5,874 research outputs found
Atom interferometry in the presence of an external test mass
The influence of an external test mass on the phase of the signal of an atom
interferometer is studied theoretically. Using traditional techniques in atom
optics based on the density matrix equations in the Wigner representation, we
are able to extract the various contributions to the phase of the signal
associated with the classical motion of the atoms, the quantum correction to
this motion resulting from atomic recoil that is produced when the atoms
interact with Raman field pulses, and quantum corrections to the atomic motion
that occur in the time between the Raman field pulses. By increasing the
effective wave vector associated with the Raman field pulses using modified
field parameters, we can increase the sensitivity of the signal to the point
where the quantum corrections can be measured. The expressions that are derived
can be evaluated numerically to isolate the contribution to the signal from an
external test mass. The regions of validity of the exact and approximate
expressions are determined.Comment: 23 pages, 3 figures, 2 table
Landau equations and asymptotic operation
The pinched/non-pinched classification of intersections of causal
singularities of propagators in Minkowski space is reconsidered in the context
of the theory of asymptotic operation as a first step towards extension of the
latter to non-Euclidean asymptotic regimes. A highly visual
distribution-theoretic technique of singular wave fronts is tailored to the
needs of the theory of Feynman diagrams. Besides a simple derivation of the
usual Landau equations in the case of the conventional singularities, the
technique naturally extends to other types of singularities e.g. due to linear
denominators in non-covariant gauges etc. As another application, the results
of Euclidean asymptotic operation are extended to a class of quasi-Euclidean
asymptotic regimes in Minkowski space.Comment: 15p PS (GSview), IJMP-A (accepted
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Immune interferon inhibits proliferation and induces 2'-5'-oligoadenylate synthetase gene expression in human vascular smooth muscle cells.
Proliferation of vascular smooth muscle cells (SMC) contributes to formation of the complicated human atherosclerotic plaque. These lesions also contain macrophages, known to secrete SMC mitogens, and T lymphocytes. Many of the SMC in the lesions express class II major histocompatibility antigens, an indication that activated T cells secrete immune IFN-gamma locally in the plaque. We therefore studied the effect of IFN-gamma on the proliferation of cultured SMC derived from adult human blood vessels. IFN-gamma (1,000 U/ml) reduced [3H]thymidine (TdR) incorporation into DNA by SMC stimulated with the well-defined mitogens IL 1 (from 15.3 +/- 0.7 to 6.2 +/- 0.7 dpm X 10(-3)/24 h) or platelet-derived growth factor (PDGF) (from 18.5 +/- 1.0 to 7.3 +/- 0.7 dpm X 10(-3)/24 h). Kinetic and nuclear labeling studies indicated that this effect of IFN-gamma was not due to altered thymidine transport or specific radioactivity of TdR in the cell. In longer term experiments (4-16 d) IFN-gamma prevented net DNA accumulation by SMC cultures stimulated by PDGF. IFN-gamma also delayed (from 30 to 60 min) the time to peak level of c-fos RNA in IL 1-treated SMC. It is unlikely that cytotoxicity caused these effects of IFN-gamma, as the inhibition of growth was reversible and we detected no cell death in SMC cultures exposed to this cytokine. Activation of 2'-5' oligoadenylate synthetase gene expression may mediate certain antiproliferative and antiviral effects of interferons. Both IFN-gamma and type I IFNs (IFN-alpha or IFN-beta) induced 2'-5' oligoadenylate synthetase mRNA and enzyme activity in SMC cultures, but with concentration dependence and time course that may not account for all of IFN-gamma's cytostatic effect on SMC. The accumulation of SMC in human atherosclerotic lesions is a long-term process that must involve altered balance between growth stimulatory and inhibitory factors. The cytostatic effect of IFN-gamma on human SMC demonstrated here may influence this balance during human atherogenesis, because T cells present in the complicated atherosclerotic plaque likely produce this cytokine
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Interleukin 1: a mitogen for human vascular smooth muscle cells that induces the release of growth-inhibitory prostanoids.
There is much interest in defining the signals that initiate abnormal proliferation of cells in a variety of states characterized by the presence of mononuclear phagocytes. Since IL-1 is a major secretory product of activated human monocytes we examined whether this cytokine can stimulate the growth of human vascular smooth muscle cells (SMC). Neither recombinant IL-1 (rIL-1) alpha (less than or equal to 5.0 ng/ml) nor beta (less than or equal to 100 ng/ml) stimulated SMC growth during 2-d incubations under usual conditions. IL-1 did stimulate SMC to produce prostanoids such as PGE1 or PGE2 that can inhibit SMC proliferation. When prostaglandin synthesis was inhibited by indomethacin or aspirin both rIL-1 alpha and beta (greater than or equal to 1 ng/ml) markedly increased SMC growth. In longer-term experiments (7-28 d) rIL-1 stimulated the growth of SMC even in the absence of cyclooxygenase inhibitors. The addition of exogenous PGE1 or PGE2 (but not PGF1 alpha, PGF2 alpha, PGI2) to indomethacin-treated SMC blocked their mitogenic response to rIL-1. Antibody to IL-1 (but not to platelet-derived growth factor [PDGF]) abolished the mitogenic response of SMC to rIL-1. Exposure of SMC to rIL-1 or PDGF caused rapid (maximal at 1 h) and transient (baseline by 3 h) expression of the c-fos proto-oncogene, determined by Northern analysis. We conclude that IL-1 is a potent mitogen for human SMC. Endogenous prostanoid production simultaneously induced by IL-1 appears to antagonize this growth-promoting effect in the short term (2 d) but not during more prolonged exposures. IL-1 produced by activated monocytes at sites of tissue inflammation or injury may thus mediate both positive and negative effects on SMC proliferation that are temporally distinct
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Stellar Astrophysics and a Fundamental Description of Thermonuclear Reactions ? 04-ERD-058 Final Report
Report on the progress achieved in 04-ERD-058. The primary goal of the project was to investigate new methods to provide a comprehensive understanding of how reactions between light nuclei proceed in hot, dense environments, such as stellar interiors. The project sought to develop an entirely new theoretical framework to describe the dynamics of nuclear collisions based on the fundamental nuclear interactions. Based on the new theoretical framework, new computational tools were developed to address specific questions in nuclear structure and reactions. A full study of the true nature of the three-nucleon interaction was undertaken within the formalism of effective field theory. We undertook a preliminary theoretical study of the quantum corrections to electron screening in thermal plasmas to resolve a discrepancy exhibited in previous theoretical approaches
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