505 research outputs found
Compressive Inverse Scattering II. SISO Measurements with Born scatterers
Inverse scattering methods capable of compressive imaging are proposed and
analyzed. The methods employ randomly and repeatedly (multiple-shot) the
single-input-single-output (SISO) measurements in which the probe frequencies,
the incident and the sampling directions are related in a precise way and are
capable of recovering exactly scatterers of sufficiently low sparsity.
For point targets, various sampling techniques are proposed to transform the
scattering matrix into the random Fourier matrix. The results for point targets
are then extended to the case of localized extended targets by interpolating
from grid points. In particular, an explicit error bound is derived for the
piece-wise constant interpolation which is shown to be a practical way of
discretizing localized extended targets and enabling the compressed sensing
techniques.
For distributed extended targets, the Littlewood-Paley basis is used in
analysis. A specially designed sampling scheme then transforms the scattering
matrix into a block-diagonal matrix with each block being the random Fourier
matrix corresponding to one of the multiple dyadic scales of the extended
target. In other words by the Littlewood-Paley basis and the proposed sampling
scheme the different dyadic scales of the target are decoupled and therefore
can be reconstructed scale-by-scale by the proposed method. Moreover, with
probes of any single frequency \om the coefficients in the Littlewood-Paley
expansion for scales up to \om/(2\pi) can be exactly recovered.Comment: Add a new section (Section 3) on localized extended target
OEMC D2.5 Feasibility and Impact Assessment
This deliverable of the Open-Earth-Monitor project presents a feasibility analysis of the stakeholder needs for the project's 32 use-cases, in addition to an impact assessment and methods for measuring use-case impact
POLRMT regulates the switch between replication primer formation and gene expression of mammalian mtDNA
Mitochondria are vital in providing cellular energy via their oxidative phosphorylation system, which requires the coordinated expression of genes encoded by both the nuclear and mitochondrial genomes (mtDNA). Transcription of the circular mammalian mtDNA depends on a single mitochondrial RNA polymerase (POLRMT). Although the transcription initiation process is well understood, it is debated whether POLRMT also serves as the primase for the initiation of mtDNA replication. In the nucleus, the RNA polymerases needed for gene expression have no such role. Conditional knockout of Polrmt in the heart results in severe mitochondrial dysfunction causing dilated cardiomyopathy in young mice. We further studied the molecular consequences of different expression levels of POLRMT and found that POLRMT is essential for primer synthesis to initiate mtDNA replication in vivo. Furthermore, transcription initiation for primer formation has priority over gene expression. Surprisingly, mitochondrial transcription factor A (TFAM) exists in an mtDNA-free pool in the Polrmt knockout mice. TFAM levels remain unchanged despite strong mtDNA depletion, and TFAM is thus protected from degradation of the AAA(+) Lon protease in the absence of POLRMT. Last, we report that mitochondrial transcription elongation factor may compensate for a partial depletion of POLRMT in heterozygous Polrmt knockout mice, indicating a direct regulatory role of this factor in transcription. In conclusion, we present in vivo evidence that POLRMT has a key regulatory role in the replication of mammalian mtDNA and is part of a transcriptional mechanism that provides a switch between primer formation for mtDNA replication and mitochondrial gene expression
OEMC D2.1 Report "Stakeholder Committee and Open- Earth-Monitor Design" workshop
This deliverable of the Open-Earth-Monitor project describes the approach taken to compile and categorize the project's stakeholders, and provides recommendations for the future stakeholder interactions based on the results of a survey from the OEMC design workshop, which took place during the project's kick-off meeting in July, 2022
Epidermolysa bullosa in Danish Hereford calves is caused by a deletion in LAMC2 gene
BACKGROUND
Heritable forms of epidermolysis bullosa (EB) constitute a heterogeneous group of skin disorders of genetic aetiology that are characterised by skin and mucous membrane blistering and ulceration in response to even minor trauma. Here we report the occurrence of EB in three Danish Hereford cattle from one herd.
RESULTS
Two of the animals were necropsied and showed oral mucosal blistering, skin ulcerations and partly loss of horn on the claws. Lesions were histologically characterized by subepidermal blisters and ulcers. Analysis of the family tree indicated that inbreeding and the transmission of a single recessive mutation from a common ancestor could be causative. We performed whole genome sequencing of one affected calf and searched all coding DNA variants. Thereby, we detected a homozygous 2.4 kb deletion encompassing the first exon of the LAMC2 gene, encoding for laminin gamma 2 protein. This loss of function mutation completely removes the start codon of this gene and is therefore predicted to be completely disruptive. The deletion co-segregates with the EB phenotype in the family and absent in normal cattle of various breeds. Verifying the homozygous private variants present in candidate genes allowed us to quickly identify the causative mutation and contribute to the final diagnosis of junctional EB in Hereford cattle.
CONCLUSIONS
Our investigation confirms the known role of laminin gamma 2 in EB aetiology and shows the importance of whole genome sequencing in the analysis of rare diseases in livestock
What is the effectiveness of surgical and non-surgical therapies in the treatment of ischemic priapism in patients with sickle cell disease? A systematic review by the EAU Sexual and Reproductive Health Panel
The authors acknowledge the participants for their cooperation Conflict of Interest: None of the authors declare any interest. Formatting of funding sources: This research did not receive any specific grant from funding agencies in the public, commercial, or not-for-profit sectors.Peer reviewedPostprin
Surgical and minimally invasive treatment of ischaemic and non-ischaemic priapism : A systematic review by the EAU Sexual and Reproductive Health Guidelines panel
Peer reviewedPostprin
Glypican-5 stimulates rhabdomyosarcoma cell proliferation by activating Hedgehog signaling
Binding between the Hedgehog ligand and its receptor Patched 1 is stabilized by Glypican-5
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