Helix orientations in membrane-associated Bcl-XL determined by 15N-solid-state NMR spectroscopy

Helix orientations in membrane-associated Bcl-XL determined by 15N-solid-state NMR spectroscopy

Controlled cell death is fundamental to tissue hemostasis and apoptosis malfunctions can lead to a wide range of diseases. Bcl-x^sub L^ is an anti-apoptotic protein the function of which is linked to its reversible interaction with mitochondrial outer membranes. Its interfacial and intermittent bila...

Full description

Saved in:
Bibliographic Details
Published in:European biophysics journal Vol. 37; no. 1; pp. 71 - 80
Main Authors: Aisenbrey, Christopher, Sudheendra, U. S., Ridley, Helen, Bertani, Philippe, Marquette, Arnaud, Nedelkina, Svetlana, Lakey, Jeremy H., Bechinger, Burkhard
Format: Journal Article
Language:English
Published: Heidelberg Springer Nature B.V 01-12-2007
Subjects:
Apoptosis
Cancer
Helix tilt angle
Membrane protein structure
Membranes
Oriented lipid bilayer
Proteins
Protein–protein interactions
Spectroscopy
Topology
Online Access:Get full text
Tags: Add Tag
No Tags, Be the first to tag this record!
Description
Summary:Controlled cell death is fundamental to tissue hemostasis and apoptosis malfunctions can lead to a wide range of diseases. Bcl-x^sub L^ is an anti-apoptotic protein the function of which is linked to its reversible interaction with mitochondrial outer membranes. Its interfacial and intermittent bilayer association makes prediction of its bound structure difficult without using methods able to extract data from dynamic systems. Here we investigate Bcl-x^sub L^ associated with oriented lipid bilayers at physiological pH using solid-state NMR spectroscopy. The data are consistent with a C-terminal transmembrane anchoring sequence and an average alignment of the remaining helices, i.e. including helices 5 and 6, approximately parallel to the membrane surface. Data from several biophysical approaches confirm that after removal of the C-terminus from Bcl-x^sub L^ its membrane interactions are weak. In the presence of membranes Bcl-x^sub L^ can still interact with a Bak BH3 domain peptide suggesting a model where the hydrophobic C-terminus of the protein unfolds and inserts into the membrane. During this conformational change the Bcl-x^sub L^ hydrophobic binding pocket becomes accessible for protein-protein interactions whilst the structure of the N-terminal region remains intact.[PUBLICATION ABSTRACT]
ISSN:0175-7571
1432-1017
DOI:10.1007/s00249-007-0165-z