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Nejvíce citované: 20479471

4 citací v PubMed Filtry

Nejvíce citovaný článek - PubMed ID 20479471

Záznam nenalezen v Medvik. Navštivte PubMed 20479471

Článek

Autologous T-Cell-Free Antigen Presentation System Unveils hCMV-Specific NK Cell Response

Ustiuzhanina, Maria O
Autor Ustiuzhanina, Maria O ORCID Shemyakin and Ovchinnikov Institute of Bioorganic Chemistry, Russian Academy of Sciences, 117997 Moscow, Russia
Streltsova, Maria A
Autor Streltsova, Maria A ORCID Shemyakin and Ovchinnikov Institute of Bioorganic Chemistry, Russian Academy of Sciences, 117997 Moscow, Russia
Timofeev, Nikita D
Autor Timofeev, Nikita D Shemyakin and Ovchinnikov Institute of Bioorganic Chemistry, Russian Academy of Sciences, 117997 Moscow, Russia
Kryukov, Maxim A
Autor Kryukov, Maxim A ORCID Ecole Polytechnique Federale de Lausanne, 1015 Lausanne, Switzerland
Chudakov, Dmitriy M
Autor Chudakov, Dmitriy M Shemyakin and Ovchinnikov Institute of Bioorganic Chemistry, Russian Academy of Sciences, 117997 Moscow, Russia Institute of Translational Medicine, Pirogov Russian National Research Medical University, 117997 Moscow, Russia Central European Institute of Technology, Masaryk University, 60200 Brno, Czech Republic Abu Dhabi Stem Cells Center, Abu Dhabi, United Arab Emirates
Kovalenko, Elena I
Autor Kovalenko, Elena I Shemyakin and Ovchinnikov Institute of Bioorganic Chemistry, Russian Academy of Sciences, 117997 Moscow, Russia

Cells. 2024 Mar 17 ; 13 (6) : . [epub] 20240317

ISSN 2073-4409
Zdroj

NK cells play a decisive role in controlling hCMV infection by combining innate and adaptive-like immune reactions. The hCMV-derived VMAPRTLFL (LFL) peptide is a potent activator of NKG2C+ NK cells. Proposed here is an autologous system of LFL stimulation without T lymphocytes and exogenous cytokines that allows us to evaluate NK-cell hCMV-specific responses in more native settings. In this model, we evaluated LFL-induced IFNγ production, focusing on signaling pathways and the degranulation and proliferation of NK cells orchestrated by microenvironment cytokine production and analyzed the transcriptome of expanded NK cells. NK cells of individuals having high anti-hCMV-IgG levels, in contrast to NK cells of hCMV-seronegative and low-positive donors, displayed increased IFNγ production and degranulation and activation levels and enhanced proliferation upon LFL stimulation. Cytokine profiles of these LFL-stimulated cultures demonstrated a proinflammatory shift. LFL-induced NK-cell IFNγ production was dependent on the PI3K and Ras/Raf/Mek signaling pathways, independently of cytokines. In hCMV-seropositive individuals, this model allowed obtaining NK-cell antigen-specific populations proliferating in response to LFL. The transcriptomic profile of these expanded NK cells showed increased adaptive gene expression and metabolic activation. The results complement the existing knowledge about hCMV-specific NK-cell response. This model may be further exploited for the identification and characterization of antigen-specific NK cells.

Klíčová slova
ERK1/2, HLA-E, IFNγ, NKG2C, RNAseq, cytokines, hCMV, memory NK cells,
MeSH
buňky NK MeSH
cytokiny metabolismus MeSH
cytomegalovirové infekce * MeSH
Cytomegalovirus MeSH
lidé MeSH
prezentace antigenu * MeSH
Check Tag
lidé MeSH
Publikační typ
časopisecké články MeSH
práce podpořená grantem MeSH
Názvy látek
cytokiny MeSH

Článek

Human Cytomegalovirus Genomes Sequenced Directly From Clinical Material: Variation, Multiple-Strain Infection, Recombination, and Gene Loss

The Journal of infectious diseases. 2019 Jul 31 ; 220 (5) : 781-791.

J Infect Dis
ISSN 1537-6613 | 0022-1899
Zdroj

The genomic characteristics of human cytomegalovirus (HCMV) strains sequenced directly from clinical pathology samples were investigated, focusing on variation, multiple-strain infection, recombination, and gene loss. A total of 207 datasets generated in this and previous studies using target enrichment and high-throughput sequencing were analyzed, in the process enabling the determination of genome sequences for 91 strains. Key findings were that (i) it is important to monitor the quality of sequencing libraries in investigating variation; (ii) many recombinant strains have been transmitted during HCMV evolution, and some have apparently survived for thousands of years without further recombination; (iii) mutants with nonfunctional genes (pseudogenes) have been circulating and recombining for long periods and can cause congenital infection and resulting clinical sequelae; and (iv) intrahost variation in single-strain infections is much less than that in multiple-strain infections. Future population-based studies are likely to continue illuminating the evolution, epidemiology, and pathogenesis of HCMV.

Klíčová slova
gene loss, genome sequence, genotype, human cytomegalovirus, multiple-strain infection, mutation, recombination, target enrichment, variation,
MeSH
cytomegalovirové infekce virologie MeSH
Cytomegalovirus genetika MeSH
databáze nukleových kyselin MeSH
datové soubory jako téma MeSH
DNA virů genetika MeSH
genetická variace MeSH
genom virový * genetika MeSH
genotyp MeSH
lidé MeSH
molekulární evoluce MeSH
mutace MeSH
rekombinace genetická * MeSH
sekvence nukleotidů * MeSH
sekvenční analýza DNA MeSH
sekvenování celého genomu MeSH
virové geny MeSH
vysoce účinné nukleotidové sekvenování MeSH
Check Tag
lidé MeSH
Publikační typ
časopisecké články MeSH
práce podpořená grantem MeSH
Názvy látek
DNA virů MeSH

Článek

High-throughput analysis of human cytomegalovirus genome diversity highlights the widespread occurrence of gene-disrupting mutations and pervasive recombination

Journal of virology. 2015 Aug 01 ; 89 (15) : 7673-7695. [epub] 20150513

J Virol
ISSN 1098-5514 | 0022-538X
Zdroj

UNLABELLED: Human cytomegalovirus is a widespread pathogen of major medical importance. It causes significant morbidity and mortality in the immunocompromised and congenital infections can result in severe disabilities or stillbirth. Development of a vaccine is prioritized, but no candidate is close to release. Although correlations of viral genetic variability with pathogenicity are suspected, knowledge about strain diversity of the 235kb genome is still limited. In this study, 96 full-length human cytomegalovirus genomes from clinical isolates were characterized, quadrupling the available information for full-genome analysis. These data provide the first high-resolution map of human cytomegalovirus interhost diversity and evolution. We show that cytomegalovirus is significantly more divergent than all other human herpesviruses and highlight hotspots of diversity in the genome. Importantly, 75% of strains are not genetically intact, but contain disruptive mutations in a diverse set of 26 genes, including immunomodulative genes UL40 and UL111A. These mutants are independent from culture passaging artifacts and circulate in natural populations. Pervasive recombination, which is linked to the widespread occurrence of multiple infections, was found throughout the genome. Recombination density was significantly higher than in other human herpesviruses and correlated with strain diversity. While the overall effects of strong purifying selection on virus evolution are apparent, evidence of diversifying selection was found in several genes encoding proteins that interact with the host immune system, including UL18, UL40, UL142 and UL147. These residues may present phylogenetic signatures of past and ongoing virus-host interactions. IMPORTANCE: Human cytomegalovirus has the largest genome of all viruses that infect humans. Currently, there is a great interest in establishing associations between genetic variants and strain pathogenicity of this herpesvirus. Since the number of publicly available full-genome sequences is limited, knowledge about strain diversity is highly fragmented and biased towards a small set of loci. Combined with our previous work, we have now contributed 101 complete genome sequences. We have used these data to conduct the first high-resolution analysis of interhost genome diversity, providing an unbiased and comprehensive overview of cytomegalovirus variability. These data are of major value to the development of novel antivirals and a vaccine and to identify potential targets for genotype-phenotype experiments. Furthermore, they have enabled a thorough study of the evolutionary processes that have shaped cytomegalovirus diversity.

Publikační typ
časopisecké články MeSH

Článek

HCMV pUL135 remodels the actin cytoskeleton to impair immune recognition of infected cells

Cell host & microbe. 2014 Aug 13 ; 16 (2) : 201-214.

Cell Host Microbe
ISSN 1934-6069 | 1931-3128
Zdroj

Immune evasion genes help human cytomegalovirus (HCMV) establish lifelong persistence. Without immune pressure, laboratory-adapted HCMV strains have undergone genetic alterations. Among these, the deletion of the UL/b' domain is associated with loss of virulence. In a screen of UL/b', we identified pUL135 as a protein responsible for the characteristic cytopathic effect of clinical HCMV strains that also protected from natural killer (NK) and T cell attack. pUL135 interacted directly with abl interactor 1 (ABI1) and ABI2 to recruit the WAVE2 regulatory complex to the plasma membrane, remodel the actin cytoskeleton and dramatically reduce the efficiency of immune synapse (IS) formation. An intimate association between F-actin filaments in target cells and the IS was dispelled by pUL135 expression. Thus, F-actin in target cells plays a critical role in synaptogenesis, and this can be exploited by pathogens to protect against cytotoxic immune effector cells. An independent interaction between pUL135 and talin disrupted cell contacts with the extracellular matrix.

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