keyword
https://read.qxmd.com/read/38308843/structural-and-functional-insight-into-the-interaction-of-clostridioides-difficile-toxin-b-and-fzd-7
#21
JOURNAL ARTICLE
Julia Kinsolving, Julien Bous, Pawel Kozielewicz, Sara Košenina, Rawan Shekhani, Lukas Grätz, Geoffrey Masuyer, Yuankai Wang, Pål Stenmark, Min Dong, Gunnar Schulte
The G protein-coupled receptors of the Frizzled (FZD) family, in particular FZD1,2,7 , are receptors that are exploited by Clostridioides difficile toxin B (TcdB), the major virulence factor responsible for pathogenesis associated with Clostridioides difficile infection. We employ a live-cell assay examining the affinity between full-length FZDs and TcdB. Moreover, we present cryoelectron microscopy structures of TcdB alone and in complex with full-length FZD7 , which reveal that large structural rearrangements of the combined repetitive polypeptide domain are required for interaction with FZDs and other TcdB receptors, constituting a first step for receptor recognition...
February 1, 2024: Cell Reports
https://read.qxmd.com/read/38308564/the-mechanistic-basis-of-the-membrane-permeabilizing-activities-of-the-virulence-associated-protein-a-vapa-from-rhodococcus-equi
#22
JOURNAL ARTICLE
Christian Nehls, Marcel Schröder, Thomas Haubenthal, Albert Haas, Thomas Gutsmann
Pathogenic Rhodococcus equi release the virulence-associated protein A (VapA) within macrophage phagosomes. VapA permeabilizes phagosome and lysosome membranes and reduces acidification of both compartments. Using biophysical techniques, we found that VapA interacts with model membranes in four steps: (i) binding, change of mechanical properties, (ii) formation of specific membrane domains, (iii) permeabilization within the domains, and (iv) pH-specific transformation of domains. Biosensor data revealed that VapA binds to membranes in one step at pH 6...
February 3, 2024: Molecular Microbiology
https://read.qxmd.com/read/38301890/klebicin-e-a-pore-forming-bacteriocin-of-klebsiella-pneumoniae-exploits-the-porin-ompc-and-the-ton-system-for-translocation
#23
JOURNAL ARTICLE
Xinxin Zhao, Wenyu Wang, Xiaoli Zeng, Rong Xu, Bing Yuan, Wenyao Yu, Mingshu Wang, Renyong Jia, Shun Chen, Dekang Zhu, Mafeng Liu, Qiao Yang, Ying Wu, Shaqiu Zhang, Juan Huang, Xumin Ou, Di Sun, Anchun Cheng
Bacteriocins, which have narrow-spectrum activity and limited adverse effects, are promising alternatives to antibiotics. In this study, we identified klebicin E (KlebE), a small bacteriocin derived from Klebsiella pneumoniae. KlebE exhibited strong efficacy against multidrug-resistant K. pneumoniae isolates and conferred a significant growth advantage to the producing strain during intraspecies competition. A giant unilamellar vesicle leakage assay demonstrated the unique membrane permeabilization effect of KlebE, suggesting it is a pore-forming toxin...
January 30, 2024: Journal of Biological Chemistry
https://read.qxmd.com/read/38300478/engineering-of-bacillus-thuringiensis-cry2ab-toxin-for-improved-insecticidal-activity
#24
JOURNAL ARTICLE
Bai-Wen Fu, Lian Xu, Mei-Xia Zheng, Yan Shi, Yu-Jing Zhu
Bacillus thuringiensis Cry2Ab toxin was a widely used bioinsecticide to control lepidopteran pests all over the world. In the present study, engineering of Bacillus thuringiensis Cry2Ab toxin was performed for improved insecticidal activity using site-specific saturation mutation. Variants L183I were screened with lower LC50 (0.129 µg/cm2 ) against P. xylostella when compared to wild-type Cry2Ab (0.267 µg/cm2 ). To investigate the molecular mechanism behind the enhanced activity of variant L183I, the activation, oligomerization and pore-formation activities of L183I were evaluated, using wild-type Cry2Ab as a control...
February 1, 2024: AMB Express
https://read.qxmd.com/read/38281302/mutational-analysis-of-the-transmembrane-%C3%AE-4-helix-of-bacillus-thuringiensis-mosquito-larvicidal-cry4aa-toxin
#25
JOURNAL ARTICLE
Hirokazu Takahashi, Mami Asakura, Toru Ide, Tohru Hayakawa
Cry4Aa, produced by Bacillus thuringiensis subsp. israelensis, exhibits specific toxicity to larvae of medically important mosquito genera. Cry4Aa functions as a pore-forming toxin, and a helical hairpin (α4-loop-α5) of domain I is believed to be the transmembrane domain that forms toxin pores. Pore formation is considered to be a central mode of Cry4Aa action, but the relationship between pore formation and toxicity is poorly understood. In the present study, we constructed Cry4Aa mutants in which each polar amino acid residues within the transmembrane α4 helix was replaced with glutamic acid...
January 28, 2024: Current Microbiology
https://read.qxmd.com/read/38276916/antibody-response-to-the-sneathia-vaginalis-cytopathogenic-toxin-a-during-pregnancy
#26
JOURNAL ARTICLE
Zion T McCoy, Myrna G Serrano, Laahirie Edupuganti, Katherine M Spaine, David J Edwards, Gregory A Buck, Kimberly K Jefferson
Sneathia vaginalis is a Gram-negative vaginal species that is associated with pregnancy complications. It produces cytopathogenic toxin A (CptA), a pore-forming toxin. To determine whether CptA is expressed in vivo and to examine the mucosal Ab response to the toxin, we examined human midvaginal swab samples obtained during pregnancy for IgM, IgA, and IgG Abs with CptA affinity. This subcohort study included samples from 93 pregnant people. S. vaginalis relative abundance was available through 16S rRNA survey...
January 1, 2024: ImmunoHorizons
https://read.qxmd.com/read/38261662/prmt-7-prmt7-activates-hlh-30-tfeb-to-guard-plasma-membrane-integrity-compromised-by-bacterial-pore-forming-toxins
#27
JOURNAL ARTICLE
Hui-Chen Hsieh, I-Hsiang Huang, Shao-Wen Chang, Po-Lin Chen, Yu-Cheng Su, Shuying Wang, Wei-Jiun Tsai, Ping-Hung Chen, Raffi V Aroian, Chang-Shi Chen
Bacterial pore-forming toxins (PFTs) that disrupt host plasma membrane integrity (PMI) significantly contribute to the virulence of various pathogens. However, how host cells protect PMI in response to PFT perforation in vivo remains obscure. Previously, we demonstrated that the HLH-30/TFEB-dependent intrinsic cellular defense (INCED) is elicited by PFT to maintain PMI in Caenorhabditis elegans intestinal epithelium. Yet, the molecular mechanism for the full activation of HLH-30/TFEB by PFT remains elusive...
January 23, 2024: Autophagy
https://read.qxmd.com/read/38248700/there-are-no-insurmountable-barriers-passage-of-the-helicobacter-pylori-vaca-toxin-from-bacterial-cytoplasm-to-eukaryotic-cell-organelle
#28
REVIEW
Miroslaw Jarzab, Joanna Skorko-Glonek
The Gram-negative bacterium Helicobacter pylori is a very successful pathogen, one of the most commonly identified causes of bacterial infections in humans worldwide. H. pylori produces several virulence factors that contribute to its persistence in the hostile host habitat and to its pathogenicity. The most extensively studied are cytotoxin-associated gene A (CagA) and vacuolating cytotoxin A (VacA). VacA is present in almost all H. pylori strains. As a secreted multifunctional toxin, it assists bacterial colonization, survival, and proliferation during long-lasting infections...
December 28, 2023: Membranes
https://read.qxmd.com/read/38236820/jak-stat-signaling-regulated-intestinal-regeneration-defends-insect-pests-against-pore-forming-toxins-produced-by-bacillus-thuringiensis
#29
JOURNAL ARTICLE
Zeyu Wang, Yanchao Yang, Sirui Li, Weihua Ma, Kui Wang, Mario Soberón, Shuo Yan, Jie Shen, Frederic Francis, Alejandra Bravo, Jie Zhang
A variety of coordinated host-cell responses are activated as defense mechanisms against pore-forming toxins (PFTs). Bacillus thuringiensis (Bt) is a worldwide used biopesticide whose efficacy and precise application methods limits its use to replace synthetic pesticides in agricultural settings. Here, we analyzed the intestinal defense mechanisms of two lepidopteran insect pests after intoxication with sublethal dose of Bt PFTs to find out potential functional genes. We show that larval intestinal epithelium was initially damaged by the PFTs and that larval survival was observed after intestinal epithelium regeneration...
January 2024: PLoS Pathogens
https://read.qxmd.com/read/38235972/-staphylococcus-aureus-senses-human-neutrophils-via-perr-to-coordinate-the-expression-of-the-toxin-lukab
#30
JOURNAL ARTICLE
Avital Savin, Exene E Anderson, Sophie Dyzenhaus, Magdalena Podkowik, Bo Shopsin, Alejandro Pironti, Victor J Torres
Staphylococcus aureus utilizes a diverse set of virulence factors, such as leukocidins, to subvert human neutrophils, but how these toxins are regulated is incompletely defined. Here, we identified the peroxide-sensitive repressor, PerR, as a required protein involved in the induction of lukAB in the presence of primary human neutrophils, a phenotype directly linked to the ability of PerR to sense H2 O. Thus, we show that S. aureus coordinates sensing and resistance to oxidative stress with toxin production to promote pathogen survival...
January 18, 2024: Infection and Immunity
https://read.qxmd.com/read/38181093/litaf-protects-against-pore-forming-protein-induced-cell-death-by-promoting-membrane-repair
#31
JOURNAL ARTICLE
Caroline Stefani, Anna M Bruchez, Mario G Rosasco, Anna E Yoshida, Kayla J Fasano, Paula F Levan, Alina Lorant, Nicholas W Hubbard, Andrew Oberst, Lynda M Stuart, Adam Lacy-Hulbert
Pore-forming toxins (PFTs) are the largest class of bacterial toxins and contribute to virulence by triggering host cell death. Vertebrates also express endogenous pore-forming proteins that induce cell death as part of host defense. To mitigate damage and promote survival, cells mobilize membrane repair mechanisms to neutralize and counteract pores, but how these pathways are activated is poorly understood. Here, we use a transposon-based gene activation screen to discover pathways that counteract the cytotoxicity of the archetypal PFT Staphylococcus aureus α-toxin...
January 5, 2024: Science Immunology
https://read.qxmd.com/read/38175929/-bacillus-thuringiensis-cry9aa-insecticidal-protein-domain-i-helices-%C3%AE-3-and-%C3%AE-4-are-two-core-regions-involved-in-oligomerization-and-toxicity
#32
JOURNAL ARTICLE
Xiang He, Yanchao Yang, Mario Soberón, Alejandra Bravo, Lihong Zhang, Jie Zhang, Zeyu Wang
Bacillus thuringiensis Cry9 proteins show high insecticidal activity against different lepidopteran pests. Cry9 could be a valuable alternative to Cry1 proteins because it showed a synergistic effect with no cross-resistance. However, the pore-formation region of the Cry9 proteins is still unclear. In this study, nine mutations of certain Cry9Aa helices α3 and α4 residues resulted in a complete loss of insecticidal activity against the rice pest Chilo suppressalis ; however, the protein stability and receptor binding ability of these mutants were not affected...
January 4, 2024: Journal of Agricultural and Food Chemistry
https://read.qxmd.com/read/38161000/structural-analysis-of-membrane-associated-forms-of-helicobacter-pylori-vaca-toxin
#33
JOURNAL ARTICLE
Sarah M Connolly, Amanda L Erwin, Megan Sabb, Jessica L Hanks, Louise Chang, Rachel M Torrez, Georgia C Caso, Anne M Campbell, Shyamal Mosalaganti, Timothy L Cover, Melanie D Ohi
Helicobacter pylori colonizes the stomach in about half of the human population, leading to an increased risk of peptic ulcer disease and gastric cancer. H. pylori secretes an 88 kDa VacA toxin that contributes to pathogenesis. VacA assembles into oligomeric complexes in solution and forms anion-selective channels in cell membranes. Cryo-electron microscopy (cryo-EM) analyses of VacA oligomers in solution provided insights into VacA oligomerization but failed to reveal the structure of the hydrophobic N-terminal region predicted to be a pore-forming domain...
December 29, 2023: Journal of Molecular Biology
https://read.qxmd.com/read/38141971/unveiling-sticholysin-ii-and-plasmid-dna-interaction-implications-for-developing-non-viral-vectors
#34
JOURNAL ARTICLE
Felipe A Escalona-Rodriguez, Yoelys Cruz Leal, Javier La O-Bonet, Julio A PerezErviti, Mario Ernesto Valdés Tresanco, Ada L Rivero-Hernández, Maricary Sifontes-Niebla, Alexis MansoVargas, Belinda Sánchez, Carlos Alvarez, Leandro R S Barbosa, Rosangela Itri, María E Lanio
Non-viral gene delivery systems offer significant potential for gene therapy due to their versatility, safety, and cost advantages over viral vectors. However, their effectiveness can be hindered by the challenge of efficiently releasing the genetic cargo from endosomes to prevent degradation in lysosomes. To overcome this obstacle, functional components can be incorporated into these systems. Sticholysin II (StII) is one of the pore-forming proteins derived from the sea anemone Stichodactyla helianthus, known for its high ability to permeabilize cellular and model membranes...
December 21, 2023: Toxicon: Official Journal of the International Society on Toxinology
https://read.qxmd.com/read/38133199/cellular-uptake-and-cytotoxicity-of-clostridium-perfringens-iota-toxin
#35
REVIEW
Masahiro Nagahama, Masaya Takehara, Soshi Seike, Yoshihiko Sakaguchi
Clostridium perfringens iota-toxin is composed of two separate proteins: a binding protein (Ib) that recognizes a host cell receptor and promotes the cellular uptake of a catalytic protein and (Ia) possessing ADP-ribosyltransferase activity that induces actin cytoskeleton disorganization. Ib exhibits the overall structure of bacterial pore-forming toxins (PFTs). Lipolysis-stimulated lipoprotein receptor (LSR) is defined as a host cell receptor for Ib. The binding of Ib to LSR causes an oligomer formation of Ib in lipid rafts of plasma membranes, mediating the entry of Ia into the cytoplasm...
December 11, 2023: Toxins
https://read.qxmd.com/read/38132307/random-mutational-analysis-targeting-residue-k-155-within-the-transmembrane-%C3%AE-hairpin-of-the-mosquitocidal-mpp46ab-toxin
#36
JOURNAL ARTICLE
Midoka Miyazaki, Mami Asakura, Toru Ide, Tohru Hayakawa
Mpp46Ab is a mosquito-larvicidal pore-forming toxin derived from Bacillus thuringiensis TK-E6. Pore formation is believed to be a central mode of Mpp46Ab action, and the cation selectivity of the channel pores, in particular, is closely related to its mosquito-larvicidal activity. In the present study, we constructed a mutant library in which residue K155 within the transmembrane β-hairpin was randomly replaced with other amino acid residues. Upon mutagenesis and following primary screening using Culex pipiens mosquito larvae, we obtained 15 mutants in addition to the wild-type toxin...
December 1, 2023: Biology
https://read.qxmd.com/read/38112538/deep-learning-assisted-single-molecule-detection-of-protein-post-translational-modifications-with-a-biological-nanopore
#37
JOURNAL ARTICLE
Chan Cao, Pedro Magalhães, Lucien F Krapp, Juan F Bada Juarez, Simon Finn Mayer, Verena Rukes, Anass Chiki, Hilal A Lashuel, Matteo Dal Peraro
Protein post-translational modifications (PTMs) play a crucial role in countless biological processes, profoundly modulating protein properties on both spatial and temporal scales. Protein PTMs have also emerged as reliable biomarkers for several diseases. However, only a handful of techniques are available to accurately measure their levels, capture their complexity at a single molecule level, and characterize their multifaceted roles in health and disease. Nanopore sensing provides high sensitivity for the detection of low-abundance proteins, holding the potential to impact single-molecule proteomics and PTM detection, in particular...
December 19, 2023: ACS Nano
https://read.qxmd.com/read/38102952/selective-block-of-human-kv1-1-channels-and-an-epilepsy-associated-gain-of-function-mutation-by-aetx-k-peptide
#38
JOURNAL ARTICLE
Ruiming Zhao, Arwa Qasim, Punyanuch Sophanpanichkul, Hui Dai, Maha Nayak, Inbal Sher, Jordan Chill, Steve A N Goldstein
Dysfunction of the human voltage-gated K+ channel Kv1.1 has been associated with epilepsy, multiple sclerosis, episodic ataxia, myokymia, and cardiorespiratory dysregulation. We report here that AETX-K, a sea anemone type I (SAK1) peptide toxin we isolated from a phage display library, blocks Kv1.1 with high affinity (Ki  ~ 1.6 pM) and notable specificity, inhibiting other Kv channels we tested a million-fold less well. Nuclear magnetic resonance (NMR) was employed both to determine the three-dimensional structure of AETX-K, showing it to employ a classic SAK1 scaffold while exhibiting a unique electrostatic potential surface, and to visualize AETX-K bound to the Kv1...
January 2024: FASEB Journal: Official Publication of the Federation of American Societies for Experimental Biology
https://read.qxmd.com/read/38089811/-staphylococcus-aureus-activates-nrlp3-dependent-il-1%C3%AE-secretion-from-human-conjunctival-goblet-cells-using-%C3%AE-toxin-and-toll-like-receptors-2-and-1
#39
JOURNAL ARTICLE
Dayu Li, Robin Hodges, Maria AukrustNaqvi, Jeffrey Bair, Paulo J M Bispo, Michael S Gilmore, Meredith Gregory-Ksander, Darlene A Dartt
We used cultured human conjunctival goblet cells to determine (i) whether the toxigenic S. aureus- induced activation of the epithelial goblet cells requires two signals to activate the NLRP3 inflammasome, (ii) if one signal is mediated by TLR1, TLR2, or TLR6, and (iii) if the S. aureus toxin α toxin is another signal for the activation of the inflammasome and secretion of mature IL-1β. Cultured cells were incubated with siRNA to knock down the different TLRs. After stimulation with toxigenic S...
2023: Frontiers in Cellular and Infection Microbiology
https://read.qxmd.com/read/38087059/phagocytic-cell-death-leads-to-enhanced-release-of-pro-inflammatory-s100a12-in-familial-mediterranean-fever
#40
JOURNAL ARTICLE
G Varga, S Schleifenbaum, U Koenig, J Waldkirch, C Hinze, C Kessel, W Geluk, T Pap, Elke Lainka, Tilmann Kallinich, D Foell, H Wittkowski
BACKGROUND: Familial Mediterranean fever (FMF) is a prototypical autoinflammatory syndrome associated with phagocytic cell activation. Pyrin mutations are the genetic basis of this disease, and its expression has been shown in monocytes, granulocytes, dendritic cells, and synovial fibroblasts. Pyrin functions as a cytosolic pattern recognition receptor and forms a distinct pyrin inflammasome. The phagocyte-specific protein S100A12 is predominantly expressed in granulocytes and belongs to the group of damage associated molecular patterns (DAMP)...
December 13, 2023: Molecular and Cellular Pediatrics
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