4,743 research outputs found
Hidden Translation and Translating Coset in Quantum Computing
We give efficient quantum algorithms for the problems of Hidden Translation
and Hidden Subgroup in a large class of non-abelian solvable groups including
solvable groups of constant exponent and of constant length derived series. Our
algorithms are recursive. For the base case, we solve efficiently Hidden
Translation in , whenever is a fixed prime. For the induction
step, we introduce the problem Translating Coset generalizing both Hidden
Translation and Hidden Subgroup, and prove a powerful self-reducibility result:
Translating Coset in a finite solvable group is reducible to instances of
Translating Coset in and , for appropriate normal subgroups of
. Our self-reducibility framework combined with Kuperberg's subexponential
quantum algorithm for solving Hidden Translation in any abelian group, leads to
subexponential quantum algorithms for Hidden Translation and Hidden Subgroup in
any solvable group.Comment: Journal version: change of title and several minor update
Special aspects in pediatric surgical inpatient care of refugee children : a comparative cohort study
Background: Recently, the number of refugees in Germany has skyrocketed, leading to a marked increase in refugee children admitted to hospitals. This study describes the special characteristics encountered in pediatric surgical inpatient refugees compared to locally residing patients. Methods: Hospital records of minor refugees admitted to our department from 2005 up to and including 2015 were retrospectively reviewed. Demographic data, diagnoses, comorbidities, body mass indexes, hemoglobin values, and lengths of stay were extracted and statistically compared to local patients. Results: A total of 63 refugee children were analyzed and compared to 24,983 locally residing children. There was no difference in median body mass index (16.2 vs. 16.3, respectively, p = 0.26). However, refugee children had significantly lower hemoglobin values (11.95 vs. 12.79 g/dL, p < 0.0001) and were more likely to be colonized with methicillin-resistant Staphylococcus. aureus (8% vs. 0.04%, p < 0.01). Refugees were much more likely to present with burn injuries (16% versus 3% of admissions, p < 0.001), esophageal foreign bodies (4% vs. 0.5%, p < 0.001), as well as trauma, except for closed head injury. Conclusion: The cohort of refugee children in this study was found to be at a particular risk for suffering from burn injuries, trauma, foreign body aspirations, and anemia. Appropriate preventive measures and screening programs should be implemented accordingly
Aerodynamic Analysis of Turboprop Engine Air Intake
The objective of this paper is to present CFD computation of a LET L-410 engine nacelle equipped with a Walter M-601E turboprop engine. The main purpose is to estimate the air intake fluid characteristics of different air intake geometries. The results of these computations are part of an optimisation process focused on increasing the performance and reducing the losses in the ‘engine - nacelle` system. A problem with flow separation in the input section was observed. This project is supported by Ministry of Industry and Trade of the Czech Republic
Computational Modeling of Single-Cell Migration::The Leading Role of Extracellular Matrix Fibers
Cell migration is vitally important in a wide variety of biological contexts ranging from embryonic development and wound healing to malignant diseases such as cancer. It is a very complex process that is controlled by intracellular signaling pathways as well as the cell's microenvironment. Due to its importance and complexity, it has been studied for many years in the biomedical sciences, and in the last 30 years it also received an increasing amount of interest from theoretical scientists and mathematical modelers. Here we propose a force-based, individual-based modeling framework that links single-cell migration with matrix fibers and cell-matrix interactions through contact guidance and matrix remodelling. With this approach, we can highlight the effect of the cell's environment on its migration. We investigate the influence of matrix stiffness, matrix architecture, and cell speed on migration using quantitative measures that allow us to compare the results to experiments
High rate locally-correctable and locally-testable codes with sub-polynomial query complexity
In this work, we construct the first locally-correctable codes (LCCs), and
locally-testable codes (LTCs) with constant rate, constant relative distance,
and sub-polynomial query complexity. Specifically, we show that there exist
binary LCCs and LTCs with block length , constant rate (which can even be
taken arbitrarily close to 1), constant relative distance, and query complexity
. Previously such codes were known to exist
only with query complexity (for constant ), and
there were several, quite different, constructions known.
Our codes are based on a general distance-amplification method of Alon and
Luby~\cite{AL96_codes}. We show that this method interacts well with local
correctors and testers, and obtain our main results by applying it to suitably
constructed LCCs and LTCs in the non-standard regime of \emph{sub-constant
relative distance}.
Along the way, we also construct LCCs and LTCs over large alphabets, with the
same query complexity , which additionally have
the property of approaching the Singleton bound: they have almost the
best-possible relationship between their rate and distance. This has the
surprising consequence that asking for a large alphabet error-correcting code
to further be an LCC or LTC with query
complexity does not require any sacrifice in terms of rate and distance! Such a
result was previously not known for any query complexity.
Our results on LCCs also immediately give locally-decodable codes (LDCs) with
the same parameters
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Interplay between motility and cell-substratum adhesion in amoeboid cells
The effective migration of amoeboid cells requires a fine regulation of cell-substratum adhesion. These entwined processes have been shown to be regulated by a host of biophysical and biochemical cues. Here, we reveal the pivotal role played by calcium-based mechanosensation in the active regulation of adhesion resulting in a high migratory adaptability. Using mechanotactically driven Dictyostelium discoideum amoebae, we uncover the existence of optimal mechanosensitive conditions—corresponding to specific levels of extracellular calcium—for persistent directional migration over physicochemically different substrates. When these optimal mechanosensitive conditions are met, noticeable enhancement in cell migration directionality and speed is achieved, yet with significant differences among the different substrates. In the same narrow range of calcium concentrations that yields optimal cellular mechanosensory activity, we uncovered an absolute minimum in cell-substratum adhesion activity, for all considered substrates, with differences in adhesion strength among them amplified. The blocking of the mechanosensitive ion channels with gadolinium—i.e., the inhibition of the primary mechanosensory apparatus—hampers the active reduction in substrate adhesion, thereby leading to the same undifferentiated and drastically reduced directed migratory response. The adaptive behavioral responses of Dictyostelium cells sensitive to substrates with varying physicochemical properties suggest the possibility of novel surface analyses based on the mechanobiological ability of mechanosensitive and guidable cells to probe substrates at the nanometer-to-micrometer level.SUTD-MIT International Design Centre (IDC) (IDG31400104
Undifferentiated human mesenchymal stem cells (hMSCs) are highly sensitive to mechanical strain: transcriptionally controlled early osteo-chondrogenic response in vitro
SummaryObjectivePhysical cues play a crucial role in skeletogenesis and osteochondral regeneration. Although human mesenchymal stem cells (hMSCs) offer considerable therapeutic potential, little is known about the molecular mechanisms that control their differentiation. We hypothesized that mechanical strain might be an inherent stimulus for chondrogenic and/or osteogenic differentiation in undifferentiated hMSCs, where c-Fos (FOS) might play a major role in mechanotransduction.MethodhMSCs from 10 donors were intermittently stimulated by cyclic tensile strain (CTS) at 3000 μstrain for a period of 3 days. Differential gene expression of strained and unstrained hMSCs was analysed by real-time RT-PCR for several marker genes, including the transcription factors FOS, RUNX2, SOX9, and others. Additionally, alkaline phosphatase activity (ALP) was determined kinetically.ResultsThe application of CTS significantly stimulated the expression levels of the early chondrogenic and osteogenic marker genes (SOX9, LUM, DCN; RUNX2, SPARC, SPP1, ALPL); this was accompanied by stimulation of ALP activity (+38%±12 standard error of mean, P<0.05). Matrix analysis revealed that the osteo-chondrogenic response followed a coordinated expression pattern, in which FOS was attributed to early osteogenic but not chondrogenic differentiation.ConclusionUndifferentiated hMSCs are highly sensitive to mechanical strain with a transcriptionally controlled osteo-chondrogenic differentiation response in vitro
The Optimal Single Copy Measurement for the Hidden Subgroup Problem
The optimization of measurements for the state distinction problem has
recently been applied to the theory of quantum algorithms with considerable
successes, including efficient new quantum algorithms for the non-abelian
hidden subgroup problem. Previous work has identified the optimal single copy
measurement for the hidden subgroup problem over abelian groups as well as for
the non-abelian problem in the setting where the subgroups are restricted to be
all conjugate to each other. Here we describe the optimal single copy
measurement for the hidden subgroup problem when all of the subgroups of the
group are given with equal a priori probability. The optimal measurement is
seen to be a hybrid of the two previously discovered single copy optimal
measurements for the hidden subgroup problem.Comment: 8 pages. Error in main proof fixe
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