A high-throughput cloning system for reverse genetics in <Emphasis Type="Italic">Trypanosoma cruzi</Emphasis>

Background  

The three trypanosomatids pathogenic to men, Trypanosoma cruzi, Trypanosoma brucei and Leishmania major, are etiological agents of Chagas disease, African sleeping sickness and cutaneous leishmaniasis, respectively. The complete sequencing of these trypanosomatid genomes represented a breakthrough in the understanding of these organisms. Genome sequencing is a step towards solving the parasite biology puzzle, as there are a high percentage of genes encoding proteins without functional annotation. Also, technical limitations in protein expression in heterologous systems reinforce the evident need for the development of a high-throughput reverse genetics platform. Ideally, such platform would lead to efficient cloning and compatibility with various approaches. Thus, we aimed to construct a highly efficient cloning platform compatible with plasmid vectors that are suitable for various approaches.     

Matriptase: potent proteolysis on the cell surface

Matriptase is a type II transmembrane serine protease expressed in most human epithelia, where it is coexpressed with its cognate transmembrane inhibitor, hepatocyte growth factor activator inhibitor (HAI)-1. Activation of the matriptase zymogen requires sequential N-terminal cleavage, activation site autocleavage, and transient association with HAI-1. Matriptase has an essential physiological role in profilaggrin processing, corneocyte maturation, and lipid matrix formation associated with terminal differentiation of the oral epithelium and the epidermis, and is also critical for hair follicle growth. Matriptase and HAI expression are frequently dysregulated in human cancer, and matriptase expression that is unopposed by HAI-1 potently promotes carcinogenesis and metastatic dissemination in animal models.     

Immunoprophylaxis of respiratory syncytial virus: global experience

In sarcoidosis, host genetic factors are discussed as contributing to disease susceptibility and course. Since tumor necrosis factor (TNF)-α is a central mediator of granuloma formation and since elevated TNF-α levels are found during active phases of sarcoidosis, genetic polymorphisms correlating with influences on TNF-α levels are of special interest. The complete sequencing of the MHC region and the increase in the number of identified gene polymorphisms in this locus associated with TNF-α production offer the opportunity of detecting new genes associated with sarcoidosis and perhaps of defining disease-associated haplotypes that bear the potential of serving as predictive markers for this disease.     

A model for predicting growth responses in plants to changes in external water potential: Zea mays primary roots

In response to osmotic step changes, three distinct phases have been noted in the growth response of Zea mays primary roots. They are cessation or slowing of growth over a period of 15–20 minutes, tissue contraction, and a damped oscillatory return to nearly normal growth rate, all within a period of about one hour. A system model of the tissue response is presented to explain such behavior and to serve in a predictive capacity to govern future experiments.It is supposed that for turgor pressure in excess of a cell wall yield threshold, plastic flow is the major component of wall deformation, and that when turgor falls below yield threshold, elastic deformation is dominant. The equations of the model describe growth rate as a function of time in terms of the following properties; plastic flow, elastic deformation, permeability to water, and solute uptake. They are derived from basic equations of feedback interactions between internal osmotic pressure and growth rate, and between wall softening, turgor and growth rate.The model predicts oscillatory growth rate regulation, and phase and amplitude relationships between turgor pressure and growth rate. The simplest model which accounts for all observations is that of biphasic deformation, two modes of wall softening, and a dual feedback system involving osmotic and yield threshold control of growth rate.It should be noted that to predict the time course of turgor pressure, osmotic pressure, yield pressure, and growth rate, two initial conditions and six system parameter values are sufficient. So far only the initial values of growth rate and its derivative can be obtained for Zea mays primary roots. However, values for wall softening and hardening coefficients (including the strain and turgor independent component), plastic extensibility, water permeability and dilution rate coefficients have not been obtained as yet for Zea roots. Values for some of these parameters have been obtained for other roots, coleoptiles, and giant algal cells.Lest the reader despair, it should be pointed out that experimental observations coupled with simulation studies will help establish restricted ranges of values that the system parameters might assume. These can then be compared with known values in the literature and values experimentally obtained in the future.     

Mathematical Analysis of Plant Growth zea mays Primary Roots

A new mathematical treatment is given to the concept of relative elemental growth rate, the limiting value at a point of the relative rate of tissue growth. The new point of view requires consideration of a coordinate system in which each point on the root surface is defined by its initial position on the root axis. The resultant technique of plotting growth parameters provides the ability to distinguish between waves of growth propagating toward the root tip away from cells and waves which tend to propagate along with the cells. Thus it is possible to model the plant growth-regulatory process in terms of auxin and other regulators, considering both cell-associated maxima of regulator concentration and maxima which propagate through the tissue.     

Posttranslational modifications of serine protease TMPRSS13 regulate zymogen activation,proteolytic activity,and cell surface localization

TMPRSS13, a member of the type II transmembrane serine protease (TTSP) family, harbors four N-linked glycosylation sites in its extracellular domain. Two of the glycosylated residues are located in the scavenger receptor cysteine-rich (SRCR) protein domain, while the remaining two sites are in the catalytic serine protease (SP) domain. In this study, we examined the role of N-linked glycosylation in the proteolytic activity, autoactivation, and cellular localization of TMPRSS13. Individual and combinatory site-directed mutagenesis of the glycosylated asparagine residues indicated that glycosylation of the SP domain is critical for TMPRSS13 autoactivation and catalytic activity toward one of its protein substrates, the prostasin zymogen. Additionally, SP domain glycosylation-deficient TMPRSS13 displayed impaired trafficking of TMPRSS13 to the cell surface, which correlated with increased retention in the endoplasmic reticulum. Importantly, we showed that N-linked glycosylation was a critical determinant for subsequent phosphorylation of endogenous TMPRSS13. Taken together, we conclude that glycosylation plays an important role in regulating TMPRSS13 activation and activity, phosphorylation, and cell surface localization.     

Growth hormone receptor gene disruption in mature‐adult mice improves male insulin sensitivity and extends female lifespan

Studies in multiple species indicate that reducing growth hormone (GH) action enhances healthy lifespan. In fact, GH receptor knockout (GHRKO) mice hold the Methuselah prize for the world''s longest‐lived laboratory mouse. We previously demonstrated that GHR ablation starting at puberty (1.5 months), improved insulin sensitivity and female lifespan but results in markedly reduced body size. In this study, we investigated the effects of GHR disruption in mature‐adult mice at 6 months old (6mGHRKO). These mice exhibited GH resistance (reduced IGF‐1 and elevated GH serum levels), increased body adiposity, reduced lean mass, and minimal effects on body length. Importantly, 6mGHRKO males have enhanced insulin sensitivity and reduced neoplasms while females exhibited increased median and maximal lifespan. Furthermore, fasting glucose and oxidative damage was reduced in females compared to males irrespective of Ghr deletion. Overall, disrupted GH action in adult mice resulted in sexual dimorphic effects suggesting that GH reduction at older ages may have gerotherapeutic effects.     

Group decisions in humans and animals: a survey

Humans routinely make many decisions collectively, whether they choose a restaurant with friends, elect political leaders or decide actions to tackle international problems, such as climate change, that affect the future of the whole planet. We might be less aware of it, but group decisions are just as important to social animals as they are for us. Animal groups have to collectively decide about communal movements, activities, nesting sites and enterprises, such as cooperative breeding or hunting, that crucially affect their survival and reproduction. While human group decisions have been studied for millennia, the study of animal group decisions is relatively young, but is now expanding rapidly. It emerges that group decisions in animals pose many similar questions to those in humans. The purpose of the present issue is to integrate and combine approaches in the social and natural sciences in an area in which theoretical challenges and research questions are often similar, and to introduce each discipline to the other''s key ideas, findings and successful methods. In order to make such an introduction as effective as possible, here, we briefly review conceptual similarities and differences between the sciences, and provide a guide to the present issue.