151 research outputs found
Genome-Wide Association Study of Cryptosporidiosis in Infants Implicates PRKCA.
Diarrhea is a major cause of both morbidity and mortality worldwide, especially among young children. Cryptosporidiosis is a leading cause of diarrhea in children, particularly in South Asia and sub-Saharan Africa, where it is responsible for over 200,000 deaths per year. Beyond the initial clinical presentation of diarrhea, it is associated with long-term sequelae such as malnutrition and neurocognitive developmental deficits. Risk factors include poverty and overcrowding, and yet not all children with these risk factors and exposure are infected, nor do all infected children develop symptomatic disease. One potential risk factor to explain these differences is their human genome. To identify genetic variants associated with symptomatic cryptosporidiosis, we conducted a genome-wide association study (GWAS) examining 6.5 million single nucleotide polymorphisms (SNPs) in 873 children from three independent cohorts in Dhaka, Bangladesh, namely, the Dhaka Birth Cohort (DBC), the Performance of Rotavirus and Oral Polio Vaccines in Developing Countries (PROVIDE) study, and the Cryptosporidiosis Birth Cohort (CBC). Associations were estimated separately for each cohort under an additive model, adjusting for length-for-age Z-score at 12 months of age, the first two principal components to account for population substructure, and genotyping batch. The strongest meta-analytic association was with rs58296998 (P = 3.73 × 10-8), an intronic SNP and expression quantitative trait locus (eQTL) of protein kinase C alpha (PRKCA). Each additional risk allele conferred 2.4 times the odds of Cryptosporidium-associated diarrhea in the first year of life. This genetic association suggests a role for protein kinase C alpha in pediatric cryptosporidiosis and warrants further investigation.IMPORTANCE Globally, diarrhea remains one of the major causes of pediatric morbidity and mortality. The initial symptoms of diarrhea can often lead to long-term consequences for the health of young children, such as malnutrition and neurocognitive developmental deficits. Despite many children having similar exposures to infectious causes of diarrhea, not all develop symptomatic disease, indicating a possible role for human genetic variation. Here, we conducted a genetic study of susceptibility to symptomatic disease associated with Cryptosporidium infection (a leading cause of diarrhea) in three independent cohorts of infants from Dhaka, Bangladesh. We identified a genetic variant within protein kinase C alpha (PRKCA) associated with higher risk of cryptosporidiosis in the first year of life. These results indicate a role for human genetics in susceptibility to cryptosporidiosis and warrant further research to elucidate the mechanism
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Early Life Inflammation and Neurodevelopmental Outcome in Bangladeshi Infants Growing Up in Adversity
Abstract. Exposure to profound adversity can negatively affect the neurodevelopment of children, but biologic mechanisms that underlie this association remain unknown. We sought to determine whether elevated levels of the inflammatory markers C-reactive protein (CRP) and soluble CD14 (sCD14) are associated with neurodevelopmental outcomes in Bangladeshi children. A total of 422 infant–mother pairs from an urban slum in Dhaka, Bangladesh were enrolled at birth and followed prospectively. Inflammation was measured with sCD14, interleukin (IL)-1β, and IL-6 at 18 weeks, and CRP at 6, 18, 40, and 53 weeks. Psychologists assessed cognitive, language, motor, and social emotional development using the Bayley Scales of Infant and Toddler Development at 78 and 104 weeks of age. We tested for the association of inflammatory markers with developmental outcomes, independent of previously identified associations such as malnutrition, family income, and maternal education. Every 10 pg/mL increase in sCD14 was associated with a 1.1–2.0 decrement in cognitive and motor scores at 78 weeks and in all domains at 104 weeks. The cumulative number of CRP elevations that a child experienced in the first year of life, as well as IL-1β and IL-6 at 18 weeks of age, were also negatively associated with Bayley Scales results. CRP, sCD14, IL-1β, and IL-6 were associated with lower neurodevelopmental outcomes. Our findings implicate a role of inflammation in the neurodevelopment of children growing up in adversity
Microbial activity in the marine deep biosphere: progress and prospects
The vast marine deep biosphere consists of microbial habitats within sediment, pore waters, upper basaltic crust and the fluids that circulate throughout it. A wide range of temperature, pressure, pH, and electron donor and acceptor conditions exists—all of which can combine to affect carbon and nutrient cycling and result in gradients on spatial scales ranging from millimeters to kilometers. Diverse and mostly uncharacterized microorganisms live in these habitats, and potentially play a role in mediating global scale biogeochemical processes. Quantifying the rates at which microbial activity in the subsurface occurs is a challenging endeavor, yet developing an understanding of these rates is essential to determine the impact of subsurface life on Earth\u27s global biogeochemical cycles, and for understanding how microorganisms in these “extreme” environments survive (or even thrive). Here, we synthesize recent advances and discoveries pertaining to microbial activity in the marine deep subsurface, and we highlight topics about which there is still little understanding and suggest potential paths forward to address them. This publication is the result of a workshop held in August 2012 by the NSF-funded Center for Dark Energy Biosphere Investigations (C-DEBI) “theme team” on microbial activity (www.darkenergybiosphere.org)
Effect of substituting IPV for tOPV on immunity to poliovirus in Bangladeshi infants: An open-label randomized controlled trial
AbstractBackgroundThe Polio Endgame strategy includes phased withdrawal of oral poliovirus vaccines (OPV) coordinated with introduction of inactivated poliovirus vaccine (IPV) to ensure population immunity. The impact of IPV introduction into a primary OPV series of immunizations in a developing country is uncertain.MethodsBetween May 2011 and November 2012, we enrolled 700 Bangladeshi infant-mother dyads from Dhaka slums into an open-label randomized controlled trial to test whether substituting an injected IPV dose for the standard Expanded Program on Immunization (EPI) fourth tOPV dose at infant age 39 weeks would reduce fecal shedding and enhance systemic immunity. The primary endpoint was mucosal immunity to poliovirus at age one year, measured by fecal excretion of any Sabin virus at five time points up to 25 days post-52 week tOPV challenge, analyzed by the intention to treat principle.FindingsWe randomized 350 families to the tOPV and IPV vaccination arms. Neither study arm resulted in superior intestinal protection at 52 weeks measured by the prevalence of infants shedding any of three poliovirus serotypes, but the IPV dose induced significantly higher seroprevalence and seroconversion rates. This result was identical for poliovirus detection by cell culture or RT-qPCR. The non-significant estimated culture-based shedding risk difference was −3% favoring IPV, and the two vaccination schedules were inferred to be equivalent within a 95% confidence margin of −10% to +4%. Results for shedding analyses stratified by poliovirus type were similar.ConclusionsNeither of the vaccination regimens is superior to the other in enhancing intestinal immunity as measured by poliovirus shedding at 52 weeks of age and the IPV regimen provides similar intestinal immunity to the four tOPV series, although the IPV regimen strongly enhances humoral immunity. The IPV-modified regimen may be considered for vaccination programs without loss of intestinal protection
A site assessment tool for inpatient controlled human infection models for enteric disease pathogens
The use of the controlled human infection model to facilitate product development and to advance understanding of host-pathogen interactions is of increasing interest. While administering a virulent (or infective) organism to a susceptible host necessitates an ongoing evaluation of safety and ethical considerations, a central theme in conducting these studies in a safe and ethical manner that yields actionable data is their conduct in facilities well-suited to address their unique attributes. To that end, we have developed a framework for evaluating potential sites in which to conduct inpatient enteric controlled human infection model to ensure consistency and increase the likelihood of success.publishedVersio
Deep z-band observations of the coolest y dwarf
Taisiya G. Kopytova, et al., “Deep z-band observations of the coolest y dwarf”, The Astrophysical Journal, Vol. 797(1), November 2014. © 2014. The American Astronomical Society.WISE J085510.83-071442.5 (hereafter, WISE 0855-07) is the coolest Y dwarf known to date and is located at a distance of 2.31 ± 0.08 pc, giving it the fourth largest parallax of any known star or brown dwarf system. We report deep z-band observations of WISE 0855-07 using FORS2 on UT1/Very Large Telescope. We do not detect any counterpart to WISE 0855-07 in our z-band images and estimate a brightness upper limit of AB mag > 24.8 (F ν <0.45 μJy) at 910 ± 65 nm with 3σ confidence. We combine our z-band upper limit with previous near- and mid-infrared photometry to place constraints on the atmospheric properties of WISE 0855-07 via comparison to models which implement water clouds in the atmospheres of T eff <300 K substellar objects. We find that none of the available models that implement water clouds can completely reproduce the observed spectral energy distribution of WISE 0855-07. Every model significantly disagrees with the (3.6 μm/4.5 μm) flux ratio and at least one other bandpass. Since methane is predicted to be the dominant absorber at 3-4 μm, these mismatches might point to an incorrect or incomplete treatment of methane in current models. We conclude that (a) WISE0855-07 has T eff 200-250 K, (b)Peer reviewe
The Wide-field Infrared Survey Explorer (WISE): Mission Description and Initial On-orbit Performance
The all sky surveys done by the Palomar Observatory Schmidt, the European
Southern Observatory Schmidt, and the United Kingdom Schmidt, the InfraRed
Astronomical Satellite and the 2 Micron All Sky Survey have proven to be
extremely useful tools for astronomy with value that lasts for decades. The
Wide-field Infrared Survey Explorer is mapping the whole sky following its
launch on 14 December 2009. WISE began surveying the sky on 14 Jan 2010 and
completed its first full coverage of the sky on July 17. The survey will
continue to cover the sky a second time until the cryogen is exhausted
(anticipated in November 2010). WISE is achieving 5 sigma point source
sensitivities better than 0.08, 0.11, 1 and 6 mJy in unconfused regions on the
ecliptic in bands centered at wavelengths of 3.4, 4.6, 12 and 22 microns.
Sensitivity improves toward the ecliptic poles due to denser coverage and lower
zodiacal background. The angular resolution is 6.1, 6.4, 6.5 and 12.0
arc-seconds at 3.4, 4.6, 12 and 22 microns, and the astrometric precision for
high SNR sources is better than 0.15 arc-seconds.Comment: 22 pages with 19 included figures. Updated to better match the
accepted version in the A
Longitudinal analysis of acute and convalescent B cell responses in a human primary dengue serotype 2 infection model
Background: Acute viral infections induce a rapid and transient increase in antibody-secreting plasmablasts. At
convalescence, memory B cells (MBC) and long-lived plasma cells (LLPC) are responsible for long-term humoral
immunity. Following an acute viral infection, the specific properties and relationships between antibodies
produced by these B cell compartments are poorly understood.
Methods:Weutilized a controlled human challenge model of primary dengue virus serotype 2 (DENV2) infection
to study acute and convalescent B-cell responses.
Findings: The level of DENV2 replication was correlated with the magnitude of the plasmablast response. Functional
analysis of plasmablast-derived monoclonal antibodies showed that the DENV2-specific response was
dominated by cells producing DENV2 serotype-specific antibodies. DENV2-neutralizing antibodies targeted quaternary
structure epitopes centered on domain III of the viral envelope protein (EDIII). Functional analysis ofMBC
and serum antibodies from the same subjects six months post-challenge revealed maintenance of the serotypespecific
response in both compartments. The serumresponse mainly targeted DENV2 serotype-specific epitopes
on EDIII.
Interpretation: Our data suggest overall functional alignment of DENV2-specific responses from the plasmablast,
through the MBC and LLPC compartments following primary DENV2 inflection. These results provide enhanced
resolution of the temporal and specificity of the B cell compartment in viral infection and serve as framework for
evaluation of B cell responses in challenge models
A map of transcriptional heterogeneity and regulatory variation in human microglia.
Microglia, the tissue-resident macrophages of the central nervous system (CNS), play critical roles in immune defense, development and homeostasis. However, isolating microglia from humans in large numbers is challenging. Here, we profiled gene expression variation in primary human microglia isolated from 141 patients undergoing neurosurgery. Using single-cell and bulk RNA sequencing, we identify how age, sex and clinical pathology influence microglia gene expression and which genetic variants have microglia-specific functions using expression quantitative trait loci (eQTL) mapping. We follow up one of our findings using a human induced pluripotent stem cell-based macrophage model to fine-map a candidate causal variant for Alzheimer's disease at the BIN1 locus. Our study provides a population-scale transcriptional map of a critically important cell for human CNS development and disease
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