The role of phosphometabolites in cell proliferation, energy metabolism, and tumor therapy

被引：139

作者：

Mazurek, S ^{[1
]}

Boschek, CB ^{[1
]}

Eigenbrodt, E ^{[1
]}

机构：

[1] UNIV GIESSEN, FAC MED, INST MED VIROL, GIESSEN, GERMANY

来源：

JOURNAL OF BIOENERGETICS AND BIOMEMBRANES | 1997年 / 29卷 / 04期

关键词：

glycolysis; pyruvate kinase type M-2; glutaminolysis; hydrogen shuttles; phosphometabolites; AMP; NADH; NADPH; apoptosis; tumor therapy;

D O I：

10.1023/A:1022490512705

中图分类号：

Q6 [生物物理学];

学科分类号：

071011 ;

摘要：

A common characteristic of tumor cells is the constant overexpression of glycolytic and glutaminolytic enzymes. In tumor cells the hyperactive hexokinase and the partly inactive pyruvate kinase lead to an expansion of all phosphometabolites from glucose 6-phosphate to phosphoenolpyruvate. In addition to the glycolytic phosphometabolites, synthesis of their metabolic derivatives such as P-ribose-PP, NADH, NADPH, UTP, CTP, and UDP-N-acetyl glucosamine is also enhanced during cell proliferation. Another phosphometabolite derived from P-ribose-PP, AMP, inhibits cell proliferation. The accumulation of AMP inhibits both P-ribose-PP-synthetase and the increase in concentration of phosphometabolites derived from P-ribose-PP. In cells with low glycerol 3-phosphate and malate-aspartate shuttle capacities the inhibition of the lactate dehydrogenase by low NADH levels leads to an inhibition of glycolytic ATP production. Several tumor-therapeutic drugs reduce NAD and NADH levels, thereby inhibiting glycolytic energy production. The role of AMP, NADH, and NADPH levels in the success of chemotherapeutic treatment is discussed.

引用

页码：315 / 330

页数：16

共 213 条

[111]

LILLIE JW, 1993, CANCER RES, V53, P3172

[112] Mimosine targets serine hydroxymethyltransferase [J].

Lin, HB ;

Falchetto, R ;

Mosca, PJ ;

Shabanowitz, J ;

Hunt, DF ;

Hamlin, JL .

JOURNAL OF BIOLOGICAL CHEMISTRY, 1996, 271 (05) :2548-2556

[113] THE BIOSYNTHETIC-PATHWAY OF PYRIMIDINE (DEOXY)NUCLEOTIDES - A SENSOR OF OXYGEN-TENSION NECESSARY FOR MAINTAINING CELL-PROLIFERATION [J].

LOFFLER, M .

EXPERIMENTAL CELL RESEARCH, 1989, 182 (02) :673-680

[114] EVIDENCE FOR THE OXIDATION OF GLYCOLYTIC NADH BY THE MALATE-ASPARTATE SHUTTLE IN EHRLICH ASCITES TUMOR-CELLS [J].

LOPEZALARCON, L ;

EBOLI, ML ;

LIBERALI, ED ;

PALOMBINI, G ;

GALEOTTI, T .

ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS, 1979, 192 (02) :391-395

[115] REQUIREMENT OF AN ICE/CED-3 PROTEASE FOR FAS/APO-1-MEDIATED APOPTOSIS [J].

LOS, M ;

VANDECRAEN, M ;

PENNING, LC ;

SCHENK, H ;

WESTENDORP, M ;

BAEUERLE, PA ;

DROGE, W ;

KRAMMER, PH ;

FIERS, W ;

SCHULZEOSTHOFF, K .

NATURE, 1995, 375 (6526) :81-83

[116]

LYON RC, 1988, CANCER RES, V48, P870

[117]

MACDONALD MJ, 1990, CANCER RES, V50, P7203

[118] BIOCHEMICAL AND GENETIC-CHARACTERIZATION OF RESPIRATION-DEFICIENT MUTANTS OF CHINESE-HAMSTER CELLS WITH A GAL- PHENOTYPE [J].

MAITI, IB ;

DESOUZA, AC ;

THIRION, JP .

SOMATIC CELL GENETICS, 1981, 7 (05) :567-582

[119] SELECTION OF CARCINOGEN-ALTERED RAT TRACHEAL EPITHELIAL-CELLS PREEXPOSED TO 7,12-DIMETHYLBENZ[A]ANTHRACENE BY THEIR LOSS OF A NEED FOR PYRUVATE TO SURVIVE IN CULTURE [J].

MARCHOK, AC ;

HUANG, SF ;

MARTIN, DH .

CARCINOGENESIS, 1984, 5 (06) :789-796

[120] DNA DAMAGE, POLY (ADP-RIBOSYL)ATION AND APOPTOTIC CELL-DEATH AS A POTENTIAL COMMON PATHWAY OF CYTOTOXIC DRUG-ACTION [J].

MARKS, DI ;

FOX, RM .

BIOCHEMICAL PHARMACOLOGY, 1991, 42 (10) :1859-1867

← 7 8 9 10 11 12 13 14 15 16 →