Issue February 2001

category image Volume 18
No. 4 (p 493-646)
February 2001
ISSN 0739-1102

Interactions Between Mastoparan B and the Membrane Studied by 1H NMR Spectroscopy (p. 595-606)

Mastoparan B (MP-B) is an antimicrobial cationic tetradecapeptide amide isolated from the venom of the hornet Vespa basalis. NMR spectroscopy was used to study the membrane associated structures of MP-B in various model membrane systems such as 120 mM DPC micelles, 200 mM SDS micelles, and 3%(w/v) DMPC/DHPC (1:2) bicelles. In all systems, MP-B has an amphiphilic α-helical structure from Lys2 to Leu14. NOESY experiments performed on MP-B in nondeuterated SDS micelles show that protons in the indole ring of Trp9 are in close contact with methylene protons of SDS micelles. T1 relaxation data and NOE data revealed that the bound form of MP-B may be dominant in SDS micelles. The interactions between MP-B and zwitterionic DPC micelles were much weaker than those between MP-B and anionic SDS micelles. By substitution of Trp9 with Ala9 , the pore-forming activity of MP-B was decreased dramatically. All of these results imply that strong electrostatic interactions between the positively charged Lys residues in MP-B and the anionic phospholipid head groups must be the primary factor for MP-B binding to the cell membrane. Then, insertion of the indole ring of Trp9 into the membrane, as well as the amphiphilic α-helical structures of MP-B may allow MP-B to span the lipid bilayer through the C-terminal portion. These structural features are crucial for the potent antibiotic activities of MP-B.

Kyeunghee Yu1
Shinwon Kang2
Sun Don Kim3
Pan Dong Ryu3
Yangmee Kim1*

1Department of Chemistry
Konkuk University
Seoul 143-701, Korea
2Department of Chemistry
Pusan National University
Pusan 609-735, Korea
3Department of Veterinary Pharmacology
College of Veterinary Medicine
Seoul National University
Suwon 441-744, Korea
*ymkim@kkucc.konkuk.ac.kr

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