Biosynthesis of poly(ester amide)s in engineered Escherichia coli
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Escherichia Coli K1-colibactin meningitis induces microglial NLRP3/IL-18 exacerbating H3K4me3-synucleinopathy in human inflammatory gut-brain axis
Escherichia coli K1 (E. coli K1) meningitis early occurs in the gastrointestinal and causes severe damage to the central nervous system, including lifelong neurological complications in survivors. However, the cellular mechanism by which E. coli K1 may cause neuropathies is not well understood due to the lack of relevant human multi-organ models for studying multifaceted systemic inflammation across the gut-brain axis. Here, we reconstruct a multicellular model of the human gut-brain axis to identify the neuropathogenic mechanism driven by E. coli K1-colibactin meningitis. We observed that E. coli K1-genotoxic colibactin induced intestinal and peripheral interleukin 6, causing the blood-brain barrier injury and endothelial inflammation via the p38/p65 pathways. Serpin-E1 from the damaged cerebral endothelia induces reactive astrocytes to release IFN-γ, which reduces microglial phagocytosis of E. coli K1 and exacerbates detrimental neuroinflammation via NLRP3/IL-18 axis. Microglial IL-18 elevates neuronal reactive oxidative stress that worsens DNA double-strand breaks in E. coli K1-infected neurons, leading to H3K4 trimethylation and phosphorylation of alpha-synuclein. Our findings suggest therapeutic strategies for post-bacterial meningitis treatment to potentially prevent the initiation of synucleinopathy.
Unveiling mechanistic intricacies of Chlorella pyrenoidosa-mediated pathogen removal from sewage
Amidst the global sanitation challenges of water pollution, waterborne diseases, and the alarming presence of pathogens in disinfected water, microalgal technology has emerged as a viable alternative for wastewater treatment. Recently, the ability of microalgae to remove pathogens from wastewater has been highlighted. However, a critical knowledge gap exists regarding microalgae-mediated pathogen removal mechanisms. The present study uncovers the intricate mechanisms of Chlorella pyrenoidosa-mediated Escherichia coli removal from sewage. Microalgae-induced pH increase was identified as the most crucial mechanism, followed by photooxidation and attachment, mediated by the hydroxyl group. Longer photoperiods or ultraviolet irradiation produced high oxidative stress, promoting microalgal exopolysaccharides’ production and increasing pathogen entrapment. The knowledge of crucial removal mechanisms can be harnessed for the development of more efficient, innovative, and scalable microalgal systems. Such improved systems offer a sustainable solution to address water-related issues by improving wastewater treatment, increasing access to clean water, and reducing the transmission risk of waterborne diseases.
Maternal immune activation imprints translational dysregulation and differential MAP2 phosphorylation in descendant neural stem cells
Alterations induced by maternal immune activation (MIA) during gestation impact the subsequent neurodevelopment of progeny, a process that in humans, has been linked to the development of several neuropsychiatric conditions. To undertake a comprehensive examination of the molecular mechanisms governing MIA, we have devised an in vitro model based on neural stem cells (NSCs) sourced from fetuses carried by animals subjected to Poly I:C treatment. These neural progenitors demonstrate proliferative capacity and can be effectively differentiated into both neurons and glial cells. Transcriptomic, proteomic, and phosphoproteomic analyses conducted on these cellular models, in conjunction with counterparts from control treatments, revealed discernible shifts in the expression levels of a specific subset of proteins implicated in neuronal function. Furthermore, the phosphoproteomic data highlighted a discernible discrepancy in the basal phosphorylation of proteins between differentiated cells from both experimental groups, particularly within proteins associated with cytoskeletal architecture and synaptic functionality, notably those belonging to the MAP family. Observed alterations in MAP phosphorylation were found to potentially have functional consequences as they correlate with changes in neuronal plasticity and the establishment of neuronal synapses. Our data agrees with previous published observations and further underscore the importance of MAP2 phosphorylation state on its function and the impact that this protein has in neuronal structure and function.
Rapid and highly efficient recombination of crosslinking points in hydrogels generated via the template polymerization of dynamic covalent three-dimensional nanoparticle crosslinkers
Dynamic covalent bonds (DCBs) can be used as crosslinking points to induce self-healing and thermoplastic properties in hydrogels because the bonding and dissociation between molecules can be controlled by external stimuli. However, once DCBs dissociate, molecules diffuse inside the gel, delaying DCB reformation. In this study, a hydrogel was prepared via template polymerization using phenylboronic acid-coated nanoparticles to control the mobility of the molecules and the density of the DCB crosslinking points. Interestingly, the loss modulus, but not the storage modulus, of the hydrogel changed with temperature according to the formation/dissociation of boronic ester bonds. Furthermore, compared with conventional hydrogels, the hydrogels prepared here exhibited very rapid changes in physicochemical properties in response to changes in temperature because the high density of three-dimensional DCB crosslinking points limits the diffusion of molecules inside the gel. As a result, the prepared hydrogel showed rapid self-healing and thermoplastic properties as the temperature changed.
A historical perspective on the multifunctional outer membrane channel protein TolC in Escherichia coli
Since its discovery nearly 60 years ago, TolC has been associated with various cellular functions in Escherichia coli, including the efflux of environmental stressors and virulence factors. It also acts as a receptor for specific bacteriophages and the colicin E1 toxin. This review highlights key discoveries over the past six decades and emphasizes the remaining gaps in understanding how TolC contributes to physiological functions in E. coli.
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