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急性白血病患者体内存在高水平的可溶性L-选择素,其可抑制原始细胞与活化内皮细胞的黏附。

High levels of the shed form of L-selectin are present in patients with acute leukemia and inhibit blast cell adhesion to activated endothelium.

作者信息

Spertini O, Callegari P, Cordey A S, Hauert J, Joggi J, von Fliedner V, Schapira M

机构信息

Division of Hematology, University of Lausanne, Switzerland.

出版信息

Blood. 1994 Aug 15;84(4):1249-56.

PMID:7519478
Abstract

L-selectin is expressed by most leukocytes and mediates the initial step of adhesion to vascular endothelium. A feature of this adhesion receptor is to be shed from the cell surface. We report here the presence of high levels of the shed form of L-selectin (sL-selectin) in plasma from patients with acute leukemia. We also show that sL-selectin purified from acute leukemia plasma exhibits functional activity. The mean (+/- 1 SD) plasma level of sL-selectin among 100 healthy individuals was 2.1 +/- 0.7 micrograms/mL. This value was increased (> 2 SD above the mean) in 63% of 58 patients with acute lymphoblastic leukemia (ALL) and 59% of 93 patients with acute myelogenous leukemia ([AML] P < .001). Repeated measurements in 24 patients showed normal-range levels in 16 of 16 patients in complete remission and high levels in eight of eight patients with therapy-resistant acute leukemia or leukemia relapse. Furthermore, elevated sL-selectin levels were detected in cerebrospinal fluid of three patients with ALL suffering from a relapse limited to the central nervous system. Epitope mapping with monoclonal antibodies demonstrated that L-selectin shedding from leukemic blasts was accompanied by conformational changes of its epidermal growth factor-like domain. A functional role for sL-selectin purified from leukemic plasma was supported by its ability to completely inhibit L-selectin-dependent adhesion of blast cells to tumor necrosis factor-alpha (TNF-alpha)-activated endothelium in vitro. These results suggest that sL-selectin may have an important role in the regulation of leukemic cell adhesion to endothelium. In addition, monitoring of the sL-selectin level may be useful for evaluating leukemia activity, in particular for the detection of leukemia relapse.

摘要

L-选择素由大多数白细胞表达,并介导与血管内皮细胞粘附的起始步骤。这种粘附受体的一个特点是可从细胞表面脱落。我们在此报告,急性白血病患者血浆中存在高水平的脱落形式的L-选择素(sL-选择素)。我们还表明,从急性白血病血浆中纯化的sL-选择素具有功能活性。100名健康个体的sL-选择素血浆平均水平(±1标准差)为2.1±0.7微克/毫升。在58例急性淋巴细胞白血病(ALL)患者中的63%以及93例急性髓细胞白血病(AML)患者中的59%,该值升高(高于平均值2个标准差以上)(P<0.001)。对24例患者的重复测量显示,16例完全缓解患者中的16例水平在正常范围内,而8例治疗抵抗性急性白血病或白血病复发患者中的8例水平较高。此外,在3例ALL复发局限于中枢神经系统的患者的脑脊液中检测到sL-选择素水平升高。用单克隆抗体进行表位作图表明,白血病母细胞上L-选择素的脱落伴随着其表皮生长因子样结构域的构象变化。从白血病血浆中纯化的sL-选择素在体外能够完全抑制母细胞与肿瘤坏死因子-α(TNF-α)激活的内皮细胞之间依赖L-选择素的粘附,这支持了其功能作用。这些结果表明,sL-选择素可能在白血病细胞与内皮细胞粘附的调节中起重要作用。此外,监测sL-选择素水平可能有助于评估白血病活性,特别是用于检测白血病复发。

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