SOLVENT EFFECTS ON BETA-PROTEIN TOXICITY INVIVO

被引：84

作者：

WAITE, J

COLE, GM

FRAUTSCHY, SA

CONNOR, DJ

THAL, LJ

机构：

[1] VET ADM MED CTR,DEPT NEUROL V-127,3350 LA JOLLA VILLAGE DR,SAN DIEGO,CA 92161

[2] WHITTIER INST,DEPT NEUROSCI,LA JOLLA,CA 92037

[3] WHITTIER INST,DEPT MOLEC & CELLULAR GROWTH BIOL,LA JOLLA,CA 92037

来源：

NEUROBIOLOGY OF AGING | 1992年 / 13卷 / 05期

关键词：

BETA-PROTEIN; BETA-AMYLOID; TOXICITY; INVIVO; RAT;

D O I：

10.1016/0197-4580(92)90062-3

中图分类号：

R592 [老年病学]; C [社会科学总论];

学科分类号：

03 ; 0303 ; 100203 ;

摘要：

Human beta (1-40) and rat beta (1-42) were dissolved in three different solvents and stereotaxically injected into rat hippocampus with the contralateral side injected with control reverse sequence peptide or vehicle alone. Results at 1 week showed gross toxicity of the 35% acetonitrile solvent which was markedly enhanced by 3 nmol of beta protein but not by reverse sequence peptide. Beta peptide in water also appeared more toxic than reverse sequence, but the results were less clear cut. In contrast, 3 nmol of beta peptide in a cyclodextrin/PBS solution produced no marked short-term toxic effects. Peripheral injection of substance P failed to prevent toxicity. We conclude that solvent effects play a major role in acute beta protein neurotoxicity.

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页码：595 / 599

页数：5

相关论文

共 14 条

[1] USE OF 2-HYDROXYPROPYL-BETA-CYCLODEXTRIN AS A SOLUBILIZING AND STABILIZING EXCIPIENT FOR PROTEIN DRUGS [J].

BREWSTER, ME ;

HORA, MS ;

SIMPKINS, JW ;

BODOR, N .

PHARMACEUTICAL RESEARCH, 1991, 8 (06) :792-795

[2] EFFECTS OF INJECTED ALZHEIMER BETA-AMYLOID CORES IN RAT-BRAIN [J].

FRAUTSCHY, SA ;

BAIRD, A ;

COLE, GM .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1991, 88 (19) :8362-8366

[3] MICROSOMAL METABOLISM OF ACETONITRILE TO CYANIDE - EFFECTS OF ACETONE AND OTHER COMPOUNDS [J].

FREEMAN, JJ ;

HAYES, EP .

BIOCHEMICAL PHARMACOLOGY, 1988, 37 (06) :1153-1159

[4] BETA-PLEATED SHEET FIBRILS - COMPARISON OF NATIVE AMYLOID WITH SYNTHETIC PROTEIN FIBRILS [J].

GLENNER, GG ;

EANES, ED ;

BLADEN, HA ;

LINKE, RP ;

TERMINE, JD .

JOURNAL OF HISTOCHEMISTRY & CYTOCHEMISTRY, 1974, 22 (12) :1141-1158

[5]

GOLDBERG MP, 1987, J PHARMACOL EXP THER, V243, P784

[6] BETA-AMYLOID PROTEIN INCREASES THE VULNERABILITY OF CULTURED CORTICAL-NEURONS TO EXCITOTOXIC DAMAGE [J].

KOH, JY ;

YANG, LL ;

COTMAN, CW .

BRAIN RESEARCH, 1990, 533 (02) :315-320

[7] AN INVIVO MODEL FOR THE NEURODEGENERATIVE EFFECTS OF BETA-AMYLOID AND PROTECTION BY SUBSTANCE-P [J].

KOWALL, NW ;

BEAL, MF ;

BUSCIGLIO, J ;

DUFFY, LK ;

YANKNER, BA .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1991, 88 (16) :7247-7251

[8] BETA-AMYLOID PEPTIDES DESTABILIZE CALCIUM HOMEOSTASIS AND RENDER HUMAN CORTICAL-NEURONS VULNERABLE TO EXCITOTOXICITY [J].

MATTSON, MP ;

CHENG, B ;

DAVIS, D ;

BRYANT, K ;

LIEBERBURG, I ;

RYDEL, RE .

JOURNAL OF NEUROSCIENCE, 1992, 12 (02) :376-389

[9] INVITRO AGING OF BETA-AMYLOID PROTEIN CAUSES PEPTIDE AGGREGATION AND NEUROTOXICITY [J].

PIKE, CJ ;

WALENCEWICZ, AJ ;

GLABE, CG ;

COTMAN, CW .

BRAIN RESEARCH, 1991, 563 (1-2) :311-314

[10] AMORPHOUS WATER-SOLUBLE DERIVATIVES OF CYCLODEXTRINS - NONTOXIC DISSOLUTION ENHANCING EXCIPIENTS [J].

PITHA, J ;

PITHA, J .

JOURNAL OF PHARMACEUTICAL SCIENCES, 1985, 74 (09) :987-990