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本-周蛋白的合成与代谢以及本-周蛋白骨髓瘤患者肿瘤负荷的计算

Synthesis and metabolism of Bence Jones protein and calculation of tumour burden in patients with Bence Jones myeloma.

作者信息

Durie B G, Cole P W, Chen H S, Himmelstein K J, Salmon S E

出版信息

Br J Haematol. 1981 Jan;47(1):7-19. doi: 10.1111/j.1365-2141.1981.tb02757.x.

Abstract

Synthesis and metabolism of Bence Jones protein was measured in seven patients with Bence Jones myeloma. Using the plasma and urine levels of 125I-labelled Bence Jones protein, it was possible to calculate the fractional catabolic rate (FCR), fractional proteinuric rate (FPR), and fractional metabolic rate (FMR) for the individual patients. There was a high degree of correlation between decreased metabolism and reduced creatinine clearance (P < 0.001). Ideal regression equations (linear and nonlinear) relating FCR, FPR and FMR with fractional creatinine clearance (FCC) were calculated. Using these regression equations plus measured values for the synthetic rates of light chain for bone marrow plasma cells, the myeloma cell mass or tumour burden was measured in each patient. Correlations between these measured cell mass values and those derived from clinical staging were reasonably good. However, for the lambda (gamma) Bence Jones myeloma patients, the measured cell mass values were significantly higher than predicted from clinical staging. Further studies will be necessary to validate this latter observation. It is hoped that this study will serve as a basis for a comprehensive schema allowing accurate cell mass measurement and staging of Bence Jones myeloma.

摘要

对7例本-周蛋白骨髓瘤患者的本-周蛋白合成及代谢情况进行了测定。利用125I标记的本-周蛋白的血浆和尿液水平,能够计算出各个患者的分数分解代谢率(FCR)、分数蛋白尿率(FPR)以及分数代谢率(FMR)。代谢降低与肌酐清除率降低之间存在高度相关性(P < 0.001)。计算出了将FCR、FPR和FMR与分数肌酐清除率(FCC)相关联的理想回归方程(线性和非线性)。利用这些回归方程以及骨髓浆细胞轻链合成率的测量值,对每位患者的骨髓瘤细胞量或肿瘤负荷进行了测量。这些测量得到的细胞量值与临床分期得出的值之间的相关性相当良好。然而,对于λ(γ)本-周蛋白骨髓瘤患者,测量得到的细胞量值显著高于临床分期所预测的值。需要进一步研究来验证后一观察结果。希望本研究将作为一个全面方案的基础,以实现本-周蛋白骨髓瘤细胞量的准确测量和分期。

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