Protein engineering modulates the transport properties and ion selectivity of the pores formed by staphylococcal gamma-hemolysins in lipid membranes
Academic Article
Publication Date:
2002
abstract:
Staphylococcal gamma-haemolysins are bicomponent toxins in a family
including other leucocidins and alpha-toxin. Two active toxins are formed
combining HlgA or HlgC with HlgB. Both open pores in lipid membranes with
conductance, current voltage characteristics and stability similar to
alpha-toxin, but different selectivity (cation instead of anion).
Structural analogies between gamma-haemolysins and alpha-toxin indicate
the presence, at the pore entry, of a conserved region containing four
positive charges in alpha-toxin, but either positive or negative in gamma-
haemolysins. Four mutants were produced (HlgA D44K, HlgB D47K, HlgB D49K
and HlgB D47K/D49K) converting those negative charges to positive in HlgA
and HlgB. When all charges were positive, the pores had the same
selectivity and conductance as alpha-toxin, suggesting that the cluster
may form an entrance electrostatic filter. As mutated HlgC-HlgB pores
were less affected, additional charges in the lumen of the pore were
changed (HlgB E107Q, HlgB D121N, HlgB T136D and HlgA K108T). Removing a
negative charge from the lumen made the selectivity of both HlgA-HlgB
D121N and HlgC-HlgB D121N more anionic. Residue D121 of HlgB is
compensated by a positive residue (HlgA K108) in the HlgA-HlgB pore, but
isolated in the more cation-selective HlgC-HlgB pore. Interestingly, the
pore formed by HlgA K108T-HlgB, in which the positive charge of HlgA was
removed, was as cation selective as HlgC-HlgB. Meanwhile, the pore formed
by HlgA K108T-HlgB D121N, in which the two charge changes compensated,
retrieved the properties of wild-type HlgA-HlgB. We conclude that the
conductance and selectivity of the gamma-haemolysin pores depend
substantially on the presence and location of charged residues in the
channel.
Iris type:
01.01 Articolo in rivista
List of contributors:
Menestrina, Gianfranco
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