Ki67免疫组织化学表达水平≥70%,大块显示≥7.5cm,脑膜淋巴瘤,4个治疗周期后的中期PETΔSUVmax<71%,作为预测弥漫性大B细胞淋巴瘤无进展生存期和总生存期的实用评分系统的一部分

Vincent Rebière, Meriem Maajem, Ronan Le Calloch, Leela Raj, Anne-Sophie Le Bris, Mohamed Malou, François Salmon, Isabelle Quintin-Roué, Adrian Tempescul, David Bourhis, Laura Samaison, Hussam Saad, Pierre-Yves Salaun, Christian Berthou, Jean-Christophe Ianotto, Ronan Abgral, Jean-Richard Eveillard
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引用次数: 0

摘要

目前,弥漫性大B细胞淋巴瘤(DLBCL)的预后模型未能密切反映患者的生物学、临床和生存异质性。因此,我们评估了尚未纳入任何评分系统的临床、生物学、免疫组织化学(IHC)、基线(0)和中期(2个和4个治疗周期后)PET(PET0、PET2和PET4)数据对DLBCL结果的影响。该分析对Finistere Observatory队列(O.Ly.Fin)中89名先前未经治疗的成年患者进行,这些患者在2010年1月至2017年12月期间招募,并记录了DLBCL,无进展生存期(PFS)和总生存期(OS)分别作为主要和次要终点。78名患者接受利妥昔单抗、环磷酰胺、羟基阿霉素、长春新碱和泼尼松(R-CHOP)治疗,11名患者接受R-剂量调整的依托泊苷、泼尼松、长春新碱、环磷酰胺和羟基阿霉素(EPOCH)治疗。患者随访至2020年6月20日。在多变量分析中,IHC(K)的Ki67≥70%、体积表现≥7.5 cm(B)、脑膜淋巴瘤(M)和PET0–PET4ΔSUVmax<71%(P4)被确定为PFS的强独立预测因子,除体积疾病外的所有变量也强独立预测OS。使用这4个参数,我们设计了一个名为KBMP4的评分模型,通过Kaplan–Meier分析将患者分为低(0参数)、中(1或2)和高风险(≥3)亚组。在43个月的中位随访中,低风险亚组的PFS和OS均为100%,中风险亚组分别为71.4%和90.5%,高风险亚组则分别为0和55.5%。在临床实践中使用KBMP4模型可以提高新发DLBCL患者预后预测和治疗决策的准确性。
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Ki67 Immunohistochemical Expression Level ≥70%, Bulky Presentation ≥7.5 cm, Meningeal Lymphomatosis, and Interim PET ΔSUVmax After 4 Treatment Cycles <71% as Parts of a Practical Scoring System to Predict Progression-Free Survival and Overall Survival in Diffuse Large B-Cell Lymphoma.

Currently, prognostic models in diffuse large B-cell lymphoma (DLBCL) fail to closely reflect patients' biological, clinical, and survival heterogeneity. We, therefore, assessed the impact of clinical, biological, immunohistochemical (IHC), baseline (0), and interim (after 2 and 4 treatment cycles) PET (PET0, PET2, and PET4) data not yet included in any scoring system on DLBCL outcome. The analysis was conducted on 89 previously untreated adult patients of the Finistere Observatory Cohort (O.Ly.Fin) with documented DLBCL, recruited between January 2010 and December 2017, with progression-free survival (PFS) and overall survival (OS) as primary and secondary endpoints, respectively. Seventy-eight patients were treated with rituximab, cyclophosphamide, hydroxyadriamycin, vincristine, and prednisone (R-CHOP), while 11 received R-dose-adjusted etoposide, prednisone, vincristine, cyclophosphamide, and hydroxyadriamycin (EPOCH). Patients were followed up until June 20, 2020. On multivariate analysis, Ki67 ≥ 70% on IHC (K), bulky presentation ≥7.5 cm (B), meningeal lymphomatosis (M), and PET0-PET4 ΔSUVmax <71% (P4) were identified as strong independent predictors of PFS, and all variables but bulky disease also strongly and independently predicted OS. Using these 4 parameters, we designed a scoring model named KBMP4 stratifying patients into low- (0 parameter), intermediate- (1 or 2), and high-risk (≥3) subgroups by the Kaplan-Meier analysis. At a median follow-up of 43 months, PFS and OS were both 100% in the low-risk subgroup, 71.4 and 90.5%, respectively, in the intermediate-risk subgroup, and 0 and 55.5%, respectively, in the high-risk subgroup. Use of the KBMP4 model in clinical practice may improve accuracy in prognostic prediction and treatment decisions in de novo DLBCL patients.

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