Knockdown of serine/threonine protein phosphatase 5 enhances gemcitabine sensitivity by promoting apoptosis in pancreatic cancer cells inï¿½vitro

Zhu, Jinhui; Ji, Yun; Yu, Yuanquan; Yun, Jimmy; Zhang, Xiaoxiao; Zhou, Jiale; Chen, Yan

doi:10.3892/ol.2018.8363

Cited by 6 publications

(8 citation statements)

References 52 publications

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“…It is unquestionable that p53 also plays a crucial role in the drug resistance of various cancers . Thus, we investigated whether SRPK2 regulated drug resistance in a p53‐dependent manner.…”

Section: Resultsmentioning

confidence: 99%

Serine/arginine protein‐specific kinase 2 promotes the development and progression of pancreatic cancer by downregulating Numb and p53

et al. 2019

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Serine/arginine protein‐specific kinase 2 (SRPK2) plays a vital role in the progression of a range of different malignancies, including pancreatic cancer. However, the mechanisms are poorly understood. Previous studies have shown that in hepatocellular carcinoma, SRPK2 knockdown leads to the upregulation of the cell fate determining protein Numb, and in pancreatic cancer cells, Numb knockdown prevents ubiquitin‐mediated degradation of p53. In this study, we investigated the relationship between SRPK2, Numb and p53 in the development of pancreatic cancer with or without chemical agent treatment in vitro. SRPK2 expression was upregulated in pancreatic cancer tissues and associated with decreased overall survival in pancreatic cancer patients, indicating that expression of this protein can be used as a marker of unfavourable prognosis. Expression of SRPK2 was positively associated with tumour T stage and Union for International Cancer Control (UICC) stage, and negatively associated with Numb expression in serial tissue sections. In pancreatic cancer cells, SRPK2 downregulation or overexpression led to modulation of Numb and wild‐type p53 protein expression in response to oxaliplatin treatment. Furthermore, these three endogenous proteins could be coimmunoprecipitated as a triple complex. Numb or p53 knockdown reversed the upregulation of p53 that was induced by silencing SRPK2. SRPK2 overexpression promoted cell invasion and migration, and decreased chemosensitivity of cancer cells to gemcitabine or oxaliplatin treatment. Conversely, SRPK2 silencing decreased cell invasion and migration and increased chemosensitivity; these effects were reversed by silencing p53 in oxaliplatin‐treated pancreatic cancer cells. Our data suggest that SRPK2 negatively regulates p53 by downregulating Numb under chemical agent treatment. Thus, SRPK2 promotes the development and progression of pancreatic cancer in a p53‐dependent manner.

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Section: Resultsmentioning

confidence: 99%

Serine/arginine protein‐specific kinase 2 promotes the development and progression of pancreatic cancer by downregulating Numb and p53

et al. 2019

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“…PPP5C plays a pivotal role in regulating cell growth, and studies have shown thatPPP5C knockdown could inhibit cancer cell proliferation [ 40–42 ]. Zhu et al found that knockdown of PPP5C could enhance gemcitabine sensitivity by promoting apoptosis of pancreatic cancer cells; and more cells in G0/G1 phase arrest were observed in this condition [ 43 ]. In this work, we found that the mRNA expression of PPP5C was higher in pancreatic adenocarcinoma than in normal tissues and that its level correlated with tumor stage.…”

Section: Discussionmentioning

confidence: 99%

The role of phosphoprotein phosphatases catalytic subunit genes in pancreatic cancer

et al. 2021

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Compelling evidence suggests that phosphoprotein phosphatases (PPPs) are involved in a large spectrum of physiological and pathological processes, but little is known about their roles in pancreatic cancer. We investigated the expression level, prognostic value, and potential function of PPPs with data from Oncomine, GEPIA, THPA, and TCGA databases and an independent cohort of patients with pancreatic cancer. Among all the PPP catalytic subunits (PPPcs), the transcription levels of PPP1CA, PPP1CB, PPP3CA, PPP3CB, and PPP4C were higher in pancreatic cancer than in normal pancreas (P<0.01, fold change > 2). Kaplan–Meier analysis showed that high transcription levels of PPP1CA, PPP1CB, PPP2CA, PPP2CB, PPP3CA, and PPP4C correlated with poorer survival. In contrast, patients with high levels of PPP3CB, PPP3CC, PPP5C, PPP6C, and PPEF2 had much better prognoses. Data from THPA and patients with pancreatic cancer enrolled in our hospital also confirmed the prognostic value of PPP1CA, PPP1CB, PPP2CA, PPP2CB, PPP3CA, PPP3CB, and PPP6C at the protein level. In addition, the Pearson Chi-square test showed that PPP3CB level was significantly correlated with T and N stages. GO and KEGG analyses showed that the genes and pathways related to the pathogenesis and progression of pancreatic cancer were greatly affected by alterations in PPPcs. Results of the present study suggest that PPP1CA, PPP1CB, PPP2CA, PPP2CB, and PPP3CA have deleterious effects but PPP3CB, PPP5C, and PPP6C have beneficial effects on pancreatic cancer.

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“…In contrast, PPP5C mentioned in this study is a cancer-promoting factor in many cancers ( 20 , 21 ). It has been less studied in pancreatic cancer and is only known to make tumors resistant to gemcitabine ( 16 ). In this section, we would analyze our results through the lens of relevant literature in order to find the immune-related genes of colon cancer, establish a prognostic risk score model, and verify its accuracy.…”

Section: Discussionmentioning

confidence: 99%

“…On the cancer side, the role of PPP5C in proliferation and cell survival and its unique structure make it a potentially attractive therapeutic target, and elevated PPP5C expression has been found to increase proliferation in most cells in breast and renal cancer clinical studies ( 15 ). The role of PPP5C in pancreatic cancer is similar to that in other cancers: it leads to the progression of pancreatic cancer by enabling tumors to develop resistance to gemcitabine ( 16 ). Therefore, targeting the inhibition of PPP5C is particularly important in the treatment of pancreatic cancer, while miRNAs regulate the properties of mRNA expression by binding to its 3’-UTR ( 17 , 18 ).…”

Section: Introductionmentioning

confidence: 99%

MiR-520a-5p/PPP5C regulation pattern is identified as the key to gemcitabine resistance in pancreatic cancer

Shao

Yang

et al. 2022

Front. Oncol.

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ObjectiveTo explore the effects of the expression level of miR-520-5p/PPP5C in pancreatic cancer cells and exosomes on cell viability, angiogenesis, autophagy, which involved in the mechanism of gemcitabine resistance in pancreatic cancer.MethodsAPSC-1 cell line was treated with gemcitabine, after which its exosomes were extracted for NTA assay. Subsequently, the drug resistance of APSC-1 cells was assayed using CCK8, as well as the activity of HUVEC cells treated with exosomes from each group of APSC-1 cells after drug resistance treatment as well as overexpression treatment. Five groups of HUVEC cells treated with exosomes were subjected to in vitro tubule formation assay. levels of PPP5C in each group of ASPC-1 cells and their exosomes, levels of overexpressed PPP5C, and related exosomal proteins were examined by WB. mRNA expression levels of PPP5C and levels of miR-520a were examined by qPCR The relationship between miR-520a-5p and PPP5C was investigated. After that, the autophagy of PPP5C was detected. Finally, it was analyzed by TCGA database for survival prognosis analysis.ResultsAPSC-1 cells had an IC50 value of 227.1 μM for gemcitabine, elevated PPP5C expression, drug resistance, and enhanced HUVEC cell activity; exosomes CD9, CD63, and CD81 were significantly expressed in all groups; meanwhile, enhanced PPP5C expression not only promoted in vitro tubule formation but also increased autophagy levels; meanwhile, its relationship with miR-520-5p and There was a targeted inhibitory relationship between its level and miR-520-5p and PPP5C, and its elevated level also led to a decrease in the survival level of patients over 3-5 years.ConclusionPPP5C has a prognostic role in pancreatic cancer by promoting the value-added and invasion of pancreatic cancer cells, and a targeted inhibitory relationship between miR-520-5p and PPP5C was found.

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Knockdown of serine/threonine protein phosphatase 5 enhances gemcitabine sensitivity by promoting apoptosis in pancreatic cancer cells inï¿½vitro

Cited by 6 publications

References 52 publications

Serine/arginine protein‐specific kinase 2 promotes the development and progression of pancreatic cancer by downregulating Numb and p53

Serine/arginine protein‐specific kinase 2 promotes the development and progression of pancreatic cancer by downregulating Numb and p53

The role of phosphoprotein phosphatases catalytic subunit genes in pancreatic cancer

MiR-520a-5p/PPP5C regulation pattern is identified as the key to gemcitabine resistance in pancreatic cancer

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