6,111 research outputs found
A massive proto-cluster of galaxies at a redshift of z {\approx} 5.3
Massive clusters of galaxies have been found as early as 3.9 Billion years
(z=1.62) after the Big Bang containing stars that formed at even earlier
epochs. Cosmological simulations using the current cold dark matter paradigm
predict these systems should descend from "proto-clusters" - early
over-densities of massive galaxies that merge hierarchically to form a cluster.
These proto-cluster regions themselves are built-up hierarchically and so are
expected to contain extremely massive galaxies which can be observed as
luminous quasars and starbursts. However, observational evidence for this
scenario is sparse due to the fact that high-redshift proto-clusters are rare
and difficult to observe. Here we report a proto-cluster region 1 billion years
(z=5.3) after the Big Bang. This cluster of massive galaxies extends over >13
Mega-parsecs, contains a luminous quasar as well as a system rich in molecular
gas. These massive galaxies place a lower limit of >4x10^11 solar masses of
dark and luminous matter in this region consistent with that expected from
cosmological simulations for the earliest galaxy clusters.Comment: Accepted to Nature, 16 Pages, 6 figure
Maternal inflammatory and microbial drivers of low birthweight in low- and middle-income countries.
BACKGROUND: Low birthweight (LBW) is when an infant is born too soon or too small, and it affects one in seven infants in low- and middle-income countries. LBW has a significant impact on short-term morbidity and mortality, and it impairs long-term health and human capital. Antenatal microbial and inflammatory exposure may contribute to LBW. METHODS: Ovid-Medline, Embase and Cochrane databases were searched for English-language articles evaluating inflammatory, microbial or infective causes of LBW, small-for-gestational age, intra-uterine growth restriction or prematurity. Inclusion criteria were human studies including published data; conference abstracts and grey literature were excluded. A narrative synthesis of the literature was conducted. RESULTS: Local infections may drive the underlying causes of LBW: for example, vaginitis and placental infection are associated with a greater risk of prematurity. Distal infection and inflammatory pathways are also associated with LBW, with an association between periodontitis and preterm delivery and environmental enteric dysfunction and reduced intra-uterine growth. Systemic maternal infections such as malaria and HIV are associated with LBW, even when infants are exposed to HIV but not infected. This latter association may be driven by chronic inflammation, co-infections and socio-economic confounders. Antimicrobial prophylaxis against other bacteria in pregnancy has shown minimal impact in most trials, though positive effects on birthweight have been found in some settings with a high infectious disease burden. CONCLUSION: Maternal inflammatory and infective processes underlie LBW, and provide treatable pathways for interventions. However, an improved understanding of the mechanisms and pathways underlying LBW is needed, given the impact of LBW on life-course
International Perspectives: Birth-Associated Neonatal Encephalopathy: Postresuscitation Care in West African Newborns
The West African subregion has the highest burden of neonatal mortality globally and the neonatal mortality rate is decreasing very slowly. A high proportion of newborn deaths are preventable and improved quality of care can reduce long-term morbidity in survivors. Perinatal asphyxia is the major cause of death and disability in term infants in the subregion. Neonatal resuscitation training programs have reduced stillbirths and early neonatal mortality but the overall effect on survival to discharge, population-based perinatal mortality, and long-term impairment is uncertain. Gaps in the health system and quality of postresuscitation care for affected newborns may defeat gains from global efforts to improve care around the time of birth. The aim of this review is to discuss the current situation of postresuscitation care of term infants with presumed birth-associated neonatal encephalopathy in West Africa. Limitations in diagnosing and treating affected infants and feasible interventions to improve acute and postdischarge care are discussed
Linking dwarf galaxies to halo building blocks with the most metal-poor star in Sculptor
Current cosmological models indicate that the Milky Way's stellar halo was
assembled from many smaller systems. Based on the apparent absence of the most
metal-poor stars in present-day dwarf galaxies, recent studies claimed that the
true Galactic building blocks must have been vastly different from the
surviving dwarfs. The discovery of an extremely iron-poor star (S1020549) in
the Sculptor dwarf galaxy based on a medium-resolution spectrum cast some doubt
on this conclusion. However, verification of the iron-deficiency and
measurements of additional elements, such as the alpha-element Mg, are
mandatory for demonstrating that the same type of stars produced the metals
found in dwarf galaxies and the Galactic halo. Only then can dwarf galaxy stars
be conclusively linked to early stellar halo assembly. Here we report
high-resolution spectroscopic abundances for 11 elements in S1020549,
confirming the iron abundance of less than 1/4000th that of the Sun, and
showing that the overall abundance pattern mirrors that seen in low-metallicity
halo stars, including the alpha-elements. Such chemical similarity indicates
that the systems destroyed to form the halo billions of years ago were not
fundamentally different from the progenitors of present-day dwarfs, and
suggests that the early chemical enrichment of all galaxies may be nearly
identical.Comment: 16 pages, including 2 figures. Accepted for publication in Nature. It
is embargoed for discussion in the press until formal publication in Natur
Stem cell differentiation increases membrane-actin adhesion regulating cell blebability, migration and mechanics
This work is licensed under a Creative Commons Attribution 4.0 International License. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in the credit line; if the material is not included under the Creative Commons license, users will need to obtain permission from the license holder in order to reproduce the material. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/K. S. is funded by an EPSRC PhD studentship. S.T. is funded by an EU Marie Curie Intra European Fellowship (GENOMICDIFF)
"I am your mother and your father!": In vitro derived gametes and the ethics of solo reproduction
In this paper, we will discuss the prospect of human reproduction achieved with gametes originating from only one person. According to statements by a minority of scientists working on the generation of gametes in vitro, it may become possible to create eggs from men’s non-reproductive cells and sperm from women’s. This would enable, at least in principle, the creation of an embryo from cells obtained from only one individual: ‘solo reproduction’. We will consider what might motivate people to reproduce in this way, and the implications that solo reproduction might have for ethics and policy. We suggest that such an innovation is unlikely to revolutionise reproduction and parenting. Indeed, in some respects it is less revolutionary than in vitro fertilisation as a whole. Furthermore, we show that solo reproduction with in vitro created gametes is not necessarily any more ethically problematic than gamete donation—and probably less so. Where appropriate, we draw parallels with the debate surrounding reproductive cloning. We note that solo reproduction may serve to perpetuate reductive geneticised accounts of reproduction, and that this may indeed be ethically questionable. However, in this it is not unique among other technologies of assisted reproduction, many of which focus on genetic transmission. It is for this reason that a ban on solo reproduction might be inconsistent with continuing to permit other kinds of reproduction that also bear the potential to strengthen attachment to a geneticised account of reproduction. Our claim is that there are at least as good reasons to pursue research towards enabling solo reproduction, and eventually to introduce solo reproduction as an option for fertility treatment, as there are to do so for other infertility related purposes
The Caenorhabditis chemoreceptor gene families
Background: Chemoreceptor proteins mediate the first step in the transduction of environmental chemical stimuli, defining the breadth of detection and conferring stimulus specificity. Animal genomes contain families of genes encoding chemoreceptors that mediate taste, olfaction, and pheromone responses. The size and diversity of these families reflect the biology of
chemoperception in specific species.
Results: Based on manual curation and sequence comparisons among putative G-protein-coupled chemoreceptor genes in the nematode Caenorhabditis elegans, we identified approximately 1300 genes and 400 pseudogenes in the 19 largest gene families, most of which fall into larger
superfamilies. In the related species C. briggsae and C. remanei, we identified most or all genes in each of the 19 families. For most families, C. elegans has the largest number of genes and C. briggsae the smallest number, suggesting changes in the importance of chemoperception among the species.
Protein trees reveal family-specific and species-specific patterns of gene duplication and gene loss. The frequency of strict orthologs varies among the families, from just over 50% in two families to less than 5% in three families. Several families include large species-specific expansions, mostly in C. elegans and C. remanei.
Conclusion: Chemoreceptor gene families in Caenorhabditis species are large and evolutionarily dynamic as a result of gene duplication and gene loss. These dynamics shape the chemoreceptor gene complements in Caenorhabditis species and define the receptor space available for
chemosensory responses. To explain these patterns, we propose the gray pawn hypothesis: individual genes are of little significance, but the aggregate of a large number of diverse genes is required to cover a large phenotype space.JHT was supported by NIH grant RO1GM48700 and HMR by R01AI56081
Measuring the water retention curve of rock fragments: A novel repacked core methodology
We describe a novel suction plate experiment that uses large, repacked soil cores comprising clasts and a fine-textured matrix to accurately measure the water retention curve of rock fragments (RFs) of high and low porosity. The method incorporates a suction plate-core containment system that can be weighed as a unit, to overcome typical core size restrictions. The method relies on analysing the relationship between total core volumetric water content and RF concentration. Cores are packed with a mix of glass and RFs to maintain a uniform volumetric total clast proportion of 30% while RF concentration varies. A constant total clast volume improves accuracy and precision by ensuring the water-holding characteristics of the matrix varies as little as possible among cores
What’s in a Name? Parents’ and Healthcare Professionals’ Preferred Terminology for Pathogenic Variants in Childhood Cancer Predisposition Genes
Current literature/guidelines regarding the most appropriate term to communicate a cancer-related disease-causing germline variant in childhood cancer lack consensus. Guidelines also rarely address preferences of patients/families. We aimed to assess preferences of parents of children with cancer, genetics professionals, and pediatric oncologists towards terminology to describe a disease-causing germline variant in childhood cancer. Using semi-structured interviews we asked participants their most/least preferred terms from; ‘faulty gene,’ ‘altered gene,’ ‘gene change,’ and ‘genetic variant,’ analyzing responses with directed content analysis. Twenty-five parents, 6 genetics professionals, and 29 oncologists participated. An equal number of parents most preferred ‘gene change,’ ‘altered gene,’ or ‘genetic variant’ (n = 8/25). Parents least preferred ‘faulty gene’ (n = 18/25). Half the genetics professionals most preferred ‘faulty gene’ (n = 3/6); however this was least preferred by the remaining genetics professionals (n = 3/6). Many oncologists most preferred ‘genetic variant’ (n = 11/29) and least preferred ‘faulty gene’ (n = 19/29). Participants across all groups perceived ‘faulty gene’ as having negative connotations, potentially placing blame/guilt on parents/children. Health professionals described challenges selecting a term that was scientifically accurate, easily understood and not distressing to families. Lack of consensus highlights the need to be guided by families’ preferred terminology, while providing accurate explanations regarding implications of genetic findings
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