Use of integrated spatial transcriptomics and histopathological analysis in adamantinomatous craniopharyngiomas to identify stromal cells as a new cellular source of leukemia inhibitory factor.

IF 3.6 2区医学 Q1 CLINICAL NEUROLOGY

Journal of neurosurgery Pub Date : 2025-08-01 DOI:10.3171/2025.4.JNS243146

Wenxin Hu, Chuan Zhao, Wenrong Zheng, Yi Lin, Ning Luo, Hongxing Liu, Xingfu Wang, Xueling Qi, Xianlong Wang, Xiao-Nan Li, Zhixiong Lin

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引用次数: 0

Abstract

Objective: Adamantinomatous craniopharyngioma (ACP) is an epithelial tumor that occurs in the sellar region of the human brain. Despite resection, relapse is frequent with poor prognosis. To facilitate the development of new therapy for ACP, the authors examined the spatial distribution, cell of origin, and potential biological functions of leukemia inhibitory factor (LIF), an important stem cell self-renewal regulator, in a series of ACP tumors.

Methods: The transcriptional sites of LIF and LIF receptor (LIFR) were determined by single-cell sequencing and space transcriptome analysis. LIF and LIFR distribution characteristics in different histopathological regions were detected with immunohistochemistry and immunofluorescence analysis. The relationships between the regional distributions of different tissues and tumor imaging characteristics, tumor cell stemness, cell proliferation, LIF expression, and patient prognosis were analyzed.

Results: The authors' analysis of 39 ACPs detected LIF overexpression that was selectively enriched in cell clusters. In addition to the discovery of the stromal cells in the interstitial region, palisade epithelium, and stellate reticulum as the source cells of LIF production, the authors also revealed that LIFR was primarily generated by the cell clusters. Examination of differentially expressed genes between LIF-high and LIF-low ACP tumors indicated that the binding of LIF to LIFR may lead to the activation of the PI3K-AKT signaling pathway. Further analysis showed enrichment of LIF expression in β-catenin-positive cell clusters expressing stem cell markers of CD44, supporting its role in stem cell self-renewal. Integrated analysis with diagnostic imaging found higher level expression of LIF in cystic tumors than in solid tumors, displaying a trend toward poorer prognosis.

Conclusions: This study confirmed for the first time that LIF in ACP mainly originates from tumor microenvironment stroma. The authors' data suggest that future efforts should also include tumor stromal cells as a novel cellular and/or molecular target when developing new anticancer therapies against ACP.

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利用综合空间转录组学和组织病理学分析在金刚烷瘤性颅咽管瘤中鉴定基质细胞作为白血病抑制因子的新细胞来源。

目的：金刚素瘤性颅咽管瘤（ACP）是一种发生在人脑鞍区的上皮性肿瘤。尽管切除，复发频繁，预后差。为了促进ACP新疗法的发展，作者研究了白血病抑制因子（LIF）的空间分布、细胞起源和潜在的生物学功能，LIF是一种重要的干细胞自我更新调节因子，在一系列ACP肿瘤中。方法：通过单细胞测序和空间转录组分析确定LIF和LIF受体（LIFR）的转录位点。采用免疫组织化学和免疫荧光法检测不同组织病理区域的LIF和LIFR分布特征。分析不同组织的区域分布与肿瘤影像学特征、肿瘤细胞干性、细胞增殖、LIF表达及患者预后的关系。结果：作者对39个ACPs的分析检测到LIF过表达，并在细胞簇中选择性富集。除了发现间质区基质细胞、栅栏上皮和星状网是产生LIFR的细胞来源外，作者还发现LIFR主要由细胞团产生。对liff -高和liff -低ACP肿瘤之间差异表达基因的检测表明，LIF与LIFR的结合可能导致PI3K-AKT信号通路的激活。进一步分析表明，在表达CD44干细胞标志物的β-catenin阳性细胞簇中，LIF表达富集，支持其在干细胞自我更新中的作用。结合诊断影像学分析发现，囊性肿瘤中LIF的表达水平高于实体瘤，表现出预后较差的趋势。结论：本研究首次证实ACP中的LIF主要来源于肿瘤微环境间质。作者的数据表明，在开发针对ACP的新抗癌疗法时，未来的努力还应包括将肿瘤基质细胞作为新的细胞和/或分子靶点。

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来源期刊

Journal of neurosurgery 医学-临床神经学

CiteScore

7.20

自引率

7.30%

发文量

1003

审稿时长

1 months

期刊介绍： The Journal of Neurosurgery, Journal of Neurosurgery: Spine, Journal of Neurosurgery: Pediatrics, and Neurosurgical Focus are devoted to the publication of original works relating primarily to neurosurgery, including studies in clinical neurophysiology, organic neurology, ophthalmology, radiology, pathology, and molecular biology. The Editors and Editorial Boards encourage submission of clinical and laboratory studies. Other manuscripts accepted for review include technical notes on instruments or equipment that are innovative or useful to clinicians and researchers in the field of neuroscience; papers describing unusual cases; manuscripts on historical persons or events related to neurosurgery; and in Neurosurgical Focus, occasional reviews. Letters to the Editor commenting on articles recently published in the Journal of Neurosurgery, Journal of Neurosurgery: Spine, and Journal of Neurosurgery: Pediatrics are welcome.