Part I: An X-ray scattering study of cholera toxin penetration and induced phase transformations in lipid membranes

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Abstract

Cholera toxin is a highly efficient biotoxin, which is frequently used as a tool to investigate protein-membrane interactions and as a reporter for membrane rafts. Cholera toxin binds selectively to gangliosides with highest affinity to GM1. However, the mechanism by which cholera toxin crosses the membrane remains unresolved. Using x-ray reflectivity and grazing incidence diffraction, we have been able to monitor the binding and penetration of cholera toxin into a model lipid monolayer containing the receptor GM 1 at the air-water interface. Very high toxin coverage was obtained allowing precise measurements of how toxin binding alters lipid packing. Grazing incidence x-ray diffraction revealed the coexistence of two monolayer phases after toxin binding. The first was identical to the monolayer before toxin binding. In regions where toxin was bound, a second membrane phase exhibited a decrease in order as evidenced by a larger area per molecule and tilt angle with concomitant thinning of the monolayer. These results demonstrate that cholera toxin binding induces the formation of structurally distinct, less ordered domains in gel phases. Furthermore, the largest decrease in lateral order to the monolayer occurred at low pH, supporting a low endosomal pH in the infection pathway. Surprisingly, at pH = 8 toxin penetration by the binding portion of the toxin, the B5 pentamer, was also observed.

Original languageEnglish
Pages (from-to)629-640
Number of pages12
JournalBiophysical Journal
Volume95
Issue number2
DOIs
StatePublished - Jul 15 2008
Externally publishedYes

Funding

The Los Alamos Neutron Science Center at the Los Alamos National Laboratory (LANL) is funded by the U.S. Department of Energy (DOE) under Contract W-7405-ENG-36. J.M and C.E.M. thank the LANL–Laboratory Directed Research and Development program, DOE Office of Science (Basic Energy Sciences) for financial support. C.E.M. acknowledges support from the LANL Director's Post-Doctoral Fellowship and the Institute for Complex Adaptive Matter. T.L.K. thanks the Jeff and Dianne Child/Steve Whitaker Fund for Distinguished Teaching and Scholarship for financial support.

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