43,411 research outputs found
Quantum degenerate dipolar Fermi gas
The interplay between crystallinity and superfluidity is of great fundamental
and technological interest in condensed matter settings. In particular,
electronic quantum liquid crystallinity arises in the non-Fermi liquid,
pseudogap regime neighboring a cuprate's unconventional superconducting phase.
While the techniques of ultracold atomic physics and quantum optics have
enabled explorations of the strongly correlated, many-body physics inherent in,
e.g., the Hubbard model, lacking has been the ability to create a quantum
degenerate Fermi gas with interparticle interactions---such as the strong
dipole-dipole interaction---capable of inducing analogs to electronic quantum
liquid crystals. We report the first quantum degenerate dipolar Fermi gas, the
realization of which opens a new frontier for exploring strongly correlated
physics and, in particular, the quantum melting of smectics in the pristine
environment provided by the ultracold atomic physics setting. A quantum
degenerate Fermi gas of the most magnetic atom 161Dy is produced by laser
cooling to 10 uK before sympathetically cooling with ultracold, bosonic 162Dy.
The temperature of the spin-polarized 161Dy is a factor T/TF=0.2 below the
Fermi temperature TF=300 nK. The co-trapped 162Dy concomitantly cools to
approximately Tc for Bose-Einstein condensation, thus realizing a novel, nearly
quantum degenerate dipolar Bose-Fermi gas mixture.Comment: 6 pages, 3 figure
Scalable Text and Link Analysis with Mixed-Topic Link Models
Many data sets contain rich information about objects, as well as pairwise
relations between them. For instance, in networks of websites, scientific
papers, and other documents, each node has content consisting of a collection
of words, as well as hyperlinks or citations to other nodes. In order to
perform inference on such data sets, and make predictions and recommendations,
it is useful to have models that are able to capture the processes which
generate the text at each node and the links between them. In this paper, we
combine classic ideas in topic modeling with a variant of the mixed-membership
block model recently developed in the statistical physics community. The
resulting model has the advantage that its parameters, including the mixture of
topics of each document and the resulting overlapping communities, can be
inferred with a simple and scalable expectation-maximization algorithm. We test
our model on three data sets, performing unsupervised topic classification and
link prediction. For both tasks, our model outperforms several existing
state-of-the-art methods, achieving higher accuracy with significantly less
computation, analyzing a data set with 1.3 million words and 44 thousand links
in a few minutes.Comment: 11 pages, 4 figure
Transfer-matrix renormalization group study of the spin ladders with cyclic four-spin interactions
The temperature dependence of the specific heat and spin susceptibility of
the spin ladders with cyclic four-spin interactions in the rung-singlet phase
is explored by making use of the transfer-matrix renormalization group method.
The values of spin gap are extracted from the specific heat and susceptibility,
respectively. It is found that for different relative strength between
interchain and intrachain interactions, the spin gap is approximately linear
with the cyclic four-spin interaction in the region far away from the critical
point. Furthermore, we show that the dispersion for the one-triplet magnon
branch can be obtained by numerically fitting on the partition function.Comment: 7 pages, 7 figures, 1 tabl
Donor hematopoietic progenitor cells in nonmyeloablated rat recipients of allogeneic bone marrow and liver grafts
Background. Although the persistence of multilineage microchimerism in recipients of long-surviving organ transplants implies engraftment of migratory pluripotent donor stem cells, the ultimate localization in the recipient of these cells has not been determined in any species. Methods. Progenitor cells were demonstrated in the bone marrow and nonparenchymal liver cells of naive rats and in Brown Norway (BN) recipients of Lewis (LEW) allografts by semiquantitative colony-forming unit in culture (CFU-C) assays. The LEW allografts of bone marrow cells (BMC) (2.5xl08), orthotopic livers, or heterotopic hearts (abdominal site) were transplanted under a 2-week course of daily tacrolimus, with additional single doses on days 20 and 27. Donor CFU-C colonies were distinguished from recipient colonies in the allografts and recipient bone marrow with a donor-specific MHC class II monoclonal antibody. The proportions of donor and recipient colonies were estimated from a standard curve created by LEW and BN bone marrow mixtures of known concentrations. Results. After the BMC infusions, 5-10% of the CFU-C in the bone marrow of BN recipients were of the LEW phenotype at 14, 30, and 60 days after transplantation. At 100 days, however, donor CFU-C could no longer be found at this site. The pattern of LEW CFU-C in the bone marrow of BN liver recipients up to 60 days was similar to that in recipients of 2.5 x 108 BMC, although the donor colonies were only 1/20 to 1/200 as numerous. This was expected, because the progenitor cells in the passenger leukocytes of a single liver are equivalent to those in 1-5x106 BMC. Using a liquid CFU-C assay, donor progenitor cells were demonstrated among the nonparenchymal cells of liver allografts up to 100 days. In contrast, after heart transplantation, donor CFU-C could not be identified in the recipient bone marrow, even at 14 days. Conclusion. Under effective immunosuppression, allogeneic hematopoietic progenitors compete effectively with host cells for initial engraftment in the bone marrow of noncytoablated recipients, but disappear from this location between 60 and 100 days after transplantation, coincident with the shift of donor leukocyte chimerism from the lymphoid to the nonlymphoid compartment that we previously have observed in this model. It is possible that the syngeneic parenchymal environment of the liver allografts constitutes a privileged site for persistent progenitor donor cells
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