Warning: Undefined array key "mm" in /www/wwwroot/www.ai-bt.com/si.php on line 10 Deprecated: trim(): Passing null to parameter #1 ($string) of type string is deprecated in /www/wwwroot/www.ai-bt.com/si.php on line 10 Tripartite haemolysin BL: isolation and characterization of two distinct homologous sets of components from a single Bacillus cereus isolate.

Literature DB >> 10846215

Tripartite haemolysin BL: isolation and characterization of two distinct homologous sets of components from a single Bacillus cereus isolate.

Abstract

Haemolysin BL (HBL), a three-component enterotoxic/necrotizing/vascular permeability toxin, is a likely virulence factor of Bacillus cereus diarrhoeal food poisoning and necrotic infections. This paper describes the isolation of two distinct homologous sets of all three HBL components from a single B. cereus isolate, MGBC 145. The proteins of one set (designated HBL, consisting of B, L(1) and L(2)), were about 87-100% identical in N-terminal amino acid sequences to their respective prototype components from strain F837/76, and the proteins of the homologous set (HBL(a), consisting of B(a), L(1a) and L(2a)) were all about 62-65% identical. Only the latter homologues differed immunochemically and physicochemically from the prototypes. HBL and HBL(a) exhibited similar haemolytic and vascular permeability potencies, and the homologues could be interchanged freely. There were no notable differences in activity between the L component homologues. However, components B and B(a) were significantly different. Both were secreted as monomers, but unlike B, B(a) was isolated as a relatively inactive complex that could be reactivated with urea. When B(a) was substituted for B in gel-diffusion assays the distinct discontinuous haemolysis pattern typical of the presence of B did not occur. In suspension assays, excess B inhibited the haemolysis of B-primed cells by L(1) (as previously described), but not that of B(a)-primed cells. Excess B(a) had the opposite effect and enhanced lysis of B(a)-primed cells, but not that of B-primed cells. These differences reveal details about how the toxin components interact on target cell membranes. The authors' observations indicate that HBL represents a new family of multicomponent toxins that was generated by a process of gene and operon duplication that occurred either intracellularly or by horizontal transfer, and raise the possibility of the existence of other related toxins in the genetically diverse B. cereus taxonomic group.

Entities: Chemical Disease Species

Mesh：

Substances：

Year: 2000 PMID： 10846215 DOI： 10.1099/00221287-146-6-1371

Source DB: PubMed Journal: Microbiology ISSN： 1350-0872 Impact factor: 2.777

Keyword Cloud
Cited

18 in total

1. Putative virulence factor expression by clinical and food isolates of Bacillus spp. after growth in reconstituted infant milk formulae.

Authors: N J Rowan; K Deans; J G Anderson; C G Gemmell; I S Hunter; T Chaithong
Journal: Appl Environ Microbiol Date: 2001-09 Impact factor: 4.792

2. Evidence for contribution of tripartite hemolysin BL, phosphatidylcholine-preferring phospholipase C, and collagenase to virulence of Bacillus cereus endophthalmitis.

Authors: D J Beecher; T W Olsen; E B Somers; A C Wong
Journal: Infect Immun Date: 2000-09 Impact factor: 3.441

3. A Genomic Island of Vibrio cholerae Encodes a Three-Component Cytotoxin with Monomer and Protomer Forms Structurally Similar to Alpha-Pore-Forming Toxins.

Authors: Alfa Herrera; Youngchang Kim; Andrzej Joachimiak; Karla J F Satchell; Jiexi Chen; Robert Jedrzejczak; Shantanu Shukla; Natalia Maltseva; Grazyna Joachimiak; Lukas Welk; Grant Wiersum; Lukasz Jaroszewski; Adam Godzik
Journal: J Bacteriol Date: 2022-04-18 Impact factor: 3.476

4. Disassembly of F-actin cytoskeleton after interaction of Bacillus cereus with fully differentiated human intestinal Caco-2 cells.

Authors: Jessica Minnaard; Vanessa Lievin-Le Moal; Marie-Helene Coconnier; Alain L Servin; Pablo F Pérez
Journal: Infect Immun Date: 2004-06 Impact factor: 3.441

Review 5. Production, secretion and biological activity of Bacillus cereus enterotoxins.

Authors: Sonia Senesi; Emilia Ghelardi
Journal: Toxins (Basel) Date: 2010-06-29 Impact factor: 4.546

6. From genome to toxicity: a combinatory approach highlights the complexity of enterotoxin production in Bacillus cereus.

Authors: Nadja Jeßberger; Viktoria M Krey; Corinna Rademacher; Maria-Elisabeth Böhm; Ann-Katrin Mohr; Monika Ehling-Schulz; Siegfried Scherer; Erwin Märtlbauer
Journal: Front Microbiol Date: 2015-06-10 Impact factor: 5.640

7. Prevalence, virulence factor genes and antibiotic resistance of Bacillus cereus sensu lato isolated from dairy farms and traditional dairy products.

Authors: James Owusu-Kwarteng; Alhassan Wuni; Fortune Akabanda; Kwaku Tano-Debrah; Lene Jespersen
Journal: BMC Microbiol Date: 2017-03-14 Impact factor: 3.605

8. Bacillus cereus in infant foods: prevalence study and distribution of enterotoxigenic virulence factors in Isfahan Province, Iran.

Authors: Ebrahim Rahimi; Fahimeh Abdos; Hassan Momtaz; Zienab Torki Baghbadorani; Mohammad Jalali
Journal: ScientificWorldJournal Date: 2013-05-27

9. Cereulide synthetase gene cluster from emetic Bacillus cereus: structure and location on a mega virulence plasmid related to Bacillus anthracis toxin plasmid pXO1.

Authors: Monika Ehling-Schulz; Martina Fricker; Harald Grallert; Petra Rieck; Martin Wagner; Siegfried Scherer
Journal: BMC Microbiol Date: 2006-03-02 Impact factor: 3.605

10. Massive horizontal gene transfer, strictly vertical inheritance and ancient duplications differentially shape the evolution of Bacillus cereus enterotoxin operons hbl, cytK and nhe.

Authors: Maria-Elisabeth Böhm; Christopher Huptas; Viktoria Magdalena Krey; Siegfried Scherer
Journal: BMC Evol Biol Date: 2015-11-10 Impact factor: 3.260