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膜流动性对肌浆网Ca2+泵活性的调节作用。

Modulation of sarcoplasmic reticulum Ca2+-pump activity by membrane fluidity.

作者信息

Almeida L M, Vaz W L, Zachariasse K A, Madeira V M

出版信息

Biochemistry. 1984 Sep 25;23(20):4714-20. doi: 10.1021/bi00315a029.

DOI:10.1021/bi00315a029
PMID:6238620
Abstract

Intramolecular excimerization of 1,3-di-1-pyrenylpropane [Py(3)Py] was used to assess the fluidity of sarcoplasmic reticulum membranes (SR); on the basis of the spectral data, the probe incorporates completely inside the membrane probably somewhere close to the polar head groups of phospholipid molecules, however not in the very hydrophobic core. The excimerization rate is very sensitive to lipid phase transitions, as revealed by thermal profiles of dimyristoyl-phosphatidylcholine (DMPC) and dipalmitoylphosphatidylcholine (DPPC) bilayers. Cholesterol abolishes pretransitions and broadens the thermal profiles of the main transitions which vanish completely at 50 mol % sterol. Excimer formation in liposomes of SR total lipid extracts does not show any sharp transitions, as in the case of DMPC and DPPC. However, the plots display discontinuities at about 20 degrees C which are broadened by cholesterol and not observed at 50 mol % sterol. Also cholesterol has been incorporated in native SR membranes by an exchange technique allowing progressive enrichment without changing the phospholipid/protein molar ratio. As in liposomes, discontinuities of excimer formation at 20 degrees C are broadened by cholesterol enrichment. The full activity of uncoupled Ca2+-ATPase is only affected by cholesterol above a molar ratio to phospholipid of 0.4. However, a significant decrease in activity (about 20%) is only noticed at a ratio of 0.6 (the highest technically achieved); at this ratio, about 28 lipid molecules per Ca2+-ATPase are expected to be relatively free from cholesterol interaction. The vesicle structure is still intact at this high ratio, as judged from the absence of basal activity (not Ca2+ stimulated).(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

1,3 - 二 - 1 - 芘基丙烷[Py(3)Py]的分子内激基缔合物形成被用于评估肌浆网膜(SR)的流动性;根据光谱数据,该探针完全嵌入膜内,可能靠近磷脂分子的极性头部基团,但不在非常疏水的核心区域。激基缔合物形成速率对脂质相变非常敏感,这在二肉豆蔻酰磷脂酰胆碱(DMPC)和二棕榈酰磷脂酰胆碱(DPPC)双层膜的热谱图中有所体现。胆固醇消除了预转变,并拓宽了主要转变的热谱图,当甾醇含量达到50摩尔%时,主要转变完全消失。SR总脂质提取物脂质体中的激基缔合物形成没有显示出任何尖锐的转变,如同DMPC和DPPC的情况。然而,图谱在约20℃处显示出不连续性,这些不连续性会因胆固醇而变宽,在50摩尔%甾醇时未观察到。此外,通过交换技术将胆固醇掺入天然SR膜中,可实现逐步富集而不改变磷脂/蛋白质摩尔比。与脂质体情况一样,20℃时激基缔合物形成的不连续性会因胆固醇富集而变宽。未偶联的Ca2 + - ATP酶的完全活性仅在胆固醇与磷脂的摩尔比高于0.4时受到影响。然而,仅在比例为0.6(技术上能达到的最高比例)时才注意到活性有显著下降(约20%);在此比例下,预计每个Ca2 + - ATP酶约有28个脂质分子相对不受胆固醇相互作用的影响。从无基础活性(未受Ca2 + 刺激)判断,在此高比例下囊泡结构仍然完整。(摘要截断于250字)

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