Many modern theories predict that the fundamental constants depend on time, position or the local density of matter. Here we develop a spectroscopic method for pulsed beams of cold molecules, and use it to measure the frequencies of microwave transitions in CH with accuracy down to 3 Hz. By comparing these frequencies with those measured from sources of CH in the Milky Way, we test the hypothesis that fundamental constants may differ between the high- and low-density environments of the Earth and the interstellar medium. For the fine structure constant we find Δα/α=(0.3±1.1) × 10−7, the strongest limit to date on such a variation of α. For the electron-to-proton mass ratio we find Δμ/μ=(−0.7±2.2) × 10−7. We suggest how dedicated astrophysical measurements can improve these constraints further and can also constrain temporal variation of the constants.
SUMMARY:There is increasing evidence that antiproteases are able to affect the inflammatory response. To further examine this question, we administered human ␣-1-antitrypsin (␣1AT) or a synthetic metalloprotease inhibitor (RS113456) to C57 mice followed by a single intratracheal dose of quartz, a dust that evokes a marked, lasting, polymorphonuclear leukocyte (PMN) infiltrate. At 2 hours after dust administration, both antiproteases completely suppressed silica-induced PMN influx into the lung and macrophage inflammatory protein-2 (MIP-2)/monocyte chemotactic protein-1 (MCP-1) (neutrophil/macrophage chemoattractant) gene expression, partially suppressed nuclear transcription factor B (NF-B) translocation, and increased inhibitor of NF-B (IB) levels. By 24 hours, PMN influx and connective tissue breakdown measured as lavage desmosine or hydroxyproline were still at, or close to, control levels after antiprotease treatment, and increases in NF-B translocation and MIP-2/MCP-1 gene expression were variably suppressed. At both time points, neither agent prevented silica-induced increases in amount of whole lung MIP-2 or MCP-1 protein, but both did prevent increases in whole lung intercellular adhesion molecule-1 (ICAM-1) at 24 hours. Inactivating the ␣1AT by oxidation to the point that it no longer possessed antiproteolytic properties did not affect its ability to suppress inflammation. Both antiproteases also prevented the silica-induced acute inflammatory response in mice with knocked out genes for macrophage metalloelastase (MME Ϫ/Ϫ), mice that develop inflammation, but not connective tissue breakdown, and the pattern of ␣1AT breakdown fragments was identical in control and MME Ϫ/Ϫ animals. These findings suggest that, in this model of acute PMN mediated inflammation, a serine protease inhibitor and a metalloprotease inhibitor have similar anti-inflammatory properties, that inflammation is not mediated by proteolysis with generation of chemotactic matrix fragments, and that classic antiproteolysis (complexing of protease to antiprotease) probably does not play a role in suppression of inflammation. The antiproteolytic effects of these agents do not seem to be mediated by protection of endogenous ␣1AT. (Lab Invest 2001, 81:1119 -1131.
Abstract. We demonstrate the implementation of a spin qubit with a single 40 Ca + ion in a micro ion trap. The qubit is encoded in the Zeeman ground state levels m J = +1/2 and m J = −1/2 of the S 1/2 state of the ion. We show sideband cooling close to the vibrational ground state and demonstrate the initialization and readout of the qubit levels with 99.5% efficiency. We employ a Raman transition close to the S 1/2 -P 1/2 resonance for coherent manipulation of the qubit. We observe single qubit rotations with 96% fidelity and gate times below 5µs. Rabi oscillations on the blue motional sideband are used to extract the phonon number distribution. The dynamics of this distribution is analyzed to deduce the trap-induced heating rate of 0.3(1) phonons/ms.
Experiments with cold molecules usually begin with a molecular source. We describe the construction and characteristics of a cryogenic buffer gas source of CaF molecules. The source emits pulses with a typical duration of 240 µs, a mean speed of about 150 m/s, and a flux of 5 × 10 10 molecules per steradian per pulse in a single rotational state. ARTICLE HISTORY
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