234,672 research outputs found
Mining Brain Networks using Multiple Side Views for Neurological Disorder Identification
Mining discriminative subgraph patterns from graph data has attracted great
interest in recent years. It has a wide variety of applications in disease
diagnosis, neuroimaging, etc. Most research on subgraph mining focuses on the
graph representation alone. However, in many real-world applications, the side
information is available along with the graph data. For example, for
neurological disorder identification, in addition to the brain networks derived
from neuroimaging data, hundreds of clinical, immunologic, serologic and
cognitive measures may also be documented for each subject. These measures
compose multiple side views encoding a tremendous amount of supplemental
information for diagnostic purposes, yet are often ignored. In this paper, we
study the problem of discriminative subgraph selection using multiple side
views and propose a novel solution to find an optimal set of subgraph features
for graph classification by exploring a plurality of side views. We derive a
feature evaluation criterion, named gSide, to estimate the usefulness of
subgraph patterns based upon side views. Then we develop a branch-and-bound
algorithm, called gMSV, to efficiently search for optimal subgraph features by
integrating the subgraph mining process and the procedure of discriminative
feature selection. Empirical studies on graph classification tasks for
neurological disorders using brain networks demonstrate that subgraph patterns
selected by the multi-side-view guided subgraph selection approach can
effectively boost graph classification performances and are relevant to disease
diagnosis.Comment: in Proceedings of IEEE International Conference on Data Mining (ICDM)
201
A Pattern Language for High-Performance Computing Resilience
High-performance computing systems (HPC) provide powerful capabilities for
modeling, simulation, and data analytics for a broad class of computational
problems. They enable extreme performance of the order of quadrillion
floating-point arithmetic calculations per second by aggregating the power of
millions of compute, memory, networking and storage components. With the
rapidly growing scale and complexity of HPC systems for achieving even greater
performance, ensuring their reliable operation in the face of system
degradations and failures is a critical challenge. System fault events often
lead the scientific applications to produce incorrect results, or may even
cause their untimely termination. The sheer number of components in modern
extreme-scale HPC systems and the complex interactions and dependencies among
the hardware and software components, the applications, and the physical
environment makes the design of practical solutions that support fault
resilience a complex undertaking. To manage this complexity, we developed a
methodology for designing HPC resilience solutions using design patterns. We
codified the well-known techniques for handling faults, errors and failures
that have been devised, applied and improved upon over the past three decades
in the form of design patterns. In this paper, we present a pattern language to
enable a structured approach to the development of HPC resilience solutions.
The pattern language reveals the relations among the resilience patterns and
provides the means to explore alternative techniques for handling a specific
fault model that may have different efficiency and complexity characteristics.
Using the pattern language enables the design and implementation of
comprehensive resilience solutions as a set of interconnected resilience
patterns that can be instantiated across layers of the system stack.Comment: Proceedings of the 22nd European Conference on Pattern Languages of
Program
Mining Representative Unsubstituted Graph Patterns Using Prior Similarity Matrix
One of the most powerful techniques to study protein structures is to look
for recurrent fragments (also called substructures or spatial motifs), then use
them as patterns to characterize the proteins under study. An emergent trend
consists in parsing proteins three-dimensional (3D) structures into graphs of
amino acids. Hence, the search of recurrent spatial motifs is formulated as a
process of frequent subgraph discovery where each subgraph represents a spatial
motif. In this scope, several efficient approaches for frequent subgraph
discovery have been proposed in the literature. However, the set of discovered
frequent subgraphs is too large to be efficiently analyzed and explored in any
further process. In this paper, we propose a novel pattern selection approach
that shrinks the large number of discovered frequent subgraphs by selecting the
representative ones. Existing pattern selection approaches do not exploit the
domain knowledge. Yet, in our approach we incorporate the evolutionary
information of amino acids defined in the substitution matrices in order to
select the representative subgraphs. We show the effectiveness of our approach
on a number of real datasets. The results issued from our experiments show that
our approach is able to considerably decrease the number of motifs while
enhancing their interestingness
A convolutional autoencoder approach for mining features in cellular electron cryo-tomograms and weakly supervised coarse segmentation
Cellular electron cryo-tomography enables the 3D visualization of cellular
organization in the near-native state and at submolecular resolution. However,
the contents of cellular tomograms are often complex, making it difficult to
automatically isolate different in situ cellular components. In this paper, we
propose a convolutional autoencoder-based unsupervised approach to provide a
coarse grouping of 3D small subvolumes extracted from tomograms. We demonstrate
that the autoencoder can be used for efficient and coarse characterization of
features of macromolecular complexes and surfaces, such as membranes. In
addition, the autoencoder can be used to detect non-cellular features related
to sample preparation and data collection, such as carbon edges from the grid
and tomogram boundaries. The autoencoder is also able to detect patterns that
may indicate spatial interactions between cellular components. Furthermore, we
demonstrate that our autoencoder can be used for weakly supervised semantic
segmentation of cellular components, requiring a very small amount of manual
annotation.Comment: Accepted by Journal of Structural Biolog
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