CHROMATOFOCUSING PROFILE OF PURIFIED HUMAN ALPHA-FETOPROTEIN AND ALBUMIN DIFFERS FROM THOSE OF CRUDE SAMPLES - EFFECT OF PROTEIN-CONCENTRATION ON THE ELUTION OF THE SAMPLE

被引：5

作者：

LEAL, JA ^{[1
]}

EDDY, KB ^{[1
]}

KEEL, BA ^{[1
]}

机构：

[1] UNIV KANSAS,SCH MED,WOMENS RES INST,DEPT OBSTET & GYNECOL,2903 E CENT,WICHITA,KS 67214

来源：

ANALYTICAL BIOCHEMISTRY | 1991年 / 192卷 / 02期

关键词：

D O I：

10.1016/0003-2697(91)90557-A

中图分类号：

Q5 [生物化学];

学科分类号：

071010 ; 081704 ;

摘要：

Chromatofocusing was utilized to characterize charge microheterogeneity of purified human α-fetoprotein (AFP) and human serum albumin (HSA). Crude cord blood samples yielded three isoforms: AFP-IA, IB, and II, with pIs 4,57 (52%), 4,27 (43%), and <4,00 (5%), respectively. In contrast, 10 μg of purified AFP or 250,000 cpm of 125I-AFP eluted entirely as isoform AFP-II. 125I-AFP focused in the presence of crude cord blood, amniotic fluid, adult male serum, or 25 mg purified HSA resulted in elution profiles similar to those of crude cord blood. Pure AFP focused along with 0.1, 1.0, 5.0, or 10 mg HSA showed a gradual shift from AFP-II to AFP-I. With ≥5 mg HSA, isoform I was further resolve into AFP-IA and IB. Similarly, 250,000 cpm of 125I-HSA, which also eluted entirely as isoform II, showed a gradual shift to isoform I when increasing concentrations of unlabeled HSA were added. The resolution of isoform HSA-I in HSA-IA, IB, and IC was again improved with ≥5 mg unlabeled HSA. When carrier proteins of varying pI values were chromatofocused along with purified AFP, it was observed that only those proteins withpIs in the range of AFP caused significant alteration in the relative distribution of AFP. We conclude that sample protein concentration and composition must be carefully considered when chromatofocusing is being used for purified samples and when the elution profiles of samples from different origins and varying protein concentrations are being compared. © 1991.

引用

页码：411 / 418

页数：8

共 19 条

[1] ON THE HETEROGENEITY OF SERUM-ALBUMIN [J].

DARCEL, CL .

INTERNATIONAL JOURNAL OF BIOCHEMISTRY, 1987, 19 (04) :295-301

[2] FAST CHROMATOFOCUSING OF HUMAN-SERUM PROTEINS WITH SPECIAL REFERENCE TO ALPHA-1-ANTITRYPSIN AND GC-GLOBULIN [J].

FAGERSTAM, LG ;

LIZANA, J ;

AXIOFREDRIKSSON, UB ;

WAHLSTROM, L .

JOURNAL OF CHROMATOGRAPHY, 1983, 266 (AUG) :523-532

[3] CHARACTERIZATION OF RAT LUTROPIN CHARGE MICROHETEROGENEITY USING CHROMATOFOCUSING [J].

KEEL, BA ;

GROTJAN, HE .

ANALYTICAL BIOCHEMISTRY, 1984, 142 (02) :267-270

[4] CHARACTERIZATION OF HUMAN ALPHA-FETOPROTEIN CHARGE MICROHETEROGENEITY DURING FETAL DEVELOPMENT [J].

KEEL, BA ;

HARMS, RL ;

LEAL, JA ;

CHO, SC .

MOLECULAR REPRODUCTION AND DEVELOPMENT, 1990, 27 (04) :281-287

[5] CHARGE MICROHETEROGENEITY OF OVINE FOLLICLE-STIMULATING-HORMONE IN RAMS AND STEROID-TREATED WETHERS [J].

KEEL, BA ;

SCHANBACHER, BD .

BIOLOGY OF REPRODUCTION, 1987, 37 (04) :786-796

[6]

KEEL BA, 1989, MICROHETEROGENEITY G, P149

[7]

KEEL BA, 1989, MICROHETEROGENEITY G

[8]

KEEL BA, 1989, BIOL ACTIVITIES ALPH, V2, P23

[9]

LEAL JA, 1990, IN PRESS J MED PRIMA

[10] HETEROGENEITY OF HUMAN ALPHA-FETOPROTEIN AS REVEALED BY ISOELECTRIC-FOCUSING IN UREA-CONTAINING GELS [J].

LESTER, EP ;

MILLER, JB ;

YACHNIN, S .

BIOCHIMICA ET BIOPHYSICA ACTA, 1978, 536 (01) :165-171

← 1 2 →