Rokotteen POXvirus VACV ilmentää immunomodulatorisia proteiineja kuten BTB-BACK-Kelch-kaltaisia(BBK) proteiineja. Muita POX viruksia ja niiden koodaamia proteiineja

 1.2 LSDV  cluster 

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1

Genomic Analysis of Lumpy Skin Disease Virus from Western and Central Africa Suggests a Distinct Sub-Lineage Within the 1.2 LSDV Cluster.

Fadele J, Ogunsanya O, Adedokun O, Ayinla A, Pami M, Sijuwola A, Saibu F, Soumare H, Fanou U, Brown C, Faburay B, Happi C, Happi A. Pathogens. 2025 Sep 12;14(9):922. doi: 10.3390/pathogens14090922. PMID: 41011822 Free PMC article.

Phylogenetic evaluation revealed that LSDV strains from Nigeria and Cameroon cluster within the classical 1.2 lineage. Furthermore, the two sequences from this study cluster with the only publicly available sequence from West and Central Africa, supporting earlier findings of the presence of a West/Central African sub-lineage. Functional genomic analysis identified mutations in genes encoding ankyrin repeat Kelch-like proteins, and envelope proteins involved in immune evasion and viral virulence, raising concerns about vaccine effectiveness. Furthermore, the detection of LSDV in flesh flies (Sarcophaga spp.) underlines their potential role in virus transmission. These findings highlight the importance of genomic monitoring and targeted surveillance.toistoisia KELCH-proteiinien kaltaisia 

2

Genetic Evolutionary Analysis of Lumpy Skin Disease Virus Strain Under Immune Pressure Exerted by Heterologous Goat Poxvirus Vaccines.

Chang W, Fang J, Zhai T, Han S, Fan W, Lei C, Wang L, Qi X, Xue Q, Wang J. Transbound Emerg Dis. 2025 Feb 23;2025:2883245. doi: 10.1155/tbed/2883245. eCollection 2025. PMID: 40302761 Free PMC article.

Recently, LSD has occurred frequently in Asia. The attenuated goat poxvirus (GTPV) vaccine is widely used to prevent LSD in cattle in China; however, sporadic cases of LSD still occur in immunized cattle. ...There are several open reading frames (ORFs) differences between …

3

Genomic characterization of Lumpy Skin Disease virus (LSDV) from India: Circulation of Kenyan-like LSDV strains with unique kelch-like proteins.

Kumar A, Venkatesan G, Kushwaha A, Poulinlu G, Saha T, Ramakrishnan MA, Dhar P, Kumar GS, Singh RK. Acta Trop. 2023 May;241:106838. doi: 10.1016/j.actatropica.2023.106838. Epub 2023 Feb 15. PMID: 36796571

Phylogenetic analysis based on complete genome sequence suggested that LSDV-WB/IND/19 is closely related to Kenyan LSDV strains with 10-12 variants with non-synonymous changes confined to LSD_019, LSD_049, LSD_089, LSD_094, LSD_096, LSD_140, and LSD_144 genes. In contrast to comp …

4

Emergence of a new lumpy skin disease virus variant in Kurgan Oblast, Russia, in 2018.

Aleksandr K, Pavel P, Olga B, Svetlana K, Vladimir R, Yana P, Alexander S. Arch Virol. 2020 Jun;165(6):1343-1356. doi: 10.1007/s00705-020-04607-5. Epub 2020 Apr 11. PMID: 32279139

Due to these incongruent phylogenetic patterns, the sequences of three additional loci ORF19 (Kelch-like protein), ORF52 (putative transcriptional elongation factor), and ORF87 (mutT motif protein) were investigated. ...

5

Kelch-like proteins: Physiological functions and relationships with diseases.

Shi X, Xiang S, Cao J, Zhu H, Yang B, He Q, Ying M. Pharmacol Res. 2019 Oct;148:104404. doi: 10.1016/j.phrs.2019.104404. Epub 2019 Aug 20. PMID: 31442578 Review.

Kelch-like gene family members (KLHLs) encode proteins with a bric-a-brac, tramtrack, broad complex (BTB)/poxvirus and zinc finger (POZ) domain, a BACK domain, and six Kelch motifs, which frequently interact with Cullin3 to form E3 ligase complexes tha …

6

Extended sequencing of vaccine and wild-type capripoxvirus isolates provides insights into genes modulating virulence and host range.

Biswas S, Noyce RS, Babiuk LA, Lung O, Bulach DM, Bowden TR, Boyle DB, Babiuk S, Evans DH. Transbound Emerg Dis. 2020 Jan;67(1):80-97. doi: 10.1111/tbed.13322. Epub 2019 Aug 30. PMID: 31379093

The genus Capripoxvirus in the subfamily Chordopoxvirinae, family Poxviridae, comprises sheeppox virus (SPPV), goatpox virus (GTPV) and lumpy skin disease virus (LSDV), which cause the eponymous diseases across parts of Africa, the Middle East and Asia. ...In particular, s …

7

Vaccinia Virus BBK E3 Ligase Adaptor A55 Targets Importin-Dependent NF-κB Activation and Inhibits CD8⁺ T-Cell Memory.

Pallett MA, Ren H, Zhang RY, Scutts SR, Gonzalez L, Zhu Z, Maluquer de Motes C, Smith GL. J Virol. 2019 May 1;93(10):e00051-19. doi: 10.1128/JVI.00051-19. Print 2019 May 15. PMID: 30814284 Free PMC article.

Viral infection of cells is sensed by pathogen recognition receptors that trigger an antiviral innate immune response, and consequently viruses have evolved countermeasures. Vaccinia virus (VACV) evades the host immune response by expressing scores of immunomodulatory proteins. One family of VACV proteins are the BTB-BACK (broad-complex, tram-trac, and bric-a-brac [BTB] and C-terminal Kelch [BACK]) domain-containing, Kelch-like (BBK) family of predicted cullin-3 E3 ligase adaptors: A55, C2, and F3. Previous studies demonstrated that gene A55R encodes a protein that is nonessential for VACV replication yet affects viral virulence in vivo Here, we report that A55 is an NF-κB inhibitor acting downstream of IκBα degradation, preventing gene transcription and cytokine secretion in response to cytokine stimulation. A55 targets the host importin α1 (KPNA2), acting to reduce p65 binding and its nuclear translocation. Interestingly, while A55 was confirmed to coprecipitate with cullin-3 in a BTB-dependent manner, its NF-κB inhibitory activity mapped to the Kelch domain, which alone is sufficient to coprecipitate with KPNA2 and inhibit NF-κB signaling. Intradermal infection of mice with a virus lacking A55R (vΔA55) increased VACV-specific CD8⁺ T-cell proliferation, activation, and cytotoxicity in comparison to levels of the wild-type (WT) virus. Furthermore, immunization with vΔA55 induced increased protection to intranasal VACV challenge compared to the level with control viruses. In summary, this report describes the first target of a poxvirus-encoded BBK protein and a novel mechanism for DNA virus immune evasion, resulting in increased CD8⁺ T-cell memory and a more immunogenic vaccine.

IMPORTANCE NF-κB is a critical transcription factor in the innate immune response to infection and in shaping adaptive immunity. The identification of host and virus proteins that modulate the induction of immunological memory is important for improving virus-based vaccine design and efficacy. In viruses, the expression of BTB-BACK Kelch-like (BBK) proteins is restricted to poxviruses and conserved within them, indicating the importance of these proteins for these medically important viruses. Using vaccinia virus (VACV), the smallpox vaccine, we report that the VACV BBK protein A55 dysregulates NF-κB signaling by disrupting the p65-importin interaction, thus preventing NF-κB translocation and blocking NF-κB-dependent gene transcription. Infection with VACV lacking A55 induces increased VACV-specific CD8⁺ T-cell memory and better protection against VACV challenge. Studying viral immunomodulators therefore expands not only our understanding of viral pathogenesis and immune evasion strategies but also of the immune signaling cascades controlling antiviral immunity and the development of immune memory.

Keywords: BTB-Kelch; E3 ligase; NF-κB; cullin-3; importins; protein A55; vaccinia virus.

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8

VARV B22R homologue as phylogenetic marker gene for Capripoxvirus classification and divergence time dating.

Mishra B, Mondal P, Patel CL, Zafir I, Gangwar R, Singh N, Sonowal J, Bisht D, Sahu AR, Baig M, Sajjanar B, Singh RK, Gandham RK. Virus Genes. 2019 Feb;55(1):51-59. doi: 10.1007/s11262-018-1613-9. Epub 2018 Nov 16. PMID: 30446925

…Sheeppox disease is associated with significant losses in sheep production world over. The sheep pox virus, the goatpox virus, and the lumpy skin disease virus cannot be distinguished by conventional serological tests. Identification of these pathogens needs molecular methods. In this study, seven genes viz. EEV maturation protein-F12L, Virion protein-D3R, RNA polymerase subunit-A5R, Virion core protein-A10L, EEV glycoprotein-A33R, VARV B22R homologue, and Kelch like protein-A55R that cover the start, middle, and end of the genome were selected. These genes were amplified from Roumanian-Fanar vaccine strain and Jaipur virulent strain, cloned, and sequenced. On analysis with the available database sequences, VARV B22R homologue was identified as a marker for phylogenetic reconstruction for classifying the sheeppox viruses of the ungulates. Further, divergence time dating with VARV B22R gene accurately predicted the sheeppox disease outbreak involving Jaipur virulent strain.

9

Isolation and genetic characterization of swinepox virus from pigs in India.

Riyesh T, Barua S, Kumar N, Jindal N, Bera BC, Narang G, Mahajan NK, Arora D, Anand T, Vaid RK, Yadav M, Chandel SS, Malik P, Tripathi BN, Singh RK. Comp Immunol Microbiol Infect Dis. 2016 Jun;46:60-5. doi: 10.1016/j.cimid.2016.04.001. Epub 2016 Apr 4. PMID: 27260812 Keywords: Ankyrin- repeat protein; Extracellular enveloped protein; Host-range genes; Kelch-like protein; Swinepox virus.

10

Klhl31 attenuates β-catenin dependent Wnt signaling and regulates embryo myogenesis.

Abou-Elhamd A, Alrefaei AF, Mok GF, Garcia-Morales C, Abu-Elmagd M, Wheeler GN, Münsterberg AE. Dev Biol. 2015 Jun 1;402(1):61-71. doi: 10.1016/j.ydbio.2015.02.024. Epub 2015 Mar 19. PMID: 25796573 Free article.

Klhl31 is a member of the Kelch-like family in vertebrates, which are characterized by an amino-terminal broad complex tram-track, bric-a-brac/poxvirus and zinc finger (BTB/POZ) domain, carboxy-terminal Kelch repeats and a central linker region (Back domain). … Klhl31 interferes with β-catenin dependent Wnt signaling. Klhl31 reduced the Wnt-mediated activation of a luciferase reporter in cultured cells. Furthermore, Klhl31 attenuated secondary axis formation in Xenopus embryos in response to Wnt1 or β-catenin. Klhl31 mis-expression in the developing neural tube affected its dorso-ventral patterning and led to reduced dermomyotome and myotome size. Co-transfection of a Wnt3a expression vector with Klhl31 in somites or in the neural tube rescued the phenotype and restored the size of dermomyotome and myotome. Thus, Klhl31 is a novel modulator of canonical Wnt signaling, important for vertebrate myogenesis. We propose that Klhl31 acts in the myotome to support cell cycle withdrawal and differentiation.