Panel of serum long non-coding RNAs as potential non-invasive biomarkers for gallbladder carcinoma

IF 5.9 3区生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY Non-coding RNA Research Pub Date : 2024-02-06 DOI:10.1016/j.ncrna.2024.02.005

Sridhar Mishra , Pallavi Srivastava , Anshuman Pandey , Akash Agarwal , Saumya Shukla , Nuzhat Husain

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引用次数: 0

Abstract

Gallbladder carcinoma (GBC) is a common malignancy and is usually diagnosed in the late stages of the disease. The identification of new effective early diagnostic biomarkers could represent an effective approach in reducing mortality in GBC. Altered expression of long non-coding RNAs (lncRNAs) is believed to be associated with the emergence and development of GBC. Our study aims to identify the expression of a range of circulating lncRNAs, including HOTAIR, ANRIL, H19, CCAT1 and MEG3, in matched serum and tissues of GBC for diagnosis and its association with clinicopathological features. The case and control study included matched serum and tissues from 63 GBC, 19 cholecystitis (CC), and 46 normal controls (NC). RNA extraction and cDNA synthesis from serum and fresh tissue match were performed using commercially available kits. Relative expression was assessed using SYBR Green real-time quantitative polymerase chain reaction. Circulating lncRNA levels including HOTAIR, ANRIL and H19 were upregulated in serum samples, while MEG3 and CCAT1 were downregulated in GBC compared to controls. The trend towards upregulation and downregulation was comparable in the tissue. HOTAIR and MEG3 levels were significantly different between serum CC and early-stage GBC (p = 0.0373, 0.0020), while H19 was significantly upregulated comparing early-stage GBC to advanced-stage GBC (p = 0.018). The expression of ANRIL was significant with M stage (p = 0.0488), H19 with stage (p = 0.009), M stage (p=<0.0001) & stage (0.009) and CCAT1 with M stage (0.044). When distinguishing GBC and NC, AUC for HOTAIR was 0.75, ANRIL 0.78, H19 0.74, CCAT1 0.80 and 0.96 for MEG3. The combination sensitivity for lncRNAs ranged from 84.13% (CI: 72.74–92.12%) to 100.0% (CI: 94.31–100.0%). Significant diagnostic value in discriminating pathologic stage was observed for ANRIL and MEG3 (p = 0.022, p = 0.0005). LncRNA show a significant change in expression in GBC and in discrimination of early stage from late-stage disease. The detection of 2 lncRNAs in panels, in coordination with radiology, could represent a potential serum-based biomarker for early-stage GBC diagnosis.

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作为胆囊癌潜在非侵入性生物标记物的血清长非编码 RNA 小组

胆囊癌（GBC）是一种常见的恶性肿瘤，通常在疾病晚期才被诊断出来。确定新的有效早期诊断生物标志物是降低胆囊癌死亡率的有效方法。长非编码 RNA（lncRNA）表达的改变被认为与 GBC 的出现和发展有关。我们的研究旨在确定一系列循环lncRNA（包括HOTAIR、ANRIL、H19、CCAT1和MEG3）在GBC配对血清和组织中的表达，以用于诊断及其与临床病理特征的关联。病例和对照研究包括63例GBC、19例胆囊炎（CC）和46例正常对照（NC）的匹配血清和组织。使用市售试剂盒从血清和新鲜组织中提取 RNA 并合成 cDNA。使用 SYBR Green 实时定量聚合酶链反应评估相对表达。与对照组相比，包括HOTAIR、ANRIL和H19在内的循环lncRNA水平在血清样本中上调，而MEG3和CCAT1在GBC中下调。组织中的上调和下调趋势相当。HOTAIR和MEG3水平在血清CC和早期GBC之间存在显著差异（p = 0.0373，0.0020），而H19在早期GBC和晚期GBC之间存在显著上调（p = 0.018）。ANRIL的表达与M期（p = 0.0488）、H19的表达与M期（p = 0.009）、M期（p=<0.0001）&期（0.009）和CCAT1的表达与M期（0.044）有显著关系。在区分 GBC 和 NC 时，HOTAIR 的 AUC 为 0.75，ANRIL 为 0.78，H19 为 0.74，CCAT1 为 0.80，MEG3 为 0.96。lncRNAs 的组合灵敏度从 84.13%（CI：72.74-92.12%）到 100.0%（CI：94.31-100.0%）不等。ANRIL 和 MEG3 在鉴别病理分期方面具有显著的诊断价值（P = 0.022，P = 0.0005）。LncRNA 在 GBC 中的表达发生了显著变化，在鉴别早期和晚期疾病方面也是如此。通过与放射学研究合作，检测出两个lncRNA，这可能是诊断早期GBC的一种基于血清的生物标志物。

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来源期刊

Non-coding RNA Research Medicine-Biochemistry (medical)

CiteScore

7.70

自引率

6.00%

发文量

审稿时长

49 days

期刊介绍： Non-coding RNA Research aims to publish high quality research and review articles on the mechanistic role of non-coding RNAs in all human diseases. This interdisciplinary journal will welcome research dealing with all aspects of non-coding RNAs-their biogenesis, regulation and role in disease progression. The focus of this journal will be to publish translational studies as well as well-designed basic studies with translational and clinical implications. The non-coding RNAs of particular interest will be microRNAs (miRNAs), small interfering RNAs (siRNAs), small nucleolar RNAs (snoRNAs), U-RNAs/small nuclear RNAs (snRNAs), exosomal/extracellular RNAs (exRNAs), Piwi-interacting RNAs (piRNAs) and long non-coding RNAs. Topics of interest will include, but not limited to: -Regulation of non-coding RNAs -Targets and regulatory functions of non-coding RNAs -Epigenetics and non-coding RNAs -Biological functions of non-coding RNAs -Non-coding RNAs as biomarkers -Non-coding RNA-based therapeutics -Prognostic value of non-coding RNAs -Pharmacological studies involving non-coding RNAs -Population based and epidemiological studies -Gene expression / proteomics / computational / pathway analysis-based studies on non-coding RNAs with functional validation -Novel strategies to manipulate non-coding RNAs expression and function -Clinical studies on evaluation of non-coding RNAs The journal will strive to disseminate cutting edge research, showcasing the ever-evolving importance of non-coding RNAs in modern day research and medicine.