Hydrophobic surfactant-associated polypeptides: SP-C is a lipopeptide with two palmitoylated cysteine residues, whereas SP-B lacks covalently linked fatty acyl groups.

Curstedt, Tore; Johansson, Jan; Persson, Per; Eklúnd, Anders; Robertson, Bengt; Löwenadler, Björn; Jörnvall, Hans

doi:10.1073/pnas.87.8.2985

Cited by 201 publications

(152 citation statements)

References 35 publications

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“…Native SP-C (LRIPCCPVNLKRLLVVVVVVVLVVVVIVGALL-MGL with both cysteines palmitoylated [6]) was purified from porcine lungs [21].…”

Section: Peptide Synthesis and Purificationmentioning

confidence: 99%

“…SP-B, a homodimer of two 79-residue polypeptide chains [6,7], has an a-helical content of about 45% as shown by Fourier transform infrared (FTIR) [8] and circular dichroism (CD) spectroscopy [9]. SP-B has been proposed to contain four amphipathic helices interacting preferentially with superficial parts of a phospholipid bilayer [9].…”

Section: Introductionmentioning

confidence: 99%

“…SP-B has been proposed to contain four amphipathic helices interacting preferentially with superficial parts of a phospholipid bilayer [9]. SP-C is a 35-residue polypeptide [10] with palmitoyl groups thioester-linked to the cysteine residues in the N-terminal part of the molecule [6]. FTIR spectroscopy revealed that SP-C adopts mainly an ahelical conformation with its a-helix oriented parallel to the lipid acyl chains [11,12].…”

Section: Introductionmentioning

confidence: 99%

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The 21‐residue surfactant peptide (LysLeu₄)₄Lys(KL₄) is a transmembrane α‐helix with a mixed nonpolar/polar surface

et al. 1996

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The 21-residue peptide KLLLLKLLLLKLL-LLKLLLLK (KL4) has been synthesized and analyzed regarding its secondary structure and orientation in lipid environments. Fourier transform infrared and circular dichroism spectroscopy shows that the peptide exhibits approximately 80% a-helical content both in dodecylphosphocholine micelles and in 1,2-dipalmitoyl-sn-glycero-3-phosphocholine (DPPC)/phosphatidylglycerol (PG) 7:3 (w/w) bilayers. The positively charged lysine residues are evenly distributed over the entire, otherwise nonpolar, circumference of the helix. This is in sharp contrast to the uneven distribution of polar and nonpolar residues in amphipathic helices. Fourier transform infrared spectroscopy of the peptide inserted in DPPC/PG bilayers shows that the helical axis is oriented parallel to the lipid acyl chains. These data do not support a previous hypothesis that the KL4 peptide interacts with peripheral parts of a phospholipid monolayer and mimics the pulmonary surfactant protein SP-B, which is composed of several amphipathic ¢x-helices. KL4 accelerates the spreading of phospholipid mixtures at an air/water interface but does so less efficiently than other transmembranous helical polypeptides studied.

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“…Native SP-C (LRIPCCPVNLKRLLVVVVVVVLVVVVIVGALL-MGL with both cysteines palmitoylated [6]) was purified from porcine lungs [21].…”

Section: Peptide Synthesis and Purificationmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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The 21‐residue surfactant peptide (LysLeu₄)₄Lys(KL₄) is a transmembrane α‐helix with a mixed nonpolar/polar surface

et al. 1996

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“…In particular antipeptide antibodies offer a sensitive approach for the detection of conformational changes in surface accessible sequences of proteins [16]. This approach is especially useful in the study of the native SP-B protein domains because, with the possible exception of disulfide dependent oligomerization, SP-B is not known to undergo post translational modification such as phosphorylation or glycosylation [5]. In this report we describe the binding characteristics of two antibodies raised against synthetic peptides containing surface seeking segments of surfactant protein B.…”

Section: Introductionmentioning

confidence: 99%

Antibodies against synthetic amphipathic helical sequences of surfactant protein SP‐B detect a conformational change in the native protein

Fan¹,

Bruni²,

Taeusch³

et al. 1991

FEBS Letters

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Syntltetic peptides based on the native human sequen¢~ of surfactant protein B have I~,en used to generate polyclonal monospecific antibodies against specific segments of the native SP-B protein, Circular dichroism analysis or the synthr.tic p, have a dominant helical content in structure promotinll environments and tensiometric measurements indicate these peptides lower surface tension at air=water interfaces implyin~ that they contain amphipathic alpha helical motifs, Antibodies directed aBainst the C-terminal segment of SP.B react with the native protein in the oxidized and reduced state, Antibodies directed against the N.tem~inal sequence of SP-B react with the native protein only in the reduced stat~ suue..aiai| that this domain has a conformation dependent on disulfide bond formation.Surfactant pcptide; Amphtpathie helix: lmmunodominance

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“…The lack of exact agreement between the molecular mass calculated from the amino acid sequence (8.7 kDa for the monomer and 17.4 kDa for the dimer) and the masses observed by gel electrophoresis could be due to abnormal binding of SDS by the hydrophobic SP-B polypeptide, the fact that SP-B retains a folded structure in SDS and/or additional factors. Covalent linkage of non-protein constituents to SP-B have been ruled out by mass spectrometry (Curstedt et al, 1990;Voss et al, 1992). Each polypeptide chain of the dimer contains three disulphide bridges: Cys8-Cys77, Cysll -Cys71 and Cys35-Cys46.…”

Section: Structures Of the Hydrophobic Proteins Sp-b And Sp-cmentioning

confidence: 99%

Molecular Structures and Interactions of Pulmonary Surfactant Components

Johansson

Curstedt

1997

European Journal of Biochemistry

269

217

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The dominating functional property of pulmonary surfactant is to reduce the surface tension at the alveolar aidliquid interface, and thereby prevent the lungs from collapsing at the end of expiration. In addition, the system exhibits host-defense properties. Insufficient amounts of pulmonary surfactant in premature infants causes respiratory distress syndrome, a serious threat which nowadays can be effectively treated by airway instillation of surfactant preparations. Surfactant is a mixture of many molecular species, mainly phospholipids and specific proteins, surfactant protein A (SP-A), SP-B, SP-C and SP-D. SP-A and SP-D are water-soluble and belong to the collectins, a family of large multimeric proteins which structurally exhibit collagenousAectin hybrid properties and functionally are Caz+-dependent carbohydrate binding proteins involved in innate host-defence functions. SP-A and SP-D also bind lipids and SP-A is involved in organization of alveolar surfactant phospholipids. SP-B belongs to another family of proteins, which includes also lipid-interacting polypeptides with antibacterial and lytic properties. SP-B is a 17.4-kDa homodimer and each subunit contains three intrachain disulphides and has been proposed to contain four amphipathic helices oriented pairwise in an antiparallel fashion. SP-A, SP-B and SP-D all have been detected also in the gastrointestinal tract. SP-C, in contrast, appears to be a unique protein with extreme structural and stability properties and to exist exclusively in the lungs. SP-C is a lipopeptide containing covalently linked palmitoyl chains and is folded into a 3.7-nm a-helix with a central 2.3-nm all-aliphatic part, making it perfectly suited to interact in a transmembranous way with a fluid bilayer composed of dipalmitoylglycerophosphocholine, the main component of surfactant. Homozygous genetic deficiency of proSP-B causes lethal respiratory distress soon after birth and is associated with aberrant processing of the precursor of SP-C. This review focuses on the chemical composition, structures and interactions of the pulmonary surfactant, in particular the associated proteins.

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Hydrophobic surfactant-associated polypeptides: SP-C is a lipopeptide with two palmitoylated cysteine residues, whereas SP-B lacks covalently linked fatty acyl groups.

Cited by 201 publications

References 35 publications

The 21‐residue surfactant peptide (LysLeu₄)₄Lys(KL₄) is a transmembrane α‐helix with a mixed nonpolar/polar surface

The 21‐residue surfactant peptide (LysLeu₄)₄Lys(KL₄) is a transmembrane α‐helix with a mixed nonpolar/polar surface

Antibodies against synthetic amphipathic helical sequences of surfactant protein SP‐B detect a conformational change in the native protein

Molecular Structures and Interactions of Pulmonary Surfactant Components

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Hydrophobic surfactant-associated polypeptides: SP-C is a lipopeptide with two palmitoylated cysteine residues, whereas SP-B lacks covalently linked fatty acyl groups.

Cited by 201 publications

References 35 publications

The 21‐residue surfactant peptide (LysLeu4)4Lys(KL4) is a transmembrane α‐helix with a mixed nonpolar/polar surface

The 21‐residue surfactant peptide (LysLeu4)4Lys(KL4) is a transmembrane α‐helix with a mixed nonpolar/polar surface

Antibodies against synthetic amphipathic helical sequences of surfactant protein SP‐B detect a conformational change in the native protein

Molecular Structures and Interactions of Pulmonary Surfactant Components

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Product

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The 21‐residue surfactant peptide (LysLeu₄)₄Lys(KL₄) is a transmembrane α‐helix with a mixed nonpolar/polar surface

The 21‐residue surfactant peptide (LysLeu₄)₄Lys(KL₄) is a transmembrane α‐helix with a mixed nonpolar/polar surface