Seroprevalence of human T-lymphotropic virus type 1 in Papua New Guinea and Irian Jaya measured using different Western blot criteria

Background: Endemic foci of HTLV-1 carriers have been found in the world, however, the origin of HTLV-1 in humans is still unclear. Since a distinct type of virus strain was isolated from the Solomon Islands, detailed surveys on HTLV-1 prevalence in New Guinea are important to shed light on its history of dissemination. Objecti6e: To clarify the seroprevalence of HTLV-1 in different regions of New Guinea Island. Study design: Sera from 1221 individuals (649 males, 454 females and 118 unknown) in New Guinea Island were studied for the presence of antibodies to HTLV-1 by a particle agglutination and the Western blot (WB) tests. Two different sets of criteria, proposed by WHO and Kiyokawa et al., were employed to interpret the WB test. Since the latter seemed to lack adequate specificity, the WHO criteria was used for the evaluation of the seroprevalence throughout the study. Results: Seroprevalence of HTLV-1 differed by the WB criteria. By the more stringent criteria, HTLV-1 carriers were found in Madang, Chimbu and one hinterland province, Enga, in Papua New Guinea. An overall seroprevalence rate in different regions ranged from 0 to 14.6%. No seropositive individuals were found in Irian Jaya. Conclusions: To avoid overestimating the seropositivity rates, the WHO criteria would be more appropriate to employ for WB test by using the samples obtained from tropical and:or malaria endemic areas. This study is the first to show HTLV-1 infected individuals in the hinterland of New Guinea Island

Germline recombination by conditional gene targeting with Parvalbumin-Cre lines

Conditional gene targeting allows us to study gene function in specific tissues or cell types. This is commonly achieved by Cre DNA recombinase and its 34–base pair target sequences called loxP sites. Through the efforts of individual labs and large-scale projects, a sizable collection of Cre mouse lines has been generated to express or delete specific genes in a wide range of cell types throughout the nervous sys-tem (Madisen et al., 2010; Taniguchi et al., 2011). Typically, the specificity of Cre transgene expression is controlled by tissue or cell-type promoters. However, increas-ing evidence has revealed that the desire

Adequacy of Approximations in GW Theory

We use an all-electron implementation of the GW approximation to analyze several possible sources of error in the theory and its implementation. Among these are convergence in the polarization and Green's functions, the dependence of QP levels on choice of basis sets, and differing approximations for dealing with core levels. In all GW calculations presented here, G and W are generated from the local-density approximation (LDA), which we denote as the \GLDA\WLDA approximation. To test its range of validity, the \GLDA\WLDA approximation is applied to a variety of materials systems. We show that for simple sp semiconductors, \GLDA\WLDA always underestimates bandgaps; however, better agreement with experiment is obtained when the self-energy is not renormalized, and we propose a justification for it. Some calculations for Si are compared to pseudopotential-based \GLDA\WLDA calculations, and some aspects of the suitability of pseudopotentials for GW calculations are discussed.Comment: 38 pages,6 figures. Minor Revision

Targeting Oxidative Stress and Aberrant Critical Period Plasticity in the Developmental Trajectory to Schizophrenia

Schizophrenia is a neurodevelopmental disorder reflecting a convergence of genetic risk and early life stress. The slow progression to first psychotic episode represents both a window of vulnerability as well as opportunity for therapeutic intervention. Here, we consider recent neurobiological insight into the cellular and molecular components of developmental critical periods and their vulnerability to redox dysregulation. In particular, the consistent loss of parvalbumin-positive interneuron (PVI) function and their surrounding perineuronal nets (PNNs) as well as myelination in patient brains is consistent with a delayed or extended period of circuit instability. This linkage to critical period triggers (PVI) and brakes (PNN, myelin) implicates mistimed trajectories of brain development in mental illness. Strategically introduced antioxidant treatment or later reinforcement of molecular brakes may then offer a novel prophylactic psychiatr