The efficacy and safety of KL4-surfactant in preterm infants with respiratory distress syndrome.

Cochrane, C. G.; Revak, Susan D.; Merritt, T. Allen; Heldt, Gregory P.; Hallman, Mikko; Cunningham, M. Douglas; Easa, David; Pramanik, Arun K.; Edwards, David K.; Alberts, Michael S.

doi:10.1164/ajrccm.153.1.8542150

Cited by 156 publications

(85 citation statements)

References 24 publications

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“…In summary, we have shown that the 21-residue peptide KL4 is a transmembranous helix with a mixed polar/nonpolar surface. The helix is oriented parallel to the lipid acyl chains and the structure and orientation of KL4 indicate that its mechanism of action is similar to that of SP-C, in contrast to previous suggestions [15][16][17][18]. This knowledge is useful for designing peptide analogues for further studies of the mechanism of action of pulmonary surfactant polypeptides.…”

Section: Discussionmentioning

confidence: 75%

“…The small sizes of SP-B and SP-C have raised the possibility of producing bioactive analogues, for formulating synthetic peptide-containing surfactant preparations. Cochrane and Revak designed a 21-residue polypeptide, KL4, with a repetitive sequence of leucine and lysine residues [15][16][17][18]. This peptide mimics the pattern of hydrophobic and hydrophilic residues in SP-B and was supposed to stabilize the phospholipid bilayer by interactions with the lipid headgroups and superficial parts of the acyl chains [15].…”

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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Section: Discussionmentioning

confidence: 75%

Section: Introductionmentioning

confidence: 99%

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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“…Two important conceptual approaches being followed to develop synthetic exogenous surfactants are: (1) Combining human sequence recombinant proteins or synthetic amphipathic peptides with synthetic biological glycerophospholipids; and (2) combining synthetic amphipathic peptides with novel synthetic lipids designed to have favorable physicochemical properties such as high surface activity and structural resistance to inflammatory phospholipases during lung injury. Surfaxin® (KL4) [87,107,123,[189][190][191][192][193][194][195] and Venticute® (recombinant SPC surfactant) [26,[196][197][198][199][200][201] are two current examples of the first of these approaches (Table 3). However, the 21 amino acid KL4 peptide is only a very rough structural analog to native SP-B, and advances in peptide molecular modeling and synthesis technology support the feasibility of preparing new SP-B peptides with significantly greater sequence and molecular folding specificity, and correspondingly higher activity ( [202][203][204] for review).…”

Section: Examples Of Research On New Synthetic Exogenous Surfactamentioning

confidence: 99%

Surfactant for Pediatric Acute Lung Injury

Willson¹,

Chess²,

Notter³

2008

Pediatric Clinics of North America

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SynopsisThis article reviews exogenous surfactant therapy and its use in mitigating acute lung injury (ALI) and the acute respiratory distress syndrome (ARDS) in infants, children, and adults. Biophysical and animal research documenting surfactant dysfunction in ALI/ARDS is described, and the scientific rationale for treatment with exogenous surfactant is discussed. Major emphasis is on reviewing clinical studies of surfactant therapy in pediatric and adult patients with ALI/ARDS. Particular advantages from surfactant therapy in direct pulmonary forms of these syndromes are described. Also discussed are additional factors affecting the efficacy of exogenous surfactants in ALI/ARDS, including the multifaceted pathology of inflammatory lung injury, the effectiveness of surfactant delivery in injured lungs, and composition-based activity differences among clinical exogenous surfactant preparations.

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“…This surfactant has greater resistance to oxidation and peroxidation than beractant and was shown to improve pulmonary function in an animal model of RDS and a pilot study involving preterm infants with established RDS. [20][21][22] Lucinactant comes in a solution containing 30 mg of phospholipids per ml for a total recommended dose of 5.8 ml kg -1 or 175 mg of phospholipids. It requires warming to 44 1C followed by vigorous shaking and cooling to body temperature before administration.…”

Section: New-generation Protein-containing Synthetic Surfactantmentioning

confidence: 99%

Synthetic surfactants: where are we? Evidence from randomized, controlled clinical trials

Moya

2009

J Perinatol

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The benefits of exogenous synthetic or animal-derived surfactants for prevention or treatment of respiratory distress syndrome (RDS) are well established. Data from head-to-head trials comparing animal-derived surfactants primarily with the synthetic surfactant colfosceril suggest that the major clinical advantages afforded by the presence of surfactant protein (SP)-B and SP-C in animal-derived preparations relate to faster onset of action, a reduction in the incidence of RDS when used prophylactically, and a lower incidence of air leaks and RDS-related deaths. However, no benefits in terms of overall mortality or BPD have been shown in these head-to-head comparisons. Findings from trials of a new-generation synthetic surfactant containing a peptide that mimics SP-B, as well as their follow-up study suggest that its administration improves short-term clinical outcomes compared with colfosceril and results in survival through 1 year of age, which is at least comparable, if not perhaps superior, to that seen with animal-derived surfactants.

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The efficacy and safety of KL4-surfactant in preterm infants with respiratory distress syndrome.

Cited by 156 publications

References 24 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

Surfactant for Pediatric Acute Lung Injury

Synthetic surfactants: where are we? Evidence from randomized, controlled clinical trials

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The efficacy and safety of KL4-surfactant in preterm infants with respiratory distress syndrome.

Cited by 156 publications

References 24 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

Surfactant for Pediatric Acute Lung Injury

Synthetic surfactants: where are we? Evidence from randomized, controlled clinical trials

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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