Three‐dimensional chromatin landscapes in somatotroph tumour

Jing Guo; Yiyuan Chen; Haibo Zhu; Xinyu Tong; Lei Cao; Yazhuo Zhang; Weiyan Xie; Chuzhong Li

doi:10.1002/ctm2.1682

Clinical and Translational Medicine (May 2024)

Three‐dimensional chromatin landscapes in somatotroph tumour

Jing Guo,
Yiyuan Chen,
Haibo Zhu,
Xinyu Tong,
Lei Cao,
Yazhuo Zhang,
Weiyan Xie,
Chuzhong Li

Affiliations

Jing Guo: Department of Neurosurgery Beijing Tiantan Hospital affiliated to Capital Medical University Beijing China
Yiyuan Chen: Department of Neurosurgery Beijing Tiantan Hospital affiliated to Capital Medical University Beijing China
Haibo Zhu: Department of Neurosurgery Beijing Tiantan Hospital affiliated to Capital Medical University Beijing China
Xinyu Tong: Annoroad Gene Technology Co., Ltd Beijing China
Lei Cao: Department of Neurosurgery Beijing Tiantan Hospital affiliated to Capital Medical University Beijing China
Yazhuo Zhang: Beijing Neurosurgical Institute Capital Medical University Beijing China
Weiyan Xie: Beijing Neurosurgical Institute Capital Medical University Beijing China
Chuzhong Li: Department of Neurosurgery Beijing Tiantan Hospital affiliated to Capital Medical University Beijing China

DOI: https://doi.org/10.1002/ctm2.1682
Journal volume & issue: Vol. 14, no. 5
pp. n/a – n/a

Abstract

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Abstract Background The three‐dimensional (3D) genome architecture plays a critical role inregulating gene expression. However, the specific alterations in thisarchitecture within somatotroph tumors and their implications for gene expression remain largely unexplored. Methods We employed Hi‐C and RNA‐seq analyses to compare the 3D genomic structures of somatotroph tumors with normal pituitary tissue. This comprehensive approachenabled the characterization of A/B compartments, topologically associateddomains (TADs), and chromatin loops, integrating these with gene expression patterns. Results We observed a decrease in both the frequency of chromosomal interactions andthe size of TADs in tumor tissue compared to normal tissue. Conversely, the number of TADs and chromatin loops was found to be increased in tumors. Integrated analysis of Hi‐C and RNA‐seq data demonstrated that changes inhigher‐order chromat in structure were associated with alterations in gene expression. Specifically, genes in A compartments showed higher density and increased expression relative to those in B compartments. Moreover, the weakand enhanced insulation boundaries were identified, and the associated genes were enriched in the Wnt/β‐Catenin signaling pathway. We identified the gainedand lost loops in tumor and integrated these differences with transcriptional changes to examine the functional relevance of the identified loops. Notably, we observed an enhanced insulation boundary and a greater number of loops in the TCF7L2 gene region within tumors, which was accompanied by an upregulation of TCF7L2 expression. Subsequently, TCF7L2 expression was confirmed through qRT‐PCR, and upregulated TCF7L2 prompted cell proliferation and growth hormone (GH) secretion in vitro. Conclusion Our results provide comprehensive 3D chromatin architecture maps of somatotroph tumors and offer a valuable resource for furthering the understanding of the underlying biology and mechanisms of gene expression regulation.

Published in Clinical and Translational Medicine

ISSN: 2001-1326 (Online)
Publisher: Wiley
Country of publisher: Australia
LCC subjects: Medicine: Medicine (General)
Website: https://onlinelibrary.wiley.com/journal/20011326

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