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- Deacylated Pulmonary Surfactant Protein SP-C Transforms From...Deacylated Pulmonary Surfactant Protein SP-C Transforms From α-Helical to Amyloid Fibril Structure via a pH-Dependent Mechanism: An Infrared Structural Investigation
Biophysical Journal, Volume 85, Issue 4, 1 October 2003, Pages 2417-2429
Richard A. Dluhy, Saratchandra Shanmukh, J. Brian Leapard, Peter Krüger and John E. Baatz
AbstractBovine pulmonary surfactant protein C (SP-C) is a hydrophobic, -helical membrane-associated lipoprotein in which cysteines C4 and C5 are acylated with palmitoyl chains. Recently, it has been found that the -helix form of SP-C is metastable, and under certain circumstances may transform from an -helix to a -strand conformation that resembles amyloid fibrils. This transformation is accelerated when the protein is in its deacylated form (dSP-C). We have used infrared spectroscopy to study the structure of dSP-C in solution and at membrane interfaces. Our results show that dSP-C transforms from an -helical to a -type amyloid fibril structure via a pH-dependent mechanism. In solution at low pH, dSP-C is -helical in nature, but converts to an amyloid fibril structure composed of short -strands or -hairpins at neutral pH. The -helix structure of dSP-C is fully recoverable from the amyloid -structure when the pH is once again lowered. Attenuated total reflectance infrared spectroscopy of lipid-protein monomolecular films showed that the fibril -form of dSP-C is not surface-associated at the air-water interface. In addition, the lipid-associated -helix form of dSP-C is only retained at the surface at low surface pressures and dissociates from the membrane at higher surface pressures. In situ polarization modulation infrared spectroscopy of protein and lipid-protein monolayers at the air-water interface confirmed that the residual dSP-C helix conformation observed in the attenuated total reflectance infrared spectra of transferred films is randomly or isotropically oriented before exclusion from the membrane interface. This work identifies pH as one of the mechanistic causes of amyloid fibril formation for dSP-C, and a possible contributor to the pathogenesis of pulmonary alveolar proteinosis.
Abstract | Full Text | PDF (266 kb) - Structural Study of Poly(β-Benzyl-l-Aspartate) Monolayers at...Structural Study of Poly(β-Benzyl-l-Aspartate) Monolayers at Air-Liquid Interfaces
Biophysical Journal, Volume 75, Issue 5, 1 November 1998, Pages 2451-2460
S.A. Riou, S.L. Hsu and H.D. Stidham
AbstractAs normally studied, in the solid state or in solution, poly(-benzyl--aspartate) (PBLA) differs from the other helical polyamino acids in that its -helical conformation is most stable in the left-handed rather than in the right-handed form. The slightly lower energy per residue for the left-handed form in PBLA is easily perturbed, however. The helical screw sense can be inverted in a polar environment and, upon heating above 100°C, a distorted left-handed helix or ω-helix is irreversibly formed. From external reflectance Fourier transform infrared measurements at the air-water interface, the conformation of PBLA in the monolayer state is directly established for the first time. The infrared frequencies of the amide bands suggest that right-handed -helices are formed on the surface of water immediately after spreading the monolayers and independently of the polypeptide conformational distribution in the spreading solution. The right-handed helical form prevails throughout the slow compression of the Langmuir monolayers to collapsed films. The helical screw sense can be reversed by lowering the polarity of the aqueous phase. In addition, an alternate conformation similar to the ω-helix forms on addition of small amounts of isopropanol to the aqueous subphase, and appears to be an intermediate in the helix–helix transition.
Abstract | Full Text | PDF (198 kb) - Infrared Reflection Absorption Spectroscopy of Amphipathic M...Infrared Reflection Absorption Spectroscopy of Amphipathic Model Peptides at the Air/Water Interface
Biophysical Journal, Volume 86, Issue 6, 1 June 2004, Pages 3750-3758
Andreas Kerth, Andreas Erbe, Margitta Dathe and Alfred Blume
AbstractThe linear sequence KLAL (KLALKLALKALKAALKLA-NH) and its corresponding ,-isomers ka-KLAL (KLALKLALkaLKAALKLA-NH) and lk-KLAL (KLALKLALKAlkAALKLA-NH) are model compounds for potentially amphipathic -helical peptides which are able to bind to membranes and to increase the membrane permeability in a structure- and target-dependent manner (Dathe and Wieprecht, 1999) We first studied the secondary structure of KLAL and its analogs bound to the air/water using infrared reflection absorption spectroscopy. For the peptide films the shape and position of the amide I and amide II bands indicate that the KLAL adopts at large areas per molecule an -helical secondary structure, whereas at higher surface pressures or smaller areas it converts into a -sheet structure. This transition could be observed in the compression isotherm as well as during the adsorption at the air/water interface from the subphase as a function of time. The secondary structures are essentially orientated parallel to the air/water interface. The analogs with -amino acids in two different positions of the sequence, ka-KLAL and lk-KLAL, form only -sheet structures at all surface pressures. The observed results are interpreted using a comparison of hydrophobic moments calculated for -helices and -sheets. The differences between the hydrophobic moments calculated using the consensus scale are not large. Using the optimal matching hydrophobicity scale or the whole-residue hydrophobicity scale the -sheet even has the larger hydrophobic moment.
Abstract | Full Text | PDF (183 kb) - …more
Copyright © 1995 The Biophysical Society. All rights reserved.
Biophysical Journal, Volume 69, Issue 6, 2770-2781, 1 December 1995
doi:10.1016/S0006-3495(95)80150-5
Research Article
The infrared dichroism of transmembrane helical polypeptides
P.H. Axelsen, B.K. Kaufman, R.N. McElhaney and R.N. Lewis
Abstract
Polarized attenuated total internal reflectance techniques were applied to study the infrared dichroism of the amide I transition moment in two membrane-bound peptides that are known to form oriented transmembrane helices: gramicidin A in a supported phospholipid monolayer and Ac-Lys2-Leu24-Lys2-amide (L24) in oriented multibilayers. These studies were performed to test the ability of these techniques to determine the orientation of these peptides, to verify the value of optical parameters used to calculate electric field strengths, to examine the common assumptions regarding the amide I transition moment orientation, and to ascertain the effect of surface imperfections on molecular disorder. The two peptides exhibit marked differences in the shape and frequency of their amide I absorption bands. Yet both peptides are highly ordered and oriented with their helical axes perpendicular to the membrane surface. In the alpha-helix formed by L24, there is evidence for a mode with type E1 symmetry contributing to amide I, and the amide I transition moment must be more closely aligned with the peptide C=O (< 34 degrees) than earlier studies have suggested. These results indicate that long-standing assumptions about the orientation of amide I in a peptide require some revision, but that in general, infrared spectroscopy yields reliable information about the orientation of membrane-bound helical peptides.
