SUCCINATE-DEPENDENT METABOLISM IN TRYPANOSOMA-CRUZI EPIMASTIGOTES

被引：64

作者：

DENICOLASEOANE, A

RUBBO, H

PRODANOV, E

TURRENS, JF

机构：

[1] UNIV REPUBLICA, SCH MED, DEPT BIOCHEM, MONTEVIDEO 11800, URUGUAY

[2] UNIV SO ALABAMA, COLL ALLIED HLTH, DEPT BIOMED SCI, MOBILE, AL 36688 USA

来源：

MOLECULAR AND BIOCHEMICAL PARASITOLOGY | 1992年 / 54卷 / 01期

关键词：

CARBOHYDRATE METABOLISM; CHAGAS DISEASE; FUMARATE REDUCTASE; HYDROGEN PEROXIDE; RESPIRATORY CHAIN; SUCCINATE; TRYPANOSOMA-CRUZI;

D O I：

10.1016/0166-6851(92)90093-Y

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Trypanosoma cruzi epimastigotes permeabilized with digitonin (65-mu-g (mg protein)-1) to measure mitochondrial respiration were exposed to different substrates. Although none of the NADH-dependent substrates stimulated respiration, succinate supported not only oxygen consumption but also oxidative phosphorylation (respiratory control ratio of 1.9 +/- 0.3) indicating that the mitochondria were coupled. The rate of NADH-dependent oxygen consumption by membrane fractions (9.4 +/- 0.7 nmol min-1 (mg protein)-1) was reduced by 50% upon addition of catalase indicating that the electrons from NADH oxidation reduced oxygen to H2O2. NADH-dependent H2O2 production (16 +/- 1 nmol min-1 (mg protein)-1) was confirmed using cytochrome c peroxidase. This activity was inhibited by fumarate by 70%, suggesting a competition between fumarate and oxygen for the electrons from NADH, probably at the fumarate reductase level. The respiratory chain inhibitor antimycin blocked both respiration by intact cells and succinate-dependent cytochrome c by isolated membranes. No inhibition by antimycin was observed when NADH replaced succinate as an electron donor, indicating that the electrons from NADH oxidation reduced cytochrome c through a different route. Malonate blocked not only succinate-cytochrome c reductase and fumarate reductase, but also intact cell motility. These results suggest that succinate has a central role in the intermediate metabolism of i. cruzi, as it may be used for respiration or excreted to the extracellular space under anaerobic conditions. In addition, 2 potential sources of H2O2 were tentatively identified as: (a) the enzyme fumarate reductase; and (b) a succinate-dependent site, which may be the semiquinone form of Coenzyme Q9, as in mammalian mitochondria.

引用

页码：43 / 50

页数：8

共 30 条

[1] RESPIRATORY CONTROL IN MITOCHONDRIA FROM TRYPANOSOMA-CRUZI
AFFRANCHINO, JL
DETARLOVSKY, MNS
STOPPANI, AOM
[J]. MOLECULAR AND BIOCHEMICAL PARASITOLOGY, 1985, 16 (03) : 289 - 298
[2] MITOCHONDRIAL DEVELOPMENT IN TRYPANOSOMA-BRUCEI-BRUCEI TRANSITIONAL BLOOD-STREAM FORMS
BIENEN, EJ
SARIC, M
POLLAKIS, G
GRADY, RW
CLARKSON, AB
[J]. MOLECULAR AND BIOCHEMICAL PARASITOLOGY, 1991, 45 (02) : 185 - 192
[3] DEFICIENT METABOLIC UTILIZATION OF HYDROGEN-PEROXIDE IN TRYPANOSOMA-CRUZI
BOVERIS, A
SIES, H
MARTINO, EE
DOCAMPO, R
TURRENS, JF
STOPPANI, OM
[J]. BIOCHEMICAL JOURNAL, 1980, 188 (03) : 643 - 648
[4] HYDROGEN-PEROXIDE GENERATION IN TRYPANOSOMA-CRUZI
BOVERIS, A
STOPPANI, AOM
[J]. EXPERIENTIA, 1977, 33 (10): : 1306 - 1308
[5] FUMARATE REDUCTASE AND OTHER MITOCHONDRIAL ACTIVITIES IN TRYPANOSOMA-CRUZI
BOVERIS, A
HERTIG, CM
TURRENS, JF
[J]. MOLECULAR AND BIOCHEMICAL PARASITOLOGY, 1986, 19 (02) : 163 - 169
[6] ROLE OF UBIQUINONE IN MITOCHONDRIAL GENERATION OF HYDROGEN-PEROXIDE
BOVERIS, A
CADENAS, E
STOPPANI, AOM
[J]. BIOCHEMICAL JOURNAL, 1976, 156 (02) : 435 - 444
[7] CELLULAR PRODUCTION OF HYDROGEN-PEROXIDE
BOVERIS, A
CHANCE, B
OSHINO, N
[J]. BIOCHEMICAL JOURNAL, 1972, 128 (03) : 617 - &
[8] THE AEROBIC FERMENTATION OF GLUCOSE BY TRYPANOSOMA-CRUZI
CANNATA, JJB
CAZZULO, JJ
[J]. COMPARATIVE BIOCHEMISTRY AND PHYSIOLOGY B-BIOCHEMISTRY & MOLECULAR BIOLOGY, 1984, 79 (03): : 297 - 308
[9] GLYCOSOMAL AND MITOCHONDRIAL MALATE-DEHYDROGENASES IN EPIMASTIGOTES OF TRYPANOSOMA-CRUZI
CANNATA, JJB
CAZZULO, JJ
[J]. MOLECULAR AND BIOCHEMICAL PARASITOLOGY, 1984, 11 (APR) : 37 - 49
[10] HYDROPEROXIDE METABOLISM IN MAMMALIAN ORGANS
CHANCE, B
SIES, H
BOVERIS, A
[J]. PHYSIOLOGICAL REVIEWS, 1979, 59 (03) : 527 - 605

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