PTEN status determines chemosensitivity to proteasome inhibition in cholangiocarcinoma

Jiang, Tianyi; Wan, Zhenghua; Lin, Yun-Kai; Zhu, Bin; Yuan, Zhen-gang; Ma, Yunhan; Shi, Yuanyuan; Zeng, Tian-Mei; Dong, Lixue; Tan, Ye-Xiong; Wang, Hongyang

doi:10.1126/scitranslmed.aay0152

Cited by 30 publications

(33 citation statements)

References 55 publications

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“…( 80 ) Cholangiocarcinoma PMSA5 a Proteasome Repression ChIP, RT-PCR Jiang et al. ( 144 ) Colorectal melanoma CDKN2A b Cell cycle Repression ChIP, RT-PCR Fang et al. ( 126 , 127 ) Abbreviation: ChIP, chromatin immunoprecipitation.…”

Section: Functions Of Bach1 In Cancer Metastasismentioning

confidence: 99%

The transcription factor BACH1 at the crossroads of cancer biology: From epithelial–mesenchymal transition to ferroptosis

Igarashi

Nishizawa

Saiki

et al. 2021

Journal of Biological Chemistry

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The progression of cancer involves not only the gradual evolution of cells by mutations in DNA but also alterations in the gene expression induced by those mutations and input from the surrounding microenvironment. Such alterations contribute to cancer cells' abilities to reprogram metabolic pathways and undergo epithelial-to-mesenchymal transition (EMT), which facilitate the survival of cancer cells and their metastasis to other organs. Recently, BTB and CNC homology 1 (BACH1), a heme-regulated transcription factor that represses genes involved in iron and heme metabolism in normal cells, was shown to shape the metabolism and metastatic potential of cancer cells. The growing list of BACH1 target genes in cancer cells reveals that BACH1 promotes metastasis by regulating various sets of genes beyond iron metabolism. BACH1 represses the expression of genes that mediate cell–cell adhesion and oxidative phosphorylation but activates the expression of genes required for glycolysis, cell motility, and matrix protein degradation. Furthermore, BACH1 represses FOXA1 gene encoding an activator of epithelial genes and activates SNAI2 encoding a repressor of epithelial genes, forming a feedforward loop of EMT. By synthesizing these observations, we propose a “two-faced BACH1 model”, which accounts for the dynamic switching between metastasis and stress resistance along with cancer progression. We discuss here the possibility that BACH1-mediated promotion of cancer also brings increased sensitivity to iron-dependent cell death (ferroptosis) through crosstalk of BACH1 target genes, imposing programmed vulnerability upon cancer cells. We also discuss the future directions of this field, including the dynamics and plasticity of EMT.

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Section: Functions Of Bach1 In Cancer Metastasismentioning

confidence: 99%

The transcription factor BACH1 at the crossroads of cancer biology: From epithelial–mesenchymal transition to ferroptosis

Igarashi

Nishizawa

Saiki

et al. 2021

Journal of Biological Chemistry

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“…Therefore, PDX model provides an alternative preclinical model for the discovery of novel treatment regimens for patients with malignant tumors. Recently, Wang et al constructed a cholangiocarcinoma PDX biobank with an engraftment rate of 83.3% (30 of 36) and used these models to reveal the chemosensitivity of proteasome inhibition in cholangiocarcinoma, which further broadened the application in medical research (17). The first report on ICC PDX model was published in 2016 by Giuliana et al, who successfully established and confirmed the histological and genetic similarity between primary tumor and PDX model (18).…”

Section: Introductionmentioning

confidence: 99%

Patient-Derived Xenograft Models for Intrahepatic Cholangiocarcinoma and Their Application in Guiding Personalized Medicine

et al. 2021

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BackgroundIntrahepatic cholangiocarcinoma (ICC) remains one of the most intractable malignancies. The development of effective drug treatments for ICC is seriously hampered by the lack of reliable tumor models. At present, patient derived xenograft (PDX) models prove to accurately reflect the genetic and biological diversity required to decipher tumor biology and therapeutic vulnerabilities. This study was designed to investigate the establishment and potential application of PDX models for guiding personalized medicine and identifying potential biomarker for lenvatinib resistance.MethodsWe generated PDX models from 89 patients with ICC and compared the morphological and molecular similarities of parental tumors and passaged PDXs. The clinicopathologic features affecting PDX engraftment and the prognostic significance of PDX engraftment were analyzed. Drug treatment responses were analyzed in IMF-138, IMF-114 PDX models and corresponding patients. Finally, lenvatinib treatment response was examined in PDX models and potential drug resistance mechanism was revealed.ResultsForty-nine PDX models were established (take rate: 55.1%). Successful PDX engraftment was associated with negative HbsAg (P = 0.031), presence of mVI (P = 0.001), poorer tumor differentiation (P = 0.023), multiple tumor number (P = 0.003), presence of lymph node metastasis (P = 0.001), and later TNM stage (P = 0.039). Moreover, patients with tumor engraftment had significantly shorter time to recurrence (TTR) (P < 0.001) and worse overall survival (OS) (P < 0.001). Multivariate analysis indicated that PDX engraftment was an independent risk factor for shortened TTR (HR = 1.84; 95% CI, 1.05–3.23; P = 0.034) and OS (HR = 2.13; 95% CI, 1.11–4.11; P = 0.024). PDXs were histologically and genetically similar to their parental tumors. We also applied IMF-138 and IMF-114 PDX drug testing results to guide clinical treatment for patients with ICC and found similar treatment responses. PDX models also facilitated personalized medicine for patients with ICC based on drug screening results using whole exome sequencing data. Additionally, PDX models reflected the heterogeneous sensitivity to lenvatinib treatment and CDH1 might be vital to lenvatinib-resistance.ConclusionPDX models provide a powerful platform for preclinical drug discovery, and potentially facilitate the implementation of personalized medicine and improvement of survival of ICC cancer patient.

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“…Meanwhile, one rejoices in surprise realizing that PNO1 de cient caused a signi cant increase in protein levels of PTEN and p53 in vivo. A previous study reported that PTEN inhibited proteasome activity and attenuated bortezomib e cacy in CHOL [39]. PTEN might modulate the function of proteasomes [40].…”

Section: Discussionmentioning

confidence: 96%

“…In addition, co-IP analysis indicated that PNO1 knockdown increased the binding of p53 to PTEN ( Figure 6B). It has been reported that PTEN attenuated bortezomib e cacy in CHOL treatment [17]. To explore the effect of manipulating PNO1 abundance on sensitivity to bortezomib, cell models in vitro and PDXs models in vivo were established.…”

Section: Pno1 Facilitates the Therapeutic Effect Of Bortezomib In Cholmentioning

confidence: 99%

PNO1 promotes human cholangiocarcinoma tumorigenesis and chemosensitivity

Chen

Huang

et al. 2021

Preprint

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Background The partner of NOB1 homolog (PNO1) is important for ribosome biogenesis and serves as an oncogene in several cancers. However, the role of PNO1 in cholangiocarcinoma (CHOL) remains largely unknown. Methods The method of mRNA microarray analysis, high-throughput screening technologies, on-line databases analysis, PDXs models, biochemistry and molecular biology have been utilized to reveal the role of PNO1 in the progression of CHOL. Results PNO1 was significantly upregulated in CHOL tissues and predicted poor prognosis. PNO1 could induce cell proliferation and metastasis in vitro and in vivo. In CHOL cells expressing wild-type p53, PNO1 knockdown increased expression of p53 and its downstream gene p21 and decreased cell viability; these effects were blocked by p53 knockout and attenuated by the p53 inhibitor PFT-a. Furthermore, PNO1 knockdown reduced global protein synthesis and inhibiting MDM2-mediated ubiquitination and p53 degradation. Moreover, PNO1 overexpression enhanced the sensitivity to bortezomib treatment in CHOL. In addition, MYC overexpression promoted PNO1 promoter activity while MYC knockdown decreased PNO1 mRNA and protein, which led to decreased cell viability and clone formation. The expression of MYC was found positively correlated with PNO1 in CHOL patients. Conclusions Collectively, upregulation of PNO1 by MYC promotes cholangiocarcinoma tumorigenesis through suppressing p53 signaling pathway and enhanced the sensitivity to bortezomib treatment. PNO1 serves as a candidate of therapeutic target in CHOL treatment and clinical chemotherapy regimen.

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PTEN status determines chemosensitivity to proteasome inhibition in cholangiocarcinoma

Cited by 30 publications

References 55 publications

The transcription factor BACH1 at the crossroads of cancer biology: From epithelial–mesenchymal transition to ferroptosis

The transcription factor BACH1 at the crossroads of cancer biology: From epithelial–mesenchymal transition to ferroptosis

Patient-Derived Xenograft Models for Intrahepatic Cholangiocarcinoma and Their Application in Guiding Personalized Medicine

PNO1 promotes human cholangiocarcinoma tumorigenesis and chemosensitivity

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