PREDOMINANT ABNORMALITY IN CEREBRAL GLUCOSE-UTILIZATION IN LATE-ONSET DEMENTIA OF THE ALZHEIMER TYPE - A CROSS-SECTIONAL COMPARISON AGAINST ADVANCED LATE-ONSET AND INCIPIENT EARLY-ONSET CASES

被引：147

作者：

HOYER, S ^{[1
]}

NITSCH, R ^{[1
]}

OESTERREICH, K ^{[1
]}

机构：

[1] UNIV HEIDELBERG,PSYCHIAT CLIN,W-6900 HEIDELBERG,GERMANY

来源：

JOURNAL OF NEURAL TRANSMISSION-PARKINSONS DISEASE AND DEMENTIA SECTION | 1991年 / 3卷 / 01期

关键词：

GLUCOSE UTILIZATION; DEMENTIA OF ALZHEIMER TYPE; LATE-ONSET; BRAIN INSULIN; INSULIN RECEPTOR;

D O I：

10.1007/BF02251132

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

Global cerebral blood flow and the cerebral metabolic rates of oxygen, CO2, glucose and lactate were studied in 11 patients aged 61-78 years who had been clinically diagnosed as suffering from incipient late-onset dementia of the Alzheimer type (DAT), and in 7 patients aged 66-83 years, in whom advanced late-onset DAT had been diagnosed, using the Kety-Schmidt technique. In incipient late-onset DAT, the predominant abnormality was a 45% reduction in cerebral glucose utilization, whereas cerebral blood flow and the cerebral metabolic rate of oxygen were diminished by only 17% and 18%, respectively. A severe imbalance between oxygen utilization and glucose utilization thus became obvious. In contrast, in advanced stages of late-onset DAT, this imbalance between oxygen and glucose utilization rates in the brain became smaller and smaller, and cerebral blood flow diminished markedly; these biological brain parameters finally all settled down at between 55% and 65% of the corresponding control values. The predominant abnormality in brain glucose utilization in incipient late-onset DAT may be associated with an impairment of its control mechanism(s), which are assumed to be either an influence of brain insulin action, or brain insulin receptor function, or both.

引用

页码：1 / 14

页数：14

共 55 条

[1] *DIE MESSUNG DER HIRNDURCHBLUTUNG MIT DER STICKOXYDULMETHODE [J].

BERNSMEIER, A ;

SIEMONS, K .

PFLUGERS ARCHIV FUR DIE GESAMTE PHYSIOLOGIE DES MENSCHEN UND DER TIERE, 1953, 258 (02) :149-162

[2] INDUCTION OF ALZHEIMER ANTIGENS BY AN UNCOUPLER OF OXIDATIVE-PHOSPHORYLATION [J].

BLASS, JP ;

BAKER, AC ;

KO, LW ;

BLACK, RS .

ARCHIVES OF NEUROLOGY, 1990, 47 (08) :864-869

[3] BIOCHEMICAL-STUDIES OF NERVE-CELLS AND ENERGY-METABOLISM IN ALZHEIMERS-DISEASE [J].

BOWEN, DM ;

DAVISON, AN .

BRITISH MEDICAL BULLETIN, 1986, 42 (01) :75-80

[4]

BOWEN DM, 1979, LANCET, V1, P11

[5] CHEMICAL PATHOLOGY OF ORGANIC DEMENTIAS .2. QUANTITATIVE ESTIMATION OF CELLULAR CHANGES IN POSTMORTEM BRAINS [J].

BOWEN, DM ;

SMITH, CB ;

WHITE, P ;

FLACK, RHA ;

CARRASCO, LH ;

GEDYE, JL ;

DAVISON, AN .

BRAIN, 1977, 100 (SEP) :427-453

[6]

BROER Y, 1987, CR ACAD SCI III-VIE, V304, P31

[7] RELATIONSHIPS OF SENILE MANIFESTATIONS AND CHRONIC BRAIN SYNDROMES TO CEREBRAL-CIRCULATION AND METABOLISM [J].

BUTLER, RN ;

DASTUR, DK ;

PERLIN, S .

JOURNAL OF PSYCHIATRIC RESEARCH, 1965, 3 (04) :229-238

[8] CEREBRAL BLOOD-FLOW AND METABOLISM IN NORMAL HUMAN AGING, PATHOLOGICAL AGING, AND SENILE DEMENTIA [J].

DASTUR, DK .

JOURNAL OF CEREBRAL BLOOD FLOW AND METABOLISM, 1985, 5 (01) :1-9

[9] POSITRON EMISSION TOMOGRAPHY STUDIES OF NORMAL AGING - A REPLICATION OF PET-III AND 18-FDG USING PET-VI AND 11-CDG [J].

DELEON, MJ ;

GEORGE, AE ;

TOMANELLI, J ;

CHRISTMAN, D ;

KLUGER, A ;

MILLER, J ;

FERRIS, SH ;

FOWLER, J ;

BRODIE, JD ;

VANGELDER, P ;

KLINGER, A ;

WOLF, AP .

NEUROBIOLOGY OF AGING, 1987, 8 (04) :319-323

[10] TRANSMISSION AND AGE-AT-ONSET PATTERNS IN FAMILIAL ALZHEIMERS-DISEASE - EVIDENCE FOR HETEROGENEITY [J].

FARRER, LA ;

MYERS, RH ;

CUPPLES, LA ;

GEORGEHYSLOP, PHS ;

BIRD, TD ;

ROSSOR, MN ;

MULLAN, MJ ;

POLINSKY, R ;

NEE, L ;

HESTON, L ;

VAN BROECKHOVEN, C ;

MARTIN, JJ ;

CRAPPERMCLACHLAN, D ;

GROWDON, JH .

NEUROLOGY, 1990, 40 (03) :395-403

← 1 2 3 4 5 6 →