14,859 research outputs found
Employability and Social Capital: An Exploration of the Missing Link in the Enhancement of Employability of Business School Graduates
This study explores the role of social capital in the development of employability skills and attributes of first generation undergraduate students in a business school.
The research, based on the reflections of graduates, examines the impact of social capital on participation in higher education and investigates the conditions within the learning environment which enhance or inhibit the development of bridging and linking social capital, as students connect with networks within the institution and with the wider business community.
The findings suggest that the ability to recognise and activate bridging and linking social capital is an important determinant of employability. The analysis illustrates that when students have opportunities to connect with and work within a variety of networks, they build a range of employability skills and capabilities, particularly the interpersonal and social skills valued by employers.
Students, who are confident and have the necessary skills to participate in a variety of networks within the immediate environment and with the wider business community, are not only able to access a greater range of resources but are more able to recognise the potential benefits that these activities have to offer. The reflections of the participants also illustrate that the skills and competencies which enable them to network effectively need to be developed deliberately. By supporting students in recognising the relationship between bridging and linking social capital and employability, and giving them the opportunity to reflect upon the achievement of interpersonal skills and affective capabilities, including the importance of relating to diverse others, their understanding and acknowledgement of employability will be enhanced.
The study also reflects on Quinnâs concept of imagined social capital and considers its impact on the development of employability. Building on her work, the analysis identifies two new typologies; unimagined and unimaginable social capital. Both categories are important in understanding how students acknowledge the potential networks and resources available to them
Relative proximity of chromosome territories influences chromosome exchange partners in radiation-induced chromosome rearrangements in primary human bronchial epithelial cells
Copyright © 2013 The Authors. This article is made available through the Brunel Open Access Publishing Fund. This is an open access article distributed under the terms of the Creative Commons Attribution-NonCommercial-No Derivative Works License, which permits non-commercial use, distribution, and reproduction in any medium, provided the original author and source are credited.Copyright © 2013 The Authors. It is well established that chromosomes exist in discrete territories (CTs) in interphase and are positioned in a cell-type specific probabilistic manner. The relative localisation of individual CTs within cell nuclei remains poorly understood, yet many cancers are associated with specific chromosome rearrangements and there is good evidence that relative territorial position influences their frequency of exchange. To examine this further, we characterised the complexity of radiation-induced chromosome exchanges in normal human bronchial epithelial (NHBE) cells by M-FISH analysis of PCC spreads and correlated the exchanges induced with their preferred interphase position, as determined by 1/2-colour 2D-FISH analysis, at the time of irradiation. We found that the frequency and complexity of aberrations induced were reduced in ellipsoid NHBE cells in comparison to previous observations in spherical cells, consistent with aberration complexity being dependent upon the number and proximity of damaged CTs, i.e. lesion proximity. To ask if particular chromosome neighbourhoods could be identified we analysed all radiation-induced pair-wise exchanges using SCHIP (statistics for chromosome interphase positioning) and found that exchanges between chromosomes (1;13), (9;17), (9;18), (12;18) and (16;21) all occurred more often than expected assuming randomness. All of these pairs were also found to be either sharing similar preferred positions in interphase and/or sharing neighbouring territory boundaries. We also analysed a human small cell lung cancer cell line, DMS53, by M-FISH observing the genome to be highly rearranged, yet possessing rearrangements also involving chromosomes (1;13) and (9;17). Our findings show evidence for the occurrence of non-random exchanges that may reflect the territorial organisation of chromosomes in interphase at time of damage and highlight the importance of cellular geometry for the induction of aberrations of varying complexity after exposure to both low and high-LET radiation.Department of Healt
Continuity of Local Time: An applied perspective
Continuity of local time for Brownian motion ranks among the most notable
mathematical results in the theory of stochastic processes. This article
addresses its implications from the point of view of applications. In
particular an extension of previous results on an explicit role of continuity
of (natural) local time is obtained for applications to recent classes of
problems in physics, biology and finance involving discontinuities in a
dispersion coefficient. The main theorem and its corollary provide physical
principles that relate macro scale continuity of deterministic quantities to
micro scale continuity of the (stochastic) local time.Comment: To appear in: "The fascination of Probability, Statistics and Their
Applications. In honour of Ole E. Barndorff-Nielsen on his 80th birthday
Topological Interactions in Warped Extra Dimensions
Topological interactions will be generated in theories with compact extra
dimensions where fermionic chiral zero modes have different localizations. This
is the case in many warped extra dimension models where the right-handed top
quark is typically localized away from the left-handed one. Using
deconstruction techniques, we study the topological interactions in these
models. These interactions appear as trilinear and quadrilinear gauge boson
couplings in low energy effective theories with three or more sites, as well as
in the continuum limit. We derive the form of these interactions for various
cases, including examples of Abelian, non-Abelian and product gauge groups of
phenomenological interest. The topological interactions provide a window into
the more fundamental aspects of these theories and could result in unique
signatures at the Large Hadron Collider, some of which we explore.Comment: 40 pages, 10 figures, 2 tables; modifications in the KK parity
discussion, final version at JHE
Vancomycin toxicity in neonates: a review of the evidence.
PURPOSE OF REVIEW: Vancomycin is a first-line agent in the treatment of serious Gram-positive infections in the neonatal population. The published evidence on vancomycin toxicity in neonates is limited. This review summarizes preclinical studies and clinical trials describing vancomycin toxicity. We discuss proposed pathophysiology and summarize evidence supporting dose-response relationships, genetic and environmental determinants, and consider future research required to further define vancomycin toxicity. RECENT FINDINGS: Current dosing regimens for vancomycin result in subtherapeutic levels in a large proportion of patients. Higher daily doses have been proposed, which have led to concerns regarding increased toxicity. Nephrotoxicity occurs in 1-9% of neonates receiving currently recommended doses. The incidence is highest in those receiving concomitant nephrotoxic drugs. Vancomycin-associated ototoxicity is rare in patients of all ages. Exposure-toxicity relationships in relation to nephrotoxicity and ototoxicity have not been clearly defined in neonates receiving vancomycin. SUMMARY: Current evidence supports the favourable safety profile of vancomycin in neonates. Further studies that address safety concerns relating to high-dose intermittent dosing regimens are needed. Such studies must include robust and standardized definitions of renal and hearing impairment, and include follow-up of sufficient length to establish the long-term implications of experimental findings
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Diversity in the oligodendrocyte lineage: Plasticity or heterogeneity?
Heterogeneity is a widely recognized phenomenon within the majority of cell types in the body including cells of the central nervous system (CNS). The heterogeneity of neurons based on their distinct transmission modes and firing patterns has been recognized for decades, and is necessary to coordinate the immense variety of functions of the CNS. More recently, heterogeneity in glial cells has been identified, including heterogeneity in oligodendrocyte progenitor cells (OPCs) and oligodendrocytes. OPC subpopulations have been described based on their developmental origin, anatomical location in the grey or white matter, and expression of surface receptors. Oligodendrocytes are categorised according to differences in gene expression, myelinogenic potential, and axon specificity. Much of what is described as heterogeneity in oligodendrocyte lineage cells (OLCs) is based on phenotypic differences. However, without evidence for functional differences between putative subgroups of OLCs, distinguishing heterogeneity from plasticity and lineage state is difficult. Identifying functional differences between phenotypically distinct groups are therefore necessary for a deeper understanding of the role of OLCs in health and disease.The authors acknowledge the support of funding from the UK Multiple Sclerosis Society, MedImmune, The Adelson Medical Research Foundation and a core support grant from the Wellcome Trust and MRC to the Wellcome Trust-Medical Research Council Cambridge Stem Cell Institute. SF and MFEH have been recipients of Wellcome Trust funded PhD studentships
Mitochondrial calcium uptake pathways as a potential therapeutic target
It has been known since the 1960âs that mitochondria have a huge capacity to take up and accumulate calcium from the cytosol, regulating energy production, autophagy, and mitochondrial morphology. Dysfunctional mitochondrial calcium homeostasis is also involved in the pathology of many disease states. Therefore, mitochondrial calcium handling represents an interesting therapeutic target. In this thesis I aimed to investigate related therapeutic avenues and further understand the role of mitochondrial calcium handling machinery. When mitochondrial calcium uptake exceeds the calcium buffering capacity of the mitochondrial matrix, the mitochondrial permeability transition pore (mPTP) opens in the inner mitochondrial membrane. Pore opening causes mitochondrial depolarisation, energetic collapse, swelling, rupture, and cell death. Using isolated mitochondria, I screened a range of novel mitochondrial targeted derivatives of the canonical mPTP inhibitor, cyclosporin A (CsA), to assess their efficacy as mPTP inhibitors, and as potential therapeutics for neurological disease. Two compounds were found to be more effective than CsA at low concentrations, and one was selected for further study. The compoundâs target was investigated and found to be Cyclophilin D, and itâs effect on various mitochondrial parameters was assessed, and it was found to be non-toxic ex vivo and in vitro. The molecular identity of the mitochondrial calcium uniporter (MCU) was only recently discovered, followed by discovery of several associated proteins â MCUb, MICU1, MICU2, MICU3, EMRE, and MCUR1. I developed a screen using the bioluminescent protein aequorin to identify mitochondrial specific inhibitors of the MCU, and I developed a stable cell line in which the MCU protein was knocked down, in order to further examine the role of MCU and investigate the effect of reduced mitochondrial calcium uptake on mitochondrial and cellular properties. While mitochondrial calcium uptake was significantly reduced upon stimulation in these cells, cytosolic calcium, oxygen consumption, cell growth and mitochondrial morphology were not affected. I also investigated the protein expression level of the components of the MCU complex in the rat brain throughout development
Reconfiguring experimental archaeology using 3D reconstruction
Experimental archaeology has long yielded valuable insights into the tools and techniques that featured in past peoplesâ relationship with the material world around them. We can determine, for example, how many trees would need to be felled to construct a large round-house of the southern British Iron Age (over one hundred), infer the exact angle needed to strike a flint core in order to knap an arrowhead in the manner of a Neolithic hunter-gatherer, or recreate the precise environmental conditions needed to store grain in underground silos over the winter months, with only the technologies and materials available to Romano-Briton villagers (see Coles 1973; Reynolds 1993). However, experimental archaeology has, hitherto, confined itself to rather rigid, empirical and quantitative questions such as those posed in these examples. This is quite understandable, and in line with good scientific practice, which stipulates that any âexperimentâ must be based on replicable data, and be reproducible. Despite their potential in this area however, it is notable that digital reconstruction technologies have yet to play a significant role in experimental archaeology. Whilst many excellent examples of digital 3D reconstruction of heritage sites exist (for example the Digital Roman Forum project: http://dlib.etc.ucla.edu/projects/Forum) most, if not all, of these are characterized by a drive to establish a photorealistic re-creation of physical features. This paper will discuss possibilities that lie beyond straightforward positivist re-creation of heritage sites, in the experimental reconstruction of intangible heritage. Between 2010 and 2012, the authors led the Motion in Place Platform project (MiPP: http://www.motioninplace.org/), a capital grant under the AHRC's DEDEFI scheme developing motion capture and analysis tools for exploring how people move through spaces. In the course of MiPP, a series of experiments were conducted using motion capture hardware and software at the Silchester Roman town archaeological excavation in Hampshire, and at the Butser Ancient Farm facility, where Romano-British and Iron Age dwellings have been constructed according to the best experimental practice. As well as reconstructing such Roman and early British dwellings in 3D, the authors were able to use motion capture to reconstruct the kind of activities that â according to the material evidence â are likely to have been carried out by the occupants who used them. Bespoke motion capture suits developed for the project were employed, and the traces captured and rendered with a combination of Autodesk and Unity3D software. This sheds new light on how the reconstructed spaces - and, by inference, their ancient counterparts - were most likely to have been used. In particular the exercises allowed the evaluation and visualisation of changes in behaviour which occur as a result of familiarity with an environment and the acquisition of expertise over time; and to assess how interaction between different actors affects how everyday tasks are carried out
Estimating ÎŽ15N fractionation and adjusting the lipid correction equation using Southern African freshwater fishes
Stable isotope analysis is an important tool for characterising food web structure; however, interpretation of isotope data can often be flawed. For instance, lipid normalisation and trophic fractionation values are often assumed to be constant, but can vary considerably between ecosystems, species and tissues. Here, previously determined lipid normalisation equations and trophic fractionation values were re-evaluated using freshwater fish species from three rivers in the Upper Zambezian floodplain ecoregion in southern Africa. The parameters commonly used in lipid normalisation equations were not correct for the 18 model species (new D and I parameters were estimated as D = 4.46â° [95% CI: 2.62, 4.85] and constant I = 0 [95% CI: 0, 0.17]). We suggest that future isotopic analyses on freshwater fishes use our new values if the species under consideration do not have a high lipid content in their white muscle tissue. Nitrogen fractionation values varied between species and river basin; however, the average value closely matched that calculated in previous studies on other species (ÎŽ15N fractionation factor of 3.37 ± 1.30 â°). Here we have highlighted the need to treat stable isotope data correctly in food web studies to avoid misinterpretation of the data
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