Molecular alterations and targeted therapy in pancreatic ductal adenocarcinoma

Qian, Yunzhen; Gong, Yitao; Fan, Zhichao; Luo, Guopei; Huang, Qiuyi; Deng, Shengming; He, Cheng; Jin, Kaizhou; Ni, Quanxing; Lei, Yu; Liu, Chen

doi:10.1186/s13045-020-00958-3

Cited by 184 publications

(146 citation statements)

References 205 publications

(227 reference statements)

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“…Recent studies showed that targeting NDRG1 blocks the crosstalk between PC cells and matrix [ 83 ]. The TGF-β/Smad4 signaling axis plays an important role in regulating the TME and mediating tumor-stroma crosstalk [ 84 ]. The Met/HGF pathway not only involves the interaction between cancer cells and activated PSCs but also takes part in the crosstalk between tumor and matrix [ 85 ].…”

Section: The Role Of Fibrosis In Pcmentioning

confidence: 99%

Targeting Fibrosis: The Bridge That Connects Pancreatitis and Pancreatic Cancer

Huang

Iovanna

Santofimia‐Castaño

2021

IJMS

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Pancreatic fibrosis is caused by the excessive deposits of extracellular matrix (ECM) and collagen fibers during repeated necrosis to repair damaged pancreatic tissue. Pancreatic fibrosis is frequently present in chronic pancreatitis (CP) and pancreatic cancer (PC). Clinically, pancreatic fibrosis is a pathological feature of pancreatitis and pancreatic cancer. However, many new studies have found that pancreatic fibrosis is involved in the transformation from pancreatitis to pancreatic cancer. Thus, the role of fibrosis in the crosstalk between pancreatitis and pancreatic cancer is critical and still elusive; therefore, it deserves more attention. Here, we review the development of pancreatic fibrosis in inflammation and cancer, and we discuss the therapeutic strategies for alleviating pancreatic fibrosis. We further propose that cellular stress response might be a key driver that links fibrosis to cancer initiation and progression. Therefore, targeting stress proteins, such as nuclear protein 1 (NUPR1), could be an interesting strategy for pancreatic fibrosis and PC treatment.

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Section: The Role Of Fibrosis In Pcmentioning

confidence: 99%

Targeting Fibrosis: The Bridge That Connects Pancreatitis and Pancreatic Cancer

Huang

Iovanna

Santofimia‐Castaño

2021

IJMS

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“…Moreover, the survival period in these patients was significantly shorter when compared to those with a pancreatic tumor characterized by intact p16 functions[ 33 , 56 , 57 ]. CDK4/6 is a potential target in CDKN2A-deficient tumors and the efficacy of CDK4 inhibitors has been confirmed in PDAC preclinical models[ 58 ].…”

Section: Pdacmentioning

confidence: 99%

“…Different to solid pseudopapillary neoplasia (SPN), CTNNB1 mutations are uncommon in PDAC[ 15 , 71 ]. In PDAC, the frequency of NTRK (neurotrophic tropomyosin receptor kinase) fusion is very low (about 0.3%), but clinical trials revealed that the selective TRK (tropomyosin receptor kinase) inhibitors are also effective in PDAC harboring NTRK rearrangement[ 58 ]. NCCN guidelines suggest the use of a TRK inhibitor in NTRK gene fusion-positive advanced/metastatic pancreatic cancer[ 61 , 65 ].…”

Section: Pdacmentioning

confidence: 99%

Molecular alterations in pancreatic tumors

Visani¹,

Acquaviva²,

Leo³

et al. 2021

WJG

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Genetic alterations in pancreatic tumors can usually be classified in: (1) Mutational activation of oncogenes; (2) Inactivation of tumor suppressor genes; and (3) Inactivation of genome maintenance genes controlling the repair of DNA damage. Endoscopic ultrasound-guided fine-needle aspiration has improved pre-operative diagnosis, but the management of patients with a pancreatic lesion is still challenging. Molecular testing could help mainly in solving these “inconclusive” specimens. The introduction of multi-gene analysis approaches, such as next-generation sequencing, has provided a lot of useful information on the molecular characterization of pancreatic tumors. Different types of pancreatic tumors ( e.g. , pancreatic ductal adenocarcinomas, intraductal papillary mucinous neoplasms, solid pseudopapillary tumors) are characterized by specific molecular alterations. The aim of this review is to summarize the main molecular alterations found in pancreatic tumors.

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“…KRAS mutations occurs in the early stage of PDAC (5), whereas mutations of TP53 , SMAD4 , and CDKN2A arise in advanced pancreatic intraepithelial neoplasias and invasive pancreatic adenocarcinomas (6–8). These common genetic abnormalities can profoundly perturb protein interactions and specific signaling pathways related to cell survival (9, 10), DNA damage repair (11), angiogenesis (12, 13), invasion (14), metastasis (15) and immune responses (16, 17),…”

Section: Introductionmentioning

confidence: 99%

Dissection of N-, O- and glycosphingolipid glycosylation changes in PaTu-S pancreatic adenocarcinoma cells upon TGF-β challenge

Zhang

Holst

et al. 2021

Preprint

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Pancreatic ductal adenocarcinoma (PDAC) is characterized by poor prognosis and high mortality. Transforming growth factor-β (TGF-β) plays a key role in tumor progression, which is often associated with aberrant glycosylation. How PDAC cells respond to TGF-β and the role of glycosylation therein is, however, not well known. Here, we investigated the TGF-β-mediated response and glycosylation changes in SMAD4-deficient PaTu-8955S (PaTu-S) cell line. PaTu-S cells responded to TGF-β by upregulating SMAD2 phosphorylation and target gene expression. TGF-β induced expression of the mesenchymal marker N-cadherin, but did not significantly affect epithelial marker E-cadherin expression. The differences of N-glycans, O-glycans and glycosphingolipid (GSL) glycans in PaTu-S cells with TGF-β stimulation were examined. TGF-β treatment primarily induced N-glycome aberrations involving elevated levels of branching, core fucosylation, and sialylation in PaTu-S cells, in line with TGF-β-induced changes in the expression of glycosylation-related genes. In addition, we observed differences in O- and GSL-glycosylation profiles after TGF-β treatment, including lower levels of sialylated Tn antigen, and neoexpression of globosides. Furthermore, SOX4 expression was upregulated upon TGF-β stimulation, and its depletion blocked the TGF-β-induced N-glycomic changes. Thus, our study provides a mechanism by which TGF-β-induced N-glycosylation changes in SOX4 dependent and SMAD4 independent manner in pancreatic cancer cells. Our results open up avenues to study the relevance of glycosylation in TGF-β signaling in SMAD4 inactivated PDAC.

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Molecular alterations and targeted therapy in pancreatic ductal adenocarcinoma

Cited by 184 publications

References 205 publications

Targeting Fibrosis: The Bridge That Connects Pancreatitis and Pancreatic Cancer

Targeting Fibrosis: The Bridge That Connects Pancreatitis and Pancreatic Cancer

Molecular alterations in pancreatic tumors

Dissection of N-, O- and glycosphingolipid glycosylation changes in PaTu-S pancreatic adenocarcinoma cells upon TGF-β challenge

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