In this respect, the focus of the present work was to build a general mutagenicity model predicting mutagenicity with respect to any of the Ames tester strains. The use of all reactivity alerts in the model was justified by their interaction mechanisms with DNA, found in the literature. The alerts identified for the current model were analyzed by comparison with other established alerts derived from human experts. In the new model, the original NTP training set with 1341 structures was expanded by 1626 proprietary chemicals provided by BASF AG. Eventually, the training set consisted of 435 chemicals, which are mutagenic as parents, 397 chemicals that are mutagenic after S9 metabolic activation, and 2012 nonmutagenic chemicals. The general mutagenicity model was found to have 82% sensitivity, 89% specificity, and 88% concordance for training set chemicals. The model applicability domain was introduced accounting for similarity (structural, mechanistic, etc.) between predicted chemicals and training set chemicals for which the model performs correctly.
Subject(s)
Models, Biological , Mutagens/chemistry , Mutagens/pharmacology , Pharmaceutical Preparations/metabolism , Computer Simulation , DNA/genetics , Databases, Genetic , Molecular Structure , Mutagens/metabolismABSTRACT
STUDY DESIGN: An anamnestic, clinical, radiographic study of 100 girls actively engaged in rhythmic gymnastics was performed in an attempt to explain the higher incidence and the specific features of scoliosis in rhythmic gymnastic trainees. OBJECTIVES: To analyze the anthropometry, the regimen of motion and dieting, the specificity of training in rhythmic gymnastics, and the growth and maturing of the trainees, and to outline the characteristics of the scoliotic curves observed. An etiologic hypothesis for this specific subgroup of scoliosis is proposed. SUMMARY OF BACKGROUND DATA: The etiology of scoliosis remains unknown in most cases despite extensive research. In the current classifications, no separate type of sports-associated scoliosis is suggested. METHODS: The examinations included anamnesis, weight and height measurements, growth and maturing data, eating regimen, general and back status, duration, intensity, and specific elements of rhythmic gymnastic training. Radiographs were taken in all the patients with suspected scoliosis. The results obtained were compared with the parameters of normal girls not involved in sports. RESULTS: A 10-fold higher incidence of scoliosis was found in rhythmic gymnastic trainees (12%) than in their normal coevals (1.1%). Delay in menarche and generalized joint laxity are common in rhythmic gymnastic trainees. The authors observed a significant physical loading with the persistently repeated asymmetric stress on the growing spine associated with the nature of rhythmic gymnastics. Some specific features of scoliosis related to rhythmic gymnastics were found also. CONCLUSIONS: This study identified a separate scoliotic entity associated with rhythmic gymnastics. The results strongly suggest the important etiologic role of a "dangerous triad": generalized joint laxity, delayed maturity, and asymmetric spinal loading.
Subject(s)
Gymnastics/statistics & numerical data , Scoliosis/epidemiology , Scoliosis/physiopathology , Adolescent , Child , Female , Humans , Incidence , Joints/physiology , Motor Activity , Posture , Radiography , Risk Factors , Scoliosis/diagnostic imaging , Spine/physiology , Weight-BearingABSTRACT
Two cases of tubercular meningitis, with a course under the form of severe acute encephalitis are discussed. The significance of those forms are emphasized, especially from diagnostic point of view, and the importance of the paraclinical investigations are stressed upon as well as the epidemiological data for the diagnosis.
