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1
Structure and membrane interactions of the antibiotic peptide dermadistinctin K by multidimensional solution and oriented 15N and 31P solid-state NMR spectroscopy.通过多维溶液以及定向15N和31P固态核磁共振光谱研究抗生素肽皮肤特异性蛋白K的结构与膜相互作用
Biophys J. 2009 Mar 18;96(6):2194-203. doi: 10.1016/j.bpj.2008.11.063.
2
Solid-state NMR and molecular dynamics simulations reveal the oligomeric ion-channels of TM2-GABA(A) stabilized by intermolecular hydrogen bonding.固态核磁共振和分子动力学模拟揭示了通过分子间氢键稳定的TM2-GABA(A)寡聚离子通道。
Biochim Biophys Acta. 2009 Mar;1788(3):686-95. doi: 10.1016/j.bbamem.2008.11.009. Epub 2008 Nov 21.
3
Structural determinants of antimicrobial and antiplasmodial activity and selectivity in histidine-rich amphipathic cationic peptides.富含组氨酸的两亲性阳离子肽中抗菌、抗疟活性及选择性的结构决定因素
J Biol Chem. 2009 Jan 2;284(1):119-133. doi: 10.1074/jbc.M806201200. Epub 2008 Nov 4.
4
Structure and alignment of the membrane-associated peptaibols ampullosporin A and alamethicin by oriented 15N and 31P solid-state NMR spectroscopy.通过定向 15N 和 31P 固态 NMR 光谱学研究膜相关缩肽类抗生素ampullosporin A 和 alamethicin 的结构和排列。
Biophys J. 2009 Jan;96(1):86-100. doi: 10.1529/biophysj.108.136242.
5
Efficacy of the amphibian peptide distinctin in a neutropenic mouse model of staphylococcal sepsis.两栖类肽段distinctin在葡萄球菌败血症中性粒细胞减少小鼠模型中的疗效。
Crit Care Med. 2008 Sep;36(9):2629-33. doi: 10.1097/CCM.0b013e318184430d.
6
Structural features of distinctin affecting peptide biological and biochemical properties.影响肽生物学和生化特性的不同蛋白的结构特征。
Biochemistry. 2008 Jul 29;47(30):7888-99. doi: 10.1021/bi800616k. Epub 2008 Jul 3.
7
A dynamic view of peptides and proteins in membranes.膜中肽和蛋白质的动态观点。
Cell Mol Life Sci. 2008 Oct;65(19):3028-39. doi: 10.1007/s00018-008-8125-z.
8
Aggregation and membrane permeabilizing properties of designed histidine-containing cationic linear peptide antibiotics.设计的含组氨酸阳离子线性肽抗生素的聚集及膜通透特性
J Pept Sci. 2008 Apr;14(4):488-95. doi: 10.1002/psc.966.
9
Self-promoted cellular uptake of peptide/DNA transfection complexes.肽/DNA转染复合物的自促进细胞摄取。
Biochemistry. 2007 Oct 9;46(40):11253-62. doi: 10.1021/bi700766j. Epub 2007 Sep 12.
10
Helix orientations in membrane-associated Bcl-X(L) determined by 15N-solid-state NMR spectroscopy.通过15N-固态核磁共振光谱法测定膜相关Bcl-X(L)中的螺旋取向
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通过固态核磁共振光谱法研究抗生素异二聚体肽Distinctin的膜结构和构象变化。

Membrane structure and conformational changes of the antibiotic heterodimeric peptide distinctin by solid-state NMR spectroscopy.

作者信息

Resende Jarbas M, Moraes Cléria Mendonça, Munhoz Victor H O, Aisenbrey Christopher, Verly Rodrigo M, Bertani Philippe, Cesar Amary, Piló-Veloso Dorila, Bechinger Burkhard

机构信息

Université de Strasbourg, Centre National de la Recherche Scientifique, UMR 7177, Institut de Chimie, 4 rue Blaise Pascal, Strasbourg, France.

出版信息

Proc Natl Acad Sci U S A. 2009 Sep 29;106(39):16639-44. doi: 10.1073/pnas.0905069106. Epub 2009 Sep 14.

DOI:10.1073/pnas.0905069106
PMID:19805350
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2757838/
Abstract

The heterodimeric antimicrobial peptide distinctin is composed of 2 linear peptide chains of 22- and 25-aa residues that are connected by a single intermolecular S-S bond. This heterodimer has been considered to be a unique example of a previously unrecorded class of bioactive peptides. Here the 2 distinctin chains were prepared by chemical peptide synthesis in quantitative amounts and labeled with (15)N, as well as (15)N and (2)H, at selected residues, respectively, and the heterodimer was formed by oxidation. CD spectroscopy indicates a high content of helical secondary structures when associated with POPC/POPG 3:1 vesicles or in membrane-mimetic environments. The propensity for helix formation follows the order heterodimer >chain 2 >chain 1, suggesting that peptide-peptide and peptide-lipid interactions both help in stabilizing this secondary structure. In a subsequent step the peptides were reconstituted into oriented phospholipid bilayers and investigated by (2)H and proton-decoupled (15)N solid-state NMR spectroscopy. Whereas chain 2 stably inserts into the membrane at orientations close to perfectly parallel to the membrane surface in the presence or absence of chain 1, the latter adopts a more tilted alignment, which further increases in the heterodimer. The data suggest that membrane interactions result in considerable conformational rearrangements of the heterodimer. Therefore, chain 2 stably anchors the heterodimer in the membrane, whereas chain 1 interacts more loosely with the bilayer. These structural observations are consistent with the antimicrobial activities when the individual chains are compared to the dimer.

摘要

异二聚体抗菌肽Distinctin由两条线性肽链组成,分别含22个和25个氨基酸残基,通过一个分子间二硫键相连。这种异二聚体被认为是一类此前未记录的生物活性肽中的独特例子。在此,通过化学肽合成定量制备了两条Distinctin链,并分别在选定残基处用¹⁵N以及¹⁵N和²H进行标记,然后通过氧化形成异二聚体。圆二色光谱表明,当与POPC/POPG 3:1囊泡结合或处于膜模拟环境中时,其螺旋二级结构含量很高。形成螺旋的倾向顺序为异二聚体>链2>链1,这表明肽 - 肽和肽 - 脂质相互作用都有助于稳定这种二级结构。在后续步骤中,将肽重构到定向磷脂双层中,并通过²H和质子去耦¹⁵N固态核磁共振光谱进行研究。在有或没有链1存在的情况下,链2都以接近与膜表面完全平行的方向稳定插入膜中,而链1则采取更倾斜的排列方式,在异二聚体中这种排列进一步增加。数据表明,膜相互作用导致异二聚体发生相当大的构象重排。因此,链2将异二聚体稳定锚定在膜中,而链1与双层的相互作用则较为松散。当将单个链与二聚体进行比较时,这些结构观察结果与抗菌活性是一致的。