缺氧诱导因子-1 α (Hif-1 α)多态性在淋巴瘤和反应性淋巴样增生

S. Yılmaz, A. Yoruk, I. Zemheri, A. Kuskucu, O. Suakar, Nergiz Imamova, Pinar Canizci
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引用次数: 0

摘要

背景:淋巴结病是指淋巴结大小或特征的异常。它可能是传染病和恶性疾病的表现。反应性淋巴样增生是一种良性的淋巴结病。细胞在缺氧诱导因子-1 α (Hif-1 α)的调控下对缺氧胁迫产生多种适应性反应。目的:Hif-1alpha可能在癌症早期的癌变过程中发挥作用。我们的目的是研究Hif-1α C1772T和G1790A基因多态性在反应性淋巴样增生和淋巴瘤病例中最常见的多态性。方法:86例石蜡包埋组[51例(59.3%)反应性淋巴样增生;(40.7%)淋巴瘤]。从这些样本中提取DNA并进行聚合酶链反应(PCR)。DNA分离后,采用焦磷酸测序法分析Hif-1α C1772T和G1790A多态性。结果:女孩(29.1%)例,男孩61例(70.9%)。反应性淋巴样增生组和淋巴瘤组的平均年龄分别为91、47±57、96岁和142、46±41、66岁。两组均无Hif-1α C1772T基因多态性,但14例Hif-1α G1790A基因多态性(反应性淋巴样增生10例,淋巴瘤4例),反应性淋巴样增生中Hif-1α G1790A基因多态性略高于淋巴瘤,但两组间差异无统计学意义(p < 0.05)。结论:Hif-1α C1772T和G1790A基因多态性在某些癌症的病因学中有重要意义。在我们的研究中,考虑到Hif-1α G1790A基因多态性在反应性淋巴样增生组中较少,在了解Hif-1α基因多态性在淋巴结病患儿中的行为方面,需要进行大量的研究。
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Hypoxia inducible factor-1 alpha (Hif-1 alpha) polymorphism in lymphoma and reactive lymphoid hyperplasia
Background: Lymphadenopathy is an abnormality in the size or the character of the lymph node.  It may be a manifestation of infectious and malignant diseases. Reactive lymphoid hyperplasia is a benign form of lymphadenopathy. Cells develop numerous adaptive responses regulated by hypoxia inducible factor-1 alpha (Hif-1 alpha) against hypoxic stress. Purpose: Hif-1alpha may play a role in the process of carcinogenesis in the early stage of cancer. We aimed to investigate the most common polymorphism of Hif-1α  C1772T and G1790A gene polymorphisms in reactive lymphoid hyperplasia and lymphoma cases. Methods: Eighty-six paraffin-embedded blocs [51 (59,3%) reactive lymphoid hyperplasia; (40,7%) lymphoma] were examined. DNA was extracted from these samples and the polymerase chain reaction (PCR) was carried out. After DNA isolation, Hif-1α C1772T and G1790A polymorphisms were investigated with pyrosequencing. Results: Cases were  (29,1%) girls and 61 (70,9%) boys. The mean age was 91,47±57,96 and 142,46±41,66 for reactive lymphoid hyperplasia and lymphoma group, respectively. There was no Hif-1α C1772T gene polymorphism in both group, but Hif-1α G1790A gene polymorphism was recorded in 14 cases (reactive lymphoid hyperplasia 10, lymphoma 4). Although Hif-1α G1790A gene polymorphism was seen a little higher in reactive lymphoid hyperplasia cases than that of lymphoma, no meaningful relationship was found statistically between two groups (p>0,05). Conclusion: Hif-1α C1772T and G1790A gene polymorphisms had been interrogated in cancer etiology and emphasized in some cancers. In our study, considering of a few of Hif-1α G1790A gene polymorphism in reactive lymphoid hyperplasia group, it should be investigated with large studies in terms of understanding of the behavior of Hif- 1α gene polymorphisms in children with lymphadenopathy.
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