Italienische Sprüche

ITALIENISCHE SPRÜCHE Italienische Sprüche ( - ) Einband ( - ) Titelseite ( - ) Vorwort ( - ) Lektionen 1. - 39. (2) Teil II. (36) Deutsche Sprichwörter ... (70) Italienische Redensarten. (74) Postscritto. (78

Solving the post enrolment course timetabling problem by ant colony optimization.

Abstract In this work we present a new approach to tackle the problem of Post Enrolment Course Timetabling as specified for the International Timetabling Competition 2007 (ITC2007), competition track 2. The heuristic procedure is based on Ant Colony Optimization (ACO) where artificial ants successively construct solutions based on pheromones (stigmergy) and local information. The key feature of our algorithm is the use of two distinct but simplified pheromone matrices in order to improve convergence but still provide enough flexibility for effectively guiding the solution construction process. We show that by parallelizing the algorithm we can improve the solution quality significantly. We applied our algorithm to the instances used for the ITC2007. The results document that our approach is among the leading algorithms for this problem; in all cases the optimal solution could be found. Furthermore we discuss the characteristics of the instances where the algorithm performs especially well

Glucose induces anion conductance and cytosol-to-membrane transposition of ICln in INS-1E rat insulinoma cells

The metabolic coupling of insulin secretion by pancreatic beta cells is mediated by membrane depolarization due to increased glucose-driven ATP production and closure of K(ATP) channels. Alternative pathways may involve the activation of anion channels by cell swelling upon glucose uptake. In INS-1E insulinoma cells superfusion with an isotonic solution containing 20 mM glucose or a 30% hypotonic solution leads to the activation of a chloride conductance with biophysical and pharmacological properties of anion currents activated in many other cell types during regulatory volume decrease (RVD), i.e. outward rectification, inactivation at positive membrane potentials and block by anion channel inhibitors like NPPB, DIDS, 4-hydroxytamoxifen and extracellular ATP. The current is not inhibited by tolbutamide and remains activated for at least 10 min when reducing the extracellular glucose concentration from 20 mM to 5 mM, but inactivates back to control levels when cells are exposed to a 20% hypertonic extracellular solution containing 20 mM glucose. This chloride current can likewise be induced by 20 mM 3-Omethylglucose, which is taken up but not metabolized by the cells, suggesting that cellular sugar uptake is involved in current activation. Fluorescence resonance energy transfer (FRET) experiments show that chloride current activation by 20 mM glucose and glucose-induced cell swelling are accompanied by a significant, transient redistribution of the membrane associated fraction of ICln, a multifunctional 'connector hub' protein involved in cell volume regulation and generation of RVD currents

A new gene-finding tool: Using the caenorhabditis elegans operons for identifying functional partner-proteins in human cells

Abstract: How can a large number of different phenotypes be generated by a limited number of genotypes? Promiscuity between different, structurally related and/or unrelated proteins seems to provide a plausible explanation to this pertinent question. Strategies able to predict such functional interrelations between different proteins are important to restrict the number of putative candidate proteins, which can then be subjected to time-consuming functional tests. Here we describe the use of the operon structure of the nematode genome to identify partner proteins in human cells. In this work we focus on ion channels proteins, which build an interface between the cell and the outside world and are responsible for a growing number of diseases in humans. However, the proposed strategy for the partner protein quest is not restricted to this scientific area but can be adopted in virtually every field of human biology where protein-protein interactions are assume