Transcriptomic profiling of insulinomas reveals a new “low-endocrine” subtype with low YY1 expressions

IF 2.7 2区医学 Q2 GASTROENTEROLOGY & HEPATOLOGY

Pancreatology Pub Date : 2026-05-01 Epub Date: 2026-02-13 DOI:10.1016/j.pan.2026.02.006

Yongzheng Li , Xingwu Zhang , Qiang Xu , Xianlin Han , Dan Guo , Yixi Jiao , Hao Zhang , Bohui Yin , Xiafei Hong , Wenming Wu

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引用次数: 0

Abstract

Background

Insulinoma is the most common functional pancreatic neuroendocrine tumors, typically originating from pancreatic β cells. However, the transcriptional heterogeneity and the regulatory role of transcription factor YY1 remain incompletely understood.

Methods

High-throughput bulk-RNA sequencing was conducted on insulinoma tumor samples. Unsupervised clustering algorithms were employed to identify molecular subtypes of insulinomas. YY1 mutation status was analyzed by whole-exome sequencing. Functional roles of YY1 were analyzed by Yy1-overexpression and knockdown in INS-1 cell line. Spatial transcriptomic characteristics of insulinoma were analyzed using Visium HD platform.

Results

Transcriptomic analysis identified two distinct expression patterns: a low-endocrine subtype and an endocrine subtype. The low-endocrine subtype was characterized by reduced PDX1 and insulin synthesis pathways, with an enrichment in exocrine-related functions. However, these two subtypes exhibited similar clinicopathological features. Notably, while YY1 mutation rates were comparable between the two subtypes, YY1 expression levels were significantly reduced in the low-endocrine subtype. Functional experiments demonstrated that Yy1 levels directly correlated with insulin production, as Yy1 overexpression in INS-1 cells markedly upregulated insulin processing genes and secretory pathways. Yy1 knockdown led to suppression of insulin. Furthermore, spatial transcriptomics confirmed that low-endocrine subtype possessed reduced insulin scores compared to the endocrine subtype.

Conclusion

We found a low-endocrine subtype insulinoma with reduced YY1 expression and insulin synthesis transcriptomic signature. This highlights the transcriptomic heterogeneity of insulinomas.

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胰岛素瘤的转录组学分析揭示了一种具有低YY1表达的新“低内分泌”亚型。

背景：胰岛素瘤是最常见的功能性胰腺神经内分泌肿瘤，通常起源于胰腺β细胞。然而，转录因子YY1的转录异质性和调控作用尚不完全清楚。方法：对胰岛素瘤标本进行高通量bulk-RNA测序。采用无监督聚类算法识别胰岛素瘤的分子亚型。通过全外显子组测序分析YY1突变状态。通过在INS-1细胞系中过表达和敲低YY1来分析YY1的功能作用。利用Visium HD平台分析胰岛素瘤的空间转录组学特征。结果：转录组学分析确定了两种不同的表达模式：低内分泌亚型和内分泌亚型。低内分泌亚型的特征是PDX1和胰岛素合成途径减少，外分泌相关功能丰富。然而，这两种亚型表现出相似的临床病理特征。值得注意的是，虽然YY1突变率在两种亚型之间具有可比性，但YY1的表达水平在低内分泌亚型中显著降低。功能实验表明，Yy1水平与胰岛素产生直接相关，因为在INS-1细胞中，Yy1过表达可显著上调胰岛素加工基因和分泌途径。Yy1敲低导致胰岛素抑制。此外，空间转录组学证实，与内分泌亚型相比，低内分泌亚型具有更低的胰岛素评分。结论：我们发现了一种低内分泌亚型胰岛素瘤，其YY1表达和胰岛素合成转录组特征均降低。这突出了胰岛素瘤的转录组异质性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Pancreatology 医学-胃肠肝病学

CiteScore

7.20

自引率

5.60%

发文量

194

审稿时长

44 days

期刊介绍： Pancreatology is the official journal of the International Association of Pancreatology (IAP), the European Pancreatic Club (EPC) and several national societies and study groups around the world. Dedicated to the understanding and treatment of exocrine as well as endocrine pancreatic disease, this multidisciplinary periodical publishes original basic, translational and clinical pancreatic research from a range of fields including gastroenterology, oncology, surgery, pharmacology, cellular and molecular biology as well as endocrinology, immunology and epidemiology. Readers can expect to gain new insights into pancreatic physiology and into the pathogenesis, diagnosis, therapeutic approaches and prognosis of pancreatic diseases. The journal features original articles, case reports, consensus guidelines and topical, cutting edge reviews, thus representing a source of valuable, novel information for clinical and basic researchers alike.