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一种用于预测小儿胶质瘤预后和免疫微环境的新型HOX相关分类器特征的鉴定与验证

Identification and validation of a novel HOX-related classifier signature for predicting prognosis and immune microenvironment in pediatric gliomas.

作者信息

Zhang Jiao, Zhang Xueguang, Su Junyan, Zhang Jiali, Liu Siyao, Han Li, Liu Mengyuan, Sun Dawei

机构信息

Department of Cardiology, Capital Medical University Electric Power Teaching Hospital, State Grid Beijing Electric Power Hospital, Beijing, China.

Department of Nephrology, Capital Medical University Electric Power Teaching Hospital, State Grid Beijing Electric Power Hospital, Beijing, China.

出版信息

Front Cell Dev Biol. 2023 Jul 21;11:1203650. doi: 10.3389/fcell.2023.1203650. eCollection 2023.

Abstract

Pediatric gliomas (PGs) are highly aggressive and predominantly occur in young children. In pediatric gliomas, abnormal expression of Homeobox (HOX) family genes (HFGs) has been observed and is associated with the development and progression of the disease. Studies have found that overexpression or underexpression of certain HOX genes is linked to the occurrence and prognosis of gliomas. This aberrant expression may contribute to the dysregulation of important pathological processes such as cell proliferation, differentiation, and metastasis. This study aimed to propose a novel HOX-related signature to predict patients' prognosis and immune infiltrate characteristics in PGs. The data of PGs obtained from publicly available databases were utilized to reveal the relationship among abnormal expression of HOX family genes (HFGs), prognosis, tumor immune infiltration, clinical features, and genomic features in PGs. The HFGs were utilized to identify heterogeneous subtypes using consensus clustering. Then random forest-supervised classification algorithm and nearest shrunken centroid algorithm were performed to develop a prognostic signature in the training set. Finally, the signature was validated in an internal testing set and an external independent cohort. Firstly, we identified HFGs significantly differentially expressed in PGs compared to normal tissues. The individuals with PGs were then divided into two heterogeneous subtypes (HOX-SI and HOX-SII) based on HFGs expression profiles. HOX-SII showed higher total mutation counts, lower immune infiltration, and worse prognosis than HOX-SI. Then, we constructed a HOX-related gene signature (including , , , , and ) based on the cluster for subtype prediction utilizing random forest supervised classification and nearest shrunken centroid algorithm. The signature was revealed to be an independent prognostic factor for patients with PGs by multivariable Cox regression analysis. Our study provides a novel method for the prognosis classification of PGs. The findings also suggest that the HOX-related signature is a new biomarker for the diagnosis and prognosis of patients with PGs, allowing for more accurate survival prediction.

摘要

小儿胶质瘤(PGs)具有高度侵袭性,主要发生于幼儿。在小儿胶质瘤中,已观察到同源盒(HOX)家族基因(HFGs)的异常表达,且其与疾病的发生发展相关。研究发现,某些HOX基因的过表达或低表达与胶质瘤的发生及预后有关。这种异常表达可能导致细胞增殖、分化和转移等重要病理过程的失调。本研究旨在提出一种新的HOX相关特征,以预测PGs患者的预后和免疫浸润特征。利用从公开数据库获得的PGs数据,揭示HOX家族基因(HFGs)异常表达、预后、肿瘤免疫浸润、临床特征和基因组特征之间的关系。使用一致性聚类法利用HFGs识别异质性亚型。然后在训练集中执行随机森林监督分类算法和最近收缩质心算法以开发预后特征。最后,在内部测试集和外部独立队列中验证该特征。首先,我们鉴定了与正常组织相比在PGs中显著差异表达的HFGs。然后根据HFGs表达谱将PGs个体分为两种异质性亚型(HOX-SI和HOX-SII)。HOX-SII显示出比HOX-SI更高的总突变数、更低的免疫浸润和更差的预后。然后,我们基于聚类构建了一个HOX相关基因特征(包括 、 、 、 和 ),利用随机森林监督分类和最近收缩质心算法进行亚型预测。多变量Cox回归分析显示该特征是PGs患者的独立预后因素。我们的研究为PGs的预后分类提供了一种新方法。研究结果还表明,HOX相关特征是PGs患者诊断和预后的新生物标志物,能够实现更准确的生存预测。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c482/10401438/29cfa16a5ec8/fcell-11-1203650-g001.jpg

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