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利用Ki-67抗原表达检测的浆细胞生长分数可识别出国际分期系统(ISS)I期多发性骨髓瘤患者中生存期较短的一个亚组。

Plasma cell growth fraction using Ki-67 antigen expression identifies a subgroup of multiple myeloma patients displaying short survival within the ISS stage I.

作者信息

Gastinne Thomas, Leleu Xavier, Duhamel Alain, Moreau Anne-Sophie, Franck Genevieve, Andrieux Joris, Lai Jean-Luc, Coiteux Valerie, Yakoub-Agha Ibrahim, Bauters Francis, Harousseau Jean-Luc, Zandecki Marc, Facon Thierry

机构信息

Service d'Hématologie Clinique, CHU, Nantes, France.

出版信息

Eur J Haematol. 2007 Oct;79(4):297-304. doi: 10.1111/j.1600-0609.2007.00915.x. Epub 2007 Aug 10.

Abstract

The current most powerful prognostic model in Multiple Myeloma (MM) combines beta-2 microglobulin (b2m) with albumin, corresponding to the International Staging System (ISS). However, the prognosis of patients within the ISS stage I (high albumin and low b2m) may vary. Ki-67 is a nuclear protein associated with cell proliferation. We retrospectively evaluated the percentage of bone marrow plasma cells expressing Ki-67 antigen (Ki-67 index) in a series of 174 untreated MM patients at diagnosis. Median survival was 51, 41 and 20 months respectively, and median Ki-67 index was 3.0%, 6.1% and 6.5% in ISS stages I, II, and III respectively. Independently of ISS, Ki-67 index > or =4% was highly predictive of adverse prognosis. Ki-67 index correlated with markers of intrinsic malignancy and with markers of tumour burden. Within ISS stage I, median survival was of 31 months (RR of death 2.65) in patients with Ki-67 index > or =4%. Eventually, the combination of Ki-67 with b2m produced an efficient prognostic model, which appeared most effective in our series when compared with b2m and KI-67 with chromosome 13 deletion models. In this series, we demonstrated that a proliferation marker provides clear-cut additional survival prognostic information to b2m into the ISS model.

摘要

多发性骨髓瘤(MM)目前最强大的预后模型是将β2微球蛋白(b2m)与白蛋白相结合,这与国际分期系统(ISS)相对应。然而,ISS I期(高白蛋白和低b2m)患者的预后可能有所不同。Ki-67是一种与细胞增殖相关的核蛋白。我们回顾性评估了174例未经治疗的MM患者在诊断时骨髓浆细胞中表达Ki-67抗原的百分比(Ki-67指数)。ISS I期、II期和III期的中位生存期分别为51个月、41个月和20个月,Ki-67指数的中位数分别为3.0%、6.1%和6.5%。独立于ISS,Ki-67指数≥4%高度预示不良预后。Ki-67指数与内在恶性标志物以及肿瘤负荷标志物相关。在ISS I期,Ki-67指数≥4%的患者中位生存期为31个月(死亡风险比为2.65)。最终,Ki-67与b2m的组合产生了一个有效的预后模型,与b2m以及伴有13号染色体缺失的KI-67模型相比,该模型在我们的研究系列中似乎最有效。在本研究系列中,我们证明了一种增殖标志物为ISS模型中的b2m提供了明确的额外生存预后信息。

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