Monocyte-Mediated Suppression of Mitogen Responses of Lymphocytes in Uremic Patients

Our study was designed to see if peritoneal macrophages (PM) of continuous ambulatory peritoneal dialysis (CAPD) uremic patients, by weaking local defense, could contribute to an increase of peritonitis incidence. Coincubation of nonadherent control responding cells (NACRC) and PM from normal subjects or CAPD patients with low peritonitis incidence (LPI) did not modify blastogenic response of cells to PHA. Coincubation of NACRC and PM from CAPD patients with high peritonitis incidence (HPI) produced noticeable decrease in blastogenic response; these PM, unable to produce normal amounts of Interleukin-1 (IL-1), released large amounts of prostaglandin E₂ (PGE₂). CAPD patients with LPI and normal subjects produced both substances in similar amounts. PM of CAPD patients with HPI were less able to kill bacteria than those from normal subjects and CAPD patients with LPI, showing a stronger suppressor effect on local defense. This suppressor activity correlated directly to PGE₂ release and inversely to IL-1 production. We can hypothesize that in some uremic patients, subpopulations of macrophages growing in response to local stimuli produce humoral substances, negatively affecting cellular-mediated defense and favoring elevated bacterial expansion in peritoneum.

Section: Discussionmentioning

confidence: 96%

Suppressor Resident Peritoneal Macrophages and Peritonitis Incidence in Continuous Ambulatory Peritoneal Dialysis

Lamperi¹,

Carozzi²

1986

“…Decreased delayed hypersensitivity (1], decreased OKT4/OKT8 ratio [2] and reduced lymphocyte response to mitogens [1,[3][4][5] have been reported in patients on maintenance HD. A high incidence of neoplasms [6,7] and tuberculosis [8,9] has also been found in uremic patients.…”

Section: Discussionmentioning

confidence: 99%

“…Prostaglandin E2 produced by monocytes has been reported to regulate IL-2 augmentation of NK cell activ ity [25]. Moreover, in uremic patients, the depletion of adherent monocytes from PBMC [3][4][5] and the addition of indomethacin, a cyclooxygenase inhibitor [4], have been reported to restore impaired lymphocyte responses to mitogens. Although the precise mechanism of a poor response of NK cells to 1 L-2 in uremia also remains to be clarified, it is speculated that activated monocytes by uremic toxin(s) produce excessive prostaglandin E2, re sulting in the depressed response of NK cells to IL-2.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Depressed Natural Killer Cell Activity in Uremia

Asaka

Iida

Izumino

et al. 1988

We investigated the natural killer (NK) cell activity of peripheral blood mononuclear cells (PBMC) and the suppressive factor of NK cell activity in patients on maintenance hemodialysis (HD). NK cell activity was significantly lower in patients on HD than in healthy controls (20.2 ± 16.5 vs. 31.0 ± 13.2%, p < 0.01). There was no difference in NK cell activity between patients treated with cuprophane and high-permeability membrane. NK cells from patients on HD showed a poor response to interleukin-2, and uremic sera significantly suppressed NK cell activity of normal PBMC. Although urea, creatinine, methylguanidine or guanidinosuccinic acid alone did not suppress the NK cell activity of normal PBMC, the guanidino compound did so significantly. It is suggested that defective NK cell activity in uremic patients explains in part their susceptibility to malignancy and infection. The immunosuppressive effect may be exhibited by synergism or mosaic of uremic toxins.

“…The mechanisms responsible for this rela tive anergy are unknown but uremic toxins and malnutri tion are the factors more commonly implicated [1][2][3]. Although several alterations of humoral immunity have been reported [1,2,4,5] the uremic immunodeficiency is mostly attributed to a deficiency of cell-mediated immu nity [1,[6][7][8]. Lymphopenia [2], reduced numbers of OKT 4 + cells [9], impaired cell-mediated immune reactions such as unresponsiveness to skin tests [2], prolonged skin graft survival [10], poor graft versus host reaction [4] and a low response to T-dependent mitogens [1,[6][7][8] are some of the alterations that have been described in these pa tients.…”

Section: Introductionmentioning

confidence: 99%

Defective Radioresistant Suppressor Cell Activity in Hemodialysis Patients

Mirapeix¹,

Montolíu²,

Suarez³

et al. 1985

The immunologic alterations in patients on hemodialysis are only partially understood. We studied the Concanavalin A (Con A) induced suppressor cell activity of irradiated and nonirradiated cells in a mixed lymphocyte culture. Peripheral blood lymphocytes from 18 normal individuals and 14 patients on regular hemodialysis were incubated with two different concentrations of Con A (10 µg and 40 µg of Con A/million cells). Irradiated and nonirradiated cells were then tested for their capacity to suppress a standard MLC. The proliferative response to phytohemagglutinin, pokeweed mitogen and Con A was also determined. Suppressor cell activity of nonirradiated cells in hemodialysis patients was similar to that of controls, at both concentrations of Con A, while irradiated cells of hemodialysis patients showed a suppressor cell activity significantly lower than that of the controls, at a Con A concentration of 40 µg/l06 cells (25.78 ± 18.86% vs. 46.05 ± 9.79%, p < 0.001). The proliferative response of lymphocytes from hemodialysis patients to the three mitogens, did not show any difference when compared with normal controls.The normal proliferative response of lymphocytes from hemodialysis patients to mitogens and the normal suppressor cell activity of nonirradiated cells, suggest a normal T cell function. The abnormal suppressor cell activity in irradiated cells indicate that the radioresistant population has a functional defect. The cell responsible for this suppressor defect probably belongs to the monocyte/macrophage population because of its relative radioresistance.