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破骨细胞细胞形态测定显示B细胞恶性肿瘤中有异常细胞群,而多发性骨髓瘤中则没有。

Osteoclast cytomorphometry demonstrates an abnormal population in B cell malignancies but not in multiple myeloma.

作者信息

Chappard D, Rossi J F, Bataille R, Alexandre C

机构信息

LBTO--Laboratoire de Biologie du Tissu Osseux, Faculté de Médecine, Saint Etienne, France.

出版信息

Calcif Tissue Int. 1991 Jan;48(1):13-7. doi: 10.1007/BF02555791.

DOI:10.1007/BF02555791
PMID:1706639
Abstract

Increased bone resorption in the vicinity of myeloma cells is mediated by local stimulating factors. Other malignancies of the B cell lineage are also able to produce resorbing factors responsible for increased bone resorption. We have studied three groups of subjects: 10 patients with overt multiple myeloma, 10 patients with a B cell malignancy, and 10 healthy human subjects as controls. Patients were studied at the time of diagnosis and had a transiliac bone biopsy. Osteoclasts were evident on histological sections by their acid phosphatase activity. A software was developed on an automatic image analyzer (Leitz TAS+) for measuring the maximal Feret's diameter (Oc.Le) of each osteoclast (corresponding to the osteoclast length). The histogram of Oc.Le frequency distribution was supplied in each group. In myeloma patients, the Oc.Le frequency distribution was similar to that in normal subjects and showed the histogram to be asymetric with a positive skew (maximum peak at 20-25 microns). With a graphical analysis, this distribution was shown to follow a lognormal distribution corresponding to a homogeneous osteoclast population. In other B cell malignancies, Oc.Le displayed a bimodal distribution with a peak at 20-25 microns and a lower peak at 10-15 microns. The graphical analysis showed that small (mononucleated?) osteoclasts are present in B cell malignancies with normal osteoclasts. This might reflect the secretion of different soluble factors by malignant cells of the B lymphocyte lineage.

摘要

骨髓瘤细胞附近骨吸收增加是由局部刺激因子介导的。B细胞系的其他恶性肿瘤也能够产生导致骨吸收增加的吸收因子。我们研究了三组对象:10例显性多发性骨髓瘤患者、10例B细胞恶性肿瘤患者以及10名健康人体作为对照。在诊断时对患者进行研究,并进行了髂骨活检。破骨细胞因其酸性磷酸酶活性在组织学切片上清晰可见。在自动图像分析仪(Leitz TAS+)上开发了一款软件,用于测量每个破骨细胞的最大费雷特直径(Oc.Le)(对应破骨细胞长度)。每组均提供了Oc.Le频率分布直方图。在骨髓瘤患者中,Oc.Le频率分布与正常受试者相似,且直方图呈不对称的正偏态(最大峰值在20 - 25微米)。通过图形分析,该分布显示遵循对数正态分布,对应均匀的破骨细胞群体。在其他B细胞恶性肿瘤中,Oc.Le呈现双峰分布,一个峰值在20 - 25微米,另一个较低峰值在10 - 15微米。图形分析表明,在伴有正常破骨细胞的B细胞恶性肿瘤中存在小的(单核的?)破骨细胞。这可能反映了B淋巴细胞系恶性细胞分泌不同的可溶性因子。

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