409 research outputs found
Stimulated Raman Adiabatic Passage (STIRAP) Among Degenerate-Level Manifolds
We examine the conditions needed to accomplish stimulated Raman adiabatic
passage (STIRAP) when the three levels (g, e and f) are degenerate, with
arbitrary couplings contributing to the pump-pulse interaction (g - e) and to
the Stokes-pulse interaction (e-f). We show that in general a sufficient
condition for complete population removal from the g set of degenerate states
for arbitrary, pure or mixed, initial state is that the degeneracies should not
decrease along the sequence g, e and f. We show that when this condition holds
it is possible to achieve the degenerate counterpart of conventional STIRAP,
whereby adiabatic passage produces complete population transfer. Indeed, the
system is equivalent to a set of independent three-state systems, in each of
which a STIRAP procedure can be implemented. We describe a scheme of unitary
transformations that produces this result. We also examine the cases when this
degeneracy constraint does not hold, and show what can be accomplished in those
cases. For example, for angular momentum states when the degeneracy of the g
and f levels is less than that of the e level we show how a special choice for
the pulse polarizations and phases can produce complete removal of population
from the g set. Our scheme can be a powerful tool for coherent control in
degenerate systems, because of its robustness when selective addressing of the
states is not required or impossible. We illustrate the analysis with several
analytically solvable examples, in which the degeneracies originate from
angular momentum orientation, as expressed by magnetic sublevels.Comment: 21 pages, 17 figure
UV-Induced Structural Changes of Model DNA Helices Probed by Optical Spectroscopy
International audienceChemical alterations of DNA, if not repaired, may lead to carcinogenic mutations. Structural modifications of the helix around the lesion enable its recognition by repair enzymes. We have used absorption spectroscopy and mass spectrometry to detect structural changes provoked by cyclobutane thymine dimers, the major lesion induced by UV radiation. We found that formation of a cyclobutane dimer in the model duplex (dA)20 · (dT)20 destroys base stacking on the adenine strand. The physical background of this novel approach is the existence of charge-transfer states among neighboring bases, whose contribution to the hypochromism of the helix disappears following destacking
UVA-induced cyclobutane pyrimidine dimers in DNA: a direct photochemical mechanism?
International audienceThe carcinogenic action of UVA radiation is commonly attributed to DNA oxidation mediated by endogenous photosensitisers. Yet, it was recently shown that cyclobutane pyrimidine dimers (CPD), well known for their involvement in UVB genotoxicity, are produced in larger yield than oxidative lesions in UVA-irradiated cells and skin. In the present work, we gathered mechanistic information on this photoreaction by comparing formation of all possible bipyrimidine photoproducts upon UVA irradiation of cells, purified genomic DNA and dA20:dT20 oligonucleotide duplex. We observed that the distribution of photoproducts, characterized by the sole formation of CPD and the absence of (6-4) photoproducts was similar in the three types of samples. The CPD involving two thymines represented 90% of the amount of photoproducts. Moreover, the yields of formation of the DNA lesions were similar in cells and isolated DNA. In addition, the effect of the wavelength of the incident photons was found to be the same in isolated DNA and cells. This set of data shows that UVA-induced cyclobutane pyrimidine dimers are formed via a direct photochemical mechanism, without mediation of a cellular photosensitiser. This is possible because the double-stranded structure increases the capacity of DNA bases to absorb UVA photons, as evidenced in the case of the oligomer dA20:dT20. These results emphasize the need to consider UVA in the carcinogenic effects of sunlight. An efficient photoprotection is needed that can only be complete by completely blocking incident photons, rather than by systemic approaches such as antioxidant supplementation
Competitive stochastic noises in coherently driven two-level atoms and quantum interference
A system of coherently-driven two-level atoms is analyzed in presence of two
independent stochastic perturbations: one due to collisions and a second one
due to phase fluctuations of the driving field. The behaviour of the quantum
interference induced by the collisional noise is considered in detail. The
quantum-trajectory method is utilized to reveal the phase correlations between
the dressed states involved in the interfering transition channels. It is shown
that the quantum interference induced by the collisional noise is remarkably
robust against phase noise. This effect is due to the fact that the phase
noise, similarly to collisions, stabilizes the phase-difference between the
dressed states.Comment: accepted for publication in J. Opt.
The Infrared Array Camera (IRAC) for the Spitzer Space Telescope
The Infrared Array Camera (IRAC) is one of three focal plane instruments in
the Spitzer Space Telescope. IRAC is a four-channel camera that obtains
simultaneous broad-band images at 3.6, 4.5, 5.8, and 8.0 microns. Two nearly
adjacent 5.2x5.2 arcmin fields of view in the focal plane are viewed by the
four channels in pairs (3.6 and 5.8 microns; 4.5 and 8 microns). All four
detector arrays in the camera are 256x256 pixels in size, with the two shorter
wavelength channels using InSb and the two longer wavelength channels using
Si:As IBC detectors. IRAC is a powerful survey instrument because of its high
sensitivity, large field of view, and four-color imaging. This paper summarizes
the in-flight scientific, technical, and operational performance of IRAC.Comment: 7 pages, 3 figures. Accepted for publication in the ApJS. A higher
resolution version is at http://cfa-www.harvard.edu/irac/publication
The NASA X-Ray Mission Concepts Study
The 2010 Astrophysics Decadal Survey recommended a significant technology development program towards realizing the scientific goals of the International X-ray Observatory (IXO). NASA has undertaken an X-ray mission concepts study to determine alternative approaches to accomplishing IXO's high ranking scientific objectives over the next decade given the budget realities, which make a flagship mission challenging to implement. The goal of the study is to determine the degree to which missions in various cost ranges from 2B could fulfill these objectives. The study process involved several steps. NASA released a Request for Information in October 2011, seeking mission concepts and enabling technology ideas from the community. The responses included a total of 14 mission concepts and 13 enabling technologies. NASA also solicited membership for and selected a Community Science Team (CST) to guide the process. A workshop was held in December 2011 in which the mission concepts and technology were presented and discussed. Based on the RFI responses and the workshop, the CST then chose a small group of notional mission concepts, representing a range of cost points, for further study. These notional missions concepts were developed through mission design laboratory activities in early 2012. The results of all these activities were captured in the final X-ray mission concepts study report, submitted to NASA in July 2012. In this presentation, we summarize the outcome of the study. We discuss background, methodology, the notional missions, and the conclusions of the study report
Dystrophin expression in muscle following gene transfer with a fully deleted ("Gutted") adenovirus is markedly improved by Trans-acting adenoviral gene products
Helper-dependent adenoviruses (HDAd) are Ad vectors lacking all or most viral genes. They hold great promise for gene therapy of diseases such as Duchenne muscular dystrophy (DMD), because they are less immunogenic than E1/E3-deleted Ad (first-generation Ad or FGAd) and can carry the full-length (Fl) dystrophin (dys) cDNA (12 kb). We have compared the transgene expression of a HDAd (HDAdCMVDysFl) and a FGAd (FGAdCMV-dys) in cell culture (HeLa, C2C12 myotubes) and in the muscle of mdx mice (the mouse model for DMD). Both vectors encoded dystrophin regulated by the same cytomegalovirus (CMV) promoter. We demonstrate that the amount of dystrophin expressed was significantly higher after gene transfer with FGAdCMV-dys compared to HDAdCMVDysFl both in vitro and in vivo. However, gene transfer with HDAdCMVDysFl in the presence of a FGAd resulted in a significant increase of dystrophin expression indicating that gene products synthesized by the FGAd increase, in trans, the amount of dystrophin produced. This enhancement occurred in cell culture and after gene transfer in the muscle of mdx mice and dystrophic golden retriever (GRMD) dogs, another animal model for DMD. The E4 region of Ad is required for the enhancement, because no increase of dystrophin expression from HDAdCMVDysFl was observed in the presence of an E1/E4-deleted Ad in vitro and in vivo. The characterization of these enhancing gene products followed by their inclusion into an HDAd may be required to produce sufficient dystrophin to mitigate the pathology of DMD by HDAd-mediated gene transfer
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