2,558 research outputs found
Higher Order Corrections to Black Hole Entropy
A scheme for calculating corrections to all orders to the entropy of any
thermodynamic system due to statistical fluctuations around equilibrium has
been developed. It is then applied to the BTZ black hole, AdS-Schwarzschild
black Hole and Schwarzschild black Hole in a cavity. The scheme that we present
is a model-independent scheme and hence universally applicable to all classical
black holes with positive specific heat. It has been seen earlier that the
microcanonical entropy of a system can be more accurately reproduced by
considering a logarithmic correction to the canonical entropy function. The
higher order corrections will be a step further in calculating the
microcanonical entropy of a black hole.Comment: 9 pages, Revised version to appear in Classical and Quantum Gravit
End-to-end Source Separation with Adaptive Front-Ends
Source separation and other audio applications have traditionally relied on
the use of short-time Fourier transforms as a front-end frequency domain
representation step. The unavailability of a neural network equivalent to
forward and inverse transforms hinders the implementation of end-to-end
learning systems for these applications. We present an auto-encoder neural
network that can act as an equivalent to short-time front-end transforms. We
demonstrate the ability of the network to learn optimal, real-valued basis
functions directly from the raw waveform of a signal and further show how it
can be used as an adaptive front-end for supervised source separation. In terms
of separation performance, these transforms significantly outperform their
Fourier counterparts. Finally, we also propose a novel source to distortion
ratio based cost function for end-to-end source separation.Comment: 4 figures, 4 page
Modeling picking on pharmaceutical tablets
Tablets are the most popular solid dosage form in the pharmaceutical industry because they are cheap to manufacture, chemically and mechanically stable and easy to transport and fairly easy to control dosage. Pharmaceutical tableting operations have been around for decades however the process is still not well understood. One of the common problems faced during the production of pharmaceutical tablets by powder compaction is sticking of powder to the punch face, This is known as \u27sticking\u27. A more specialized case of sticking is picking when the powder is pulled away form the compact in the vicinity of debossed features. In the pharmaceutical industry, picking is solved by trial and error which is an expensive, labor intensive and time consuming affair.
The objective of this work was to develop, validate, and implement a modeling framework for predicting picking in powder compacts. The model was developed in Abaqus a commercially available finite element package. The resulting model was used to investigate the influence of debossed feature geometry viz. the stroke angle and degree of pre-pick, and, influence of lubricant on picking. (Abstract shortened by ProQuest.
Bioinformatics Techniques for Studying Drug Resistance In HIV and Staphylococcus Aureus
The worldwide HIV/AIDS pandemic has been partly controlled and treated by antivirals targeting HIV protease, integrase and reverse transcriptase, however, drug resistance has become a serious problem. HIV-1 drug resistance to protease inhibitors evolves by mutations in the PR gene. The resistance mutations can alter protease catalytic activity, inhibitor binding, and stability.
Different machine learning algorithms (restricted boltzmann machines, clustering, etc.) have been shown to be effective machine learning tools for classification of genomic and resistance data. Application of restricted boltzmann machine produced highly accurate and robust classification of HIV protease resistance. They can also be used to compare resistance profiles of different protease inhibitors.
HIV drug resistance has also been studied by enzyme kinetics and X-ray crystallography. Triple mutant HIV-1 protease with resistance mutations V32I, I47V and V82I has been used as a model for the active site of HIV-2 protease. The effects of four investigational antiviral inhibitors was measured for Triple mutant. The tested compounds had significantly worse inhibition of triple mutant with Ki values of 17-40 nM compared to 2-10 pM for wild type protease. The crystal structure of triple mutant in complex with GRL01111 was solved and showed few changes in protease interactions with inhibitor. These new inhibitors are not expected to be effective for HIV-2 protease or HIV-1 protease with changes V32I, I47V and V82I.
Methicillin-resistant Staphylococcus aureus (MRSA) is an opportunistic pathogen that causes hospital and community-acquired infections. Antibiotic resistance occurs because of newly acquired low-affinity penicillin-binding protein (PBP2a). Transcriptome analysis was performed to determine how MuM (mutated PBP2 gene) responds to spermine and how Mu50 (wild type) responds to spermine and spermine–β-lactam synergy. Exogenous spermine and oxacillin were found to alter some significant gene expression patterns with major biochemical pathways (iron, sigB regulon) in MRSA with mutant PBP2 protein
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