Abstract
A metabolic pathway of activated macrophages (M phi) involving oxidation of the guanido nitrogens of L-arginine is required for inhibition of growth and respiration of some target cells. The goal of this study was to identify the M phi metabolite(s) that induce these injuries. The stable products of the L-arginine pathway, NO2- and NO3-, were incapable of causing cytostasis under coculture conditions. However, NO2- became cytostatic upon mild acidification, which favors its transformation into nitrogen oxides of greater reactivity. This suggested that NO. (and/or NO2), recently identified as an M phi metabolite of L-arginine, could be a mediator. Authentic NO. caused cytostasis and respiratory inhibition in L1210 cells in a dose-dependent manner. The mitochondrial lesions caused by NO. were confined to complex 1 and 2, a pattern of injury identical to that seen after coculture with activated M phi. Inclusion of NO. scavenger systems prevented cytostasis from developing in M phi-L1210 cocultures. Thus, M phi-generated NO. can account for L-arginine-dependent cytostasis and respiratory inhibition.
Dates
| Type | When |
|---|---|
| Created | 21 years, 2 months ago (June 24, 2004, 3:56 a.m.) |
| Deposited | 2 years, 1 month ago (July 24, 2023, 9:31 p.m.) |
| Indexed | 1 week, 1 day ago (Aug. 23, 2025, 1 a.m.) |
| Issued | 36 years, 3 months ago (May 1, 1989) |
| Published | 36 years, 3 months ago (May 1, 1989) |
| Published Online | 36 years, 3 months ago (May 1, 1989) |
| Published Print | 36 years, 3 months ago (May 1, 1989) |
@article{Stuehr_1989, title={Nitric oxide. A macrophage product responsible for cytostasis and respiratory inhibition in tumor target cells.}, volume={169}, ISSN={1540-9538}, url={http://dx.doi.org/10.1084/jem.169.5.1543}, DOI={10.1084/jem.169.5.1543}, number={5}, journal={The Journal of experimental medicine}, publisher={Rockefeller University Press}, author={Stuehr, D J and Nathan, C F}, year={1989}, month=may, pages={1543–1555} }