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Lymphoid Neoplasia: Gene expression profiling of pulmonary mucosa-associated lymphoid tissue lymphoma identifies new biologic insights with potential diagnostic and therapeutic applications

机译:淋巴瘤形成:肺粘膜相关淋巴组织淋巴瘤的基因表达谱确定了具有潜在诊断和治疗应用的新生物学见解

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摘要

We conducted comprehensive gene expression profiling (GEP) of primary pulmonary mucosa-associated lymphoid tissue (MALT) lymphoma (n = 33) and compared the results to GEP of other B- and T-cell lymphomas and normal lymphocytes to identify novel markers and deregulated pathways. MALT has a prominent T-cell signature and a marginal zone/memory B-cell profile. Four novel transcripts were specifically overexpressed in MALT, and 2 of these, MMP7 and SIGLEC6, were validated at the protein level. GEP also revealed distinct molecular subsets in MALT. One subset, characterized by MALT1 translocations, showed overexpression of nuclear factor-κB (NF-KB) pathway genes but also was enriched for chemokine signaling pathways. Another subset showed increased plasma cells and a prominent plasma cell gene signature. By analyzing several genes with very high (“spiked”) expression in individual cases, we identified clusters with different biologic characteristics, such as samples with MALT1 translocations having high expression of MALT1 and RARA, samples with plasmacytic differentiation having high FKBP11 expression, and samples with high RGS13 expression tending to have trisomy 3 and reactive follicles. In conclusion, MALT subgroups with distinct pathologic features defined by distinct groups of deregulated genes were identified. These genes could represent novel diagnostic and therapeutic targets.
机译:我们对原发性肺黏膜相关淋巴样组织(MALT)淋巴瘤(n = 33)进行了全面的基因表达谱分析(GEP),并将结果与​​其他B细胞和T细胞淋巴瘤以及正常淋巴细胞的GEP进行了比较,以发现新的标志物并解除管制途径。 MALT具有突出的T细胞特征和边缘区/记忆B细胞特征。四种新的转录本在MALT中特异表达,其中2种MMP7和SIGLEC6在蛋白质水平得到验证。 GEP还揭示了MALT中不同的分子亚群。一个子集以MALT1易位为特征,显示核因子-κB(NF-KB)通路基因的过表达,但也富含趋化因子信号通路。另一个子集显示浆细胞增加和浆细胞基因签名突出。通过分析个别情况下几个表达水平非常高(“尖峰”)的基因,我们确定了具有不同生物学特性的簇,例如具有MALT1和RARA高表达的MALT1易位样品,具有高FKBP11表达的浆细胞分化样品和样品RGS13高表达的人倾向于具有三体性3和反应性卵泡。总之,鉴定了具有由不同的失调基因组定义的不同病理特征的MALT亚组。这些基因可能代表新的诊断和治疗目标。

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