t(14;18)阴性滤泡性淋巴瘤向浆液性淋巴瘤转化:病例报告与基因演变分析。

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2024-06-22 DOI:10.1186/s13000-024-01512-2
Sojung Lim, Jiwon Koh, Jeong Mo Bae, Hongseok Yun, Cheol Lee, Jin Ho Paik, Tae Min Kim, Yoon Kyung Jeon
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引用次数: 0

摘要

背景:滤泡性淋巴瘤(FL)的特征是涉及IGH和BCL2基因的t(14;18)(q32;q21)。然而,10%-15%的FL缺乏BCL2重排。这些BCL2重排阴性的FL在临床、病理和基因上都是异质性的。这类 FLs 的生物学行为和组织学转化特征尚不充分。在此,我们报告了首例迅速发展为浆细胞性淋巴瘤(PBL)的t(14;18)阴性FL病例:病例介绍:一名先前健康的 51 岁男性出现腿部肿胀。计算机断层扫描(CT)显示全身淋巴结(LN)肿大,包括两侧腹股沟区。腹股沟淋巴结针刺活检提示为低级别 B 细胞非霍奇金淋巴瘤。颈部淋巴结切除活检显示,中心细胞和中心母细胞增生,呈滤泡状和弥漫状生长。免疫组化分析显示,这些细胞的CD20、BCL6、CD10和CD23均呈阳性。BCL2染色在滤泡中呈阴性,在滤泡间区呈弱至中度阳性。BCL2荧光原位杂交结果为阴性。靶向新一代测序(NGS)显示,TNFRSF14、CREBBP、STAT6、BCL6、CD79B、CD79A和KLHL6基因发生了突变,但没有发现BCL2或BCL6重排的证据。病理和遗传特征与t(14;18)阴性FL一致。苯达莫司汀和利妥昔单抗化疗一个周期两个月后,患者出现左侧腹痛。正电子发射断层扫描(Positron emission tomography)/CT显示腹膜后新出现一个巨大的高代谢肿块。腹膜后肿块的针刺活检显示大浆细胞弥漫增生,B细胞标志物BCL2、BCL6和CD10阴性;MUM-1、CD138、CD38和C-MYC阳性。病理结果与 PBL 一致。通过靶向 NGS 分析了最初的 FL 与随后的 PBL 之间的克隆关系。肿瘤具有相同的CREBBP、STAT6、BCL6和CD79B突变,这强烈表明PBL是从FL克隆转化而来的。除了IGH::IRF4融合外,PBL还携带BRAF V600E突变和IGH::MYC融合:我们认为,当存在相关基因突变时,FL 向 PBL 的转化或分化克隆进化可能发生。这项研究拓宽了t(14;18)阴性FL组织学转化的范围,并强调了其生物学和临床异质性。
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Transformation of t(14;18)-negative follicular lymphoma to plasmablastic lymphoma: a case report with analysis of genetic evolution.

Background: Follicular lymphoma (FL) is characterized by t(14;18)(q32;q21) involving the IGH and BCL2 genes. However, 10-15% of FLs lack the BCL2 rearrangement. These BCL2-rearrangement-negative FLs are clinically, pathologically, and genetically heterogeneous. The biological behavior and histological transformation of such FLs are not adequately characterized. Here, we report the first case of t(14;18)-negative FL that rapidly progressed to plasmablastic lymphoma (PBL).

Case presentation: A previously healthy 51-year-old man presented with leg swelling. Computed tomography (CT) showed enlarged lymph nodes (LNs) throughout the body, including both inguinal areas. Needle biopsy of an inguinal LN suggested low-grade B-cell non-Hodgkin lymphoma. Excisional biopsy of a neck LN showed proliferation of centrocytic and centroblastic cells with follicular and diffuse growth patterns. Immunohistochemical analysis showed that the cells were positive for CD20, BCL6, CD10, and CD23. BCL2 staining was negative in the follicles and weak to moderately positive in the interfollicular areas. BCL2 fluorescence in situ hybridization result was negative. Targeted next-generation sequencing (NGS) revealed mutations in the TNFRSF14, CREBBP, STAT6, BCL6, CD79B, CD79A, and KLHL6 genes, without evidence of BCL2 or BCL6 rearrangement. The pathologic and genetic features were consistent with t(14;18)-negative FL. Two months after one cycle of bendamustine and rituximab chemotherapy, the patient developed left flank pain. Positron emission tomography/CT showed new development of a large hypermetabolic mass in the retroperitoneum. Needle biopsy of the retroperitoneal mass demonstrated diffuse proliferation of large plasmablastic cells, which were negative for the B-cell markers, BCL2, BCL6, and CD10; they were positive for MUM-1, CD138, CD38, and C-MYC. The pathologic findings were consistent with PBL. The clonal relationship between the initial FL and subsequent PBL was analyzed via targeted NGS. The tumors shared the same CREBBP, STAT6, BCL6, and CD79B mutations, strongly suggesting that the PBL had transformed from a FL clone. The PBL also harbored BRAF V600E mutation and IGH::MYC fusion in addition to IGH::IRF4 fusion.

Conclusions: We propose that transformation or divergent clonal evolution of FL into PBL can occur when relevant genetic mutations are present. This study broadens the spectrum of histological transformation of t(14;18)-negative FL and emphasizes its biological and clinical heterogeneity.

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ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
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9.40
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2.10%
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464
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