742 research outputs found

    Chiral Parametrization of QCD Vector Field in SU(3)

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    The chiral parametrization of gluons in SU(3) QCD is proposed extending an approach developed earlier for SU(2) case. A color chiral field is introduced, gluons are chirally rotated, and vector component of rotated gluons is defined on condition that no new color variables appeared with the chiral field. This condition associates such a vector component with SU(3)/U(2) coset plus an U(2) field. The topological action in SU(3) QCD is derived. It is expressed in terms of axial vector component of rotated gluons. The vector field in CP^2 sector is studied in new variables of chiral parametrization.Comment: 17 page

    Color Bosonization, Chiral Parametrization of Gluonic Field and QCD Effective Action

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    We develop a color bosonization approach to treatment of QCD gauge field (''gluons'') at low energies in order to derive an effective color action of QCD taking into account the quark chiral anomaly in the case of SU(2) color.. We have found that there exists such a region in the chiral sector of color space, where a gauge field coincides with of chirally rotated vector field, while an induced axial vector field disappears. In this region, the unit color vector of chiral field plays a defining role, and a gauge field is parametrized in terms of chiral parameters, so that no additional degrees of freedom are introduced by the chiral field. A QCD gauge field decomposition in color bosonization is a sum of a chirally rotated gauge field and an induced axial-vector field expressed in terms of gluonic variables. An induced axial-vector field defines the chiral color anomaly and an effective color action of QCD. This action admits existence of a gauge invariant d=2 condensate of induced axial-vector field and mass.Comment: 13 pages, LaTe

    Mathematical modeling of tumor therapy with oncolytic viruses: Effects of parametric heterogeneity on cell dynamics

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    One of the mechanisms that ensure cancer robustness is tumor heterogeneity, and its effects on tumor cells dynamics have to be taken into account when studying cancer progression. There is no unifying theoretical framework in mathematical modeling of carcinogenesis that would account for parametric heterogeneity. Here we formulate a modeling approach that naturally takes stock of inherent cancer cell heterogeneity and illustrate it with a model of interaction between a tumor and an oncolytic virus. We show that several phenomena that are absent in homogeneous models, such as cancer recurrence, tumor dormancy, an others, appear in heterogeneous setting. We also demonstrate that, within the applied modeling framework, to overcome the adverse effect of tumor cell heterogeneity on cancer progression, a heterogeneous population of an oncolytic virus must be used. Heterogeneity in parameters of the model, such as tumor cell susceptibility to virus infection and virus replication rate, can lead to complex, time-dependent behaviors of the tumor. Thus, irregular, quasi-chaotic behavior of the tumor-virus system can be caused not only by random perturbations but also by the heterogeneity of the tumor and the virus. The modeling approach described here reveals the importance of tumor cell and virus heterogeneity for the outcome of cancer therapy. It should be straightforward to apply these techniques to mathematical modeling of other types of anticancer therapy.Comment: 45 pages, 6 figures; submitted to Biology Direc

    Biological applications of the theory of birth-and-death processes

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    In this review, we discuss the applications of the theory of birth-and-death processes to problems in biology, primarily, those of evolutionary genomics. The mathematical principles of the theory of these processes are briefly described. Birth-and-death processes, with some straightforward additions such as innovation, are a simple, natural formal framework for modeling a vast variety of biological processes such as population dynamics, speciation, genome evolution, including growth of paralogous gene families and horizontal gene transfer, and somatic evolution of cancers. We further describe how empirical data, e.g., distributions of paralogous gene family size, can be used to choose the model that best reflects the actual course of evolution among different versions of birth-death-and-innovation models. It is concluded that birth-and-death processes, thanks to their mathematical transparency, flexibility and relevance to fundamental biological process, are going to be an indispensable mathematical tool for the burgeoning field of systems biology.Comment: 29 pages, 4 figures; submitted to "Briefings in Bioinformatics

    On diffusive stability of Eigen's quasispecies model

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    Eigen's quasispecies system with explicit space and global regulation is considered. Limit behavior and stability of the system in a functional space under perturbations of a diffusion matrix with nonnegative spectrum are investigated. It is proven that if the diffusion matrix has only positive eigenvalues then the solutions of the distributed system converge to the equilibrium solution of the corresponding local dynamical system. These results imply that the error threshold does not change if the spatial interactions under the principle of global regulation are taken into account.Comment: 16 pages, 1 figure, several typos are fixe
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