1,706 results match your criteria: "Institute of Molecular Biology and Genetics.[Affiliation]"

Defective N-glycosylation in tumor-infiltrating CD8 T cells impairs IFN-γ-mediated effector function.

Immunol Cell Biol

August 2023

School of Biological Sciences and Institute of Molecular Biology and Genetics, Seoul National University, Seoul, Republic of Korea.

Article Synopsis
  • The study examines how N-glycosylation affects T cell function, specifically focusing on exhausted CD8 T cells in a mouse model of colon cancer.
  • Researchers discovered that exhausted T cells reduce levels of the oligosaccharyltransferase complex critical for N-glycan transfer, leading to a decline in their antitumor activity.
  • By restoring this complex, they were able to enhance IFN-γ production and reduce CD8 T cell exhaustion, suggesting that modifying glycosylation could be a potential strategy for cancer immunotherapy.
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Therapeutic Effectiveness of Interferon-α2b against COVID-19 with Community-Acquired Pneumonia: The Ukrainian Experience.

Int J Mol Sci

April 2023

Biofilm Study Group, Department of Cell Regulatory Mechanisms, Institute of Molecular Biology and Genetics, National Academy of Sciences of Ukraine, 150 Zabolotnoho Str., 03680 Kyiv, Ukraine.

Despite several targeted antiviral drugs against SARS-CoV-2 currently being available, the application of type I interferons (IFNs) still deserves attention as an alternative antiviral strategy. This study aimed to assess the therapeutic effectiveness of IFN-α in hospitalized patients with COVID-19-associated pneumonia. The prospective cohort study included 130 adult patients with coronavirus disease (COVID-19).

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Coenzyme A (CoA) is an important cellular metabolite that is critical for metabolic processes and the regulation of gene expression. Recent discovery of the antioxidant function of CoA has highlighted its protective role that leads to the formation of a mixed disulfide bond with protein cysteines, which is termed protein CoAlation. To date, more than 2000 CoAlated bacterial and mammalian proteins have been identified in cellular responses to oxidative stress, with the majority being involved in metabolic pathways (60%).

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A few notes on science in Ukraine.

BBA Adv

April 2023

Institute of Molecular Biology and Genetics, Kyiv, Acad. Zabolotnogo Str. 150, 03143 Ukraine.

As a person who has had a long scientific career in Ukraine, both before and after its re-acquisition of independence thirty years ago, I would like to share my observations with the readership of this Special Issue. By no means are these observations meant to provide a systematic presentation, which requires a different format. Rather, they are highly personal notes, providing snippets of the past and present and a discussion of the future of Ukrainian science.

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Structural insights into ubiquitin chain cleavage by ovarian tumor deubiquitinases.

Life Sci Alliance

July 2023

Department of Systems Biology, College of Life Science and Biotechnology, Yonsei University, Seoul, Republic of Korea

Article Synopsis
  • Ubiquitin is a protein found in eukaryotes, but some bacteria and viruses have evolved proteins that disrupt the host's ubiquitin system, such as the Lot DUBs from a gram-negative bacterium.
  • The research outlines the unique structure of Lot DUBs, highlighting an extended helical lobe that distinguishes them from other OTU-DUBs and provides a specific site for binding ubiquitin.
  • Additionally, the study reveals that different LotA OTU domains work together to selectively cut longer K48-linked polyubiquitin chains and that LotA is also capable of cleaving K6-linked chains, showcasing their innovative mechanisms.
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The eEF1 family of mammalian translation elongation factors is comprised of the two variants of eEF1A (eEF1A1 and eEF1A2), and the eEF1B complex. The latter consists of eEF1Bα, eEF1Bβ, and eEF1Bγ subunits. The two eEF1A variants have similar translation activity but may differ with respect to their secondary, "moonlighting" functions.

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The structure of DNA fragments: Quantum-chemical modelling.

BBA Adv

February 2023

Department of Chemistry, Mellon College of Science, Carnegie Mellon University, Pittsburgh, Pennsylvania 15213, United States.

In this review, we analyze and systematize our computational studies of the nucleic acid duplex formations and thermodynamic stability under the different factors of investigation. The proposed structural models of mini-helix contains N nucleobase pairs (N = 3-5); QM structural data suggest that the helical conformations of mini-helix adopt geometrical parameters comparable to those of natural A- and B-DNA forms under specific conditions as micro hydration and charge compensation. The gas-phase models adopt non regular conformations between the helical form and a ladder form.

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Rationally designed molecularly imprinted polymer membranes as antibody and enzyme mimics in analytical biotechnology.

BBA Adv

December 2022

University of Leicester, Department of Chemistry, Leicester, University Road, Leicester, LE1 7RH, United Kingdom.

The paper is a self-review of works on development of new approaches to formation of mimics of receptor and catalytic sites of biological macromolecules in the structure of highly cross-linked polymer membranes and thin films. The general strategy for formation of the binding sites in molecularly imprinted polymer (MIP) membranes and thin films was described. A selective recognition of a number of food toxins, endocrine disruptors and metabolites is based on the results of computational modeling data for the prediction and optimization of their structure.

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Coenzyme A (CoA) is an essential cofactor in all living cells which plays critical role in cellular metabolism, the regulation of gene expression and the biosynthesis of major cellular constituents. Recently, CoA was found to function as a major antioxidant in both prokaryotic and eukaryotic cells. This unconventional function of CoA is mediated by a novel post-translational modification, termed protein CoAlation.

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Although recent advances in deep learning approaches for protein engineering have enabled quick prediction of hot spot residues improving protein solubility, the predictions do not always correspond to an actual increase in solubility under experimental conditions. Therefore, developing methods that rapidly confirm the linkage between computational predictions and empirical results is essential to the success of improving protein solubility of target proteins. Here, we present a simple hybrid approach to computationally predict hot spots possibly improving protein solubility by sequence-based analysis and empirically explore valuable mutants using split GFP as a reporter system.

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Motivation: Computational analysis of large-scale metagenomics sequencing datasets have proven to be both incredibly valuable for extracting isolate-level taxonomic, and functional insights from complex microbial communities. However, due to an ever-expanding ecosystem of metagenomics-specific methods and file-formats, designing studies which implement seamless and scalable end-to-end workflows, and exploring the massive amounts of output data have become studies unto themselves. One-click bioinformatics pipelines have helped to organize these tools into targeted workflows, but they suffer from general compatibility and maintainability issues.

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Article Synopsis
  • Parkinson's disease (PD) is a progressive neurodegenerative disorder, and understanding how different cell types contribute to its mechanisms is still a challenge.
  • Researchers analyzed over 113,000 nuclei from the substantia nigra in both healthy individuals and PD patients, revealing important changes in gene regulation specific to different cell types.
  • The study identified dysregulated regulatory elements and 656 target genes connected to PD, emphasizing unique expression patterns in cells like dopaminergic neurons and glial cells, which are crucial for understanding PD's development.
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Innate Immunity System in Patients With Cardiovascular and Kidney Disease.

Circ Res

April 2023

Division of Nephrology and Transplantation, Grande Ospedale Metropolitano, Reggio Calabria, Italy and National Research Council (CNR), Clinical Epidemiology of Hypertension and Renal Diseases Unit of the Institute of Clinical Physiology, Reggio Calabria, Italy (F.M.).

With a global burden of 844 million, chronic kidney disease (CKD) is now considered a public health priority. Cardiovascular risk is pervasive in this population, and low-grade systemic inflammation is an established driver of adverse cardiovascular outcomes in these patients. Accelerated cellular senescence, gut microbiota-dependent immune activation, posttranslational lipoprotein modifications, neuroimmune interactions, osmotic and nonosmotic sodium accumulation, acute kidney injury, and precipitation of crystals in the kidney and the vascular system all concur in determining the unique severity of inflammation in CKD.

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A large body of clinical and experimental evidence indicates that colorectal cancer is one of the most common multifactorial diseases. Although some useful prognostic biomarkers for clinical therapy have already been identified, it is still difficult to characterize a therapeutic signature that is able to define the most appropriate treatment. Gene expression levels of the epigenetic regulator histone deacetylase 2 () are deregulated in colorectal cancer, and this deregulation is tightly associated with immune dysfunction.

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Combination of radiation therapy (RT) with immune checkpoint blockade can enhance systemic anti-tumor T cell responses. Here, using two mouse tumor models, we demonstrate that adding long-acting CD122-directed IL-2 complexes (IL-2c) to RT/anti-PD1 further increases tumor-specific CD8 T cell numbers. The highest increase (>50-fold) is found in the blood circulation.

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The present study aimed to investigate the dynamic changes in peripheral blood leucocyte subpopulations, cytokine and miRNA levels, and changes in computed tomography (CT) scores in patients with severe coronavirus disease 2019 (COVID-19) (n=14) and age-matched non-COVID-19 volunteers (n=17), which were included as a reference control group. All data were collected on the day of patient admission (day 0) and on the 7th, 14th and 28th days of follow-up while CT of the lungs was performed on weeks 2, 8, 24 and 48. On day 0, lymphopenia and leucopenia were detected in most patients with COVID-19, as well as an increase in the percentage of banded neutrophils, B cells, and CD4 Treg cells, and a decrease in the content of PD-1 T cells, classical, plasmacytoid, and regulatory dendritic cells.

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Perinatal derivatives (PnD) are drawing growing interest among the scientific community as an unrestricted source of multipotent stem cells, secretome, and biological matrices. They are useful for the treatment of diseases that currently have limited or no effective therapeutic options, but they require the development of regenerative approaches. With this development, the question of regulation of donation, processing, and distribution has therefore become more important.

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Proper cellular proteostasis, essential for viability, requires a network of chaperones and cochaperones. ATP-dependent chaperonin TRiC/CCT partners with cochaperones prefoldin (PFD) and phosducin-like proteins (PhLPs) to facilitate the folding of essential eukaryotic proteins. Using cryoEM and biochemical analyses, we determine the ATP-driven cycle of TRiC-PFD-PhLP2A interaction.

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Coumarin-based fluorescent agents play an important role in the manifold fundamental scientific and technological areas and need to be carefully studied. In this research, linear photophysics, photochemistry, fast vibronic relaxations, and two-photon absorption (2PA) of the coumarin derivatives, methyl 4-[2-(7-methoxy-2-oxo-chromen-3-yl)thiazol-4-yl]butanoate () and methyl 4-[4-[2-(7-methoxy-2-oxo-chromen-3-yl)thiazol-4-yl]phenoxy]butanoate (), were comprehensively analyzed using stationary and time-resolved spectroscopic techniques, along with quantum-chemical calculations. The steady-state one-photon absorption, fluorescence emission, and excitation anisotropy spectra, as well as 3D fluorescence maps of 3-hetarylcoumarins and were obtained at room temperature in solvents of different polarities.

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Whole-brain mapping of effective connectivity by fMRI with cortex-wide patterned optogenetics.

Neuron

June 2023

Center for Neuroscience Imaging Research, Institute for Basic Science, Suwon, Republic of Korea; Department of Biomedical Engineering, Sungkyunkwan University, Suwon, Republic of Korea; Department of Intelligent Precision Healthcare Convergence, Sungkyunkwan University, Suwon, Republic of Korea. Electronic address:

Article Synopsis
  • fMRI combined with optogenetics allows researchers to map brain networks effectively by enabling precise neural manipulation in real-time.
  • By using a digital micromirror device, scientists can create customizable light patterns for stimulating specific brain areas in mice while conducting imaging.
  • This technique reveals that brain connectivity is influenced by the type of anesthetics used and opens new avenues for studying how brain functions change dynamically in individual animals.
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Aminoacyl-tRNA synthetases are crucial enzymes involved in protein synthesis and various cellular physiological reactions. Aside from their standard role in linking amino acids to the corresponding tRNAs, they also impact protein homeostasis by controlling the level of soluble amino acids within the cell. For instance, leucyl-tRNA synthetase (LARS1) acts as a leucine sensor for the mammalian target of rapamycin complex 1 (mTORC1), and may also function as a probable GTPase-activating protein (GAP) for the RagD subunit of the heteromeric activator of mTORC1.

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Benchmarking datasets for assembly-based variant calling using high-fidelity long reads.

BMC Genomics

March 2023

Institute of Molecular Biology and Genetics, Seoul National University, Seoul, 08826, Korea.

Background: Recent advances in long-read sequencing technologies have enabled accurate identification of all genetic variants in individuals or cells; this procedure is known as variant calling. However, benchmarking studies on variant calling using different long-read sequencing technologies are still lacking.

Results: We used two Caenorhabditis elegans strains to measure several variant calling metrics.

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Nicotinic acetylcholine receptors (nAChRs), initially characterized as ligand-gated ion channels mediating fast synaptic transmission, are now found in many non-excitable cells and mitochondria where they function in ion-independent manner and regulate vital cellular processes like apoptosis, proliferation, cytokine secretion. Here we show that the nAChRs of α7 subtype are present in the nuclei of liver cells and astrocytoma U373 cell line. As shown by lectin ELISA, the nuclear α7 nAChRs are mature glycoproteins that follow the standard rout of post-translational modifications in Golgi; however, their glycosylation profile is non-identical to that of mitochondrial nAChRs.

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Summary: Highly accurate protein structure predictors have generated hundreds of millions of protein structures; these pose a challenge in terms of storage and processing. Here, we present Foldcomp, a novel lossy structure compression algorithm, and indexing system to address this challenge. By using a combination of internal and Cartesian coordinates and a bi-directional NeRF-based strategy, Foldcomp improves the compression ratio by a factor of three compared to the next best method.

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Role of Molecular Singlet Oxygen in Photochemical Degradation of NTO: DFT Study.

J Phys Chem A

March 2023

Interdisciplinary Center for Nanotoxicity, Department of Chemistry, Physics & Atmospheric Sciences, Jackson State University, Jackson, Mississippi 39217, United States.

Article Synopsis
  • * A computational study explored how singlet oxygen, generated by sunlight in aquatic environments, can trigger the decomposition of NTO through a series of chemical reactions.
  • * The study revealed that NTO degradation begins with singlet oxygen reacting with a carbon bond, leading to the formation of nitrogen gas, carbon dioxide, and ammonia, with the anionic form of NTO being more reactive than its neutral counterpart.
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