Trentin L, Zambello R, Agostini C, Ambrosetti A, Chisesi T, Raimondi R, Bulian P, Pizzolo G, Semenzato G
Padua University School of Medicine, Department of Clinical Medicine, Italy.
Blood. 1990 Apr 1;75(7):1525-30.
Natural killer (NK) cell activity is severely impaired in untreated patients with hairy cell leukemia (HCL). In an attempt to investigate whether this impairment is related to a defect at the target cell binding and/or at the post target cell binding level, we evaluated the peripheral blood mononuclear cells (PBMC) of HCL patients for their ability to: (1) bind and kill K-562 NK-sensitive targets at the single cell binding level; (2) release the NK cytotoxic factor (NKCF) under different in vitro stimuli, including K-562 and phytohemoagglutinin; and (3) kill K-562 targets in a lectin-dependent cellular cytoxicity (LDCC) assay. This study demonstrates that untreated HCL patients' PBMC show a low ability to form conjugates with K-562 targets at the single cell binding level (5.7% +/- 1.0%) with respect to patients studied after treatment (9.3% +/- 1.3%) and controls (15.0% +/- 4.0%); P less than .05 and P less than .001, respectively. A decreased ability to kill the bound target was demonstrated in untreated cases (1.2% +/- 1.1%) versus patients studied after treatment and controls (12.3% +/- 1.6%, 17.0% +/- 3.1% respectively); P less than .001 in both conditions. After activation of effector cells with interleukin-2 (IL-2) in vitro, an increase in the ability of PBMC to form conjugates with K-562 targets and kill the bound target was demonstrated in each group of patients. Moreover, IL-2 was able to increase the cytotoxicity against NK-sensitive targets in all patients tested. Evaluation of NKCF production showed that untreated patients release low levels of NKCF when PBMC were incubated in the presence of K-562 stimulators (1.8% +/- 0.7%) with respect to patients after interferon-alpha (IFN-alpha) therapy (7.6% +/- 2.1%) and controls (12.9% +/- 2.2%); P less than .02 and P less than .001, respectively. When the recognition mechanisms were bypassed by triggering the cells with lectins in an LDCC assay, we demonstrated an increase of the lytic activity in both groups of patients with respect to the baseline values. However, the cytotoxic capacity observed in untreated patients was significantly lower than that observed in subjects after IFN-alpha therapy and controls (P less than .001). These findings suggest that the impaired NK activity observed in patients with HCL is related to defects both at the target and posttarget cell binding levels.
在未经治疗的毛细胞白血病(HCL)患者中,自然杀伤(NK)细胞活性严重受损。为了研究这种损害是否与靶细胞结合缺陷和/或靶细胞结合后水平的缺陷有关,我们评估了HCL患者外周血单个核细胞(PBMC)的以下能力:(1)在单细胞结合水平上结合并杀伤K-562 NK敏感靶细胞;(2)在不同的体外刺激下,包括K-562和植物血凝素,释放NK细胞毒性因子(NKCF);(3)在凝集素依赖性细胞毒性(LDCC)试验中杀伤K-562靶细胞。本研究表明,未经治疗的HCL患者的PBMC在单细胞结合水平上与K-562靶细胞形成结合物的能力较低(5.7%±1.0%),而治疗后研究的患者为(9.3%±1.3%),对照组为(15.0%±4.0%);P分别小于0.05和0.001。未经治疗的病例中杀伤结合靶细胞的能力降低(1.2%±1.1%),而治疗后研究的患者和对照组分别为(12.3%±1.6%,17.0%±3.1%);两种情况下P均小于0.001。在体外用人白细胞介素-2(IL-2)激活效应细胞后,每组患者的PBMC与K-562靶细胞形成结合物并杀伤结合靶细胞的能力均有所增加。此外,IL-2能够增强所有测试患者对NK敏感靶细胞的细胞毒性。对NKCF产生的评估表明,当PBMC在K-562刺激物存在下孵育时,未经治疗的患者释放的NKCF水平较低(1.8%±0.7%),而干扰素-α(IFN-α)治疗后的患者为(
