Detection of Single Nucleotide Polymorphism Rs2013162 of IRF6 Gene in Patient with Cleft Lip and Palate

Background: Cleft lip and palate are congenital disorders which induce affected individuals medically, socially and psychologically. The objective of this study was to investigate the association of Single Nucleotide Polymorphism(SNP); rs2013162 of IRF6 Gene in Patient with Cleft Lip and Palate. Materials and Methods: Fifty patients with non-syndromic CL/P were included in present study alongwith fifty individuals with no psychiatric history as controls. In all of the these individuals, search for Single nucleotide polymorphism was carried out by designing sequence specific primers. The sequence was amplified by using Real time PCR and products were investigated by visualizing high resolution melting curve upon HRM-PCR. Results: The logistic regression and Hardy-Weinberg equilibrium were applied to investigate the association of IRF6 SNP rs2013162 with disease. Results revealed no association of this polymorphism with non-syndromic CL/P. Conclusion: We found no association of IRF6 SNP rs2013162 in patients with non-syndromic CL/P. Further study is required with larger sample size to validate the findings of the present study in Pakistani population and along with this SNP other polymorphisms of the same gene should be analyzed to find out the association with the non-syndromic CL/P

Novel cyclic di-GMP effectors of the YajQ protein family control bacterial virulence

Bis-(3 ',5 ') cyclic di-guanylate (cyclic di-GMP) is a key bacterial second messenger that is implicated in the regulation of many critical processes that include motility, biofilm formation and virulence. Cyclic di-GMP influences diverse functions through interaction with a range of effectors. Our knowledge of these effectors and their different regulatory actions is far from complete, however. Here we have used an affinity pull-down assay using cyclic di-GMP-coupled magnetic beads to identify cyclic di-GMP binding proteins in the plant pathogen Xanthomonas campestris pv. campestris (Xcc). This analysis identified XC_3703, a protein of the YajQ family, as a potential cyclic di-GMP receptor. Isothermal titration calorimetry showed that the purified XC_3703 protein bound cyclic di-GMP with a high affinity (K-d similar to 2 mu M). Mutation of XC_3703 led to reduced virulence of Xcc to plants and alteration in biofilm formation. Yeast two-hybrid and far-western analyses showed that XC_3703 was able to interact with XC_2801, a transcription factor of the LysR family. Mutation of XC_2801 and XC_3703 had partially overlapping effects on the transcriptome of Xcc, and both affected virulence. Electromobility shift assays showed that XC_3703 positively affected the binding of XC_2801 to the promoters of target virulence genes, an effect that was reversed by cyclic di-GMP. Genetic and functional analysis of YajQ family members from the human pathogens Pseudomonas aeruginosa and Stenotrophomonas maltophilia showed that they also specifically bound cyclic di-GMP and contributed to virulence in model systems. The findings thus identify a new class of cyclic di-GMP effector that regulates bacterial virulence

A Transformation-based Implementation for CLP with Qualification and Proximity

Uncertainty in logic programming has been widely investigated in the last decades, leading to multiple extensions of the classical LP paradigm. However, few of these are designed as extensions of the well-established and powerful CLP scheme for Constraint Logic Programming. In a previous work we have proposed the SQCLP (proximity-based qualified constraint logic programming) scheme as a quite expressive extension of CLP with support for qualification values and proximity relations as generalizations of uncertainty values and similarity relations, respectively. In this paper we provide a transformation technique for transforming SQCLP programs and goals into semantically equivalent CLP programs and goals, and a practical Prolog-based implementation of some particularly useful instances of the SQCLP scheme. We also illustrate, by showing some simple-and working-examples, how the prototype can be effectively used as a tool for solving problems where qualification values and proximity relations play a key role. Intended use of SQCLP includes flexible information retrieval applications.Comment: 49 pages, 5 figures, 1 table, preliminary version of an article of the same title, published as Technical Report SIC-4-10, Universidad Complutense, Departamento de Sistemas Inform\'aticos y Computaci\'on, Madrid, Spai

Advances in Rule-based Modeling: Compartments, Energy, and Hybrid Simulation, with Application to Sepsis and Cell Signaling

Biological systems are commonly modeled as reaction networks, which describe the system at the resolution of biochemical species. Cellular systems, however, are governed by events at a finer scale: local interactions among macromolecular domains. The multi-domain structure of macromolecules, combined with the local nature of interactions, can lead to a combinatorial explosion that pushes reaction network methods to their limits. As an alternative, rule-based models (RBMs) describe the domain-based structure and local interactions found in biological systems. Molecular complexes are represented by graphs: functional domains as vertices, macromolecules as groupings of vertices, and molecular bonding as edges. Reaction rules, which describe classes of reactions, govern local modifications to molecular graphs, such as binding, post-translational modification, and degradation. RBMs can be transformed to equivalent reaction networks and simulated by differential or stochastic methods, or simulated directly with a network-free approach that avoids the problem of combinatorial complexity. Although RBMs and network-free methods resolve many problems in systems modeling, challenges remain. I address three challenges here: (i) managing model complexity due to cooperative interactions, (ii) representing biochemical systems in the compartmental setting of cells and organisms, and (iii) reducing the memory burden of large-scale network-free simulations. First, I present a general theory of energy-based modeling within the BioNetGen framework. Free energy is computed under a pattern-based formalism, and contextual variations within reaction classes are enumerated automatically. Next, I extend the BioNetGen language to permit description of compartmentalized biochemical systems, with treatment of volumes, surfaces and transport. Finally, a hybrid particle/population method is developed to reduce memory requirements of network-free simulations. All methods are implemented and available as part of BioNetGen. The remainder of this work presents an application to sepsis and inflammation. A multi-organ model of peritoneal infection and systemic inflammation is constructed and calibrated to experiment. Extra-corporeal blood purification, a potential treatment for sepsis, is explored in silico. Model simulations demonstrate that removal of blood cytokines and chemokines is a sufficient mechanism for improved survival in sepsis. However, differences between model predictions and the latest experimental data suggest directions for further exploration