356 research outputs found
Biomimetic engineered muscle with capacity for vascular integration and functional maturation in vivo.
Tissue-engineered skeletal muscle can serve as a physiological model of natural muscle and a potential therapeutic vehicle for rapid repair of severe muscle loss and injury. Here, we describe a platform for engineering and testing highly functional biomimetic muscle tissues with a resident satellite cell niche and capacity for robust myogenesis and self-regeneration in vitro. Using a mouse dorsal window implantation model and transduction with fluorescent intracellular calcium indicator, GCaMP3, we nondestructively monitored, in real time, vascular integration and the functional state of engineered muscle in vivo. During a 2-wk period, implanted engineered muscle exhibited a steady ingrowth of blood-perfused microvasculature along with an increase in amplitude of calcium transients and force of contraction. We also demonstrated superior structural organization, vascularization, and contractile function of fully differentiated vs. undifferentiated engineered muscle implants. The described in vitro and in vivo models of biomimetic engineered muscle represent enabling technology for novel studies of skeletal muscle function and regeneration
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T7 RNA polymerase-driven inducible cell lysis for DNA transfer from Escherichia coli to Bacillus subtilis
The majority of the good DNA editing techniques have been developed in Escherichia coli; however, Bacillus subtilis is better host for a plethora of synthetic biology and biotechnology applications. Reliable and efficient systems for the transfer of synthetic DNA between E. coli and B. subtilis are therefore of the highest importance. Using synthetic biology approaches, such as streamlined lambda Red recombineering and Gibson Isothermal Assembly, we integrated genetic circuits pT7L123, Repr-ts-1 and pLT7pol encoding the lysis genes of bacteriophages MS2, ΦX174 and lambda, the thermosensitive repressor and the T7 RNA polymerase into the E. coli chromosome. In this system, T7 RNA polymerase regulated by the thermosensitive repressor drives the expression of the phage lysis genes. We showed that T7 RNA polymerase significantly increases efficiency of cell lysis and transfer of the plasmid and bacterial artificial chromosome-encoded DNA from the lysed E. coli into B. subtilis. The T7 RNA polymerase-driven inducible cell lysis system is suitable for the efficient cell lysis and transfer of the DNA engineered in E. coli to other naturally competent hosts, such as B. subtilis.This work was supported by the UK Engineering and Physical Sciences Research Council (EPSRC), OpenPlant Fund and SynBio Fund
Show case project: camea camea wimtronic – using long-term experience to develop of a novel weighing digital sensor for further evolution of wim technology
CAMEA Weigh-In-Motion has been equipped at almost 900 traffic lanes so far, out of
which approximately 200 are used for a direct enforcement application. Based on this
experience, the system producer was able to identify the main needs the WIM technology
has in order to evolve further. These are: facing the problem of drivers who intentionally
avoid measurement or behavior documentation, minimizing the impact on the road surface
when installing the WIM site, extending the lifetime of the installed WIM sensors.
This article suggests the tools to address these needs: Preventing the driver’s maneuvers
by taking government/law measures, recognizing such maneuvers and validating the
results of the measurement using advanced SW and using sensors with small intrusion
into the road and a long lifetime. The company’s newly developed digital weighing sensor
WIMTRONIC has numerous innovative characteristics and features. Some of its main
advantages are embedded electronics, high accuracy, easy installation, and the possibility
to measure previously unobtainable parameters of the vehicle, wheels, axles, and the
road. All the while keeping the cost low to present an affordable solution for wide use of
WIM.Papers presented at the 40th International Southern African Transport Conference on 04 -08 July 202
Cluster-mining: An approach for determining core structures of metallic nanoparticles from atomic pair distribution function data
We present a novel approach for finding and evaluating structural models of
small metallic nanoparticles. Rather than fitting a single model with many
degrees of freedom, the approach algorithmically builds libraries of
nanoparticle clusters from multiple structural motifs, and individually fits
them to experimental PDFs. Each cluster-fit is highly constrained. The
approach, called cluster-mining, returns all candidate structure models that
are consistent with the data as measured by a goodness of fit. It is highly
automated, easy to use, and yields models that are more physically realistic
and result in better agreement to the data than models based on cubic
close-packed crystallographic cores, often reported in the literature for
metallic nanoparticles
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Combining Genes from Multiple Phages for Improved Cell Lysis and DNA Transfer from to
The ability to efficiently and reliably transfer genetic circuits between the key synthetic biology chassis, such as and , constitutes one of the major hurdles of the rational genome engineering. Using lambda Red recombineering we integrated the thermosensitive lambda repressor and the lysis genes of several bacteriophages into the chromosome. The lysis of the engineered autolytic cells is inducible by a simple temperature shift. We improved the lysis efficiency by introducing different combinations of lysis genes from bacteriophages lambda, ΦX174 and MS2 under the control of the thermosensitive lambda repressor into the chromosome. We tested the engineered autolytic cells by transferring plasmid and bacterial artificial chromosome (BAC)-borne genetic circuits from to . Our engineered system combines benefits of the two main synthetic biology chassis, and B. subtilis, and allows reliable and efficient transfer of DNA edited in into .This work was supported by grants from the UK Engineering and Physical Sciences Research Council (JWA), OpenPlant Fund (MJ) and SynBio Fund (MJ)
Lipid composition of liver in rats fed diets supplemented with egg yolks of modified composition
The aim of this study was to examine the effects of diets supplemented with egg yolks of modified composition on the fatty-acid composition and lipid content in rat’s liver. During four weeks of the experiment 64 Wistar rats were divided into four groups of 16 individuals each (eight individuals of both sexes) and fed a commercial feed mixture for rats (group C) or diet containing 70% commercial mixture for rats and 30% freshly cooked egg yolks from laying hens fed diets with 3% fish oil (group F), 3% palm olein (group P) or 3% lard (group L). Dietary supplementation with egg yolks significantly increased the hepatic cholesterol pool in rats, regardless of the type of fat in the diet of laying hens from which the eggs originated. The content of α-linolenic acid in the liver of male rats in group P was 4-6 times higher compared to males in the other groups. Liver lipids and their fatty-acid composition differ by both, sex and dietary modified egg yolk composition in rats
Genomic islands: tools of bacterial horizontal gene transfer and evolution
Bacterial genomes evolve through mutations, rearrangements or horizontal gene transfer. Besides the core genes encoding essential metabolic functions, bacterial genomes also harbour a number of accessory genes acquired by horizontal gene transfer that might be beneficial under certain environmental conditions. The horizontal gene transfer contributes to the diversification and adaptation of microorganisms, thus having an impact on the genome plasticity. A significant part of the horizontal gene transfer is or has been facilitated by genomic islands (GEIs). GEIs are discrete DNA segments, some of which are mobile and others which are not, or are no longer mobile, which differ among closely related strains. A number of GEIs are capable of integration into the chromosome of the host, excision, and transfer to a new host by transformation, conjugation or transduction. GEIs play a crucial role in the evolution of a broad spectrum of bacteria as they are involved in the dissemination of variable genes, including antibiotic resistance and virulence genes leading to generation of hospital ‘superbugs', as well as catabolic genes leading to formation of new metabolic pathways. Depending on the composition of gene modules, the same type of GEIs can promote survival of pathogenic as well as environmental bacteri
Exosomal release of L-plastin by breast cancer cells facilitates metastatic bone osteolysis
Bone metastasis from breast and prostate carcinomas is facilitated by activation of bone-resorbing osteoclasts. Using proteomics approaches, we have identified peroxiredoxin-4 (PRDX4) as a cancer-secreted mediator of osteoclastogenesis. We now report characterization of L-plastin in the conditioned media (CM) of MDA-MB-231 human breast cancer cells using immunoblotting and mass spectrometry. The osteoclastogenic potential of MDAMB-231 CM with siRNA-silenced L-plastin was significantly reduced. L-plastin was detected in cancer-derived exosomes, and inhibition of exosomal release significantly decreased the osteoclastogenic capacity of MDA-MB-231 CM. When added to osteoclast precursors primed with RANKL for 2 days, recombinant L-plastin induced calcium/NFATc1-mediated osteoclastogenesis to the levels similar to continuous treatment with RANKL. Using shRNA, we generated MDA-MB-231 cells lacking L-plastin, PRDX4, or both and injected these cell populations intratibially in CD-1 immunodeficient mice. Micro-CT and histomorphometric analysis demonstrated a complete loss of osteolysis when MDA-MB-231 cells lacking both L-plastin and PRDX4 were injected. A meta-analysis established an increase in L-plastin and PRDX4 mRNA expression in numerous human cancers, including breast and prostate carcinomas. This study demonstrates that secreted L-plastin and PRDX4 mediate osteoclast activation by human breast cancer cells
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