167 research outputs found
Spatial configuration shapes student social and informal learning activities in educational complexes
Notable gains have been made in understanding the factors that influence student experiences
in higher education, particularly in the area of spatial configuration. Indeed, studies have found
that spatial configuration affects spatial behaviour and movement patterns (e.g., Hillier et
al., 1993). Increasingly physical and spatial supports are provided to ensure the efficacy and
efficiency of learning activities in higher education (Higgins et al., 2005; Brown & Long, 2006;
Dugdale & Long, 2007; Dugdale, 2009). Consequently, the informal learning spaces became
a pivotal architectural design strategy for universities to enhance interior design quality and
improve learning environments. It is definitely an effective way to improve learning performance
in the higher educational facilities if well-designed informal learning spaces could improve
student experiences within them. Even though the development of purpose-built informal
learning spaces is a strategy to enhance student experiences, it is becoming more prevalent.
The empirical research in this area is still lacking. What appears to be missing in this enquiry is
how the built environment, namely the shape of the learning environment, influences student
activities.
Using Hillierβs (2007) definition of intelligibility as the relationship between local and global
configurational factors, this paper aims to examine the impact of spatial configuration upon
frequency of student activities in an educational complex based on space syntax theory and
behavioural observation. In order to achieve this assumption, we correlated the data between
the observation data of the frequencies of six student activities: Focused Informal Learning,
Serendipitous Encounter, Intermittent Exchange, Focused Socialising, Dietary Related
Activities and Ambient Sociality. The spatial attributes were derived from space syntax theory in
an educational complex of the University Park campus in the University of Nottingham: Coates
Building - Pope Building - ESLC area. More specifically, there are five informal learning spaces
in the educational complex in total. The frequency of the six types of student activities were examined in five informal learning spaces in this educational complex. The findings confirm that
spatial configuration and patterns of spatial usage are related to each other. The main finding
is that there is a correlation between the degree of connectivity of the area and frequency of
student activities. The finding suggests that spatial configuration may play an important role in
determining frequencies of students socialising and informal learning activities
Identification of a Maturation Plasma Cell Index through a Highly Sensitive Droplet Digital PCR Assay Gene Expression Signature Validation in Newly Diagnosed Multiple Myeloma Patients
DNA microarrays and RNA-based sequencing approaches are considered important discovery tools in clinical medicine. However, cross-platform reproducibility studies undertaken so far have highlighted that microarrays are not able to accurately measure gene expression, particularly when they are expressed at low levels. Here, we consider the employment of a digital PCR assay (ddPCR) to validate a gene signature previously identified by gene expression profile. This signature included ten Hedgehog (HH) pathways' genes able to stratify multiple myeloma (MM) patients according to their self-renewal status. Results show that the designed assay is able to validate gene expression data, both in a retrospective as well as in a prospective cohort. In addition, the plasma cells' differentiation status determined by ddPCR was further confirmed by other techniques, such as flow cytometry, allowing the identification of patients with immature plasma cells' phenotype (i.e., expressing CD19+/CD81+ markers) upregulating HH genes, as compared to others, whose plasma cells lose the expression of these markers and were more differentiated. To our knowledge, this is the first technical report of gene expression data validation by ddPCR instead of classical qPCR. This approach permitted the identification of a Maturation Index through the integration of molecular and phenotypic data, able to possibly define upfront the differentiation status of MM patients that would be clinically relevant in the future
A chemically modified antibody mediates complete eradication of tumours by selective disruption of tumour blood vessels
These results reinforce the concept that vascular shutdown can induce a curative avalanche of tumour cell death. Immuno-photodynamic therapy may be particularly indicated for squamous cell carcinoma of the skin, which we show to be strongly positive for markers of angiogenesis
Distribution of laminin and fibronectin isoforms in oral mucosa and oral squamous cell carcinoma
The expression of laminin and fibronectin isoforms varies with cellular maturation and differentiation and these differences may well influence cellular processes such as adhesion and motility. The basement membrane (BM) of fetal oral squamous epithelium contains the laminin chains, Ξ±2, Ξ±3, Ξ±5, Ξ²1, Ξ²2, Ξ²3, Ξ³1 and Ξ³2. The BM of adult normal oral squamous epithelium comprises the laminin chains, Ξ±3, Ξ±5, Ξ²1, Ξ²3, Ξ³1 and Ξ³2. A re-expression of the laminin Ξ±2 and Ξ²2 chains could be shown in adult hyperproliferative, dysplastic and carcinomatous lesions. In dysplasia and oral squamous cell carcinoma (OSCC), multifocal breaks of the BM are present as indicated by laminin chain antibodies. These breaks correlate to malignancy grade in their extent. Moreover, in the invasion front the Ξ±3 and Ξ³2 chain of laminin-5 can immunohistochemically be found outside the BM within the cytoplasm of budding carcinoma cells and in the adjacent stroma. The correlation between the morphological pattern of invasive tumour clusters and a laminin-5 immunostaining in the adjacent stroma may suggest, first, that a laminin-5 deposition outside the BM is an immunohistochemical marker for invasion and second, that OSCC invasion is guided by the laminin-5 matrix. Expression of oncofetal fibronectins (IIICS de novo glycosylated fibronectin and ED-B fibronectin) could be demonstrated throughout the stromal compartment. However, the ED-B fibronectin synthesizing cells (RNA/RNA in situ hybridization) are confined to small stroma areas and to single stroma and inflammatory cells in the invasion front. A correlation of the number of ED-B fibronectin synthesizing cells to malignancy grade could not be seen. ED-B fibronectin mRNA-positive cells seem to be concentrated in areas of fibrous stroma recruitment with a linear alignment of stromal fibro-/myofibroblasts (desmoplasia). Double staining experiments (ED-B fibronectin in situ hybridization and Ξ±-smooth muscle actin immunohistochemistry) indicated that the stroma myofibroblasts are a preferential source of ED-B fibronectin. In conclusion, in OSCC, a fetal extracellular matrix conversion is demonstrable. Tumour cells (laminin Ξ±2 and Ξ²2 chain) and recruited stromal myofibroblasts (oncofetal ED-B fibronectin) contribute to the fetal extracellular matrix milieu. Β© 1999 Cancer Research Campaig
Combination of temozolomide with immunocytokine F16βIL2 for the treatment of glioblastoma
Glioblastoma patients are still not cured by the treatments available at the moment. We investigated the therapeutic properties of temozolomide in combination with F16-IL2, a clinical-stage immunocytokine consisting of human interleukin (IL)-2 fused to the human antibody F16, specific to the A1 domain of tenascin-C
Human monoclonal antibodies targeting carbonic anhydrase IX for the molecular imaging of hypoxic regions in solid tumours
BACKGROUND: Hypoxia, which is commonly observed in areas of primary tumours and of metastases, influences response to treatment. However, its characterisation has so far mainly been restricted to the ex vivo analysis of tumour sections using monoclonal antibodies specific to carbonic anhydrase IX (CA IX) or by pimonidazole staining, after the intravenous administration of this 2-nitroimidazole compound in experimental animal models.METHODS: In this study, we describe the generation of high-affinity human monoclonal antibodies (A3 and CC7) specific to human CA IX, using phage technology.RESULTS: These antibodies were able to stain CA IX ex vivo and to target the cognate antigen in vivo. In one of the two animal models of colorectal cancer studied (LS174T), CA IX imaging closely matched pimonidazole staining, with a preferential staining of tumour areas characterised by little vascularity and low perfusion. In contrast, in a second animal model (SW1222), distinct staining patterns were observed for pimonidazole and CA IX targeting. We observed a complementary pattern of tumour regions targeted in vivo by the clinical-stage vascular-targeting antibody L19 and the anti-CA IX antibody A3, indicating that a homogenous pattern of in vivo tumour targeting could be achieved by a combination of the two antibodies.CONCLUSION: The new human anti-CA IX antibodies are expected to be non-immunogenic in patients with cancer and may serve as broadly applicable reagents for the non-invasive imaging of hypoxia and for pharmacodelivery applications. British Journal of Cancer (2009) 101, 645-657. doi: 10.1038/sj.bjc.6605200 www.bjcancer.com Published online 21 July 2009 (C) 2009 Cancer Research U
Optimal MHC-II-restricted tumor antigen presentation to CD4+ T helper cells: the key issue for development of anti-tumor vaccines
Present immunoprevention and immunotherapeutic approaches against cancer suffer from the limitation of being not βsterilizingβ procedures, as very poor protection against the tumor is obtained. Thus newly conceived anti-tumor vaccination strategies are urgently needed. In this review we will focus on ways to provide optimal MHC class II-restricted tumor antigen presentation to CD4+ T helper cells as a crucial parameter to get optimal and protective adaptive immune response against tumor. Through the description of successful preventive or therapeutic experimental approaches to vaccinate the host against the tumor we will show that optimal activation of MHC class II-restricted tumor specific CD4+ T helper cells can be achieved in various ways. Interestingly, the success in tumor eradication and/or growth arrest generated by classical therapies such as radiotherapy and chemotherapy in some instances can be re-interpreted on the basis of an adaptive immune response induced by providing suitable access of tumor-associated antigens to MHC class II molecules. Therefore, focussing on strategies to generate better and suitable MHC class IIβrestricted activation of tumor specific CD4+ T helper cells may have an important impact on fighting and defeating cancer
Objectively assessed disease activity and drug persistence during ustekinumab treatment in a nationwide real-world Crohn's disease cohort
ObjectiveLong-term evidence on ustekinumab treatment response and persistence in patients with Crohn's disease in a real-world setting is scarce. We performed a retrospective nationwide chart review study of long-term clinical outcomes in Crohn's disease patients treated with ustekinumab.MethodsThe study was conducted in 17 Finnish hospitals and included adult Crohn's disease patients who received an initial intravenous dose of ustekinumab during 2017-2018. Disease activity data were collected at baseline, 16 weeks, and 1 year from health records.ResultsThe study included 155 patients. The disease was stricturing or penetrating in 69 and 59% had prior Crohn's disease-related surgeries, and 97% had a treatment history of at least one biologic agent. Of 93 patients with >= 1 year of follow-up, 77 (83%) were still on ustekinumab at 1 year. In patients with data available, from baseline to the 1-year follow-up the simple endoscopic score for Crohn's disease (SES-CD) decreased from 10 to 3 (P = 0.033), C-reactive protein from 7 to 5 mg/L, (P ConclusionsUstekinumab treatment in patients with highly refractory Crohn's disease resulted in high long-term treatment persistence and significantly reduced disease activity, assessed with objective markers for intestinal inflammatory activity.</div
The role of tenascin-C in tissue injury and tumorigenesis
The extracellular matrix molecule tenascin-C is highly expressed during embryonic development, tissue repair and in pathological situations such as chronic inflammation and cancer. Tenascin-C interacts with several other extracellular matrix molecules and cell-surface receptors, thus affecting tissue architecture, tissue resilience and cell responses. Tenascin-C modulates cell migration, proliferation and cellular signaling through induction of pro-inflammatory cytokines and oncogenic signaling molecules amongst other mechanisms. Given the causal role of inflammation in cancer progression, common mechanisms might be controlled by tenascin-C during both events. Drugs targeting the expression or function of tenascin-C or the tenascin-C protein itself are currently being developed and some drugs have already reached advanced clinical trials. This generates hope that increased knowledge about tenascin-C will further improve management of diseases with high tenascin-C expression such as chronic inflammation, heart failure, artheriosclerosis and cancer
Combining the Strengths of Qualitative Comparative Analysis with Cluster Analysis for Comparative Public Policy Research: With Reference to the Policy of Economic Convergence in the Euro Currency Area
Qualitative Comparative Analysis (QCA) is a well-established method for comparing national public policy similarities and differences. It is argued that Cluster Analysis can add additional benefits to such research when used concurrently with QCA. Cluster Analysis provides a better method for the initial exploration of multivariate data and examining how countries compare because it can work with the full range of available interval data while patterns are created and viewed. This provides the best first method for exploring patterns and likely groupings of countries. QCA then provides a more robust method for theorizing about the construction of such groupings and their relationship around similar variable scores. QCA makes such theorizing transparent. The research example used to illustrate the benefits of combining Cluster Analysis and QCA is an analysis of the evolving of macroeconomic policy for the countries sharing the Euro, comparing 2005 (precrisis) with 2010 (postcrisis)
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