A thermomechanical framework for reconciling the effects of ultraviolet radiation exposure time and wavelength on connective tissue elasticity

Augmentation of the mechanical properties of connective tissue using ultraviolet (UV) radiation—by targeting collagen cross-linking in the tissue at predetermined UV exposure time \((t)\) and wavelength \((\lambda )\) —has been proposed as a therapeutic method for supporting the treatment for structural-related injuries and pathologies. However, the effects of \(\lambda \) and \(t\) on the tissue elasticity, namely elastic modulus \((E)\) and modulus of resilience \((u_\mathrm{Y})\) , are not entirely clear. We present a thermomechanical framework to reconcile the \(t\) - and \(\lambda \) -related effects on \(E\) and \(u_\mathrm{Y}\) . The framework addresses (1) an energy transfer model to describe the dependence of the absorbed UV photon energy, \(\xi \) , per unit mass of the tissue on \(t\) and \(\lambda \) , (2) an intervening thermodynamic shear-related parameter, \(G\) , to quantify the extent of UV-induced cross-linking in the tissue, (3) a threshold model for the \(G\) versus \(\xi \) relationship, characterized by   \(t_\mathrm{C}\) —the critical \(t\) underpinning the association of \(\xi \) with \(G\) —and (4) the role of \(G\) in the tissue elasticity. We hypothesized that \(G\) regulates \(E\) (UV-stiffening hypothesis) and \(u_\mathrm{Y}\) (UV-resilience hypothesis). The framework was evaluated with the support from data derived from tensile testing on isolated ligament fascicles, treated with two levels of \(\lambda \) (365 and 254 nm) and three levels of \(t\) (15, 30 and 60 min). Predictions from the energy transfer model corroborated the findings from a two-factor analysis of variance of the effects of \(t\) and \(\lambda \) treatments. Student’s t test revealed positive change in \(E\) and \(u_\mathrm{Y}\) with increases in \(G\) —the findings lend support to the hypotheses, implicating the implicit dependence of UV-induced cross-links on \(t\) and \(\lambda \) for directing tissue stiffness and resilience. From a practical perspective, the study is a step in the direction to establish a UV irradiation treatment protocol for effective control of exogenous cross-linking in connective tissues.     

N-site Phosphorylation Systems with 2N-1 Steady States

Multisite protein phosphorylation plays a prominent role in intracellular processes like signal transduction, cell-cycle control and nuclear signal integration. Many proteins are phosphorylated in a sequential and distributive way at more than one phosphorylation site. Mathematical models of \(n\) -site sequential distributive phosphorylation are therefore studied frequently. In particular, in Wang and Sontag (J Math Biol 57:29–52, 2008), it is shown that models of \(n\) -site sequential distributive phosphorylation admit at most \(2n-1\) steady states. Wang and Sontag furthermore conjecture that for odd \(n\) , there are at most \(n\) and that, for even \(n\) , there are at most \(n+1\) steady states. This, however, is not true: building on earlier work in Holstein et al. (Bull Math Biol 75(11):2028–2058, 2013), we present a scalar determining equation for multistationarity which will lead to parameter values where a \(3\) -site system has \(5\) steady states and parameter values where a \(4\) -site system has \(7\) steady states. Our results therefore are counterexamples to the conjecture of Wang and Sontag. We furthermore study the inherent geometric properties of multistationarity in \(n\) -site sequential distributive phosphorylation: the complete vector of steady state ratios is determined by the steady state ratios of free enzymes and unphosphorylated protein and there exists a linear relationship between steady state ratios of phosphorylated protein.     

Individual-Based Model for Quorum Sensing with Background Flow

Quorum sensing is a wide-spread mode of cell–cell communication among bacteria in which cells release a signalling substance at a low rate. The concentration of this substance allows the bacteria to gain information about population size or spatial confinement. We consider a model for \(N\) cells which communicate with each other via a signalling substance in a diffusive medium with a background flow. The model consists of an initial boundary value problem for a parabolic PDE describing the exterior concentration \(u\) of the signalling substance, coupled with \(N\) ODEs for the masses \(a_i\) of the substance within each cell. The cells are balls of radius \(R\) in \(\mathbb {R} ^3\) , and under some scaling assumptions we formally derive an effective system of \(N\) ODEs describing the behaviour of the cells. The reduced system is then used to study the effect of flow on communication in general, and in particular for a number of geometric configurations.     

A locally convergent rotationally invariant particle swarm optimization algorithm

Several well-studied issues in the particle swarm optimization algorithm are outlined and some earlier methods that address these issues are investigated from the theoretical and experimental points of view. These issues are the: stagnation of particles in some points in the search space, inability to change the value of one or more decision variables, poor performance when the swarm size is small, lack of guarantee to converge even to a local optimum (local optimizer), poor performance when the number of dimensions grows, and sensitivity of the algorithm to the rotation of the search space. The significance of each of these issues is discussed and it is argued that none of the particle swarm optimizers we are aware of can address all of these issues at the same time. To address all of these issues at the same time, a new general form of velocity update rule for the particle swarm optimization algorithm that contains a user-definable function \(f\) is proposed. It is proven that the proposed velocity update rule guarantees to address all of these issues if the function \(f\) satisfies the following two conditions: (i) the function \(f\) is designed in such a way that for any input vector \(\vec {y}\) in the search space, there exists a region \(A\) which contains \(\vec {y}\) and \( f\!\left( {\vec {y}} \right) \) can be located anywhere in \(A\) , and (ii) \(f\) is invariant under any affine transformation. An example of function \(f\) is provided that satisfies these conditions and its performance is examined through some experiments. The experiments confirm that the proposed algorithm (with an appropriate function \(f)\) can effectively address all of these issues at the same time. Also, comparisons with earlier methods show that the overall ability of the proposed method for solving benchmark functions is significantly better.     

Approximation of sojourn-times via maximal couplings: motif frequency distributions

Sojourn-times provide a versatile framework to assess the statistical significance of motifs in genome-wide searches even under non-Markovian background models. However, the large state spaces encountered in genomic sequence analyses make the exact calculation of sojourn-time distributions computationally intractable in long sequences. Here, we use coupling and analytic combinatoric techniques to approximate these distributions in the general setting of Polish state spaces, which encompass discrete state spaces. Our approximations are accompanied with explicit, easy to compute, error bounds for total variation distance. Broadly speaking, if \({\mathsf{T}}_n\) is the random number of times a Markov chain visits a certain subset \({\mathsf{T}}\) of states in its first \(n\) transitions, then we can usually approximate the distribution of \({\mathsf{T}}_n\) for \(n\) of order \((1-\alpha )^{-m}\) , where \(m\) is the largest integer for which the exact distribution of \({\mathsf{T}}_m\) is accessible and \(0\le \alpha \le 1\) is an ergodicity coefficient associated with the probability transition kernel of the chain. This gives access to approximations of sojourn-times in the intermediate regime where \(n\) is perhaps too large for exact calculations, but too small to rely on Normal approximations or stationarity assumptions underlying Poisson and compound Poisson approximations. As proof of concept, we approximate the distribution of the number of matches with a motif in promoter regions of C. elegans. Mathematical properties of the proposed ergodicity coefficients and connections with additive functionals of homogeneous Markov chains as well as ergodicity of non-homogeneous Markov chains are also explored.     

Fishermen’s Profits Maximization: Case of Generalized Nash Equilibrium of a Non-symmetrical Game

In the present paper, we consider a bio-economic equilibrium model which describes the dynamics of a fish population fished by several fishermen seeking to maximize their profits. Each fisherman tries to find the fishing effort which maximizes his profit at biological equilibrium without any consultation with others, but all of them have to respect two constraints: (1) the sustainable management of the resources ; and (2) the preservation of the biodiversity. With all these considerations, our problem leads to a generalized Nash equilibrium problem. The objective is to show that even when a fisherman \(i\) provides a fishing effort equal to twice the fishing effort of a fisherman \(j\) , then the profit of fisherman \(i\) is not necessarily double that of fisherman \(j\) .     

On linear birth-and-death processes in a random environment

We study the probability of extinction for single-type and multi-type continuous-time linear birth-and-death processes in a finite Markovian environment. The probability of extinction is equal to 1 almost surely if and only if the basic reproduction number \(R_0\) is \(\le 1\) , the key point being to identify a suitable definition of \(R_0\) for such a result to hold.     

Elastic behavior of a red blood cell with the membrane’s nonuniform natural state: equilibrium shape,motion transition under shear flow,and elongation during tank-treading motion

Direct numerical simulations of the mechanics of a single red blood cell (RBC) were performed by considering the nonuniform natural state of the elastic membrane. A RBC was modeled as an incompressible viscous fluid encapsulated by an elastic membrane. The in-plane shear and area dilatation deformations of the membrane were modeled by Skalak constitutive equation, while out-of-plane bending deformation was formulated by the spring model. The natural state of the membrane with respect to in-plane shear deformation was modeled as a sphere ( \(\alpha =0\) ), biconcave disk shape ( \(\alpha =1\) ) and their intermediate shapes ( \(0<\alpha <1\) ) with the nonuniformity parameter \(\alpha \) , while the natural state with respect to out-of-plane bending deformation was modeled as a flat plane. According to the numerical simulations, at an experimentally measured in-plane shear modulus of \(2.5\times 10^{-6}\,\hbox {N}/\hbox {m}\) and an out-of-plane bending rigidity of \(2.0\times 10^{-19}\,\hbox {N}\cdot \hbox {m}\) of the cell membrane, the following results were obtained. (i) The RBC shape at equilibrium was biconcave discoid for \(\alpha >0.22\) and cupped otherwise; (ii) the experimentally measured fluid shear stress at the transition between tumbling and tank-treading motions under shear flow was reproduced for \(0.05<\alpha <0.34\) ; (iii) the elongation deformation of the RBC during tank-treading motion from the simulation was consistent with that from in vitro experiments, irrespective of the \(\alpha \) value. Based on our RBC modeling, the three phenomena (i), (ii), and (iii) were mechanically consistent for \(0.22<\alpha <0.34\) . The condition \(0.05<\alpha <0.22\) precludes a biconcave discoid shape at equilibrium (i); however, it gives appropriate fluid shear stress at the motion transition under shear flow (ii), suggesting that a combined effect of \(\alpha \) and the natural state with respect to out-of-plane bending deformation is necessary for understanding details of the RBC mechanics at equilibrium. Our numerical results demonstrate that moderate nonuniformity in a membrane’s natural state with respect to in-plane shear deformation plays a key role in RBC mechanics.     

The Basic Reproduction Number for Cellular SIR Networks

The basic reproduction number \(R_0\) is the average number of new infections produced by a typical infective individual in the early stage of an infectious disease, following the introduction of few infective individuals in a completely susceptible population. If \(R_0<1\) , then the disease dies, whereas for \(R_0>1\) the infection can invade the host population and persist. This threshold quantity is well studied for SIR compartmental or mean field models based on ordinary differential equations, and a general method for its computation has been proposed by van den Driessche and Watmough. We concentrate here on SIR epidemiological models that take into account the contact network N underlying the transmission of the disease. In this context, it is generally admitted that \(R_{0}\) can be approximated by the average number \(R_{2,3}\) of infective individuals of generation three produced by an infective of generation two. We give here a simple analytic formula of \(R_{2,3}\) for SIR cellular networks. Simulations on two-dimensional cellular networks with von Neumann and Moore neighborhoods show that \(R_{2,3}\) can be used to capture a threshold phenomenon related the dynamics of SIR cellular network and confirm the good quality of the simple approach proposed recently by Aparicio and Pascual for the particular case of Moore neighborhood.     

Biaxial mechanical properties of the human thoracic and abdominal aorta,common carotid,subclavian, renal and common iliac arteries

The biomechanics of large- and medium-sized arteries influence the pathophysiology of arterial disease and the response to therapeutic interventions. However, a comprehensive comparative analysis of human arterial biaxial mechanical properties has not yet been reported. Planar biaxial extension was used to establish the passive mechanical properties of human thoracic (TA, \(n=8\) ) and abdominal (AA, \(n=7\) ) aorta, common carotid (CCA, \(n=21\) ), subclavian (SA, \(n=12\) ), renal (RA, \(n=13\) ) and common iliac (CIA, \(n=16\) ) arteries from 11 deceased subjects ( \(54\pm 21\)  years old). Histological evaluation determined the structure of each specimen. Experimental data were used to determine constitutive parameters for a structurally motivated nonlinear anisotropic constitutive model. All arteries demonstrated appreciable anisotropy and large nonlinear deformations. Most CCA, SA, TA, AA and CIA specimens were stiffer longitudinally, while most RAs were stiffer circumferentially. A switch in anisotropy was occasionally demonstrated for all arteries. The CCA was the most compliant, least anisotropic and least frequently diseased of all arteries, while the CIA and AA were the stiffest and the most diseased. The severity of atherosclerosis correlated with age, but was not affected by laterality. Elastin fibers in the aorta, SA and CCA were uniformly and mostly circumferentially distributed throughout the media, while in the RA and CIA, elastin was primarily axially aligned and concentrated in the external elastic lamina. Constitutive modeling provided good fits to the experimental data for most arteries. Biomechanical and architectural features of major arteries differ depending on location and functional environment. A better understanding of localized arterial mechanical properties may support the development of site-specific treatment modalities for arterial disease.     

Threshold dynamics in an SEIRS model with latency and temporary immunity

A disease transmission model of SEIRS type with distributed delays in latent and temporary immune periods is discussed. With general/particular probability distributions in both of these periods, we address the threshold property of the basic reproduction number \(R_0\) and the dynamical properties of the disease-free/endemic equilibrium points present in the model. More specifically, we 1. show the dependence of \(R_0\) on the probability distribution in the latent period and the independence of \(R_0\) from the distribution of the temporary immunity, 2. prove that the disease free equilibrium is always globally asymptotically stable when \(R_0<1\) , and 3. according to the choice of probability functions in the latent and temporary immune periods, establish that the disease always persists when \(R_0>1\) and an endemic equilibrium exists with different stability properties. In particular, the endemic steady state is at least locally asymptotically stable if the probability distribution in the temporary immunity is a decreasing exponential function when the duration of the latency stage is fixed or exponentially decreasing. It may become oscillatory under certain conditions when there exists a constant delay in the temporary immunity period. Numerical simulations are given to verify the theoretical predictions.     

Vaccination Strategies for SIR Vector-Transmitted Diseases

Vector-borne diseases are one of the major public health problems in the world with the fastest spreading rate. Control measures have been focused on vector control, with poor results in most cases. Vaccines should help to reduce the diseases incidence, but vaccination strategies should also be defined. In this work, we propose a vector-transmitted SIR disease model with age-structured population subject to a vaccination program. We find an expression for the age-dependent basic reproductive number \(R_0\) , and we show that the disease-free equilibrium is locally stable for \(R_0 \le 1\) , and a unique endemic equilibrium exists for \(R_0 >1\) . We apply the theoretical results to public data to evaluate vaccination strategies, immunization levels, and optimal age of vaccination for dengue disease.     

Principal trabecular structural orientation predicted by quantitative ultrasound is strongly correlated with \upmu FEA determined anisotropic apparent stiffness

The microarchitecture and alignment of trabecular bone adapts to the particular mechanical milieu applied to it. Due to this anisotropic mechanical property, measurement orientation has to be taken into consideration when assessing trabecular bone quality and fracture risk prediction. Quantitative ultrasound (QUS) has demonstrated the ability in predicting the principal structural orientation (PSO) of trabecular bone. Although the QUS prediction for PSO is very close to that of \(\upmu \) CT, certain angle differences still exist. It remains unknown whether this angle difference can induce significant differences in mechanical properties or not. The objective of this study was to evaluate the mechanical properties in different PSOs predicted using different methods, QUS and \(\upmu \) CT, thus to investigate the ability of QUS as a means to predict the PSO of trabecular bone noninvasively. By validating the ability of QUS to predict the PSO of trabecular bone, it is beneficial for future QUS applications because QUS measurements in the PSO can provide information more correlated with the mechanical properties than with other orientations. In this study, seven trabecular bone balls from distal bovine femurs were used to generate finite element models based on the 3-dimensional \(\upmu \) CT images. Uniaxial compressive loading was performed on the bone ball models in the finite element analysis (FEA) in six different orientations (three anatomical orientations, two PSOs predicted by QUS and the longest vector of mean intercept length (MIL) tensor calculated by \(\upmu \) CT). The stiffness was calculated based on the reaction force of the bone balls under loading, and the von Mises stress results showed that both the mechanical properties in the PSOs predicted by QUS are significantly higher than the anatomical orientations and comparatively close to the longest vector of MIL tensor. The stiffness in the PSOs predicted by QUS is also highly correlated with the stiffness in the MIL tensor orientation (ATTmax vs. MIL, \(R^{2}\)  = 0.98, \(p<001\) ; UVmax vs. MIL, \(R^{2}\)  = 0.92, \(p<001\) ). These results were validated by in vitro mechanical testing on the bone ball samples. This study demonstrates that the PSO of trabecular bone predicted by QUS has an equally strong apparent stiffness with the orientation predicted by \(\upmu \) CT.     

Reconstructing a Phylogenetic Level-1 Network from Quartets

We describe a method that will reconstruct an unrooted binary phylogenetic level-1 network on \(n\) taxa from the set of all quartets containing a certain fixed taxon, in \(O(n^3)\) time. We also present a more general method which can handle more diverse quartet data, but which takes \(O(n^6)\) time. Both methods proceed by solving a certain system of linear equations over the two-element field \(\mathrm{GF}(2)\) . For a general dense quartet set, i.e. a set containing at least one quartet on every four taxa, our \(O(n^6)\) algorithm constructs a phylogenetic level-1 network consistent with the quartet set if such a network exists and returns an \(O(n^2)\) -sized certificate of inconsistency otherwise. This answers a question raised by Gambette, Berry and Paul regarding the complexity of reconstructing a level-1 network from a dense quartet set, and more particularly regarding the complexity of constructing a cyclic ordering of taxa consistent with a dense quartet set.     

Modulation of the cAMP Response by G\alpha _i and G\beta \gamma : A Computational Study of G Protein Signaling in Immune Cells

Cyclic AMP is important for the resolution of inflammation, as it promotes anti-inflammatory signaling in several immune cell lines. In this paper, we present an immune cell specific model of the cAMP signaling cascade, paying close attention to the specific isoforms of adenylyl cyclase (AC) and phosphodiesterase that control cAMP production and degradation, respectively, in these cells. The model describes the role that G protein subunits, including G \(\alpha _s\) , G \(\alpha _i\) , and G \(\beta \gamma \) , have in regulating cAMP production. Previously, G \(\alpha _i\) activation has been shown to increase the level of cAMP in certain immune cell types. This increase in cAMP is thought to be mediated by \(\beta \gamma \) subunits which are released upon G \(\alpha \) activation and can directly stimulate specific isoforms of AC. We conduct numerical experiments in order to explore the mechanisms through which G \(\alpha _i\) activation can increase cAMP production. An important conclusion of our analysis is that the relative abundance of different G protein subunits is an essential determinant of the cAMP profile in immune cells. In particular, our model predicts that limited availability of \(\beta \gamma \) subunits may both \((i)\) enable immune cells to link inflammatory G \(\alpha _i\) signaling to anti-inflammatory cAMP production thereby creating a balanced immune response to stimulation with low concentrations of PGE2, and \((ii)\) prohibit robust anti-inflammatory cAMP signaling in response to stimulation with high concentrations of PGE2.     

A Stuctured Discrete Model for Dengue Fever Infections and the Determination of R_0 from Age-Stratified Serological Data

A time discrete age-structured model for modeling the spread of Dengue fever is built. The demographic dynamics is introduced trough the Leslie model. The basic reproductive number is introduced, and an approximation for it is built. The final age distributions for the susceptibles, infected and removed are obtained, and we show how they can be used to produce an actual estimate for \(R_0\) from stratified serological data. An application is made using data from Recife, Brazil, and explicit estimates for \(R_0\) are given.     

Dynamic permeability of the lacunar–canalicular system in human cortical bone

A new method for the experimental determination of the permeability of a small sample of a fluid-saturated hierarchically structured porous material is described and applied to the determination of the lacunar–canalicular permeability \((K_\mathrm{LC})\) in bone. The interest in the permeability of the lacunar–canalicular pore system (LCS) is due to the fact that the LCS is considered to be the site of bone mechanotransduction due to the loading-driven fluid flow over cellular structures. The permeability of this space has been estimated to be anywhere from \(10^{-17}\;\) to \(10^{-25}\; \hbox {m}^{2}\) . However, the vascular pore system and LCS are intertwined, rendering the permeability of the much smaller-dimensioned LCS challenging to measure. In this study, we report a combined experimental and analytical approach that allowed the accurate determination of the \(K_\mathrm{LC}\) to be on the order of \(10^{-22}\; \hbox {m}^{2}\) for human osteonal bone. It was found that the \(K_\mathrm{LC}\) has a linear dependence on loading frequency, decreasing at a rate of \(2 \times 10^{-24}\; \hbox {m}^{2}\) /Hz from 1 to 100 Hz, and using the proposed model, the porosity alone was able to explain 86 % of the \(K_\mathrm{LC}\) variability.     

Interdependency and hierarchy of exact and approximate epidemic models on networks

Over the years numerous models of \(SIS\) (susceptible \(\rightarrow \) infected \(\rightarrow \) susceptible) disease dynamics unfolding on networks have been proposed. Here, we discuss the links between many of these models and how they can be viewed as more general motif-based models. We illustrate how the different models can be derived from one another and, where this is not possible, discuss extensions to established models that enables this derivation. We also derive a general result for the exact differential equations for the expected number of an arbitrary motif directly from the Kolmogorov/master equations and conclude with a comparison of the performance of the different closed systems of equations on networks of varying structure.