Qatar Foundation Annual Research Forum Volume 2012 Issue 1
- تاريخ المؤتمر: 21-23 Oct 2012
- الموقع: Qatar National Convention Center (QNCC), Doha, Qatar
- رقم المجلد: 2012
- المنشور: ٠١ أكتوبر ٢٠١٢
1 - 20 of 469 نتائج
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User engagement in the digital world
المؤلفون: Mounia LalmasIn the online world, user engagement refers to the quality of the user experience that emphasizes the positive aspects of the interaction with a web application and, in particular, the phenomena associated with wanting to use that application longer and frequently. This definition is motivated by the observation that successful web applications are not just used, but they are engaged with. Users invest time, attention, and emotion into them. User engagement is measured in many ways, through methods of self-reporting (e.g., questionnaires), observer methods (e.g., facial expression analysis, speech analysis, desktop actions, etc.), neuro-physiological signal processing methods (e.g., respiratory and cardiovascular accelerations and decelerations, muscle spasms, etc.), and from a web analytics perspective (through online behavior metrics that assess users' depth of engagement with a site). These methods represent various tradeoffs between scale of data and depth of understanding (for instance, surveys are small-scale but deep, whereas clicks are large-scale but shallow in understanding). Little work has been done to integrate these various measures into a coherent understanding of engagement success. We address this problem by combining techniques from web analytics and mining, information retrieval evaluation, and existing works on user engagement coming from the domains of information science, multimodal human computer interaction and cognitive psychology. In this way, we can combine insights from big data with deep analysis of human behavior in the lab or through crowd-sourcing experiment. This research comprises three "inter-woven" parts: (1) Definition of user engagement and its many characteristics. (2) Data-driven approaches looking at user engagement through the development of models that allow for a better representation of how users engage within and across different digital services. (3) How studying affect and cognition is providing additional insights into measuring user engagement.
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Mice as animal models for human disease
المؤلفون: Zaher Hanna and Paul JolicoeurBackground: Many human diseases lack validated animal models, hampering translational progress in several important disease areas. New and improved models can often be developed by recapitulating phenotypes related to those associated with human diseases. Objectives: Our lab has been interested in generating and characterizing several transgenic (Tg) animal models. These Tg animals were used to explore, on the cellular and molecular levels, the pathological mechanisms underlying several diseases, including immunological, neurodegenerative diseases, viral infections, cardiovascular disease, and cancer. Methods: Transgenes construction, analyzing techniques, and generation of Tg mice are as described in literature. Results: Examples of research projects that utilized animal models in our lab include: - Infectious diseases such as the acquired immunodeficiency syndrome (AIDS), which is caused by the human immunodeficiency virus type 1 (HIV-1). HIV-1 causes disease only in humans and chimpanzees. Thus, a major obstacle to explore the cellular and molecular mechanisms by which HIV-1 acts in vivo and to study how HIV-1 causes disease has been the lack of a small and cheap animal model. However, we have overcome the block to disease induction in rodents by generating Tg mice that express HIV-1 in the same immune cells that are normally infected in AIDS patients. These mice develop a severe AIDS-like disease leading to early death. Several pathological phenotypes, remarkably similar to those observed in HIV-1 infected individuals, were found. These included signs of growth retardation and wasting, atrophy of all lymphoid organs, preferential loss of CD4+ T cells, and interstitial nephritis and pneumonitis. More details will be presented. - Cancers such as leukemia and lymphoma as caused by murine leukemia viruses (MuLV) in inoculated mice. Their proviruses integrate in the vicinity of various genes involved in growth regulation, and act as insertion mutagens. We are using this retroviral insertion mutagenesis approach to identify novel oncogenes involved in T- or B-cell lymphomas induced by various MuLVs. We have succeeded in identifying novel oncogenes responsible for the onset of cancer. Among these oncogenes are members of Notch family, which are now under intense investigation to understand their role in inducing cancer. The details of these studies will be presented. Conclusions: It is likely that these novel Tg models will prove valuable in evaluating new pharmacological drugs, vaccines and disease therapies.
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The proprotein convertases in health and disease
المؤلفون: Nabil G. SeidahBackground: The mammalian proprotein convertases (PCs) constitute a family of nine secretory serine proteases related to bacterial subtilisin and yeast kexin. Seven of them (PC1/3, PC2, furin, PC4, PC5/6, PACE4 and PC7) activate cellular and pathogen precursor proteins by cleavage at single or paired basic residues, while SKI-1/S1P and PCSK9 regulate cholesterol/lipid homeostasis via cleavage at non-basic residues or through induced degradation of receptors. PCs are now considered attractive targets for the development of powerful novel therapeutics. In this poster presentation, I will summarize the physiological functions and pathological implications of the PCs and discuss proposed strategies to control some of their activities, including their therapeutic application and validation in selected disease states. Objectives: The concept of the cleavage of precursor proteins to generate active products was born 47 years ago and the cognate convertases were identified during a 13-year period that ended in 2003 with the identification of PCSK9. Since the discovery of the PCs, efforts have been deployed to identify specific functions of PCs in animal models and humans in both health and disease and they have been implicated in a wide variety of cellular processes that regulate both body homeostasis and multiple disease states. While most PCs exert their functions through cleavage of substrates either at basic or non-basic amino acids, PCSK9 only requires its enzymatic activity to autocatalytically process its prosegment in the endoplasmic reticulum, and is secreted as an inactive protease. The challenging identification of safe orally active small molecule inhibitors of some of the convertases, especially PCSK9, is definitively a future goal that should be pursued vehemently. Conclusions: The use of biologics and desirable automated injection procedures or minimally invasive methods may be the future for effective PC-based therapies. The future is indeed bright and awaits innovative and practical approaches to target these exciting and multifunctional enzymes. The topics discussed here will encourage the investigation and development of potent and effective PC-inhibitors/silencers, and minimally invasive procedures for delivery to patients, which would be highly beneficial in the clinical treatment of diseases in which PCs play a key role.
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Identification and characterization of inhibitors of G protein-coupled receptor kinase 6 (GRK6) as potential therapeutics for multiple myeloma
Multiple myeloma (MM) is one of the most common hematological malignancies, but current therapy options are limited to high-dose chemotherapy or high-risk stem-cell transplantation. In a recent kinome-wide RNAi study by Tiedemann and colleagues (2010), the G-protein coupled receptor kinase 6 (GRK6) was identified as a critical kinase required for survival of MM cells. This study also suggests that MM cells, but not other cell types, are dependent on GRK6; and that gene silencing by shRNA or siRNA of GRK6, but not other GRKs, results in decreased survival. At present, the G protein-coupled receptor (GPCR) signaling mediated by GRK6 in MM cells is not well understood. Through gene silencing techniques and expression of either the wild-type or kinase-dead form of GRK6 protein, we determined that a functional GRK6 kinase domain is required for survival of MM cells. These findings helped validate that the GRK6 kinase domain is a potential target for MM, and have spurred the investigation of small molecule kinase inhibitors of GRK6. By screening a cassette of compounds that are known as kinase inhibitors, compounds with moderate potency in preliminary biochemical assays were identified and further evaluated. As part of this effort we identified CX-4945, which is a known potent and selective ATP-competitive small molecule protein kinase CK2 inhibitor (IC₅₀ of 1 nM for recombinant human CK2α) as a moderately potent inhibitor of GRK6 (IC₅₀ on GRK6 = 300-500 nM). Herein we describe the design and synthesis of novel analogs of CX-4945 and key structure activity relationships (SAR) of this chemical series against GRK6 that serve as a platform for further optimization.
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Personalized peptide-based vaccine design for prostate cancer immunotherapy
المؤلفون: Simo Arreadouani, H. Kissick, L. Dunn, S.T. On and M.G. SandaBackground: The recent approval by the FDA of the autologous, cell-based vaccine Provenge was hailed as a major advance for the treatment of advanced prostate cancer (PCa) and reinvigorated interest in the field of PCa immunotherapy. Peptide-based vaccines represent a viable, cost-effective formulation in the field of cancer vaccine development. This approach has been used successfully to treat melanoma where vaccination with gp100-derived peptide in combination with IL-2 gave a 6.7 month improvement in overall survival compared to IL-2 alone. Objectives: Our goal was to identify immunogenic epitopes from gene rearrangement products and tumor coding mutations to generate vaccines for prostate cancer immunotherapy. Methods: We used a 3-step, in silico/in vitro/in vivo approach to identify HLA-A2.1-restricted, immunogenic epitopes derived from the highly prostate tumor-specific antigen ERG, a component of the TMPRSS2:ERG gene fusion that occurs in about 50% of PCa cases. We designed longer epitopes that exhibit helper function through activation of CD4 T lymphocytes. We screened RNAseq data from prostate tumors to identify potential immunogenic epitopes that rise from coding mutations. Predicted epitopes are tested in humanized mice for immunogenicity. Anti-tumor effect of epitope-specific cytotoxic lymphocytes is tested against human prostate tumor cell lines. Results: We have identified several epitopes from ERG that induced a strong immune response in humanized HLA-A2.1+ mice and overcame peripheral tolerance in prostate specific ERG-expressing TRAMP-HLA-A2.1-ERG+ mice. Additionally, we have designed long peptides that target both MHC-I and MHC-II molecules and overcome the need for helper peptides. These immunogenic epitopes are naturally processed and presented by tumor cells to mediate cytotoxicity. Finally, we used RNAseq to identify a high number of tumor-specific, panHLA-customized, coding mutations, including those from KRas oncogene, that exhibit immunogenicity in vivo. Conclusion: Our findings provide proof of concept for peptide-based vaccines that are tailored to the tumor's molecular profile, and lay the ground for future development of personalized vaccines for clinical use.
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Pharmacological modulators of stem cells as novel therapeutics
المؤلفون: Ramzey Abujarour, Bahram Valamehr, Monica Bennett, Megan Robinson and Peter FlynnFate Therapeutics (Fate) is pursuing the pharmacological modulation of adult stem cells to enhance tissue regeneration. Fate's lead clinical program, ProHema, consists of pharmacologically-enhanced hematopoietic stem cells (HSCs), designed to improve HSC engraftment and hematopoietic reconstitution during the normal course of a stem cell transplant for the treatment of patients with hematologic malignancies. Fate is currently conducting three clinical phase II trials of ProHema (FT1050‐enhanced umbilical cord blood). In addition, Fate is advancing a human recombinant protein, FT301, engineered for improved pharmacologic properties, and for driving the regeneration of skeletal muscle cells for use in atrophy and dystrophy. FT301 has a novel mode of action that results in the expansion of satellite stem cells. Fate has applied its proprietary induced pluripotent stem cell (iPSC) technology to test the efficacy of FT301 in a human model of Duchenne muscular dystrophy (DMD). We established iPSC lines from patients with DMD, and explored the regenerative capacity of FT301 on myoblasts generated from the DMD-specific iPSCs. Treatment of the iPSC-derived muscle fibers with FT301 induced significant hypertrophy confirming our in vitro and in vivo observed effects of FT301 in inducing productive muscular hypertrophy, and highlighting its possible application in muscular degenerative disorders.
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Selective inhibition of nuclear export function for cancer therapy
المؤلفون: Ramzi M Mohammad, Asfar S. Azmi, Sharon Shacham and Michael KauffmanBackground and Aims: Tumor suppressor proteins (TSPs) are inactivated by many different mechanisms, including nuclear exclusion by the chromosome region maintenance protein (CRM-1). Increased tumor levels of CRM-1 have been correlated with poor prognosis of patients with different cancers, making it a therapeutic target. We have developed selective inhibitors of nuclear export (SINEs) that bind to CRM-1 to irreversibly inhibit its ability to export proteins. Here we investigated our new class of SINEs in multiple tumor models. Methods: We studied the effects of SINE analogs in a panel of pancreatic, colon, triple-negative breast cancer (TNBC), prostate, non Hodgkin's lymphoma (NHL) cell lines and non-transformed/normal cells using proliferation, apoptosis, immunoblot, co-immunoprecipitation, small inhibitor (Si)-RNA, and fluorescence microscopy analyses. The effects of the SINEs were also investigated in mice with subcutaneous, orthotopic tumors and in disseminated liquid tumor models. Results: SINEs (KPT-185, KPT-127, KPT-205, and KPT-227) inhibited proliferation and promoted apoptosis of both solid liquid cancer cells, but did not affect normal lymphocytes or immortalized non-transformed cells. The nuclei of cells incubated with KPT-185 accumulated major TSPs such as p53, p73, p27, FOXO, p73, and prostate apoptosis response 4 (PAR-4) and inhibited interactions between CRM-1 and these proteins. Mutations in the region of CRM-1 that binds to SINEs (Cys-528), or siRNA knockdown of TSPs, prevented the ability of KPT-185 to block proliferation and induce apoptosis of cancer cells. Oral administration of the KPT SINEs to mice reduced growth of subcutaneous, orthotopic and disseminated xenograft tumors without major toxicity. Analysis of tumor remnants showed that KPT-SINE disrupted the interaction between CRM-1 and TSP, activated TSP function, and reduced proliferation of tumor cells. Conclusion: We identified SINEs that inhibit CRM-1 and promote nuclear accumulation of tumor suppressor proteins in multiple tumor models. Oral administration of the drug to mice reduces growth of xenograft tumors. Based on our solid preliminary studies a phase I clinical trial has been initiated for both solid tumors and hematological malignancies. Our results provide conclusive evidence in support of a global therapy for different cancers that involves targeted inhibition of nuclear export protein function and warrants advanced clinical investigations.
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Regulation of ERBB2 signaling and response to Trastuzumab by DARPP-32 in esophageal adenocarcinoma
المؤلفون: Wael El-Rifai and Jun HongBackground: Esophageal adenocarcinoma (EAC) is characterized by a poor response to therapy with less than 10% five-year survival rates. Although Herceptin, a humanized monoclonal anti-ERBB2 antibody, has been successfully used for treatment of ERBB2-positive metastatic breast and gastroesophageal junction adenocarcinoma, a significant proportion of patients either fail to achieve initial response or develop acquired resistance. Clinical trials using Herceptin for the treatment of esophageal and gastroesophageal adenocarcinomas are ongoing in several Western countries. Understanding mechanisms that could hamper the response to Herceptin could influence the therapeutic decision making options and the management of these patients. Methods and Results: Truncated DARPP-32 (t-DARPP) (dopamine and cyclic AMP-regulated phosphoprotein of Mr 32,000), located at the 17q21 region, is a commonly amplified and overexpressed gene in upper gastrointestinal malignancies. The CellTiter cell viability, clonogenic survival, and Annexin V assays results indicated that stable or transient t-DARPP expression in OE19 cells significantly promoted cell survival and blocked apoptosis after treatment with 20 μg/ml Herceptin (p<0.01). The western blot results showed that t-DARPP sustained p-ERBB2 (Y1248) and p-AKT (S473) protein levels in response to Herceptin. Conversely, knockdown of endogenous t-DARPP in OE33 cells significantly decreased cell survival and p-ERBB2 (Y1248) and p-AKT (S473) protein levels in response to Herceptin (p<0.01). Western blot results showed that transient and stable t-DARPP expression without Herceptin increased protein levels of ERBB2, p-ERBB2 (Y1248), and p-AKT (S473). We hypothesized that t-DARPP enhances ERBB2 protein stability, thus blocking ERBB2 receptor steady-state down-regulation. The cycloheximide-based chase assay results showed that stable expression of t-DARPP increased the half-life of ERBB2 protein to 43.6 hours as opposed to 29.6 hours in control cells. We next investigated the effect of t-DARPP on Herceptin binding to ERBB2 receptor. Using co-immunoprecipitation, we have also shown that t-DARPP interacts with ERBB2 protein, hence, interfering with Herceptin binding to ERBB2 receptor, blocking Herceptin-induced down-regulation of downstream signaling. We also developed a Herceptin-resistant OE19 cell model, generated after selection with Herceptin for six months. The acquired resistance cell model demonstrated upregulation of endogenous t-DARPP and recapitulated the signaling events of Herceptin resistance. Conclusions: Our data demonstrate, for the first time, that t-DARPP enhances AKT signaling and is a key contributor to Herceptin resistance in EAC. In addition, t-DARPP mediates resistance to Herceptin through blocking ERBB2 receptor drug accessibility in EAC. The studies using in vivo models are ongoing.
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Efficient siRNA delivery and gene silencing using self-assembled rosette nanotubes
المؤلفون: Hicham Fenniri, Uyen Ho and Aws AlshamsanBackground: Self-assembly and self-organization processes offer a powerful strategy for the design of nanomaterials from the ground up with predefined dimensions and properties. Central to these approaches is the design and synthesis of molecules with a built-in ability to undergo a hierarchical sequence of supramolecular reactions, culminating with the formation of a well-defined functional superstructure. The rosette nanotubes (RNTs) are a new class of biocompatible organic nanomaterials with tunable dimensions and properties. They are obtained through the hierarchical self-assembly of small synthetic organic molecules. They can be readily tailored to target and kill cancerous cells. Objectives: Our aim is to address the following issues: (i) extent to which the RNTs can capture and deliver siRNA to a tumour while retaining their activity, (ii) advantages and/or limitations of RNTs compared to clinically tested drug delivery systems (DDS), (iii) effectiveness of RNT-based formulations in cancer treatment, (iv) specificity and real-time tracking of the RNT DDS, (v) toxicity profile of the new RNT DDS, (vi) identification of optimal cancer targets for the RNT DDS, and (vii) categorization of the therapeutic advantages/challenges of this system in animal models. Methods: We have designed a family of RNTs and characterized them chemically and structurally. We have also tested their ability to capture siRNA and deliver it to cancer cells. Results: The binding efficiency was shown to be a function of RNT/siRNA ratio, net charge, and local cationic density. These formulations were reproducible at different ionic strength media and were shown to protect siRNA from degradation by serum nucleases. Moreover, the presence of siRNA also played a role in dictating the supramolecular shape of the nanocarrier, which may reflect in-cell uptake and the resulting silencing process. Fluorescence microscopy showed that Caco-2 cells can take up RNT derived assemblies very readily within 4 hours and retain siRNA up to 72 hours. Silencing experiments showed a dose-dependent reduction in VEGF protein levels secreted by Caco-2 cells reaching approximately 40% reduction at 20 nM siRNA. Conclusions: We have shown that the RNTs are effective oligonucleotide carriers. Future studies will involve animal studies and further optimization of the observed therapeutic effect.
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Insights into the mechanism of function of a protein unfolding and degradation system
المؤلفون: Walid HouryClpP is a cylindrical tetradecameric serine protease whose activity is regulated by the unfoldase ATP-dependent chaperones ClpX and ClpA of the AAA+ superfamily. The chaperones act to select substrate proteins, unfold them, and then thread them into the ClpP cylinder for degradation. ClpP can only degrade small peptides on its own. Structural and functional studies from my group have elucidated the mechanism of function of the ClpXP chaperone-protease system. These studies highlighted the importance of protein dynamics in this system. More recently, we used ClpP as a target in a high-throughput screen for compounds, which activate the protease and allow it to degrade larger proteins, hence, abolishing the specificity arising from the ATP-dependent chaperones. Our screen resulted in five structurally distinct compounds, which we designate as activators of self-compartmentalizing proteases 1 to 5 (ACP 1 to 5). The compounds are found to stabilize the ClpP double ring structure. The ACP1 chemical structure was considered to have drug-like characteristics and was further optimized to give analogs with bactericidal activity. Hence, the ACPs represent new classes of compounds that can activate ClpP and that can be developed as potential novel antibiotics.
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The cancer multi-disciplinary team from the co-ordinators' perspective:
المؤلفون: Rozh Jalil, Benjamin Lamb, Stephanie Russ, Nick Sevdalis and James GreenBackground: The multi-disciplinary team (MDT) coordinator’s role is relatively new and as such is evolving. What is apparent is that the coordinator's work is pivotal to the effectiveness and efficiency of an MDT. Objectives: This study aimed to assess the views and needs of MDT-coordinators. Methods: Views of MDT-coordinators were evaluated through an online survey that covered their current practice and role, MDT chairing, opinions on how to improve MDT meetings, and coordinators' educational/training needs. Results: 265 coordinators responded to the survey. More than one third of the respondents felt that the job plan does not reflect their actual duties. It was reported that medical members of the MDT always contribute to case discussions. 66.9% of the respondents reported that MDTs are chaired by surgeons. The majority reported having training on data management and IT skills but more than 50% reported that further training is needed in areas of oncology, anatomy and physiology, audit and research, peer-review, and leadership skills (Figure 1) Conclusions: The MDT coordinator’s role is central to the care of cancer patients. The study reveals areas of training requirements that remain unmet. Improving the resources and training available to MDT-coordinators can give them an opportunity to develop the required additional skills and contribute to improved MDT performance and ultimately cancer care. MDTs in the developmental stage should benefit from the experience of well-established organisations to enhance the cancer care. Finally, this study acknowledges the recent launch of a new e-learning training programme for MDT coordinators that is an important resource for these cancer key workers.
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Analog-to-digital conversion, a practical approach and its applications in real world system-on-chip (SOC)
المؤلفون: Maher SarrajData converters play a crucial role in interfacing real time analog signals to the digital processing circuitry. Almost every SOC (system-on-chip) silicon design has an analog front/back end, which includes either an ADC (analog-to-digital converter) or a DAC (digital-to-analog converter). There is a wide range of applications that uses data converters spanning from medical systems to industrial control to audio players like the iPod. The resolution and speed of the converter depends on the application. For example, in video processors, the ADC resolution is 8/10 bits and the clock rate is approximately 150 MHz; whereas in digital audio applications, the resolution is much higher at 16/24 bits and the clock rate is about 44 KHz. We will discuss how ADCs are used in touch screen controllers and in high-energy detectors or medical imaging systems.
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Design and fundamental limitations of large-scale coherent dynamical networks
المؤلفون: Bassam BamiehNetworks of dynamical systems occur in diverse areas of engineering, such as distributed computation, automated vehicular formations, and power systems networks. We investigate the interplay between network coherence and the network's interconnection topology. In such networks, synchronization or more general coherence under stochastic uncertainty is an important measure of performance. For example, in power systems this notion corresponds to phase and frequency coherence of multiple generators (the lack of which may lead to so-called inter-area oscillations), while in vehicular formations this notion corresponds to how well vehicles are collectively tracking their commanded trajectories. We study abstractions of all of the above problems as distributed/cooperative control problems. We investigate the asymptotic limits of performance when network sizes become large as a function of the networks' topologies. This has important implications for the design of future highly-distributed-generation power networks, as well as large vehicular formation schemes such as those in proposed automated highway systems. This talk will specifically address the notion of network coherence under stochastic disturbances, and its dependence on network topology and various notions of network dimension. Regular lattices and fractal networks provide case studies with both integer and fractional dimension. We give asymptotic lower bounds on network disorder and show its dependence on both the complexity of individual node dynamics, as well as network dimension. It turns out that higher connectivity improves coherence, while more complex node dynamics can hinder it. However, in all cases there is a critical network dimension above which purely local interactions can lead to the emergence of global order. We outline the connections between these results and those on the statistical mechanics of harmonic solids. For future highly-distributed-generation power networks, we quantify the cost of synchronization in terms of resistive line losses due to the power flow needed to achieve this synchrony. We show that this cost scales unboundedly with the number of generators in the network and is independent of the underlying connection topology. This result is a further argument for the use of information communication rather than only power flows to enhance synchrony in such large networks.
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High-Tc superconductivity: from basic research to useful applications
المؤلفون: Walid Malaeb, Yukiaki Ishida, Kozo Okazaki, Yuuichi Ota and Sik ShinBackground: Superconductivity is the complete loss of electric resistance in some elements and compounds cooled below a transition temperature (Tc). Since its discovery more than 100 years ago, this phenomenon has enriched basic science in ways that nobody could have foreseen. Moreover, superconductors have been used in various applications like power transmission, high magnetic field generation, levitated high-speed trains (MAGLEV), and magnetic resonance imaging (MRI). In a county, like Qatar, seeking to find alternative renewable energy sources, superconductors can be greatly useful in connecting the electric power generated from the renewable energy sources (solar and wind power) with superconducting devices (especially cables) to fulfill the energy saving and sustainability objectives. Objectives and methods: The effective use of superconductors in applications requires a better understanding of the basic phenomena of high-Tc superconductivity. For this purpose, several techniques are used especially photoemission spectroscopy which is considered as the most powerful tool to directly investigate the electronic structure of solids including superconductors. This technique is based on the photoelectric effect where various light sources like synchrotron radiation, lasers and others may be used. We have been using photoemission spectroscopy to investigate the electronic structure of newly discovered superconductors known as iron pnictides since their discovery in Japan in 2008. We have used several facilities like the Institute for Solid State Physics at the University of Tokyo in Japan, Photon Factory in Japan, Hiroshima Synchrotron Radiation Center at Hiroshima University in Japan, and Stanford Synchrotron Radiation Lightsource at Stanford University in USA. Our work was published in refereed scientific journals and presented at many international conferences worldwide and has had important implications on this field from the very early stage. Results and conclusions: In this paper, I will present an introduction about superconductivity and highlight on its various possible applications especially in Qatar. Also I will present an overview of our research on newly discovered iron pnictide superconductors using photoemission spectroscopy and how our results led to a better understanding of high-Tc superconductivity in these compounds.
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Integration of solar energy with post-combustion carbon capture
المؤلفون: Ali Abbas, Abdul Qadir, Rajab Khalilpour and Matteo ChiesaBackground: A techno-economic analysis has been performed for a coal-fired power plant retrofitted with solvent-based post-combustion carbon capture (PCC) technology where thermal energy is partially supplied by solar thermal collectors. The plant is compared with a generic PCC plant where all the thermal energy is provided by steam bled from the steam cycle. A suite of solar thermal collectors which include flat plate collectors, compound parabolic collectors, linear Fresnel collectors, evacuated tube collectors (ETCs) and parabolic trough collectors (PTCs) have each been tested for their viability. The plant has been simulated for several different locations in Australia: Sydney, Townsville and Melbourne. Objectives: This study investigates the integration of solar thermal energy in the energy mix of a power plant by using it to partially compensate for the debilitating energy penalty burdened by the introduction of the carbon capture process. Methods: The overall system consists of three subsystems: power plant, PCC plant and solar collector field. A base case scenario is studied in which there is no heat integration between the three subsystems and is compared to a system with heat integration. Additionally, incentives such as renewable energy certificates (RECs), carbon tax/credits and government subsidies have been considered in the economic model and a sensitivity analysis has been performed for each scenario of incentives for all five solar collector technologies at the three locations. Results: The ETC is found to be the best performer amongst solar collectors when the three subsystems have good heat integration while the PTC is the best performer in the case of no heat integration. The best location for the solar-assisted PCC (SPCC) plant is found to be Sydney. Conclusions: The SPCC plant is only economically viable in Sydney and Townsville once incentives such as RECs, carbon tax and subsidies are taken into account. By the use of solar energy and the available government incentives for their deployment, the cost of carbon capture is shown to be reduced.
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Modeling and characterization of deformation in magnesium alloys for energy efficiency
المؤلفون: Hussein Zbib, Hesam Askari, John Young, David Field and Ghassan KridliThe need to produce vehicles with improved fuel efficiency and reduced emissions has led the automotive industry to consider the use of "lightweighting" materials in the construction of automotive body and chassis systems. Towards this end, interest has been increasingly focusing on the use of sheet magnesium in the manufacture of panels and structural components by utilizing recent advances in twin-roll casting technology of magnesium. However, challenges in the areas of manufacturing, material processing and modeling need to be resolved in order to fully utilize magnesium alloys. Despite the limited formability of magnesium alloys at room temperature due to its hexagonal close-packed crystalline structure, studies have shown that the formability of magnesium alloys can be significantly improved by processing the material at elevated temperatures and by modifying the microstructure to increase ductility. Such improvements can potentially be achieved by processes such as superplastic forming and warm forming along with sheet manufacturing techniques such as Twin Roll Casting (TRC). In this work we investigate the superplastic behavior of twin-roll cast AZ31B through mechanical testing, microstructure characterization and modeling. The experimental results show that the as-received AZ31B sheet consists of relatively large gains, and while it is brittle at low temperature it is ductile at high temperature with activation energies of the deformation close to that of lattice diffusion. The material analyzed possesses medium strain-rate sensitivity of 0.27 with a relatively modest ductility of about 74%. Based on the experimental results, we use a physically-based constitutive model for deformation. The model integrates the main microstructural features, grain shape and grain orientations, within a self-consistent viscoplasticity theory with internal variables. Simulation of the deformation process at room temperature shows activity of the basal and prismatic systems at the early stages of deformation and increasing activity of pyramidal systems due to twinning. The predicted texture from the model is consistent with the experimental results. With the use of the appropriate model parameters, the stress strain relationship can be described accurately over the range of low strain rates.
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Recent progress in wide bandgap materials GaN/InGaN for concentrated photovoltaics
المؤلفون: Abdallah Ougazzaden, K. Pantzasa, T. Moudakirb, S. Sureshb, Y. El Gmilib, J. Dickersona and P. L. VossaIn recent years, concentration has been adopted as a promising strategy to high $/W ratio of photovoltaic energy conversion. In concentrated photovoltaics, the Sun's energy is focused into a smaller area allowing for the conversion of sunlight into electricity using only a small low-cost photovoltaic cell. Conventional solar concentrators, which use III-V are, however, costly to produce. Ideally, the material should perform well under high concentration and be affordable. We propose to construct solar cells based on an excellent candidate materials system, InGaN, whose band gap can be adjusted from 0.7 eV to 3.4 eV as the indium content is reduced. Recent progress has resulted in InGaN solar cells with 97% internal quantum efficiency and 57% external quantum efficiency with an active region only 60 nm thick. This work demonstrates that electron-hole pairs are very efficiently collected in InGaN materials and the absorption is very strong at the band gap. The toughness of the nitride materials translates into its excellent performances under harsh environments: high temperature and humidity and high concentration. Georgia Tech-CNRS and their partners have developed unique lift-off technologies that dramatically lower nitride cost as a result of the ability to reuse the substrates used for the growth of nitrides. These lift-off technologies are also favorable for integration of InGaN cells with building materials like glass or metal, or with other solar cells, such as those made of silicon. In this presentation InGaN solar cells progress and results will be presented.
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Chlorine dioxide production on-demand under ambient temperature and pH in water
المؤلفون: Mahdi Abu-Omar, Scott Hicks and Curt BougherThe oxyanions of chlorine have seen multiple uses from bleaching to oxidizers in rocket fuel. Concerns over their accumulation in the environment, particularly that of perchlorate, have risen over the past two decades. Both chlorate (ClO₃¯) and chlorite (ClO₂¯) are employed in the generation of chlorine dioxide gas (ClO₂), which has been used in water treatment, disinfections, the pulp bleaching industry, and as an oxidizing agent. The lack of stability of ClO₂ and difficulties associated with its storage require its generation on-demand. Current methods employ harsh and corrosive conditions that require sulfuric acid and produce large amounts of salt and unwanted byproducts. Inspired by nature and how microorganisms isolated from contaminated sites degrade the oxyanions of chlorine, our research group developed catalysts based on manganese, a cheap and earth-abundant metal, for the conversion of chlorite to ClO₂ under ambient temperature and pH in aqueous solution. Two families of catalysts have been shown effective for this reaction, water-soluble manganese porphyrin/heme complexes and manganese compounds supported by simple polypyridyl cage ligands. Several spectroscopic techniques such as UV-vis, EPR, X-ray, mass spectrometry, and ion chromatography have been employed in the characterization of intermediates and products. Study of the reaction kinetics in conjunction with isotope labeling experiments has lead to mechanistic insight on the relevant species involved in catalysis. The prevailing pathway appears to involve an unprecedented homolytic Cl-O bond cleavage of chlorite at the metal site to generate high-valent manganese oxo and solvated chlorine oxide radical. The implication of these mechanistic insights on the reaction chemistry and development of future practical catalysts will be discussed.
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Evaluation of contaminant transport and vulnerability of groundwater using the emission-transmission-immission-concept (ETI)
المؤلفون: Rafig AzzamThe evaluation of the contaminant transport is dictated by the Federal Soil Protection Regulation (BBodSchV, 1999) for sites that are suspected to endanger the groundwater. Vulnerability maps are often used for this evaluation. However, vulnerability maps consider the intrinsic vulnerability according to different methods taking some soil properties into account. Such qualitative method is not accurate when it comes to calculate the contaminant transport and looking at the specific vulnerability. Within the framework of a research project, a new investigation concept for the prediction of contaminants input into the groundwater was developed. This concept considers the estimation of the emission (E) of the contaminants, i.e., the time dependent amount and concentration of the leachate of the contamination source. The amount of leachate can be estimated by the infiltration of the groundwater recharge for every hydrological year using hydrological parameters. The expected concentration can be obtained from elution tests. In a second step, the transmission (T), i.e., the pollutant transport through the unsaturated zone into the groundwater is evaluated. This evaluation considers the transport mechanisms advection, diffusion and the retardation potential of the transmission zone. As a result, the immission (I) into the groundwater, the amount and concentration of the contaminants input can be estimated. Finally, it is important to evaluate the sensitivity of the system by classifying the groundwater according to the source value. This evaluation technique comprises a characterization of the site and an estimation of the contamination potential by conducting laboratory and in-situ tests and a numerical simulation modelling involving iteration for a contaminant mass balance. In this paper, a new testing method in a diffusion cell for the determination of the characteristic parameters for the transport mechanisms including the retardation potential is described and an evaluation concept for the contaminant transport based on the testing results is presented and discussed.
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Variation in codend selectivity parameters between hauls and years in trawl nets for swordtip squid (Loligo edulis)
المؤلفون: Mohamed Salah Mahjoub, Daisuke Shiode and Tadashi TokaiBackground: Trawl net fisheries are effective fishing activities, but often cause bycacth and discards issues for commercial species of unmarketable small size and endangered species. It is well accepted that codend mesh has size sorting properties for fish and other animals, and the codend selectivity is usually used as one of fisheries management measures to protect small animals. In the ocean, squids are abundant and still prospective fisheries resources, and especially swordtip squid is commercially important because of its good taste and high price in Japan and China. Objectives: Difference in selectivity parameters a, b and p could occur between years. This study objective is to analyze the variation between years and between hauls in selectivity parameters for swordtip squid (Loligo edulis) having a peculiar soft body type. Methods: A total of 23 experimental hauls were carried using trouser trawl onboard the research and training vessel Umitaka-Maru of the Tokyo University of Marine Science and Technology from 2006 to 2011, with 60mm mesh size test codend and 8.3mm mesh size control codend. Mantle length and girth of the swordtip squid caught were measured in cm. Catches were modeled by fitting codend selectivity parameters (a, b and p) in the Share Each LEngth Catch to the Total (SELECT) process and its variation between hauls and between years tested by the Akaike's Information Criterion (AIC) model selection. Results: The model with common logistic parameters a and b in each year and different split parameter p for each haul had a better estimation, confirmed by AIC. There was a variation in the 50% retention length (l50) from 6.04 to 7.11 cm and in the selection range, (S.R.) from 0.62 to 5.05 cm, which resulted in different selection curves annually. Conclusion: The difference in selection curves occurred although the codend used was the same. The fluctuation in S.R. was large compared with the l50, which could result from the small sample size. Others possible reasons are the yearly change in mesh size, catch size, and so on. This result is useful for fisheries managers to consider mesh size regulation for squid resource conservation.
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