共 20 条
A SYNTHETIC ANALOG OF MELITTIN AGGREGATES IN LARGE OLIGOMERS
被引:15
作者:

JOHN, E
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MAX PLANCK INST BIOL,MEMBRANBIOCHEM ABT,CORRENSSTR 38,W-7400 TUBINGEN,GERMANY MAX PLANCK INST BIOL,MEMBRANBIOCHEM ABT,CORRENSSTR 38,W-7400 TUBINGEN,GERMANY

JAHNIG, F
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MAX PLANCK INST BIOL,MEMBRANBIOCHEM ABT,CORRENSSTR 38,W-7400 TUBINGEN,GERMANY MAX PLANCK INST BIOL,MEMBRANBIOCHEM ABT,CORRENSSTR 38,W-7400 TUBINGEN,GERMANY
机构:
[1] MAX PLANCK INST BIOL,MEMBRANBIOCHEM ABT,CORRENSSTR 38,W-7400 TUBINGEN,GERMANY
关键词:
D O I:
10.1016/S0006-3495(92)81737-X
中图分类号:
Q6 [生物物理学];
学科分类号:
071011 ;
摘要:
An analogue of melittin synthesized in the group of E. T. Kaiser (DeGrado, W. F., F. J. Kezdy, and E. T. Kaiser. 1981. J. Am. Chem. Soc. 103:679-681 ) was investigated by Raman spectroscopy and fluorescence anisotropy decay. In water, the analogue is completely alpha-helical and aggregates in large oligomers of about 50 monomers. In vesicle membranes, it undergoes orientational fluctuations similar to melittin. The most significant difference from melittin, therefore, is the formation of straight helixes and their aggregation in large oligomers in water. We interpret this as a consequence of the lacking proline residue in the analogue. We, furthermore, hypothesize that the increased tendency for aggregation causes the increased hemolytic activity of the analogue.
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页码:1536 / 1543
页数:8
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共 20 条
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JAHNIG, F
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机构: Max-Planck-Institut für Biologie, Abteilung Membranbiochemie, Tübingen, D 7400