THE ROLE OF LET-7/HMGA2 LINKAGE IN THE PATHOGENESIS AND PROGNOSIS OF MYELODYSPLASTIC NEOPLASMS

IF 0.7 Q4 HEMATOLOGY Leukemia Research Reports Pub Date : 2024-01-01 DOI:10.1016/j.lrr.2024.100428
D. Vlachopoulou , C.-N. Kontandreopoulou , P.T. Diamantopoulos , S. Syriopoulou , C. Stafylidis , P. Katsiampoura , A. Galanopoulos , M. Dimou , P. Panayiotidis , N.-A. Viniou
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Abstract

Introduction

MicroRNAs (miRNAs),are significant regulators of human hematopoietic stem cells. Their deregulation contributes to hematological malignancies.The let-7 family has been found frequently deregulated in malignancies.In MDS various alterations of miRNAs have been reported.High Mobility Group AT-Hook 2 (HMGA2) protein functions as a transcriptional regulator. In this study, we investigated the HMGA2 expression in MDS and specifically in patients with fibrosis we studied the prognostic significance of four members of the let-7 family (let-7a, let-7b, let-7c, let-7d).

Methods

RNA extraction, reverse transcription, anda SYBR Green based real-time PCR were performed for the absolute quantification of HMGA2, using standard protocols. After RNA polyadenylation and reverse transcription with an oligo-dT adapter primer, miRNAs transcript levels were determined using the SYBR Green chemistry. IBM SPSS statistics, version 26 (IBM Corporation, North Castle, NY, USA) was used for the analysis.

Results

HMGA2 gene expression was investigated in 78 patients with MDS, whereas transcript levels of four members of the let-7 family (let-7a, let-7b, let-7c, let-7d) were analyzed in 11 patients with fibrosis. Let-7a transcript levels were significantly higher in MDS patients who developed acute myeloid leukemia (AML) compared to the group that did not (p=0.0141). Let-7d presented a negative correlation (p=0.0408). A moderate (p =0.0483) negative correlation of HMGA2 with let-7c, and a strong positive correlation (p =0.0481) with let-7d, were observed.

Conclusions

In literature, the let-7/HMGA2 linkage could be a signature in MDS pathogenesis. Let-7a level was found higher in transformation to AML,defining it as a poor prognostic factor, in contrast with the protective role of high let-7d.

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LET-7/HMGA2连锁在骨髓增生异常性肿瘤的发病机制和预后中的作用
导言微小RNA(miRNA)是人类造血干细胞的重要调节因子。在 MDS 中,miRNAs 的各种改变均有报道。高迁移率组 AT-Hook 2(HMGA2)蛋白具有转录调节因子的功能。在这项研究中,我们调查了 HMGA2 在 MDS 中的表达情况,特别是在纤维化患者中的表达情况,并研究了 let-7 家族四个成员(let-7a、let-7b、let-7c、let-7d)的预后意义。方法采用标准方案进行 RNA 提取、反转录和基于 SYBR Green 的实时 PCR,以绝对定量 HMGA2。用寡聚-dT 适配器引物进行 RNA 多腺苷酸化和反转录后,使用 SYBR Green 化学方法测定 miRNAs 的转录水平。结果 在 78 例 MDS 患者中调查了 HMGA2 基因的表达,在 11 例纤维化患者中分析了 let-7 家族四个成员(let-7a、let-7b、let-7c 和 let-7d)的转录水平。与未发展为急性髓性白血病(AML)的组别相比,发展为急性髓性白血病(AML)的 MDS 患者的 Let-7a 转录水平明显更高(P=0.0141)。Let-7d 呈负相关(p=0.0408)。HMGA2 与 let-7c 呈中度负相关(p=0.0483),与 let-7d 呈强正相关(p=0.0481)。Let-7a水平在向急性髓细胞性白血病转化时较高,是一个不良预后因素,与高let-7d的保护作用形成鲜明对比。
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来源期刊
Leukemia Research Reports
Leukemia Research Reports Medicine-Oncology
CiteScore
1.70
自引率
0.00%
发文量
70
审稿时长
23 weeks
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