220 research outputs found
Gaseous Electronics
Contains reports on two research projects.Joint Services Electronics Programs (U. S. Army, U. S. Navy, and U. S. Air Force) under Contract DA 28-043-AMC-02536(E
Plasmas and Controlled Nuclear Fusion
Contains reports on three research projects.U. S. Atomic Energy Commission (Contract AT(30-1)-3980
Applied Plasma Research
Contains reports on three research projects.National Science Foundation (Grant GK-18185)M. I. T. Lincoln Laboratory Purchase Order No. CC-55
Removing Orbital Debris with Lasers
Orbital debris in low Earth orbit (LEO) are now sufficiently dense that the
use of LEO space is threatened by runaway collisional cascading. A problem
predicted more than thirty years ago, the threat from debris larger than about
1 cm demands serious attention. A promising proposed solution uses a high power
pulsed laser system on the Earth to make plasma jets on the objects, slowing
them slightly, and causing them to re-enter and burn up in the atmosphere. In
this paper, we reassess this approach in light of recent advances in low-cost,
light-weight modular design for large mirrors, calculations of laser-induced
orbit changes and in design of repetitive, multi-kilojoule lasers, that build
on inertial fusion research. These advances now suggest that laser orbital
debris removal (LODR) is the most cost-effective way to mitigate the debris
problem. No other solutions have been proposed that address the whole problem
of large and small debris. A LODR system will have multiple uses beyond debris
removal. International cooperation will be essential for building and operating
such a system.Comment: 37 pages, 15 figures, in preparation for submission to Advances in
Space Researc
GISTIC2.0 facilitates sensitive and confident localization of the targets of focal somatic copy-number alteration in human cancers
We describe methods with enhanced power and specificity to identify genes targeted by somatic copy-number alterations (SCNAs) that drive cancer growth. By separating SCNA profiles into underlying arm-level and focal alterations, we improve the estimation of background rates for each category. We additionally describe a probabilistic method for defining the boundaries of selected-for SCNA regions with user-defined confidence. Here we detail this revised computational approach, GISTIC2.0, and validate its performance in real and simulated datasets
Consistency-based detection of potential tumor-specific deletions in matched normal/tumor genomes
Wittler R, Chauve C. Consistency-based detection of potential tumor-specific deletions in matched normal/tumor genomes. BMC Bioinformatics. 2011;12(Suppl. 9):S21
Near-infrared camera for the Clementine mission
The Clementine mission provided the first ever complete, systematic surface mapping of the moon from the ultra-violet to the near-infrared regions. More than 1.7 million images of the moon, earth and space were returned from this mission. The near-infrared (NIR) multi-spectral camera, one of two workhorse lunar mapping cameras (the other being the UV/visible camera), provided {approximately}200 in spatial resolution at 400 km periselene, and a 39 km across-track swath. This 1.9 kg infrared camera using a 256 x 256 InSb FPA viewed reflected solar illumination from the lunar surface and lunar horizon in the 1 to 3 {micro}m wavelength region, extending lunar imagery and mineralogy studies into the near infrared. A description of this light-weight, low power NIR camera along with a summary of lessons learned is presented. Design goals and preliminary on-orbit performance estimates are addressed in terms of meeting the mission`s primary objective for flight qualifying the sensors for future Department of Defense flights
Translational Database Selection and Multiplexed Sequence Capture for Up Front Filtering of Reliable Breast Cancer Biomarker Candidates
Biomarker identification is of utmost importance for the development of novel diagnostics and therapeutics. Here we make use of a translational database selection strategy, utilizing data from the Human Protein Atlas (HPA) on differentially expressed protein patterns in healthy and breast cancer tissues as a means to filter out potential biomarkers for underlying genetic causatives of the disease. DNA was isolated from ten breast cancer biopsies, and the protein coding and flanking non-coding genomic regions corresponding to the selected proteins were extracted in a multiplexed format from the samples using a single DNA sequence capture array. Deep sequencing revealed an even enrichment of the multiplexed samples and a great variation of genetic alterations in the tumors of the sampled individuals. Benefiting from the upstream filtering method, the final set of biomarker candidates could be completely verified through bidirectional Sanger sequencing, revealing a 40 percent false positive rate despite high read coverage. Of the variants encountered in translated regions, nine novel non-synonymous variations were identified and verified, two of which were present in more than one of the ten tumor samples
cisRED: a database system for genome-scale computational discovery of regulatory elements
We describe cisRED, a database for conserved regulatory elements that are identified and ranked by a genome-scale computational system (). The database and high-throughput predictive pipeline are designed to address diverse target genomes in the context of rapidly evolving data resources and tools. Motifs are predicted in promoter regions using multiple discovery methods applied to sequence sets that include corresponding sequence regions from vertebrates. We estimate motif significance by applying discovery and post-processing methods to randomized sequence sets that are adaptively derived from target sequence sets, retain motifs with p-values below a threshold and identify groups of similar motifs and co-occurring motif patterns. The database offers information on atomic motifs, motif groups and patterns. It is web-accessible, and can be queried directly, downloaded or installed locally
Cloning and characterization of a novel alternatively spliced transcript of the human CHD7 putative helicase
<p>Abstract</p> <p>Background</p> <p>The <it>CHD7 </it>(Chromodomain Helicase DNA binding protein 7) gene encodes a member of the chromodomain family of ATP-dependent chromatin remodeling enzymes. Mutations in the <it>CHD7 </it>gene are found in individuals with CHARGE, a syndrome characterized by multiple birth malformations in several tissues. CHD7 was identified as a binding partner of PBAF complex (Polybromo and BRG Associated Factor containing complex) playing a central role in the transcriptional reprogramming process associated to the formation of multipotent migratory neural crest, a transient cell population associated with the genesis of various tissues. <it>CHD7 </it>is a large gene containing 38 annotated exons and spanning 200 kb of genomic sequence. Although genes containing such number of exons are expected to have several alternative transcripts, there are very few evidences of alternative transcripts associated to <it>CHD7 </it>to date indicating that alternative splicing associated to this gene is poorly characterized.</p> <p>Findings</p> <p>Here, we report the cloning and characterization by experimental and computational studies of a novel alternative transcript of the human <it>CHD7 </it>(named CHD7 CRA_e), which lacks most of its coding exons. We confirmed by overexpression of CHD7 CRA_e alternative transcript that it is translated into a protein isoform lacking most of the domains displayed by the canonical isoform. Expression of the CHD7 CRA_e transcript was detected in normal liver, in addition to the DU145 human prostate carcinoma cell line from which it was originally isolated.</p> <p>Conclusions</p> <p>Our findings indicate that the splicing event associated to the CHD7 CRA_e alternative transcript is functional. The characterization of the CHD7 CRA_e novel isoform presented here not only sets the basis for more detailed functional studies of this isoform, but, also, contributes to the alternative splicing annotation of the <it>CHD7 </it>gene and the design of future functional studies aimed at the elucidation of the molecular functions of its gene products.</p
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