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弥漫性大B细胞淋巴瘤的分子谱分析确定了多种明确的亚型,其中一种以宿主炎症反应为特征。

Molecular profiling of diffuse large B-cell lymphoma identifies robust subtypes including one characterized by host inflammatory response.

作者信息

Monti Stefano, Savage Kerry J, Kutok Jeffery L, Feuerhake Friedrich, Kurtin Paul, Mihm Martin, Wu Bingyan, Pasqualucci Laura, Neuberg Donna, Aguiar Ricardo C T, Dal Cin Paola, Ladd Christine, Pinkus Geraldine S, Salles Gilles, Harris Nancy Lee, Dalla-Favera Riccardo, Habermann Thomas M, Aster Jon C, Golub Todd R, Shipp Margaret A

机构信息

The Broad Institute, Cambridge, MA, USA.

出版信息

Blood. 2005 Mar 1;105(5):1851-61. doi: 10.1182/blood-2004-07-2947. Epub 2004 Nov 18.

DOI:10.1182/blood-2004-07-2947
PMID:15550490
Abstract

Diffuse large B-cell lymphoma (DLBCL) is a heterogeneous disease with recognized variability in clinical outcome, genetic features, and cells of origin. To date, transcriptional profiling has been used to highlight similarities between DLBCL tumor cells and normal B-cell subtypes and associate genes and pathways with unfavorable outcome. To identify robust and highly reproducible DL-BCL subtypes with comprehensive transcriptional signatures, we used a large series of newly diagnosed DLBCLs, whole genome arrays, and multiple clustering methods. Tumors were also analyzed for known common genetic abnormalities in DLBCL. There were 3 discrete subsets of DLBCL-"oxidative phosphorylation," "B-cell receptor/proliferation," and "host response" (HR)-identified characterized using gene set enrichment analysis and confirmed in an independent series. HR tumors had increased expression of T/natural killer cell receptor and activation pathway components, complement cascade members, macrophage/dendritic cell markers, and inflammatory mediators. HR DLB-CLs also contained significantly higher numbers of morphologically distinct CD2+/CD3+ tumor-infiltrating lymphocytes and interdigitating S100+/gamma interferon-induced lysosomal transferase-positive (GILT+) CD1a-/CD123- dendritic cells. The HR cluster shared features of histologically defined T-cell/histiocyte-rich B-cell lymphoma, including fewer genetic abnormalities, younger age at presentation, and frequent splenic and bone marrow involvement. These studies identify tumor microenvironment and host inflammatory response as defining features in DLBCL and suggest rational treatment targets in specific DLBCL subsets.

摘要

弥漫性大B细胞淋巴瘤(DLBCL)是一种异质性疾病,在临床结局、基因特征和起源细胞方面存在公认的变异性。迄今为止,转录谱分析已被用于突出DLBCL肿瘤细胞与正常B细胞亚型之间的相似性,并将基因和信号通路与不良预后相关联。为了通过全面的转录特征识别出稳健且高度可重复的DL-BCL亚型,我们使用了一系列新诊断的DLBCL病例、全基因组阵列和多种聚类方法。还对肿瘤进行了DLBCL中已知常见基因异常的分析。通过基因集富集分析确定并在一个独立队列中得到证实,DLBCL存在3个离散亚组——“氧化磷酸化”、“B细胞受体/增殖”和“宿主反应”(HR)。HR肿瘤中T/自然杀伤细胞受体及激活信号通路成分、补体级联成员、巨噬细胞/树突状细胞标志物和炎症介质的表达增加。HR DLB-CL中形态学上不同的CD2+/CD3+肿瘤浸润淋巴细胞和指状突S100+/γ干扰素诱导的溶酶体转移酶阳性(GILT+)CD1a-/CD123-树突状细胞的数量也显著更多。HR聚类具有组织学定义的富含T细胞/组织细胞的B细胞淋巴瘤的特征,包括较少的基因异常、发病时年龄较轻以及脾脏和骨髓受累频繁。这些研究确定了肿瘤微环境和宿主炎症反应是DLBCL的决定性特征,并提出了特定DLBCL亚组的合理治疗靶点。

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