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骨髓瘤患者的骨重塑异常及骨吸收生化指标正常

Abnormal bone remodelling in patients with myelomatosis and normal biochemical indices of bone resorption.

作者信息

Taube T, Beneton M N, McCloskey E V, Rogers S, Greaves M, Kanis J A

机构信息

Department of Human Metabolism, University of Sheffield Medical School, United Kingdom.

出版信息

Eur J Haematol. 1992 Oct;49(4):192-8. doi: 10.1111/j.1600-0609.1992.tb00046.x.

Abstract

We studied bone biopsies from 26 patients with myelomatosis with apparently normal skeletal metabolism. Quantitative histomorphometric measurements suggested that skeletal disease was progressive despite normocalcaemia and normal urinary excretion rates of calcium and hydroxyproline. When biopsies were divided according to the involvement of marrow by plasma cells, bone resorption--as judged by the eroded surface--increased significantly the greater plasma cell burden. Osteoclasts were frequent with moderate tumour burdens, but there was no further increase in the number of osteoclasts when plasma cell infiltration increased by more than 50% of bone marrow. Contrary to expectation, the numbers of osteoblasts and bone formation rates were increased with bone biopsies with moderate tumour burden, but were markedly lower when plasma cell infiltration occupied more than 50% of bone marrow, due to a decreased functional capacity of osteoblasts. We conclude that skeletal bone disease in myeloma is commonly progressive despite apparently stable bone disease as judged by biochemical measurements. The major mechanism of bone loss in myelomatosis is increased osteoclastic resorption but decreased bone formation contributes to bone loss with heavy plasma cell burdens. Urinary excretion of calcium and hydroxyproline provide insensitive indices of bone resorption in myelomatosis.

摘要

我们研究了26例骨骼代谢明显正常的骨髓瘤患者的骨活检标本。定量组织形态计量学测量结果表明,尽管血钙正常、尿钙和羟脯氨酸排泄率正常,但骨骼疾病仍在进展。根据浆细胞对骨髓的累及情况对活检标本进行分类时,以侵蚀面判断的骨吸收在浆细胞负荷越大时显著增加。在肿瘤负荷中等时破骨细胞数量较多,但当浆细胞浸润增加超过骨髓的50%时,破骨细胞数量并未进一步增加。与预期相反,在肿瘤负荷中等的骨活检标本中,成骨细胞数量和骨形成率增加,但当浆细胞浸润占据骨髓超过50%时,由于成骨细胞功能能力下降,其数量和骨形成率显著降低。我们得出结论,尽管根据生化测量判断骨病明显稳定,但骨髓瘤中的骨骼疾病通常仍在进展。骨髓瘤中骨质流失的主要机制是破骨细胞吸收增加,但骨形成减少在浆细胞负荷较重时也会导致骨质流失。尿钙和羟脯氨酸排泄是骨髓瘤中骨吸收的不敏感指标。

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