STIMULATION OR INHIBITION OF THE RESPIRATORY BURST IN CULTURED MACROPHAGES IN A MYCOBACTERIUM MODEL - INITIAL STIMULATION IS FOLLOWED BY INHIBITION AFTER PHAGOCYTOSIS

被引：24

作者：

GORDON, AH ^{[1
]}

HART, PD ^{[1
]}

机构：

[1] NATL INST MED RES,LEPROSY & MYCOBACTERIAL RES LAB,LONDON NW7 1AA,ENGLAND

来源：

INFECTION AND IMMUNITY | 1994年 / 62卷 / 10期

关键词：

D O I：

10.1128/IAI.62.10.4650-4651.1994

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Microorganisms cause varying degrees of stimulation of superoxide (O-2(-)) production (respiratory burst [RB]) in macrophages but in some cases apparently inhibit the RB induced in the same monolayers by a conventional stimulator. We have explored these differences. A mycobacterium model, the slowly multiplying mouse pathogen Mycobacterium microti, induced a modest RB in resident macrophage monolayers, compared with the substantial RB induced by opsonized zymosan (Zy). However, if the 1-h M. microti pulse immediately preceded the Zy assay (instead of being concurrent), the RB was consistently less than that elicited by the Zy alone. Cytochalasin (an inhibitor of phagocytosis) enhanced Zy-induced RB, supporting the view that the burst is cell surface mediated, but his agent apparently eliminated the inhibition of the Zy-induced RB caused by prior M. microti exposure, suggesting that this inhibition may have an intracellular origin. The inhibition described extended not only to another mycobacterium (Mycobacterium bovis BCG) but also to a previous application of Zy itself. The general implications for macrophage functions of these observations on timing and sites of initiation are briefly discussed.

引用

页码：4650 / 4651

页数：2

共 18 条

[1]

ALLISON AC, 1971, NATURE-NEW BIOL, V232, P153

[2]

BRETT SJ, 1988, CLIN EXP IMMUNOL, V71, P32

[3]

BUCHMULLERROUILLER Y, 1987, INFECT IMMUN, V55, P587

[4] MACROPHAGE OXIDATIVE-METABOLISM AND INTRACELLULAR TOXOPLASMA-GONDII [J].

CHANG, HR ;

PECHERE, JC .

MICROBIAL PATHOGENESIS, 1989, 7 (01) :37-44

[5] SURVIVAL AND GROWTH OF YERSINIA-PESTIS WITHIN MACROPHAGES AND AN EFFECT OF THE LOSS OF THE 47-MEGADALTON PLASMID ON GROWTH IN MACROPHAGES [J].

CHARNETZKY, WT ;

SHUFORD, WW .

INFECTION AND IMMUNITY, 1985, 47 (01) :234-241

[6] SUPEROXIDE-DISMUTASE ACTIVITY OF MYCOBACTERIUM-AVIUM COMPLEX (MAC) STRAINS ISOLATED FROM AIDS PATIENTS [J].

DESHPANDE, RG ;

KHAN, MB ;

SAVARIAR, LS ;

WINDHAM, YZ ;

NAVALKAR, RG .

TUBERCLE AND LUNG DISEASE, 1993, 74 (05) :305-309

[7] HISTOPLASMA-CAPSULATUM FAILS TO TRIGGER RELEASE OF SUPEROXIDE FROM MACROPHAGES [J].

EISSENBERG, LG ;

GOLDMAN, WE .

INFECTION AND IMMUNITY, 1987, 55 (01) :29-34

[8] INHIBITION OF PHAGOSOME-LYSOSOME FUSION IN MACROPHAGES BY CERTAIN MYCOBACTERIA CAN BE EXPLAINED BY INHIBITION OF LYSOSOMAL MOVEMENTS OBSERVED AFTER PHAGOCYTOSIS [J].

HART, PD ;

YOUNG, MR ;

GORDON, AH ;

SULLIVAN, KH .

JOURNAL OF EXPERIMENTAL MEDICINE, 1987, 166 (04) :933-946

[9] MYCOBACTERIUM-LEPRAE FAILS TO STIMULATE PHAGOCYTIC CELL SUPEROXIDE ANION GENERATION [J].

HOLZER, TJ ;

NELSON, KE ;

SCHAUF, V ;

CRISPEN, RG ;

ANDERSEN, BR .

INFECTION AND IMMUNITY, 1986, 51 (02) :514-520

[10] GENERATION OF SUPEROXIDE ANION AND CHEMILUMINESCENCE BY HUMAN MONOCYTES DURING PHAGOCYTOSIS AND ON CONTACT WITH SURFACE-BOUND IMMUNOGLOBULIN-G [J].

JOHNSTON, RB ;

LEHMEYER, JE ;

GUTHRIE, LA .

JOURNAL OF EXPERIMENTAL MEDICINE, 1976, 143 (06) :1551-1556

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