62 research outputs found

    Spin analog of the controlled Josephson charge current

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    We propose a controlled Josephson spin current across the junction of two non-centrosymmetric superconductors like CePt_3Si. The Josephson spin current arises due to direction dependent tunneling matrix element and different momentum dependent phases of the triplet components of the gap function. Its modulation with the angle \xi between the noncentrosymmetric axes of two superconductors is proportional to \sin \xi. This particular dependence on \xi may find application of the proposed set-up in making a Josephson spin switch.Comment: 4 pages, 1 figure; title is changed; article is rewritte

    Induction of Ovarian Leiomyosarcomas in Mice by Conditional Inactivation of Brca1 and p53

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    gene is often found in patients with inherited breast and ovarian cancer syndrome..associated inherited EOC

    Spin-flip and spin-wave excitations in arbitrarily polarized quantum Hall states

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    We study spin-flip and spin-wave excitations for arbitrarily polarized quantum Hall states by employing a fermionic Chern-Simons gauge theory in the low Zeeman energy limit. We show that the spin-flip correlation functions do not get renormalized by the fluctuations of Chern-Simons gauge field. As a consequence, the excitations for a given integer quantum Hall state are identical to fractional quantum Hall states in the lowest Landau level having the same numerator equal to the integer quantum Hall state. Fully and partially polarized states possess only spin-wave excitations while spin-flip excitations are possible for all states, irrespective of their polarizations.Comment: 19 pages, 8 postscript figure

    Study of Low Energy Spin Rotons in the Fractional Quantum Hall Effect

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    Motivated by the discovery of extremely low energy collective modes in the fractional quantum Hall effect (Kang, Pinczuk {\em et al.}), with energies below the Zeeman energy, we study theoretically the spin reversed excitations for fractional quantum Hall states at ν=2/5\nu=2/5 and 3/7 and find qualitatively different behavior than for ν=1/3\nu=1/3. We find that a low-energy, charge-neutral "spin roton," associated with spin reversed excitations that involve a change in the composite-fermion Landau level index, has energy in reasonable agreement with experiment.Comment: Postscript figures included. Accepted in Phys. Rev. B (Rapid Communication

    Direct test of composite fermion model in quantum Hall systems

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    We show that neutron scattering and Raman scattering experiments can unambiguously determine a composite fermion parameter, viz., the effective number of Landau Levels filled by the composite fermions. For this purpose, one needs partially polarized or more preferably unpolarized quantum Hall states. We further find that spin correlation function acts as an order parameter in the spin transition.Comment: 18 page

    Ground State Vortex Lattice Structures in d-wave Superconductors

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    We show in a realistic dx2y2d_{x^{2}-y^{2}} symmetry gap model for a cuprate superconductor that the clean vortex lattice has discontinuous structural transitions (at and near T=0), as a function of the magnetic field BB along the c-axis. The transitions arise from the singular nonlocal and anisotropic susceptibility of the dx2y2d_{x^{2}-y^{2}} superconductor to the perturbation caused by supercurrents associated with vortices. The susceptibility, due to virtual Dirac quasiparticle-hole excitation, is calculated carefully, and leads to a ground state transition for the triangular lattice from an orientation along one of the crystal axis to one at 45o^o to them, i.e, along the gap zero direction. The field scale is seen to be 5 Tesla (Δ0/ta)2Φ0 \sim (\Delta_{0}/ta)^{2}\Phi_{0}, where Δ0\Delta_{0} is the gap maximum, tt is the nearest neighbour hopping, aa is the lattice constant, and Φ0\Phi_{0} is the flux quantum. At much higher fields (28T\sim 28T) there is a discontinuous transition to a centred square structure. The source of the differences from existing calculations, and experimental observability are discussed, the latter especially in view of the very small (a few degrees KK per vortex) differences in the ground state energy.Comment: To be published in Phys. Rev.

    Brg1 Is Required for Cdx2-Mediated Repression of Oct4 Expression in Mouse Blastocysts

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    During blastocyst formation the segregation of the inner cell mass (ICM) and trophectoderm is governed by the mutually antagonistic effects of the transcription factors Oct4 and Cdx2. Evidence indicates that suppression of Oct4 expression in the trophectoderm is mediated by Cdx2. Nonetheless, the underlying epigenetic modifiers required for Cdx2-dependent repression of Oct4 are largely unknown. Here we show that the chromatin remodeling protein Brg1 is required for Cdx2-mediated repression of Oct4 expression in mouse blastocysts. By employing a combination of RNA interference (RNAi) and gene expression analysis we found that both Brg1 Knockdown (KD) and Cdx2 KD blastocysts exhibit widespread expression of Oct4 in the trophectoderm. Interestingly, in Brg1 KD blastocysts and Cdx2 KD blastocysts, the expression of Cdx2 and Brg1 is unchanged, respectively. To address whether Brg1 cooperates with Cdx2 to repress Oct4 transcription in the developing trophectoderm, we utilized preimplantation embryos, trophoblast stem (TS) cells and Cdx2-inducible embryonic stem (ES) cells as model systems. We found that: (1) combined knockdown (KD) of Brg1 and Cdx2 levels in blastocysts resulted in increased levels of Oct4 transcripts compared to KD of Brg1 or Cdx2 alone, (2) endogenous Brg1 co-immunoprecipitated with Cdx2 in TS cell extracts, (3) in blastocysts Brg1 and Cdx2 co-localize in trophectoderm nuclei and (4) in Cdx2-induced ES cells Brg1 and Cdx2 are recruited to the Oct4 promoter. Lastly, to determine how Brg1 may induce epigenetic silencing of the Oct4 gene, we evaluated CpG methylation at the Oct4 promoter in the trophectoderm of Brg1 KD blastocysts. This analysis revealed that Brg1-dependent repression of Oct4 expression is independent of DNA methylation at the blastocyst stage. In toto, these results demonstrate that Brg1 cooperates with Cdx2 to repress Oct4 expression in the developing trophectoderm to ensure normal development

    Localisation and Function of the Endocannabinoid System in the Human Ovary

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    Although anandamide (AEA) had been measured in human follicular fluid and is suggested to play a role in ovarian follicle and oocyte maturity, its exact source and role in the human ovary remains unclear.Immunohistochemical examination of normal human ovaries indicated that the endocannabinoid system was present and widely expressed in the ovarian medulla and cortex with more intense cannabinoid receptor 2 (CB2) than CB1 immunoreactivity in the granulosa cells of primordial, primary, secondary, tertiary follicles, corpus luteum and corpus albicans. The enzymes, fatty acid amide hydrolase (FAAH) and N-acyclphosphatidylethanolamine-phospholipase D (NAPE-PLD), were only found in growing secondary and tertiary follicles and corpora lutea and albicantes. The follicular fluid (FF) AEA concentrations of 260 FF samples, taken from 37 infertile women undergoing controlled ovarian hyperstimulation for in vitro fertilisation and intracytoplasmic sperm injection with embryo transfer, were correlated with ovarian follicle size (P = 0.03). Significantly higher FF AEA concentrations were also observed in mature follicles (1.43+/-0.04 nM; mean+/-SEM) compared to immature follicles (1.26+/-0.06 nM), P = 0.0142 and from follicles containing morphologically assessed mature oocytes (1.56+/-0.11 nM) compared to that containing immature oocytes (0.99+/-0.09 nM), P = 0.0011. ROC analysis indicated that a FF AEA level of 1.09 nM could discriminate between mature and immature oocytes with 72.2% sensitivity and 77.14% specificity, whilst plasma AEA levels and FF AEA levels on oocyte retrieval day were not significantly different (P = 0.23).These data suggest that AEA is produced in the ovary, is under hormonal control and plays a role in folliculogenesis, preovulatory follicle maturation, oocyte maturity and ovulation

    CB1 Expression Is Attenuated in Fallopian Tube and Decidua of Women with Ectopic Pregnancy

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    BACKGROUND: Embryo retention in the Fallopian tube (FT) is thought to lead to ectopic pregnancy (EP), a considerable cause of morbidity. In mice, genetic/pharmacological silencing of cannabinoid receptor Cnr1, encoding CB1, causes retention of embryos in the oviduct. The role of the endocannabinoids in tubal implantation in humans is not known. METHODS AND FINDINGS: Timed FT biopsies (n = 18) were collected from women undergoing gynecological procedures for benign conditions. Endometrial biopsies and whole blood were collected from women undergoing surgery for EP (n = 11); management of miscarriage (n = 6), and termination of pregnancy (n = 8). Using RT-PCR and immunohistochemistry, CB1 mRNA and protein expression levels/patterns were examined in FT and endometrial biopsies. The distribution of two polymorphisms of CNR1 was examined by TaqMan analysis of genomic DNA from the whole blood samples. In normal FT, CB1 mRNA was higher in luteal compared to follicular-phase (p<0.05). CB1 protein was located in smooth muscle of the wall and of endothelial vessels, and luminal epithelium of FT. In FT from women with EP, CB1 mRNA expression was low. CB1 mRNA expression was also significantly lower (p<0.05) in endometrium of women with EP compared to intrauterine pregnancies (IUP). Although of 1359G/A (rs1049353) polymorphisms of CNR1 gene suggests differential distribution of genotypes between the small, available cohorts of women with EP and those with IUP, results were not statistically significant. CONCLUSIONS: CB1 mRNA shows temporal variation in expression in human FT, likely regulated by progesterone. CB1 mRNA is expressed in low levels in both the FT and endometrium of women with EP. We propose that aberrant endocannabinoid-signaling in human FT leads to EP. Furthermore, our finding of reduced mRNA expression along with a possible association between polymorphism genotypes of the CNR1 gene and EP, suggests a possible genetic predisposition to EP that warrants replication in a larger sample pool

    Fetal Programming of Adult Glucose Homeostasis in Mice

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    BACKGROUND: Emerging evidence suggests that dietary soy and phytoestrogens can have beneficial effects on lipid and glucose metabolism. We have previously shown that male mice fed from conception to adulthood with a high soy-containing diet had reduced body weight, adiposity and a decrease in glucose intolerance, an early marker of insulin resistance and diabetes. OBJECTIVES: The purpose of this study was to identify the precise periods of exposure during which phytoestrogens and dietary soy improve lipid and glucose metabolism. Since intrauterine position (IUP) has been shown to alter sensitivity to endocrine disruptors, we also investigated whether the combination of IUP and fetal exposure to dietary phytoestrogens could potentially affect adult metabolic parameters. METHODS: Male outbred mice (CD-1) were allowed ad libitum access to either a high soy-containing diet or a soy-free diet either during gestation, lactation or after weaning. Adiposity and bone mass density was assessed by dual x-ray absorptiometry. Glucose tolerance was assessed by a glucose tolerance test. Blood pressure was examined by the tail-cuff system. RESULTS: Here we show that metabolic improvements are dependent on precise windows of exposure during life. The beneficial effects of dietary soy and phytoestrogens on adiposity were apparent only in animals fed post-natally, while the improvements in glucose tolerance are restricted to animals with fetal exposure to soy. Interestingly, we observed that IUP influenced adult glucose tolerance, but not adiposity. Similar IUP trends were observed for other estrogen-related metabolic parameters such as blood pressure and bone mass density. CONCLUSION: Our results suggest that IUP and fetal exposure to estrogenic environmental disrupting compounds, such as dietary phytoestrogens, could alter metabolic and cardiovascular parameters in adult individuals independently of adipose gain
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