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Improvement of pulmonary surfactant activity by introducing D-amino acids into highly hydrophobic amphiphilic α-peptide Hel 13-5.

作者信息

Nakamura Yoshihiro, Yukitake Ko, Nakahara Hiromichi, Lee Sooyoung, Shibata Osamu, Lee Sannamu

机构信息

Muromachi Chemical Co. Ltd., Ohmuta, Fukuoka 836-0895, Japan.

Fukuoka University Hospital, Fukuoka 814-0180, Japan.

出版信息

Biochim Biophys Acta. 2014 Aug;1838(8):2046-52. doi: 10.1016/j.bbamem.2014.04.024. Epub 2014 May 2.

DOI:10.1016/j.bbamem.2014.04.024
PMID:24796503
Abstract

The high costs of artificial pulmonary surfactants, ranging in hundreds per kilogram of body weight, used for treating the respiratory distress syndrome (RDS) premature babies have limited their applications. We have extensively studied soy lecithins and higher alcohols as lipid alternatives to expensive phospholipids such as DPPC and PG. As a substitute for the proteins, we have synthesized the peptide Hel 13-5D3 by introducing D-amino acids into a highly lipid-soluble, basic amphiphilic peptide, Hel 13-5, composed of 18 amino acid residues. Analysis of the surfactant activities of lipid-amphiphilic artificial peptide mixtures using lung-irrigated rat models revealed that a mixture (Murosurf SLPD3) of dehydrogenated soy lecithin, fractionated soy lecithin, palmitic acid (PA), and peptide Hel 13-5D3 (40:40:17.5:2.5, by weight) superior pulmonary surfactant activity than a commercially available pulmonary surfactant (beractant, Surfacten®). Experiments using ovalbumin-sensitized model animals revealed that the lipid-amphiphilic artificial peptide mixtures provided significant control over an increase in the pulmonary resistance induced by premature allergy reaction and reduced the number of acidocytes and neutrophils in lung-irrigated solution. The newly developed low-cost pulmonary surfactant system may be used for treatment of a wide variety of respiratory diseases.

摘要

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