216 research outputs found
Geniculo-Cortical Projection Diversity Revealed within the Mouse Visual Thalamus
This is the final version of the article. It was first available from PLOS via http://dx.doi.org/10.1371/journal.pone.0144846All dLGN cell co-ordinates, V1 injection sites, dLGN boundary coordinates, experimental protocols and analysis scripts are available for download from figshare at https://figshare.com/s/36c6d937b1844eec80a1.The mouse dorsal lateral geniculate nucleus (dLGN) is an intermediary between retina and primary visual cortex (V1). Recent investigations are beginning to reveal regional complexity in mouse dLGN. Using local injections of retrograde tracers into V1 of adult and neonatal mice, we examined the developing organisation of geniculate projection columns: the population of dLGN-V1 projection neurons that converge in cortex. Serial sectioning of the dLGN enabled the distribution of labelled projection neurons to be reconstructed and collated within a common standardised space. This enabled us to determine: the organisation of cells within the dLGN-V1 projection columns; their internal organisation (topology); and their order relative to V1 (topography). Here, we report parameters of projection columns that are highly variable in young animals and refined in the adult, exhibiting profiles consistent with shell and core zones of the dLGN. Additionally, such profiles are disrupted in adult animals with reduced correlated spontaneous activity during development. Assessing the variability between groups with partial least squares regression suggests that 4?6 cryptic lamina may exist along the length of the projection column. Our findings further spotlight the diversity of the mouse dLGN?an increasingly important model system for understanding the pre-cortical organisation and processing of visual information. Furthermore, our approach of using standardised spaces and pooling information across many animals will enhance future functional studies of the dLGN.Funding was provided by a Wellcome Trust grant jointly awarded to IDT and SJE (083205, www.wellcome.ac.uk), and by MRC PhD Studentships awarded to MNL and ACH (http://www.mrc.ac.uk/)
Relative Impacts of Adult Movement, Larval Dispersal and Harvester Movement on the Effectiveness of Reserve Networks
Movement of individuals is a critical factor determining the effectiveness of
reserve networks. Marine reserves have historically been used for the management
of species that are sedentary as adults, and, therefore, larval dispersal has
been a major focus of marine-reserve research. The push to use marine reserves
for managing pelagic and demersal species poses significant questions regarding
their utility for highly-mobile species. Here, a simple conceptual
metapopulation model is developed to provide a rigorous comparison of the
functioning of reserve networks for populations with different admixtures of
larval dispersal and adult movement in a home range. We find that adult movement
produces significantly lower persistence than larval dispersal, all other
factors being equal. Furthermore, redistribution of harvest effort previously in
reserves to remaining fished areas (‘fishery squeeze’) and fishing
along reserve borders (‘fishing-the-line’) considerably reduce
persistence and harvests for populations mobile as adults, while they only
marginally changes results for populations with dispersing larvae. Our results
also indicate that adult home-range movement and larval dispersal are not simply
additive processes, but rather that populations possessing both modes of
movement have lower persistence than equivalent populations having the same
amount of ‘total movement’ (sum of larval and adult movement spatial
scales) in either larval dispersal or adult movement alone
Cytoskeletal control of B cell responses to antigens.
The actin cytoskeleton is essential for cell mechanics and has increasingly been implicated in the regulation of cell signalling. In B cells, the actin cytoskeleton is extensively coupled to B cell receptor (BCR) signalling pathways, and defects of the actin cytoskeleton can either promote or suppress B cell activation. Recent insights from studies using single-cell imaging and biophysical techniques suggest that actin orchestrates BCR signalling at the plasma membrane through effects on protein diffusion and that it regulates antigen discrimination through the biomechanics of immune synapses. These mechanical functions also have a role in the adaptation of B cell subsets to specialized tasks during antibody responses
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