Enhancement of Natural Killer Cell Activity by Nocardia opaca Fractions

Three molecules derived from Nocardia opaca bacteria, NDCM, NWSMP, and PG, have been shown to express immunomodulating properties. The present study was aimed al assessing the effects of these derivatives on natural killer (NK) activity. Two experimental protocols were adopted, consisting of incubat...

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Veröffentlicht in:Scandinavian journal of immunology 1989-02, Vol.29 (2), p.133-141
Hauptverfasser: BAROT‐CIORBARU, R., LINNA, T. J., PATEL, M. R., ALTMAN, J., CARNAUD, C.
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Sprache:eng
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Zusammenfassung:Three molecules derived from Nocardia opaca bacteria, NDCM, NWSMP, and PG, have been shown to express immunomodulating properties. The present study was aimed al assessing the effects of these derivatives on natural killer (NK) activity. Two experimental protocols were adopted, consisting of incubating whole or Percoll fractionated NK cells in vitro with those substances, and the other in which the derivatives were administered in vivo so mice and the activity assessed later. Incubation of spleen cells in vitro with NWSMP or its precursor NDCM promoted NK activity. This effect could be observed after only 2 h of incubation and continued until day 2. Percoll fractions 1–3, which contain most of the NK activity, were enhanced to a similar extent. Band 4, which is usually devoid of such activity, remained unresponsive even after contact with the N. opaca derivatives. PG was practically ineffective upon all the subsets. The results of experiments in vivo correlated with those obtained in vitro in that NWSMP and NDCM, but not PG, promoted NK activity. Bands 1–3 were similarly enhanced, the effect was observed after short treatment times, and could be partially cancelled by the concomitant administration of anti interferon antibodies (anti‐IFN Ab). All these findings suggest that the promoting effects of N. opaca derivatives are mediated through alpha/beta IFN. In contrast to the results observed on spleen NK cells. NK cells from the peritoneum displayed susceptibility mainly to PG, and much less to NWSMP or NDCM. The administration of PG to mice in vivo had a particularly marked promoting effect upon the cytotoxic activity of peritoneal cells. One logical explanation for the difference observed between PG and NWSMP or NDCM may be related to the specific IFN inducing properties of these compounds as well as to die different responsiveness of die NK cells present in the spleen and peritoneal cavity.
ISSN:0300-9475
1365-3083
DOI:10.1111/j.1365-3083.1989.tb01109.x