STN1 facilitates metastasis by promoting transcription of EMT-activator ZEB1 in pancreatic cancer

Pancreatic ductal adenocarcinoma (PDAC) poses a serious clinical challenge, demanding further exploration of its pathogenesis and therapeutic targets for metastasis, the main cause of mortality. Here, we identify STN1, a CST complex member crucial for maintaining telomere lengths and genome stabilit...

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Published inNature communications Vol. 16; no. 1; pp. 7815 - 16
Main Authors Dong, Di, Zhou, Zhe, Zhu, Minglu, Hou, Zhiyuan, Chen, Mo, Gong, Jingjing, Zhao, Xuyang, Yan, Aohui, Liang, Hui, Yin, Yuxin
Format Journal Article
LanguageEnglish
Published London Nature Publishing Group UK 21.08.2025
Nature Publishing Group
Nature Portfolio
Subjects
13
13/1
13/109
13/44
13/51
38/1
38/15
38/32
38/39
38/43
38/77
38/91
631/67/322
631/67/395
631/80/304
692/4020/1503/1712/1713
Adenocarcinoma
Cancer
Datasets
Genomes
Humanities and Social Sciences
Maintenance
Medical prognosis
Metastases
Metastasis
multidisciplinary
Pancreatic cancer
Pathogenesis
Patients
Proteins
Science
Science (multidisciplinary)
Single-stranded DNA
Stat3 protein
Statistical significance
Telomeres
Therapeutic targets
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Abstract Pancreatic ductal adenocarcinoma (PDAC) poses a serious clinical challenge, demanding further exploration of its pathogenesis and therapeutic targets for metastasis, the main cause of mortality. Here, we identify STN1, a CST complex member crucial for maintaining telomere lengths and genome stability, as a key factor in promoting PDAC metastasis. Elevated STN1 levels correlate with poor patient survival, with oncogenic protein HOXB7 as an upstream transcription factor regulating STN1 . Utilizing multiple PDAC experimental models, we discover STN1’s role in promoting metastasis by functioning as an upstream factor in epithelial-mesenchymal transition (EMT). Our mechanistic evidence suggests that during transcription, STN1 binds to structurally displaced single-stranded DNA flanking the R-loop, recruiting STAT3 to activate ZEB1 transcription independent of its known telomere maintenance function. Notably, STAT3 inhibitors show enhanced efficiency in restraining metastatic potential in STN1-overexpressed PDAC cells, offering a potential therapeutic avenue for targeting metastasis in STN1-overexpressed PDAC patients facing an unfavorable prognosis. Metastasis of pancreatic cancer has been associated with epithelial-mesenchymal transition (EMT). Here, the authors identify STN1 as a regulator of pancreatic cancer metastasis by promoting transcription of EMT-activator ZEB1, which is independent of its known role in telomere maintenance.
AbstractList Abstract Pancreatic ductal adenocarcinoma (PDAC) poses a serious clinical challenge, demanding further exploration of its pathogenesis and therapeutic targets for metastasis, the main cause of mortality. Here, we identify STN1, a CST complex member crucial for maintaining telomere lengths and genome stability, as a key factor in promoting PDAC metastasis. Elevated STN1 levels correlate with poor patient survival, with oncogenic protein HOXB7 as an upstream transcription factor regulating STN1. Utilizing multiple PDAC experimental models, we discover STN1’s role in promoting metastasis by functioning as an upstream factor in epithelial-mesenchymal transition (EMT). Our mechanistic evidence suggests that during transcription, STN1 binds to structurally displaced single-stranded DNA flanking the R-loop, recruiting STAT3 to activate ZEB1 transcription independent of its known telomere maintenance function. Notably, STAT3 inhibitors show enhanced efficiency in restraining metastatic potential in STN1-overexpressed PDAC cells, offering a potential therapeutic avenue for targeting metastasis in STN1-overexpressed PDAC patients facing an unfavorable prognosis.
Pancreatic ductal adenocarcinoma (PDAC) poses a serious clinical challenge, demanding further exploration of its pathogenesis and therapeutic targets for metastasis, the main cause of mortality. Here, we identify STN1, a CST complex member crucial for maintaining telomere lengths and genome stability, as a key factor in promoting PDAC metastasis. Elevated STN1 levels correlate with poor patient survival, with oncogenic protein HOXB7 as an upstream transcription factor regulating STN1 . Utilizing multiple PDAC experimental models, we discover STN1’s role in promoting metastasis by functioning as an upstream factor in epithelial-mesenchymal transition (EMT). Our mechanistic evidence suggests that during transcription, STN1 binds to structurally displaced single-stranded DNA flanking the R-loop, recruiting STAT3 to activate ZEB1 transcription independent of its known telomere maintenance function. Notably, STAT3 inhibitors show enhanced efficiency in restraining metastatic potential in STN1-overexpressed PDAC cells, offering a potential therapeutic avenue for targeting metastasis in STN1-overexpressed PDAC patients facing an unfavorable prognosis. Metastasis of pancreatic cancer has been associated with epithelial-mesenchymal transition (EMT). Here, the authors identify STN1 as a regulator of pancreatic cancer metastasis by promoting transcription of EMT-activator ZEB1, which is independent of its known role in telomere maintenance.
Pancreatic ductal adenocarcinoma (PDAC) poses a serious clinical challenge, demanding further exploration of its pathogenesis and therapeutic targets for metastasis, the main cause of mortality. Here, we identify STN1, a CST complex member crucial for maintaining telomere lengths and genome stability, as a key factor in promoting PDAC metastasis. Elevated STN1 levels correlate with poor patient survival, with oncogenic protein HOXB7 as an upstream transcription factor regulating STN1. Utilizing multiple PDAC experimental models, we discover STN1’s role in promoting metastasis by functioning as an upstream factor in epithelial-mesenchymal transition (EMT). Our mechanistic evidence suggests that during transcription, STN1 binds to structurally displaced single-stranded DNA flanking the R-loop, recruiting STAT3 to activate ZEB1 transcription independent of its known telomere maintenance function. Notably, STAT3 inhibitors show enhanced efficiency in restraining metastatic potential in STN1-overexpressed PDAC cells, offering a potential therapeutic avenue for targeting metastasis in STN1-overexpressed PDAC patients facing an unfavorable prognosis.Metastasis of pancreatic cancer has been associated with epithelial-mesenchymal transition (EMT). Here, the authors identify STN1 as a regulator of pancreatic cancer metastasis by promoting transcription of EMT-activator ZEB1, which is independent of its known role in telomere maintenance.
ArticleNumber 7815
Author Zhou, Zhe
Hou, Zhiyuan
Dong, Di
Gong, Jingjing
Zhao, Xuyang
Zhu, Minglu
Chen, Mo
Liang, Hui
Yan, Aohui
Yin, Yuxin
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Snippet Pancreatic ductal adenocarcinoma (PDAC) poses a serious clinical challenge, demanding further exploration of its pathogenesis and therapeutic targets for...
Abstract Pancreatic ductal adenocarcinoma (PDAC) poses a serious clinical challenge, demanding further exploration of its pathogenesis and therapeutic targets...
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Adenocarcinoma
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Title STN1 facilitates metastasis by promoting transcription of EMT-activator ZEB1 in pancreatic cancer
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