1,076 research outputs found

    On topological defect formation in the process of symmetry breaking phase transitions

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    By resorting to some results in quantum field theories with spontaneous breakdown of symmetry we show that an explanation based on microscopic dynamics can be given of the fact that topological defect formation is observed during the process of non-equilibrium phase transitions characterized by a non-zero order parameter. We show that the Nambu-Goldstone particle acquires an effective non-zero mass due to the boundary (finite volume) effects and this is related with the size of the defect. We also relate such volume effect with temperature effect.Comment: 12 pages, no figure

    On flavor conservation in weak interaction decays involving mixed neutrinos

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    In the context of quantum field theory (QFT), we compute the amplitudes of weak interaction processes such as W+→e++νe W^{+} \rightarrow e^{+} + \nu_{e} and W+→e++νμ W^{+} \rightarrow e^{+} + \nu_{\mu} by using different representations of flavor states for mixed neutrinos. Analyzing the short time limit of the above amplitudes, we find that the neutrino states defined in QFT as eigenstates of the flavor charges lead to results consistent with lepton charge conservation. On the contrary, the Pontecorvo flavor states produce a violation of lepton charge in the vertex, which is in contrast with what expected at tree level in the Standard Model.Comment: 15 page

    Recent developments and strategies in pediatric pharmacology research in the USA

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    Research in pediatric pharmacology has undergone major changes in the last ten years, with an expansion in both publicly and privately funded activities. A number of pharmacokinetics studies and multi-site controlled efficacy trials have been conducted, so that treatment of children and adolescents can now be better informed and evidence-based. Regulatory financial incentives to industry in return for studies on drugs still covered by patent exclusivity have resulted in a substantial increase in pediatric research funded by pharmaceutical companies. In parallel, public funding has supported research on off-patent medications and other clinical important aspects of treatment, such as comparisons between active treatments, including non-pharmacological interventions. With greater interest by industry in pediatric research, the role of government funding agencies has been redefined to avoid duplication and ensure better integration of efforts and utilization of resources. The present review discusses some of the recent developments in pediatric pharmacology with focus on psychiatric medications

    Moderation of antipsychotic-induced weight gain by energy balance gene variants in the RUPP autism network risperidone studies.

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    Second-generation antipsychotic exposure, in both children and adults, carries significant risk for excessive weight gain that varies widely across individuals. We queried common variation in key energy balance genes (FTO, MC4R, LEP, CNR1, FAAH) for their association with weight gain during the initial 8 weeks in the two NIMH Research Units on Pediatric Psychopharmacology Autism Network trials (N=225) of risperidone for treatment of irritability in children/adolescents aged 4-17 years with autism spectrum disorders. Variants in the cannabinoid receptor (CNR)-1 promoter (P=1.0 Ă— 10(-6)), CNR1 (P=9.6 Ă— 10(-5)) and the leptin (LEP) promoter (P=1.4 Ă— 10(-4)) conferred robust-independent risks for weight gain. A model combining these three variants was highly significant (P=1.3 Ă— 10(-9)) with a 0.85 effect size between lowest and highest risk groups. All results survived correction for multiple testing and were not dependent on dose, plasma level or ethnicity. We found no evidence for association with a reported functional variant in the endocannabinoid metabolic enzyme, fatty acid amide hydrolase, whereas body mass index-associated single-nucleotide polymorphisms in FTO and MC4R showed only trend associations. These data suggest a substantial genetic contribution of common variants in energy balance regulatory genes to individual antipsychotic-associated weight gain in children and adolescents, which supersedes findings from prior adult studies. The effects are robust enough to be detected after only 8 weeks and are more prominent in this largely treatment naive population. This study highlights compelling directions for further exploration of the pharmacogenetic basis of this concerning multifactorial adverse event

    First report of anti-TIF1Îł dermatomyositis in a patient with myelodysplastic syndrome.

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    Inflammatory myopathies as para-neoplastic phenomena were first described by Sterz in 1916. Recently, myositis specific autoantibodies were described in cancer-associated myositis. Anti-transcription intermediary factor 1 gamma (anti-TIF1Îł) antibodies have been found in both young adults affected by juvenile dermatomyositis and in elderly patients with cancer-associated myositis. In this regard, we report herein the first case of anti-TIF1Îł dermatomyositis secondary to a myelodysplastic syndrome
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