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Ki-67 and subtype as prognostic and predictive markers of diffuse large B-Cell lymphoma

机译:Ki-67和亚型是弥漫性大B细胞淋巴瘤的预后和预测指标

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Introduction: Since patients with similar International Prognostic Index (IPI) scores have varied outcomes, molecular signatures including Ki-67 overexpression have been studied to prognosticate diffuse large B-cell lymphoma (DLBCL), which have shown varied outcomes. Objective: To correlate Ki-67 expression with survival in two biologic subgroups of DLBCL. Materials and Methods: One hundred and twelve adults with DLBCL between 2008 and 2012 were identified. Ki-67 overexpression was determined using immunohistochemistry. Results: A total of 112 patients of DLBCL were identified and included in the study. The median age was 54 years (18–78 years), with a male/female ratio of 1.8:1. Median survival was greater in patients with low Ki-67 (n = 32) as compared to high Ki-67 (n = 44) (32 m vs. 21.5 m, P = 0.033). In the germinal center B-cell (GCB) subtype, low Ki-67 had a better survival as compared to high Ki-67 (35 m vs. 28 m, P = 0.044), whereas in the non-GCB (NGCB) subtype, the results were same but statistically insignificant (26.5 m vs. 18 m, P = 0.7). In the high IPI arm, low Ki-67 had a better survival (26.5 m vs. 17 m, P = 0.02), whereas in low IPI arm, the results were similar but statistically insignificant (39 m vs. 38 m, P = 0.837). Survival analysis was done in each treatment arm (CHOP and R-CHOP) based on Ki-67 expression (high or low) in GCB and NGCB arms. No statistically significant difference was noted in any of the four arms; 27.5 m versus 34 m (P = 0.738) in high versus low Ki-67 in CHOP-GCB arm, 15 m versus 22 m (P = 0.443) in high versus low Ki-67 in CHOP-NGCB arm, 27 m versus 44 m (P = 0.104) in high versus low Ki-67 in R-CHOP-GCB arm, and 31 m versus 35 m (P = 0.861) in high versus low Ki-67 in R-CHOP-NGCB arm. Conclusions: Ki-67 although an indicator of poor outcome, its use to predict outcomes alone in the absence of study of expression of concomitant markers such as myc/BCL6 would cause a bias in results. Furthermore, its relevance in the rituximab era needs further validation.
机译:简介:由于具有相似国际预后指数(IPI)评分的患者预后各不相同,因此已研究了包括Ki-67过表达在内的分子标记来预示弥散性大B细胞淋巴瘤(DLBCL),预后也各不相同。目的:将Ki-67表达与DLBCL的两个生物学亚组的存活率相关。材料与方法:确定了2008年至2012年之间的112名DLBCL成人。使用免疫组织化学确定Ki-67过表达。结果:总共鉴定出112例DLBCL患者并纳入研究。中位年龄为54岁(18-78岁),男女之比为1.8:1。 Ki-67低(n = 32)的患者的中位生存期高于Ki-67低(n = 44)的患者(32 m vs. 21.5 m,P = 0.033)。在生发中心B细胞(GCB)亚型中,低Ki-67的存活率比高Ki-67(35 m vs. 28 m,P = 0.044)高,而在非GCB(NGCB)亚型中,结果相同,但统计意义不明显(26.5 m和18 m,P = 0.7)。在高IPI组中,低Ki-67的生存期更好(26.5 m vs. 17 m,P = 0.02),而在低IPI组中,结果相似,但在统计学上不显着(39 m vs. 38 m,P = 0.837)。根据GCB和NGCB组中Ki-67的表达(高或低)在每个治疗组(CHOP和R-CHOP)中进行生存分析。四个组中的任何一个都没有发现统计学上的显着差异。 CHOP-GCB组的高Ki-67相对于低Ki-67为27.5 m与34 m(P = 0.738),CHOP-NGCB组的高Ki-67相对于高Ki-67为15 m与22 m(P = 0.443),27OP对44 R-CHOP-GCB组的高Ki-67臂相对于低Ki-67的m(P = 0.104),R-CHOP-NGCB组的高Ki-67臂相对于低Ki-67的m(P = 0.861)。结论:Ki-67虽然是不良预后的指标,但在缺乏对诸如myc / BCL6等伴随标志物表达的研究的情况下,仅将其用于预测预后将导致结果偏倚。此外,它在利妥昔单抗时代的相关性还需要进一步验证。

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