Trypanosoma-Brucei is Protected from the Cytostaic Effects of Nitric Oxide Under In-Vivo Conditions

N A  Mabbott; I A  Sutherland; Jeremy M Sternberg

Trypanosoma-Brucei is Protected from the Cytostaic Effects of Nitric Oxide Under In-Vivo Conditions

N A Mabbott, I A Sutherland, Jeremy M Sternberg

Aberdeen Centre For Environmental Sustainability

Research output: Contribution to journal › Article › peer-review

Abstract

In mice infected with Trypanosoma brucei, splenic and peritoneal macrophages release substantial amounts of nitric oxide (NO). The production of NO by activated macrophages has been reported to be a nonspecific immune-effector mechansism against several parasites, and in this work we investigate the role of NO in killing T. brucei. Addition of bloodstream trypanosomes to peritoneal macrophages activated in vitro resulted in an NO-dependent inhibition of parasite growth. This effect was totally abrogated when dilutions of whole blood were included in the cultures, suggesting that bloodstream parasites such as T. brucei are not susceptible to NO-mediated killing in vivo.

Original language	English
Pages (from-to)	687-690
Number of pages	4
Journal	Parasitology Research
Volume	80
Issue number	8
Publication status	Published - Nov 1994

Keywords

ACTIVATED MACROPHAGES
L-ARGININE
MURINE MACROPHAGES
GAMMA-INTERFERON
RHODESIENSE
INHIBITION
METABOLISM
GAMBIENSE
RELEASE
PATHWAY

Cite this

@article{671a33b2a85b48569b0424029eb022bc,

title = "Trypanosoma-Brucei is Protected from the Cytostaic Effects of Nitric Oxide Under In-Vivo Conditions",

abstract = "In mice infected with Trypanosoma brucei, splenic and peritoneal macrophages release substantial amounts of nitric oxide (NO). The production of NO by activated macrophages has been reported to be a nonspecific immune-effector mechansism against several parasites, and in this work we investigate the role of NO in killing T. brucei. Addition of bloodstream trypanosomes to peritoneal macrophages activated in vitro resulted in an NO-dependent inhibition of parasite growth. This effect was totally abrogated when dilutions of whole blood were included in the cultures, suggesting that bloodstream parasites such as T. brucei are not susceptible to NO-mediated killing in vivo.",

keywords = "ACTIVATED MACROPHAGES, L-ARGININE, MURINE MACROPHAGES, GAMMA-INTERFERON, RHODESIENSE, INHIBITION, METABOLISM, GAMBIENSE, RELEASE, PATHWAY",

author = "Mabbott, {N A} and Sutherland, {I A} and Sternberg, {Jeremy M}",

year = "1994",

month = nov,

language = "English",

volume = "80",

pages = "687--690",

journal = "Parasitology Research",

issn = "0932-0113",

publisher = "Springer Verlag",

number = "8",

}

TY - JOUR

T1 - Trypanosoma-Brucei is Protected from the Cytostaic Effects of Nitric Oxide Under In-Vivo Conditions

AU - Mabbott, N A

AU - Sutherland, I A

AU - Sternberg, Jeremy M

PY - 1994/11

Y1 - 1994/11

N2 - In mice infected with Trypanosoma brucei, splenic and peritoneal macrophages release substantial amounts of nitric oxide (NO). The production of NO by activated macrophages has been reported to be a nonspecific immune-effector mechansism against several parasites, and in this work we investigate the role of NO in killing T. brucei. Addition of bloodstream trypanosomes to peritoneal macrophages activated in vitro resulted in an NO-dependent inhibition of parasite growth. This effect was totally abrogated when dilutions of whole blood were included in the cultures, suggesting that bloodstream parasites such as T. brucei are not susceptible to NO-mediated killing in vivo.

AB - In mice infected with Trypanosoma brucei, splenic and peritoneal macrophages release substantial amounts of nitric oxide (NO). The production of NO by activated macrophages has been reported to be a nonspecific immune-effector mechansism against several parasites, and in this work we investigate the role of NO in killing T. brucei. Addition of bloodstream trypanosomes to peritoneal macrophages activated in vitro resulted in an NO-dependent inhibition of parasite growth. This effect was totally abrogated when dilutions of whole blood were included in the cultures, suggesting that bloodstream parasites such as T. brucei are not susceptible to NO-mediated killing in vivo.

KW - ACTIVATED MACROPHAGES

KW - L-ARGININE

KW - MURINE MACROPHAGES

KW - GAMMA-INTERFERON

KW - RHODESIENSE

KW - INHIBITION

KW - METABOLISM

KW - GAMBIENSE

KW - RELEASE

KW - PATHWAY

M3 - Article

SN - 0932-0113

VL - 80

SP - 687

EP - 690

JO - Parasitology Research

JF - Parasitology Research

IS - 8

ER -

Trypanosoma-Brucei is Protected from the Cytostaic Effects of Nitric Oxide Under In-Vivo Conditions

Abstract

Keywords

Fingerprint

Cite this