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Cellular origin of human B-cell neoplasms and Hodgkin's disease based on analysis of somatic hypermutations in the immunoglobulin variable region genes

机译:基于免疫球蛋白可变区基因体细胞超突变分析的人类B细胞肿瘤和霍奇金病的细胞起源

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In response to antigen stimulation, B cells undergo a germinal center(GC) reaction such as somatic hypermutations of the immunoglobulin variable region genes, which results in the production and selection of antigen-specific antibodies with increased affinity. Therefore, somatic hypermutations are considered to be a hallmark of GC B cells and their descendants. Pre-GC B cells(precursor B cells, immature B cells, naive B cells and CD5+ B cells) carry no somatic hypermutations, whereas GC B cells and post-GC B cells(memory B cells and plasma cells) express somatic hypermutations. This phenomenon is useful in identifying the cellular origin of various B-cell neoplasms. Precursor B-lymphoblastic leukemia/lymphoma, mantle cell lymphoma, and most B-CLL originate from pre-GC B cells, and follicular lymphoma, Burkitt's lymphoma, marginal zone B-cell lymphoma, diffuse large B-cell lymphoma and myeloma from GC B cells or post-GC B cells. Nodular lymphocyte-predominant Hodgkin's disease and most classical types of Hodgkin's disease are derived from GC B cells. Most human-B cell neoplasms including Hodgkin's disease are derived from GC B cells or their descendants. Molecular processes that modify the DNA of GC B cells, such as somatic hypermutation, class switching and receptor editing occur in the environment of the GCs, and increase the risk of malignant transformation.
机译:响应抗原刺激,B细胞发生生发中心(GC)反应,例如免疫球蛋白可变区基因的体细胞超突变,从而导致亲和力更高的抗原特异性抗体的产生和选择。因此,体细胞超突变被认为是GC B细胞及其后代的标志。前GC B细胞(前体B细胞,未成熟B细胞,幼稚B细胞和CD5 + B细胞)不携带体细胞超突变,而GC B细胞和后GC B细胞(记忆B细胞和浆细胞)表达体细胞超突变。此现象可用于识别各种B细胞肿瘤的细胞起源。前体B淋巴细胞白血病/淋巴瘤,套细胞淋巴瘤和大多数B-CLL起源于GC前B细胞,滤泡性淋巴瘤,伯基特淋巴瘤,边缘区B细胞淋巴瘤,弥漫性大B细胞淋巴瘤和骨髓瘤细胞或GC后B细胞。结节性淋巴细胞为主的霍奇金氏病和大多数经典类型的霍奇金氏病均来自GC B细胞。包括霍奇金氏病在内的大多数人B细胞瘤均来自GC B细胞或其后代。修饰GC B细胞DNA的分子过程,例如体细胞超突变,类别转换和受体编辑,发生在GC的环境中,并增加了恶性转化的风险。

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