449,505 research outputs found
On the rate of convergence to stationarity of the M/M/N queue in the Halfin-Whitt regime
We prove several results about the rate of convergence to stationarity, that
is, the spectral gap, for the M/M/n queue in the Halfin-Whitt regime. We
identify the limiting rate of convergence to steady-state, and discover an
asymptotic phase transition that occurs w.r.t. this rate. In particular, we
demonstrate the existence of a constant s.t. when a certain
excess parameter , the error in the steady-state approximation
converges exponentially fast to zero at rate . For , the
error in the steady-state approximation converges exponentially fast to zero at
a different rate, which is the solution to an explicit equation given in terms
of special functions. This result may be interpreted as an asymptotic version
of a phase transition proven to occur for any fixed n by van Doorn [Stochastic
Monotonicity and Queueing Applications of Birth-death Processes (1981)
Springer]. We also prove explicit bounds on the distance to stationarity for
the M/M/n queue in the Halfin-Whitt regime, when . Our bounds scale
independently of in the Halfin-Whitt regime, and do not follow from the
weak-convergence theory.Comment: Published in at http://dx.doi.org/10.1214/12-AAP889 the Annals of
Applied Probability (http://www.imstat.org/aap/) by the Institute of
Mathematical Statistics (http://www.imstat.org
High levels of cyclic di-GMP in Klebsiella pneumoniae attenuate virulence in the lung
ABSTRACT
The bacterial second messenger bis-(3′-5′)-cyclic dimeric GMP (c-di-GMP) has been shown to influence the expression of virulence factors in certain pathogenic bacteria, but little is known about its activity in the increasingly antibiotic-resistant pathogen
Klebsiella pneumoniae
. Here, the expression in
K. pneumoniae
of a heterologous diguanylate cyclase increased the bacterial c-di-GMP concentration and attenuated pathogenesis in murine pneumonia. This attenuation remained evident in mice lacking the c-di-GMP sensor STING, indicating that the high c-di-GMP concentration exerted its influence not on host responses but on bacterial physiology. While serum resistance and capsule expression were unaffected by the increased c-di-GMP concentration, both type 3 and type 1 pili were strongly upregulated. Importantly, attenuation of
K. pneumoniae
virulence by high c-di-GMP levels was abrogated when type 1 pilus expression was silenced. We conclude that increased type 1 piliation may hamper
K. pneumoniae
virulence in the respiratory tract and that c-di-GMP signaling represents a potential therapeutic target for antibiotic-resistant
K. pneumoniae
in this niche.
</jats:p
Comment on "Superinstantons and the Reliability of Perturbation Theory in Non-Abelian Models"
In a recent letter (hep-lat/9311019) A. Patrascioiu and E. Seiler argued that
when taking into account "superinstantons configurations" the perturbative
expansion and the beta-function of the two-dimensional non-linear sigma-model
are modified at two loops order. I point out that: (1) perturbation theory in a
superinstanton background is infra-red singular beyond three loops; (2) the new
infra-red singular terms, which change the two loop terms, come from singular
operators - describing superinstanton insertions - in the OPE; (3) taking into
account these operators, the beta-function is not modified. Therefore the
results of Patrascioiu and Seiler do not contradict perturbation theory.Comment: 1 page, REVTeX, no figure
A Critical Examination of the FDA’s Efforts to Preempt Failure-to-Warn Claims
This article explores the legality and wisdom of the FDA’s effort to persuade courts to find most failure-to-warn claims preempted. The article first analyzes the FDA’s justifications for reversing its long-held views to the contrary and explains why the FDA’s position cannot be reconciled with its governing statute. The article then examines why the FDA’s position, if ultimately adopted by the courts, would undermine the incentives drug manufacturers have to change labeling to respond to newly-discovered risks. The background possibility of failure-to-warn litigation provides important incentives for drug companies to ensure that drug labels reflect accurate and up-to-date safety information. The article next explains why the agency’s view that it is capable of singlehandedly regulating the safety of drugs is unrealistic. The agency does not have the resources to perform the Herculean task of monitoring the performance of every drug on the market. Both the Institute of Medicine and the Government Accountability Office have explained the shortcomings in the FDA’s recent performance, and they express doubt that the FDA is in capable of facing an increasingly challenging future.
The article then explains how state damages litigation helps uncover and assess risks that are not apparent to the agency during a drug’s approval process, and why this “feedback loop” enables the agency to better do its job. FDA approval of drugs is based on clinical trials that involve, at most, a few thousand patients and last a year or so. These trials cannot detect risks that are relatively rare, affect vulnerable sub-populations, or have long latency periods. For this reason, most serious adverse effects do not become evident until a drug is used in larger population groups for periods in excess of one year. Time and again, failure-to-warn litigation has brought to light information that would not otherwise be available to the FDA, to doctors, to other health care providers, and to consumers. And failure-to-warn litigation often has preceded and clearly influenced FDA decisions to modify labeling, and, at times, to withdraw drugs from the market
Extended Laguerre inequalities and a criterion for real zeros
Let where and is a real entire
function of genus 0 or 1. We give a necessary and sufficient condition in terms
of a sequence of inequalities for all of the zeros of to be real. These
inequalities are an extension of the classical Laguerre inequalities.Comment: The paper is based on a talk given at the 7th ISAAC Congress held at
Imperial College in London in July 200
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