首页> 外文期刊>Brazilian Archives of Biology and Technology >Involvement of transforming growth factor beta-1 (TGFβ1) cytokine and FOXP3 transcription factor genetic polymorphisms in hematological malignancies
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Involvement of transforming growth factor beta-1 (TGFβ1) cytokine and FOXP3 transcription factor genetic polymorphisms in hematological malignancies

机译:转化生长因子β-1(TGFβ1)细胞因子和FOXP3转录因子遗传多态性与血液系统恶性肿瘤的关系

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Hematological malignancies (HM) are a group of neoplastic diseases that arise from hematologic cell lineages. Transforming growth factor beta 1 (TGFβ1) is shown to negatively regulate normal and malignant hematopoiesis and, in immunological context, to promote T cell exhaustion and generation of regulatory T cells, which are shown to be deleterious in cancer, by the induction of transcription factor FOXP3 expression. The present study aimed to evaluate TGFB1 exon-1 rs1800470 and FOXP3 intron-1 rs2232365 polymorphisms in relation to HM susceptibility. DNA was extracted from blood samples of 43 HM patients and 142 neoplasia-free individuals and polymorphisms were analyzed by allelic-specific PCR. Association analysis was assessed by the Odds Ratio (OR) with significance level of 5%. Regarding FOXP3 polymorphism, no significant differences were observed in genotype or allele distribution among the patients and controls. However, there was a positive association between TGFB1 TT genotype and HM susceptibility (OR = 4.07; CI95% = 1.94 - 8.52). In the combined analysis, a positive association was also observed for TGFB1 TT and FOXP3 GG genotypes (OR = 4.00; CI95% = 1.54 - 10.41) in relation to HM susceptibility. Our results indicated promising new markers to be further investigated in hematological malignancies.
机译:血液恶性肿瘤(HM)是由血液细胞谱系引起的一组肿瘤性疾病。转化生长因子β1(TGFβ1)被证明对正常和恶性造血功能有负调节作用,并且在免疫学上,通过诱导转录因子,可促进T细胞衰竭和调节性T细胞的产生,而调节性T细胞在癌症中是有害的。 FOXP3表达式。本研究旨在评估与HM敏感性相关的TGFB1外显子1 rs1800470和FOXP3内含子1 rs2232365多态性。从43名HM患者和142名无瘤形成个体的血液样本中提取DNA,并通过等位基因特异性PCR分析其多态性。关联分析由显着性水平为5%的赔率(OR)评估。关于FOXP3多态性,在患者和对照之间没有观察到基因型或等位基因分布的显着差异。但是,TGFB1 TT基因型与HM敏感性之间存在正相关(OR = 4.07; CI95%= 1.94-8.52)。在组合分析中,还发现TGFB1 TT和FOXP3 GG基因型与HM易感性呈正相关(OR = 4.00; CI95%= 1.54-10.41)。我们的结果表明有希望的新标志物有待在血液系统恶性肿瘤中进一步研究。

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