), mais en plus marquée éventuellement par les intérêts divergents et des rapports de pouvoir. None of the authors have any conflict of interest. “
“The post-genomic era is characterized by a gold-rush mood, because many previously separate disciplines, ranging Galunisertib mw from biology and biochemistry to physics, mathematics and computer sciences, have grown together and contribute to the generation of enormous amounts of experimental and theoretical data. These data are published in journals and often collected in electronic data repositories. Such resources provide, as a challenge for intelligent
data mining, many potential chances to create new knowledge and to gain insights into complex biological systems. One approach of, for example, systems biologists, is not only to depict the cellular metabolic pathways such as those drawn in the well-known Boehringer poster or the KEGG pathway map but to enter in the third dimension with a higher level of information such as the e-cell project (Tomita et al., 1999 and Takahashi et al., 2004). Apart to the basic scientific understanding of metabolic networks the application of these digitized maps can also be useful for the simulation of the treatment
of diseases such as diabetes which could lead to the development of new “intelligent” drugs (Werner, 2002). However, the way to this scientific goldmine is paved with serious problems. Have you also been faced with the difficulty for comparing your kinetic data
obtained from Cobimetinib mw your experimental results with those published in the literature? Have you been interested in the effect of directed mutations within the catalytic domain or within structure determining sections of the protein on structure–function relationships regarding the catalytic properties? Oxalosuccinic acid Or did you just want to understand the experimental results in the literature and to draw the conclusion in reference to the materials and methods described? Or have you tried to construct a computer model on the basis of published data? The following brief examples will demonstrate the stumbling blocks on the way to the goldmine. Imagine you are investigating the functional properties of the enzymes of your particular interest. Appropriate, that is to say published and proven, methodologies are applied and your assays produce apparently reasonable results. Imagine you are working on the characterization of the key enzymes of a well-known metabolic pathway, which could be glycolysis in baker׳s yeast. Your primary interest could be to understand the interdependences of the metabolic control of this pathway and thus you intend to supply the simulation algorithms such as JWS Online (Olivier and Snoep, 2004) with your kinetic data. However, before doing the theoretical work you want to refer to the primary literature to seek for support for your own experimental results.