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肺表面活性物质蛋白C类似物的棕榈酰化作用会影响表面相关脂质储备和膜稳定性。

Palmitoylation of a pulmonary surfactant protein C analogue affects the surface associated lipid reservoir and film stability.

作者信息

Gustafsson M, Palmblad M, Curstedt T, Johansson J, Schürch S

机构信息

Department of Medical Biochemistry and Biophysics, Karolinska Institutet, Stockholm, Sweden.

出版信息

Biochim Biophys Acta. 2000 Jun 1;1466(1-2):169-78. doi: 10.1016/s0005-2736(00)00198-x.

Abstract

Surfactant protein C (SP-C) is a lipopeptide that contains two thioester-linked palmitoyl groups and is considered to be important for formation of the alveolar surface active lipid film. Here, a non- or dipalmitoylated SP-C analogue (SP-C(Leu)), in which all helical Val residues were replaced with Leu and Cys-5 and Cys-6 were replaced with Ser, was tested for surface activity in a captive bubble system (CBS). SP-C(Leu), either palmitoylated at Ser-5 and Ser-6 or non-palmitoylated, was added to mixtures of 1, 2-dipalmitoyl-sn-glycero-3-phosphocholine (DPPC)/phosphatidyl glycerol (PG)/palmitic acid (PA), 68:22:9, (by mass) at a concentration of 2 and 5%. With 2% peptide, surface film formation was rapid, reaching a surface tension below 25 mN/m within 5 s, but the samples with 5% SP-C(Leu) required more than 20 s to reach values below 25 mN/m. Minimum surface tension for the samples with dipalmitoylated SP-C(Leu) was below 1.5 mN/m and very stable, as the surface tension increased by less than 0.5 mN/m within 10 min at constant bubble volume. Minimum surface tension for the non-palmitoylated SP-C(Leu) was approximately 2 and 5 mN/m for 2 and 5% peptide, respectively, but the films were less stable as seen by frequent bubble clicking at low surface tensions. Films with dipalmitoylated SP-C(Leu) that were dynamically cycled at 20-30 cycles/min were substantially less compressible at a surface tension of 20 mN/m (0.007 m/mN) than those that contained the non-palmitoylated peptide (0.02 m/mN). After subphase depletion, the incorporation of lipids into the surface active film during initial bubble expansion occurred at a relatively low surface tension (about 35 mN/m) for the samples with dipalmitoylated SP-C(Leu) compared to approximately 45 mN/m for those containing the non-palmitoylated peptide. Furthermore, for samples that contained non-palmitoylated SP-C(Leu), the ability to reach near zero stable surface tension was lost after a few adsorption steps, whereas with the dipalmitoylated peptide the film quality did not deteriorate even after more than 10 expansion steps and the incorporation of reservoir material equivalent to more than two monolayers. It appears that the covalently linked palmitoyl groups of the SP-C analogue studied are important for the mechanical stability of the lipid film, for the capacity to incorporate material from the reservoir into the surface active film upon area expansion, and for the low film compressibility of dynamically cycled films.

摘要

表面活性蛋白C(SP-C)是一种脂肽,含有两个硫酯连接的棕榈酰基,被认为对肺泡表面活性脂质膜的形成很重要。在此,我们在俘获气泡系统(CBS)中测试了一种非棕榈酰化或二棕榈酰化的SP-C类似物(SP-C(Leu))的表面活性,其中所有螺旋缬氨酸残基都被亮氨酸取代,半胱氨酸-5和半胱氨酸-6被丝氨酸取代。将在丝氨酸-5和丝氨酸-6处棕榈酰化或未棕榈酰化的SP-C(Leu)以2%和5%的浓度添加到1,2-二棕榈酰-sn-甘油-3-磷酸胆碱(DPPC)/磷脂酰甘油(PG)/棕榈酸(PA)质量比为68:22:9的混合物中。添加2%肽时,表面膜形成迅速,在5秒内表面张力降至25 mN/m以下,但添加5% SP-C(Leu)的样品需要超过20秒才能达到25 mN/m以下的值。二棕榈酰化SP-C(Leu)样品的最低表面张力低于1.5 mN/m且非常稳定,因为在恒定气泡体积下10分钟内表面张力增加不到0.5 mN/m。未棕榈酰化的SP-C(Leu)在2%和5%肽时的最低表面张力分别约为2和5 mN/m,但从低表面张力下频繁的气泡破裂可以看出,这些膜不太稳定。在20 - 30次/分钟动态循环的情况下,二棕榈酰化SP-C(Leu)的膜在20 mN/m(0.007 m/mN)的表面张力下比含有未棕榈酰化肽的膜(0.02 m/mN)更难压缩。在亚相耗尽后,与含有未棕榈酰化肽的样品在约45 mN/m相比,二棕榈酰化SP-C(Leu)的样品在初始气泡膨胀期间脂质掺入表面活性膜的过程发生在相对较低的表面张力(约35 mN/m)下。此外,对于含有未棕榈酰化SP-C(Leu)的样品,经过几次吸附步骤后就失去了达到接近零的稳定表面张力的能力,而对于二棕榈酰化肽,即使经过超过10次膨胀步骤以及掺入相当于超过两个单层的储库材料后,膜质量也没有恶化。看来,所研究的SP-C类似物的共价连接棕榈酰基对于脂质膜的机械稳定性、在面积膨胀时将储库材料掺入表面活性膜的能力以及动态循环膜的低膜压缩性很重要。

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