Berlose J P, Convert O, Derossi D, Brunissen A, Chassaing G
Laboratoire de Chimie Organique Biologique, URA CNRS 493, Université P. et M. Curie, Paris, France.
Eur J Biochem. 1996 Dec 1;242(2):372-86. doi: 10.1111/j.1432-1033.1996.0372r.x.
The third helix of antennapedia homeodomain pAntp-(43-58) can translocate through cell membrane and has been used as an intracellular vehicle for delivering peptides and oligonucleotides. The conformational and associative behaviour of two peptidic vectors pAntp-(43-58) and [Pro50] pAntp-(43-58) has been analyzed by different biophysical methods. pAntp-(43-58) adopts an amphipathic helical structure in 30% (by vol.) hexafluoroisopropanol, in perfluoro-tert-butanol and in the presence of SDS micelles. CD spectra indicate that the conformation of [Pro50]pAntp-(43-58) in contrast to pAntp-(43-58) is independent of the media used. 1H-NMR spectroscopy in SDS micelles or in perfluoro-tert-butanol allows detection of aggregated peptides probably in a ribbon 2(7) type conformation. These conformations became the predominant structure when Gln50 was replaced by Pro50. Interproton-distance restraints derived from NOE measurements have been classified in two groups corresponding to two types of structures: alpha-helix and essentially extended structures. Consecutive CH alpha (i)/ CH alpha (i + 1) NOEs are only compatible with aggregates. Simulated annealing calculation of dimeric structure agrees with phi and psi angles in the beta-sheet and gamma-turn regions. Fluorescence spectroscopy analysis has shown that the indole groups of both peptides penetrate into SDS micelles; both peptides also induce the formation of micelles at very low concentration of SDS (20 microM). Similar interaction was observed with reverse-phase micelles made of bis(2-ethyhexyl) sodium sulfosuccinate and small unilamellar vesicles (SUV) made of a mixture of phosphatidylcholine/phosphatidylserine. 31P-NMR of vesicles (SUV and large unilamellar vesicles) indicated that the addition of pAntp analogues did not affect the size of phosphatidylcholine/phosphatidylserine vesicles. The addition of pAntp analogues to lipidic dispersions modulates lipid polymorphism in different ways depending on the mixtures of acidic lipids.
触角足同源结构域pAntp-(43 - 58)的第三个螺旋能够穿过细胞膜,并已被用作递送肽和寡核苷酸的细胞内载体。通过不同的生物物理方法分析了两种肽载体pAntp-(43 - 58)和[Pro50]pAntp-(43 - 58)的构象和缔合行为。pAntp-(43 - 58)在30%(体积)的六氟异丙醇、全氟叔丁醇中以及在SDS胶束存在的情况下会形成两亲螺旋结构。圆二色光谱表明,与pAntp-(43 - 58)相比,[Pro50]pAntp-(43 - 58)的构象与所用介质无关。在SDS胶束或全氟叔丁醇中的1H - NMR光谱能够检测到可能呈带状2(7)型构象的聚集肽。当Gln50被Pro50取代时,这些构象成为主要结构。源自NOE测量的质子间距离限制已被分为两组,分别对应两种类型的结构:α - 螺旋和基本伸展的结构。连续的CHα(i)/CHα(i + 1) NOE仅与聚集体兼容。二聚体结构的模拟退火计算与β - 折叠和γ - 转角区域中的φ和ψ角一致。荧光光谱分析表明,两种肽的吲哚基团都能穿透到SDS胶束中;两种肽在非常低的SDS浓度(20μM)下也能诱导胶束的形成。在用双(2 - 乙基己基)磺基琥珀酸钠制成的反相胶束和由磷脂酰胆碱/磷脂酰丝氨酸混合物制成的小单层囊泡(SUV)中也观察到了类似的相互作用。囊泡(SUV和大单层囊泡)的31P - NMR表明,添加pAntp类似物不会影响磷脂酰胆碱/磷脂酰丝氨酸囊泡的大小。根据酸性脂质的混合物不同,向脂质分散体中添加pAntp类似物会以不同方式调节脂质多态性。
