9,516 research outputs found
Generalized pairwise z-complementary codes
An approach to generate generalized pairwise Z-complementary (GPZ) codes, which works in pairs in order to offer a zero correlation zone (ZCZ) in the vicinity of zero phase shift and fit extremely well in power efficient quadrature carrier modems, is introduced in this letter. Each GPZ code has MK sequences, each of length 4NK, whereMis the number of Z-complementary mates,
K is a factor to perform Walsh–Hadamard expansions, and N is the sequence length of the Z-complementary code. The proposed GPZ codes include the generalized pairwise complementary (GPC)codes as special cases
Quasi-Local Energy Flux of Spacetime Perturbation
A general expression for quasi-local energy flux for spacetime perturbation
is derived from covariant Hamiltonian formulation using functional
differentiability and symplectic structure invariance, which is independent of
the choice of the canonical variables and the possible boundary terms one
initially puts into the Lagrangian in the diffeomorphism invariant theories.
The energy flux expression depends on a displacement vector field and the
2-surface under consideration. We apply and test the expression in Vaidya
spacetime. At null infinity the expression leads to the Bondi type energy flux
obtained by Lindquist, Schwartz and Misner. On dynamical horizons with a
particular choice of the displacement vector, it gives the area balance law
obtained by Ashtekar and Krishnan.Comment: 8 pages, added appendix, version to appear in Phys. Rev.
Tailored design of NKT-stimulatory glycolipids for polarization of immune responses.
Natural killer T (NKT) cell is a distinct population of T lymphocytes that can rapidly release massive amount of Th1 and Th2 cytokines upon the engagement of their T cell receptor with glycolipids presented by CD1d. The secreted cytokines can promote cell-mediated immunity to kill tumor cells and intracellular pathogens, or suppress autoreactive immune cells in autoimmune diseases. Thus, NKT cell is an attractive target for developing new therapeutics to manipulate immune system. The best-known glycolipid to activate NKT cells is α-galactosylceramide (α-GalCer), which has been used as a prototype for designing new NKT stimulatory glycolipids. Many analogues have been generated by modification of the galactosyl moiety, the acyl chain or the phytosphingosine chain of α-GalCer. Some of the analogues showed greater abilities than α-GalCer in polarizing immune responses toward Th1 or Th2 dominance. Among them, several analogues containing phenyl groups in the lipid tails were more potent in inducing Th1-skewed cytokines and exhibited greater anticancer efficacy than α-GalCer. Analyses of the correlation between structure and activity of various α-GalCer analogues on the activation of iNKT cell revealed that CD1d-glycolipid complexes interacted with the same population of iNKT cell expressing similar T-cell receptor Vβ as α-GalCer. On the other hand, those phenyl glycolipids with propensity for Th1 dominant responses showed greater binding avidity and stability than α-GalCer for iNKT T-cell receptor when complexed with CD1d. Thus, it is the avidity and stability of the ternary complexes of CD1d-glycolipid-iNKT TCR that dictate the polarity and potency of immune responses. These findings provide a key to the rationale design of immune modulating glycolipids with desirable Th1/Th2 polarity for clinical application. In addition, elucidation of α-GalCer-induced anergy, liver damage and accumulation of myeloid derived suppressor cells has offered explanation for its lacklustre anti-cancer activities in clinical trials. On other hand, the lack of such drawbacks in glycolipid analogues containing phenyl groups in the lipid tails of α-GalCer coupled with the greater binding avidity and stability of CD1d-glycolipid complex for iNKT T-cell receptor, account for their superior anti-cancer efficacy in tumor bearing mice. Further clinical development of these phenyl glycolipids is warranted
Resonant Subband Landau Level Coupling in Symmetric Quantum Well
Subband structure and depolarization shifts in an ultra-high mobility
GaAs/Al_{0.24}Ga_{0.76}As quantum well are studied using magneto-infrared
spectroscopy via resonant subband Landau level coupling. Resonant couplings
between the 1st and up to the 4th subbands are identified by well-separated
anti-level-crossing split resonance, while the hy-lying subbands were
identified by the cyclotron resonance linewidth broadening in the literature.
In addition, a forbidden intersubband transition (1st to 3rd) has been
observed. With the precise determination of the subband structure, we find that
the depolarization shift can be well described by the semiclassical slab plasma
model, and the possible origins for the forbidden transition are discussed.Comment: 4 pages, 2 figure
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