Identification of biomarkers for the early detection of non-small cell lung cancer: a systematic review and meta-analysis.

IF 3.3 3区 医学 Q2 ONCOLOGY Carcinogenesis Pub Date : 2024-02-12 DOI:10.1093/carcin/bgad091
Eithar Mohamed, Daniel J García Martínez, Mohammad-Salar Hosseini, Si Qi Yoong, Daniel Fletcher, Simon Hart, Barbara-Ann Guinn
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Abstract

Lung cancer (LC) causes few symptoms in the earliest stages, leading to one of the highest mortality rates among cancers. Low-dose computerised tomography (LDCT) is used to screen high-risk individuals, reducing the mortality rate by 20%. However, LDCT results in a high number of false positives and is associated with unnecessary follow-up and cost. Biomarkers with high sensitivities and specificities could assist in the early detection of LC, especially in patients with high-risk features. Carcinoembryonic antigen (CEA), cytokeratin 19 fragments and cancer antigen 125 have been found to be highly expressed during the later stages of LC but have low sensitivity in the earliest stages. We determined the best biomarkers for the early diagnosis of LC, using a systematic review of eight databases. We identified 98 articles that focussed on the identification and assessment of diagnostic biomarkers and achieved a pooled area under curve of 0.85 (95% CI 0.82-0.088), indicating that the diagnostic performance of these biomarkers when combined was excellent. Of the studies, 30 focussed on single/antigen panels, 22 on autoantibodies, 31 on miRNA and RNA panels, and 15 suggested the use of circulating DNA combined with CEA or neuron-specific enolase (NSE) for early LC detection. Verification of blood biomarkers with high sensitivities (Ciz1, exoGCC2, ITGA2B), high specificities (CYFR21-1, antiHE4, OPNV) or both (HSP90α, CEA) along with miR-15b and miR-27b/miR-21 from sputum may improve early LC detection. Further assessment is needed using appropriate sample sizes, control groups that include patients with non-malignant conditions, and standardised cut-off levels for each biomarker.

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识别早期检测非小细胞肺癌的生物标志物:系统综述和荟萃分析。
肺癌(LC)早期症状不明显,是死亡率最高的癌症之一。低剂量计算机断层扫描(LDCT)用于筛查高危人群,可将死亡率降低 20%。然而,低剂量计算机断层扫描会导致大量假阳性结果,并带来不必要的随访和费用。具有高敏感性和高特异性的生物标志物有助于早期发现乳腺癌,尤其是具有高危特征的患者。研究发现,癌胚抗原(CEA)、细胞角蛋白19片段和癌抗原125在乳腺癌晚期表达较高,但在早期敏感性较低。我们通过对八个数据库进行系统性回顾,确定了早期诊断乳腺癌的最佳生物标志物。我们共发现了 98 篇关于诊断生物标志物的鉴定和评估的文章,汇总后的曲线下面积为 0.85(95% CI 0.82-0.088),表明这些生物标志物结合在一起的诊断效果非常好。在这些研究中,30 项研究侧重于单一/抗原检测,22 项研究侧重于自身抗体检测,31 项研究侧重于 miRNA 和 RNA 检测,15 项研究建议使用循环 DNA 结合 CEA 或 NSE 进行早期 LC 检测。验证高灵敏度(Ciz1、exoGCC2、ITGA2B)、高特异性(CYFR21-1、anti-HE4、OPNV)或两者兼具(HSP90α、CEA)的血液生物标记物以及痰中的 miR-15b 和 miR-27b/miR-21 可能会提高早期肺癌的检测率。需要使用适当的样本量、包括非恶性疾病患者在内的对照组以及每种生物标记物的标准化临界值水平进行进一步评估。
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来源期刊
Carcinogenesis
Carcinogenesis 医学-肿瘤学
CiteScore
9.20
自引率
2.10%
发文量
95
审稿时长
1 months
期刊介绍: Carcinogenesis: Integrative Cancer Research is a multi-disciplinary journal that brings together all the varied aspects of research that will ultimately lead to the prevention of cancer in man. The journal publishes papers that warrant prompt publication in the areas of Biology, Genetics and Epigenetics (including the processes of promotion, progression, signal transduction, apoptosis, genomic instability, growth factors, cell and molecular biology, mutation, DNA repair, genetics, etc.), Cancer Biomarkers and Molecular Epidemiology (including genetic predisposition to cancer, and epidemiology), Inflammation, Microenvironment and Prevention (including molecular dosimetry, chemoprevention, nutrition and cancer, etc.), and Carcinogenesis (including oncogenes and tumor suppressor genes in carcinogenesis, therapy resistance of solid tumors, cancer mouse models, apoptosis and senescence, novel therapeutic targets and cancer drugs).
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