ترغب بنشر مسار تعليمي؟ اضغط هنا

Many-body effects in tracer particle diffusion with applications for single-protein dynamics on DNA

155   0   0.0 ( 0 )
 نشر من قبل Ludvig Lizana
 تاريخ النشر 2015
  مجال البحث فيزياء علم الأحياء
والبحث باللغة English




اسأل ChatGPT حول البحث

30% of the DNA in E. coli bacteria is covered by proteins. Such high degree of crowding affect the dynamics of generic biological processes (e.g. gene regulation, DNA repair, protein diffusion etc.) in ways that are not yet fully understood. In this paper, we theoretically address the diffusion constant of a tracer particle in a one dimensional system surrounded by impenetrable crowder particles. While the tracer particle always stays on the lattice, crowder particles may unbind to a surrounding bulk and rebind at another or the same location. In this scenario we determine how the long time diffusion constant ${cal D}$ (after many unbinding events) depends on (i) the unbinding rate of crowder particles $k_{rm off}$, and (ii) crowder particle line density $rho$, from simulations (Gillespie algorithm) and analytical calculations. For small $k_{rm off}$, we find ${cal D}sim k_{rm off}/rho^2$ when crowder particles are immobile on the line, and ${cal D}sim sqrt{D k_{rm off}}/rho$ when they are diffusing; $D$ is the free particle diffusion constant. For large $k_{rm off}$, we find agreement with mean-field results which do not depend on $k_{rm off}$. From literature values of $k_{rm off}$ and $D$, we show that the small $k_{rm off}$-limit is relevant for in vivo protein diffusion on a crowded DNA. Our results applies to single-molecule tracking experiments.



قيم البحث

اقرأ أيضاً

193 - O. Flomenbom , J. Klafter 2003
We study voltage driven translocation of a single stranded (ss) DNA through a membrane channel. Our model, based on a master equation (ME) approach, investigates the probability density function (pdf) of the translocation times, and shows that it can be either double or mono-peaked, depending on the system parameters. We show that the most probable translocation time is proportional to the polymer length, and inversely proportional to the first or second power of the voltage, depending on the initial conditions. The model recovers experimental observations on hetro-polymers when using their properties inside the pore, such as stiffness and polymer-pore interaction.
We consider a non-interacting many-fermion system populating levels of a unitary random matrix ensemble (equivalent to the q=2 complex Sachdev-Ye-Kitaev model) - a generic model of single-particle quantum chaos. We study the corresponding many-partic le level statistics by calculating the spectral form factor analytically using algebraic methods of random matrix theory, and match it with an exact numerical simulation. Despite the integrability of the theory, the many-body spectral rigidity is found to have a surprisingly rich landscape. In particular, we find a residual repulsion of distant many-body levels stemming from single-particle chaos, together with islands of level attraction. These results are encoded in an exponential ramp in the spectral form-factor, which we show to be a universal feature of non-ergodic many-fermion systems embedded in a chaotic medium.
We demonstrate the phenomenon of cumulative inertia in intracellular transport involving multiple motor proteins in human epithelial cells by measuring the empirical survival probability of cargoes on the microtubule and their detachment rates. We fo und the longer a cargo moves along a microtubule, the less likely it detaches from it. As a result, the movement of cargoes is non-Markovian and involves a memory. We observe memory effects on the scale of up to 2 seconds. We provide a theoretical link between the measured detachment rate and the super-diffusive Levy walk-like cargo movement.
We present a theoretical model of facilitated diffusion of proteins in the cell nucleus. This model, which takes into account the successive binding/unbinding events of proteins to DNA, relies on a fractal description of the chromatin which has been recently evidenced experimentally. Facilitated diffusion is shown quantitatively to be favorable for a fast localization of a target locus by a transcription factor, and even to enable the minimization of the search time by tuning the affinity of the transcription factor with DNA. This study shows the robustness of the facilitated diffusion mechanism, invoked so far only for linear conformations of DNA.
Diffusion of impenetrable particles in a crowded one-dimensional channel is referred as the single file diffusion. The particles do not pass each other and the displacement of each individual particle is sub-diffusive. We analyse a simple realization of this single file diffusion problem where one dimensional Brownian point particles interact only by hard-core repulsion. We show that the large deviation function which characterizes the displacement of a tracer at large time can be computed via a mapping to a problem of non-interacting Brownian particles. We confirm recently obtained results of the one time distribution of the displacement and show how to extend them to the multi-time correlations. The probability distribution of the tracer position depends on whether we take annealed or quenched averages. In the quenched case we notice an exact relation between the distribution of the tracer and the distribution of the current. This relation is in fact much more general and would be valid for arbitrary single file diffusion. It allows in particular to get the full statistics of the tracer position for the symmetric simple exclusion process (SSEP) at density 1/2 in the quenched case.
التعليقات
جاري جلب التعليقات جاري جلب التعليقات
سجل دخول لتتمكن من متابعة معايير البحث التي قمت باختيارها
mircosoft-partner

هل ترغب بارسال اشعارات عن اخر التحديثات في شمرا-اكاديميا