CCK-58 is the only detectable endocrine form of cholecystokinin in rat

被引：70

作者：

Reeve, JR

Green, GM

Chew, P

Eysselein, VE

Keire, DA

机构：

[1] Vet Affairs Greater Los Angeles Healthcare Syst, Res Serv 151, Digest Dis Res Ctr, Ctr Ulcer Res & Educ, Los Angeles, CA 90073 USA

[2] Univ Calif Los Angeles, Sch Med, Div Digest Dis, Los Angeles, CA 90024 USA

[3] Univ Texas, Hlth Sci Ctr, Dept Physiol, San Antonio, TX 78229 USA

[4] Harbor Univ Los Angeles Med Ctr, Div Gastroenterol, Torrance, CA 90509 USA

来源：

AMERICAN JOURNAL OF PHYSIOLOGY-GASTROINTESTINAL AND LIVER PHYSIOLOGY | 2003年 / 285卷 / 02期

关键词：

pancreas; radioimmunoassay; blood processing; plasma; molecular forms;

D O I：

10.1152/ajpgi.00523.2002

中图分类号：

R57 [消化系及腹部疾病];

学科分类号：

摘要：

CCK-58 differs from CCK-8 in patterns of expression of pancreatic secretion of fluid and amylase and gallbladder contraction. These differences have physiological relevance only if CCK-58 release is stimulated by nutrients entering the intestine and if CCK-58 circulates in sizeable amounts. In this study, we report that when radiolabeled CCK-58 is added to rat blood and plasma is formed, there is extensive loss and degradation of the radioactive peptide. Therefore, a new method was developed to minimize loss and degradation of this label. This method recovered >85% of the label with no detectable degradation. Furthermore, the optimized method recovered all unlabeled exogenous cholecystokinin molecular forms in >80% yields. Blood from fasted rats and rats in which cholecystokinin release was stimulated by the trypsin inhibitor camostat contained only CCK-58 (3.5 +/- 0.5 and 17 +/- 1.5 fmol/ml, respectively). Because CCK-58 predominates in the blood, this molecular form should be used in studieson the physiology and pathophysiology of cholecystokinin.

引用

页码：G255 / G265

页数：11

共 27 条

[1] DETECTION OF CHOLECYSTOKININ-58 IN HUMAN-BLOOD BY INHIBITION OF DEGRADATION [J].

EBERLEIN, GA ;

EYSSELEIN, VE ;

HESSE, WH ;

GOEBELL, H ;

SCHAEFER, M ;

REEVE, JR .

AMERICAN JOURNAL OF PHYSIOLOGY, 1987, 253 (04) :G477-G482

[2] CHOLECYSTOKININ-58 IS THE MAJOR MOLECULAR-FORM IN MAN, DOG AND CAT BUT NOT IN PIG, BEEF AND RAT INTESTINE [J].

EBERLEIN, GA ;

EYSSELEIN, VE ;

GOEBELL, H .

PEPTIDES, 1988, 9 (05) :993-998

[3] PURIFICATION AND SEQUENCING OF A RAT INTESTINAL 22 AMINO-ACID C-TERMINAL CCK FRAGMENT [J].

ENG, J ;

DU, BH ;

PAN, YC ;

CHANG, M ;

HULMES, JD ;

YALOW, RS .

PEPTIDES, 1984, 5 (06) :1203-1206

[4] CHARACTERIZATION OF THE MAJOR FORM OF CHOLECYSTOKININ IN HUMAN INTESTINE - CCK-58 [J].

EYSSELEIN, VE ;

EBERLEIN, GA ;

SCHAEFFER, M ;

GRANDT, D ;

GOEBELL, H ;

NIEBEL, W ;

ROSENQUIST, GL ;

MEYER, HE ;

REEVE, JR .

AMERICAN JOURNAL OF PHYSIOLOGY, 1990, 258 (02) :G253-G260

[5] MOLECULAR VARIANTS OF CHOLECYSTOKININ AFTER ENDOGENOUS STIMULATION IN HUMANS - A TIME STUDY [J].

EYSSELEIN, VE ;

EBERLEIN, GA ;

HESSE, WH ;

SCHAEFFER, M ;

GRANDT, D ;

WILLIAMS, R ;

GOEBELL, H ;

REEVE, JR .

AMERICAN JOURNAL OF PHYSIOLOGY, 1990, 258 (06) :G951-G957

[6] ISOLATION OF A LARGE CHOLECYSTOKININ PRECURSOR FROM CANINE BRAIN [J].

EYSSELEIN, VE ;

REEVE, JR ;

SHIVELY, JE ;

MILLER, C ;

WALSH, JH .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1984, 81 (21) :6565-6568

[7]

EYSSELEIN VE, 1987, J BIOL CHEM, V262, P214

[8]

FOLSCH UR, 1987, GASTROENTEROLOGY, V92, P449

[9] CHOLECYSTOKININ NEURON SYSTEMS AND THEIR INTERACTIONS WITH THE PRESYNAPTIC FEATURES OF THE DOPAMINE NEURON SYSTEMS - A MORPHOMETRIC AND NEUROCHEMICAL ANALYSIS INVOLVING STUDIES ON THE ACTION OF CHOLECYSTOKININ-8 AND CHOLECYSTOKININ-58 [J].

FUXE, K ;

AGNATI, LF ;

VANDERHAEGHEN, JJ ;

TATEMOTO, K ;

ANDERSSON, K ;

ENEROTH, P ;

HARFSTRAND, A ;

VONEULER, G ;

TONI, R ;

GOLDSTEIN, M ;

MUTT, V .

ANNALS OF THE NEW YORK ACADEMY OF SCIENCES, 1985, 448 (JUL) :231-254

[10]

GROSSMAN MI, 1977, FED PROC, V36, P1930

← 1 2 3 →