Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:3.4.16.2 (
PCP
)
3,761
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
To investigate the potential effects of technical pentachlorophenol (
PCP
-T, contaminated with polychlorinated dioxins and furans) and of analytical grade pentachlorophenol (
PCP
-A) on the human immune system, in vitro assays with freshly prepared human peripheral blood lymphocytes were used as an alternative to experimental animals. Both cell-mediated and humoral immune functions were examined after direct lymphocyte exposure to
PCP
-T or
PCP
-A at concentrations ranging from 0-200 microM. In each case the viability of the treated cells remained within the control value range. T lymphocyte blastogenesis after 3 days incubation with
PCP
was measured using both optimal and suboptimal mitogen (
PHA
) concentration. Interleukin-2 activity of 24.5-h supernatants of lymphocytes in response to
PHA
, pretreated with
PCP
for 20-24 h, was examined in a bioassay using the mouse IL-2-dependent CTLL-6 cell line. The synthesis of immunoglobulins was determined after stimulation with T-dependent (PWM) and T-independent (KlebsM) polyclonal B cell activators. In the proliferation assay the effects of
PCP
-T became more evident after suboptimal mitogen stimulation. Whereas after optimal mitogen stimulation blastogenesis was affected only at the highest concentration of 200 microM
PCP
-T, cell reactivity after suboptimal
PHA
stimulation was altered by all
PCP
-T doses. In the lower concentration range
PCP
-T caused enhanced proliferative responses, but at the two highest
PCP
-T concentrations cell reactivity was significantly suppressed as compared to the medium controls. Significant differences between the effects of
PCP
-T and
PCP
-A could be demonstrated only after optimal mitogen stimulation at the highest
PCP
concentration (200 microM). In contrast, lymphokine production as well as Ig secretion showed severe dose-dependent suppression after exposure to both
PCP
-T and
PCP
-A. The humoral immune response appeared to be more suppressed when cultures were stimulated with T-dependent rather than T-independent mitogens. The two different
PCP
preparations caused immunosuppression of both lymphocyte functions to the same extent. To summarize, the results of our studies indicate that
PCP
itself is directly immunotoxic to human immunocompetent cells and the T helper cell subset appears to be especially sensitive to
PCP
exposure. Furthermore, the observation of a direct effect on humoral immunity is similar to previous results showing considerable alterations of antigen specific antibody production in experimental animals after in vivo exposure.
...
PMID:Human lymphocyte reactivity after in vitro exposure to technical and analytical grade pentachlorophenol. 177 35
