Staphylococcus aureus alpha toxin

Staphylococcus aureus alpha toxin from S.aureus. PDB entry 7ahl

Alpha-toxin, also known as alpha-hemolysin (Hla), is the major cytotoxic agent released by bacterium Staphylococcus aureus and the first identified member of the pore forming beta-barrel toxin family.^[1] This toxin consists mostly of beta-sheets (68%) with only about 10% alpha-helices. The hla gene on the S. aureus chromosome encodes the 293 residue protein monomer, which forms heptameric units on the cellular membrane to form a complete beta-barrel pore. This structure allows the toxin to perform its major function, development of pores in the cellular membrane, eventually causing cell death.

Function

Alpha-toxin has been shown to play a role in pathogenesis of disease, as hla knockout strains show reductions in invasiveness and virulence.^[2] The dosage of toxin can result in two different modes of activity. Low concentrations of toxin bind to specific, but unidentified, cell surface receptors and form the heptameric pores. This pore allows the exchange of monovalent ions, resulting in DNA fragmentation and eventually apoptosis.^[3] Higher concentrations result in the toxin absorbing nonspecifically to the lipid bilayer and forming large, Ca²⁺ permissive pores. This in turn results in massive necrosis and other secondary cellular reactions triggered by the uncontrolled Ca²⁺ influx.^[3]

Structure

The structure of the protein has been solved by X-ray crystallography and is deposited in the PDB as id code 7ahl.^[4] Seven monomers each contribute a long beta-hairpin to a fourteen stranded beta barrel that forms a pore in the cell membrane. This pore is 14 Ångström wide at its narrowest point. This width equals the diameter of approximately 4 calcium ions.

Role in Apoptosis

Recently, studies have shown that alpha-toxin plays a role in inducing apoptosis in certain human immune cells. Incubation of T-cells, monocytes, and peripheral blood lymphocytes with either purified alpha-toxin or S. aureus cell lysate resulted in the induction of apoptosis via the intrinsic death pathway.^[3] This activity was inhibited when two different anti-alpha-toxin antibodies were introduced. In the same study, alpha toxin was shown to activate caspase 8 and caspase 9, which in turn activate caspase 3, which causes massive DNA degradation and apoptosis. This activity was shown to be independent of the death receptor pathway.

Vaccine Development

Alpha-toxin is also one of the key virulence factors in S. aureus pneumonia.^[5] The level of alpha-toxin expressed by a particular strain of S. aureus directly correlates with the virulence of the strain.^[2] Recent research has shown that immunization with a mutant form of alpha-toxin that is no longer able to form pores protects against S. aureus pneumonia in mice. Also, introduction of alpha-toxin specific antibodies into an unimmunized animal protects against subsequent infection. Cultures of human lung epithelial cells incubated with anti-alpha-toxin and infected with S. aureus showed marked reductions in cellular damage when compared to control cells. As many strains of S. aureus are proving to be resistant to most available antibiotics, specific targeting of virulence factors with antibodies may be the next step to treating this pathogen.

References

↑ Bhakdi S, Tranum-Jensen J (December 1991). "α-toxin of Staphylococcus aureus". Microbiol. Rev. 55 (4): 733–51. PMC 372845. PMID 1779933.
1 2 Bubeck Wardenburg J, Schneewind O (February 2008). "Vaccine protection against Staphylococcus aureus pneumonia". J. Exp. Med. 205 (2): 287–94. doi:10.1084/jem.20072208. PMC 2271014. PMID 18268041.
1 2 3 Bantel H, Sinha B, Domschke W, Peters G, Schulze-Osthoff K, Jänicke RU (November 2001). "α-Toxin is a mediator of Staphylococcus aureus-induced cell death and activates caspases via the intrinsic death pathway independently of death receptor signaling". J. Cell Biol. 155 (4): 637–48. doi:10.1083/jcb.200105081. PMC 2198876. PMID 11696559.
↑ Song L, Hobaugh MR, Shustak C, Cheley S, Bayley H, Gouaux JE (1996). "Structure of staphylococcal alpha-hemolysin, a heptameric transmembrane pore.". Science. 274 (5294): 1859–1866. doi:10.1126/science.274.5294.1859. PMID 8943190.
↑ Bubeck Wardenburg J, Bae T, Otto M, Deleo FR, Schneewind O (December 2007). "Poring over pores: α-hemolysin and Panton-Valentine leukocidin in Staphylococcus aureus pneumonia". Nat. Med. 13 (12): 1405–6. doi:10.1038/nm1207-1405. PMID 18064027.

Toxins

Clostridium:	tetani Tetanospasmin Tetanolysin perfringens Alpha toxin Enterotoxin difficile A B botulinum Botox

other:	Anthrax toxin Listeriolysin O

Cocci

Streptolysin Leukocidin Panton-Valentine leukocidin

Staphylococcus	Staphylococcus aureus alpha/beta/delta Exfoliatin Toxic shock syndrome toxin Staphylococcal Enterotoxin B (SEB)

Plant toxins

Invertebrate toxins

scorpion:	Androctonus australis hector insect toxin Charybdotoxin Maurotoxin Agitoxin Margatoxin Slotoxin Scyllatoxin Hefutoxin HgeTx1 HsTx1 Lq2 Birtoxin Bestoxin BmKAEP Phaiodotoxin Imperatoxin Pi3

spider:	Latrotoxin Alpha-latrotoxin CSTX Cupiennins PhTx3 Stromatoxin Vanillotoxin Huwentoxin

mollusca:	Conotoxin Eledoisin Onchidal Saxitoxin Tetrodotoxin

Vertebrate toxins

fish:	Ciguatera Tetrodotoxin

amphibian:	(+)-Allopumiliotoxin 267A Batrachotoxin Bufotoxins Arenobufagin Bufotalin Bufotenin Cinobufagin Marinobufagin Epibatidine Histrionicotoxin Pumiliotoxin 251D Samandarin Samandaridine Tarichatoxin

reptile/snake venom:	Bungarotoxin Alpha-Bungarotoxin Beta-Bungarotoxin Calciseptine Taicatoxin Calcicludine Cardiotoxin III

note: some toxins are produced by lower species and pass through intermediate species

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