Single-cell Landscape Analysis Reveals Distinct Regression Trajectories and Novel Prognostic Biomarkers in Primary Neuroblastoma

Overview

Journal Genes Dis

Date 2022 Sep 26

PMID 36157484

Authors

Qingqing Liu

Zhenni Wang

Yan Jiang

Fengling Shao

Yue Ma

Mingzhao Zhu

Qing Luo

Yang Bi

Lijian Cao

Liang Peng

Jianwu Zhou

Zhenzhen Zhao

Xiaobin Deng

Tong-Chuan He

Shan Wang

Affiliations

Soon will be listed here.

Abstract

Neuroblastoma (NB), which is the most common pediatric extracranial solid tumor, varies widely in its clinical presentation and outcome. NB has a unique ability to spontaneously differentiate and regress, suggesting a potential direction for therapeutic intervention. However, the underlying mechanisms of regression remain largely unknown, and more reliable prognostic biomarkers are needed for predicting trajectories for NB. We performed scRNA-seq analysis on 17 NB clinical samples and three peritumoral adrenal tissues. Primary NB displayed varied cell constitution, even among tumors of the same pathological subtype. Copy number variation patterns suggested that neuroendocrine cells represent the malignant cell type. Based on the differential expression of sets of related marker genes, a subgroup of neuroendocrine cells was identified and projected to differentiate into a subcluster of benign fibroblasts with highly expressed and , supporting a progressive pathway of spontaneous NB regression. We also identified prognostic markers ( and ) by evaluating intra-tumoral heterogeneity. Lastly, we determined that in M2-like macrophages was associated with favorable prognosis and may serve as a potential diagnostic marker and therapeutic target. In conclusion, our findings reveal novel mechanisms underlying regression and potential prognostic markers and therapeutic targets of NB.

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