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HNF1A regulates oxaliplatin resistance in pancreatic cancer by targeting 53BP1

Renpeng Xia, Chonghui Hu, Yuancheng Ye, Xiang Zhang, Tingting Li, Rihua He, Shangyou Zheng, Xiaofeng Wen, Rufu Chen

2023International Journal of Oncology13 citationsDOIOpen Access PDF

Abstract

DNA double‑strand break repair is critically involved in oxaliplatin resistance in pancreatic ductal adenocarcinoma (PDAC). Hepatocyte nuclear factor 1 homeobox A (HNF1A) has received increased attention regarding its role in cancer progression. The present study explored the role of HNF1A in oxaliplatin resistance in PDAC. The results revealed that HNF1A expression was negatively associated with oxaliplatin chemoresistance in PDAC tissues and cell lines. HNF1A inhibition promoted the proliferation, colony formation and stemness of PDAC cells, and suppressed their apoptosis. Furthermore, HNF1A inhibition switched nonhomologous end joining to homologous recombination, thereby enhancing genomic stability and oxaliplatin resistance. Mechanistically, HNF1A transcriptionally activates p53‑binding protein 1 (53BP1) expression by directly interacting with the 53BP1 promoter region. Upregulation of HNF1A and 53BP1 induced significant inhibition of PDAC growth and oxaliplatin resistance in patient‑derived PDAC xenograft models and orthotopic models. In conclusion, the findings of the present study suggested that HNF1A/53BP1 may be a promising PDAC therapeutic target for overcoming oxaliplatin resistance.

Topics & Concepts

OxaliplatinCancer researchHNF1ADownregulation and upregulationBiologyPancreatic cancerOncogeneApoptosisCell cycleCancerColorectal cancerGeneGeneticsPancreatic and Hepatic Oncology ResearchEpigenetics and DNA MethylationPancreatic function and diabetes
HNF1A regulates oxaliplatin resistance in pancreatic cancer by targeting 53BP1 | Litcius