ASSIGNMENT OF DISULFIDE BONDS IN SYNTHETIC ENDOTHELIN-1 ISOMERS BY FAST-ATOM-BOMBARDMENT MASS-SPECTROMETRY

被引：9

作者：

ISHIBASHI, Y

KIKUCHI, T

WAKIMASU, M

MIZUTA, E

FUJINO, M

机构：

[1] Tsukuba Research Laboratories, Takeda Chemical Industries Ltd, Tsukuba, Ibaraki, 300-42

来源：

BIOLOGICAL MASS SPECTROMETRY | 1991年 / 20卷 / 11期

关键词：

D O I：

10.1002/bms.1200201109

中图分类号：

Q6 [生物物理学];

学科分类号：

071011 ;

摘要：

Endothelin-1 (ET-1), a 21-residue vasoconstrictor peptide possessing four cysteinyl residues at positions 1, 3, 11 and 15, was synthesized by random oxidation of a tetrahydro-ET-1. On reverse-phase high-performance liquid chromatography, crude product was shown to be a mixture of two disulphide isomers. A method was developed to determine the disulphide structure of the isomers. The method consisted of (a) limited digestion with chymotrypsin, (b) cleavage with cyanogen bromide and (c) manual Edman degradation. Through this procedure, each isomer afforded specific fragments containing a single disulphide bond, which were identified by fast atom bombardment mass spectrometry. Isomer 1, the minor component, afforded a fragment containing Cys 3 and Cys 15, and isomer 2, the major component, afforded fragments containing Cys 3 and Cys 11. Since little disulphide exchange was observed, it could be concluded clearly that the disulphide bond pairs in isomer 1 were Cys 1-Cys 11 and Cys 3-Cys 15, while those in isomer 2 were Cys 1-Cys 15 and Cvs 3-Cys 11 (the same as natural ET-1). The procedure was successfully applied to two synthetic analogues, [Gly18]-ET-1 and [Pro16]-ET-1.

引用

页码：703 / 708

页数：6

共 12 条

[1] A DETERMINATION OF THE POSITIONS OF DISULFIDE BONDS IN PAIM-I, ALPHA-AMYLASE INHIBITOR FROM STREPTOMYCES-CORCHORUSHII, USING FAST ATOM BOMBARDMENT MASS-SPECTROMETRY
AKASHI, S
HIRAYAMA, K
SEINO, T
OZAWA, S
FUKUHARA, K
OOUCHI, N
MURAI, A
ARAI, M
MURAO, S
TANAKA, K
NOJIMA, I
[J]. BIOMEDICAL AND ENVIRONMENTAL MASS SPECTROMETRY, 1988, 15 (10): : 541 - 546
[2] KITADA C, 1991, PEPTIDE CHEMISTRY 1990, P405
[3] KUMAGAYE SI, 1988, INT J PEPT PROT RES, V32, P519
[4] A NEW METHOD FOR RAPID ASSIGNMENT OF S-S BRIDGES IN PROTEINS
MORRIS, HR
PUCCI, P
[J]. BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1985, 126 (03) : 1122 - 1128
[5] LOCATION OF DISULFIDE BONDS IN HUMAN INSULIN-LIKE GROWTH-FACTORS (IGFS) SYNTHESIZED BY RECOMBINANT DNA TECHNOLOGY
RASCHDORF, F
DAHINDEN, R
MAERKI, W
RICHTER, WJ
MERRYWEATHER, JP
[J]. BIOMEDICAL AND ENVIRONMENTAL MASS SPECTROMETRY, 1988, 16 (1-12): : 3 - 8
[6] SEQUENCING OF PEPTIDE MIXTURES BY EDMAN DEGRADATION AND FIELD-DESORPTION MASS-SPECTROMETRY
SHIMONISHI, Y
HONG, YM
KITAGISHI, T
MATSUO, T
MATSUDA, H
KATAKUSE, I
[J]. EUROPEAN JOURNAL OF BIOCHEMISTRY, 1980, 112 (02): : 251 - 264
[7] STRATEGIES FOR LOCATING DISULFIDE BONDS IN PROTEINS
SMITH, DL
ZHOU, ZR
[J]. METHODS IN ENZYMOLOGY, 1990, 193 : 374 - 389
[8] TAKAO T, 1984, J BIOL CHEM, V259, P6105
[9] FAST ATOM BOMBARDMENT (FAB) MASS-SPECTRA OF PROTEIN DIGESTS - HEN AND DUCK EGG-WHITE LYSOZYMES
TAKAO, T
YOSHIDA, M
HONG, YM
AIMOTO, S
SHIMONISHI, Y
[J]. BIOMEDICAL MASS SPECTROMETRY, 1984, 11 (11): : 549 - 556
[10] CALIBRATION IN POSITIVE AND NEGATIVE-ION FAST ATOM BOMBARDMENT USING SALT MIXTURES
VEKEY, K
[J]. ORGANIC MASS SPECTROMETRY, 1989, 24 (03): : 183 - 185

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