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10.3390/toxins7051702

http://scihub22266oqcxt.onion/10.3390/toxins7051702
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C4448169!4448169!26008232
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suck abstract from ncbi


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pmid26008232      Toxins+(Basel) 2015 ; 7 (5): 1702-21
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  • Perfringolysin O: The Underrated Clostridium perfringens Toxin? #MMPMID26008232
  • Verherstraeten S; Goossens E; Valgaeren B; Pardon B; Timbermont L; Haesebrouck F; Ducatelle R; Deprez P; Wade KR; Tweten R; Van Immerseel F
  • Toxins (Basel) 2015[May]; 7 (5): 1702-21 PMID26008232show ga
  • The anaerobic bacterium Clostridium perfringens expresses multiple toxins that promote disease development in both humans and animals. One such toxin is perfringolysin O (PFO, classically referred to as ? toxin), a pore-forming cholesterol-dependent cytolysin (CDC). PFO is secreted as a water-soluble monomer that recognizes and binds membranes via cholesterol. Membrane-bound monomers undergo structural changes that culminate in the formation of an oligomerized prepore complex on the membrane surface. The prepore then undergoes conversion into the bilayer-spanning pore measuring approximately 250?300 Å in diameter. PFO is expressed in nearly all identified C. perfringens strains and harbors interesting traits that suggest a potential undefined role for PFO in disease development. Research has demonstrated a role for PFO in gas gangrene progression and bovine necrohemorrhagic enteritis, but there is limited data available to determine if PFO also functions in additional disease presentations caused by C. perfringens. This review summarizes the known structural and functional characteristics of PFO, while highlighting recent insights into the potential contributions of PFO to disease pathogenesis.
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