The TGF-β/Smad4 Signaling Pathway in Pancreatic Carcinogenesis and Its Clinical Significance

Ahmed, Sunjida; Bradshaw, Azore Dee; Gera, Shweta; Dewan, M. Zahidunnabi; Xu, Ruliang

doi:10.3390/jcm6010005

Cited by 140 publications

(121 citation statements)

References 92 publications

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“…10,58,59 Recent studies suggest TGF-β signalling may lead to muscle atrophy by a mechanism which is ROS dependent 25 and plays a central role in fibrosis. 60 TGF-β signals can activate SMADdependent canonical pathway, 61 as well as induce the JNK/p38 MAPK signalling pathway (non-canonical). 62 However, the signalling pathway underlying TGF-β effect upon ECM expression in the tumour of cachectic patients has not been previously identified.…”

Section: Discussionmentioning

confidence: 99%

Tumour‐derived transforming growth factor‐β signalling contributes to fibrosis in patients with cancer cachexia

Lima

Simoes

Castro

et al. 2019

J cachexia sarcopenia muscle

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Background Cachexia is a paraneoplastic syndrome related with poor prognosis. The tumour micro‐environment contributes to systemic inflammation and increased oxidative stress as well as to fibrosis. The aim of the present study was to characterise the inflammatory circulating factors and tumour micro‐environment profile, as potentially contributing to tumour fibrosis in cachectic cancer patients. Methods 74 patients (weight stable cancer n = 31; cachectic cancer n = 43) diagnosed with colorectal cancer were recruited, and tumour biopsies were collected during surgery. Multiplex assay was performed to study inflammatory cytokines and growth factors. Immunohistochemistry analysis was carried out to study extracellular matrix components. Results Higher protein expression of inflammatory cytokines and growth factors such as epidermal growth factor, granulocyte–macrophage colony‐stimulating factor, interferon‐α, and interleukin (IL)‐8 was observed in the tumour and serum of cachectic cancer patients in comparison with weight‐stable counterparts. Also, IL‐8 was positively correlated with weight loss in cachectic patients (P = 0.04; r = 0.627). Immunohistochemistry staining showed intense collagen deposition (P = 0.0006) and increased presence of α‐smooth muscle actin (P < 0.0001) in tumours of cachectic cancer patients, characterizing fibrosis. In addition, higher transforming growth factor (TGF)‐β1, TGF‐β2, and TGF‐β3 expression (P = 0.003, P = 0.05, and P = 0.047, respectively) was found in the tumour of cachectic patients, parallel to p38 mitogen‐activated protein kinase alteration. Hypoxia‐inducible factor‐1α mRNA content was significantly increased in the tumour of cachectic patients, when compared with weight‐stable group (P = 0.005). Conclusions Our results demonstrate TGF‐β pathway activation in the tumour in cachexia, through the (non‐canonical) mitogen‐activated protein kinase pathway. The results show that during cachexia, intratumoural inflammatory response contributes to the onset of fibrosis. Tumour remodelling, probably by TGF‐β‐induced transdifferentiation of fibroblasts to myofibroblasts, induces unbalanced inflammatory cytokine profile, angiogenesis, and elevation of extracellular matrix components (EMC). We speculate that these changes may affect tumour aggressiveness and present consequences in peripheral organs.

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Section: Discussionmentioning

confidence: 99%

Tumour‐derived transforming growth factor‐β signalling contributes to fibrosis in patients with cancer cachexia

Lima

Simoes

Castro

et al. 2019

J cachexia sarcopenia muscle

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“…It also induces programmed cell death (PCD) or apoptosis of pancreatic cells by regulating the TIEG, a zinc-finger gene transducted by TGF-β/Smad4 signaling, and takes part in tumor inhibition. (24) Smad proteins regulate the TGF-β signaling pathway, and the absence of the tumor suppressor. Smad4 is one of the molecular mechanisms leading to TGF-β resistance.…”

Section: Discussionmentioning

confidence: 99%

Microarray screening of differentially expressed genes after up-regulating miR-205 or down-regulating miR-141 in cervical cancer cells

Fang

Yao

2019

Preprint

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10 11 12 13 14 15 16 17 18 19 20 2 21 Microarray screening of differentially expressed genes after up-regulating miR-205 or 22 down-regulating miR-141 in cervical cancer cells 23 Abstract 24 Cervical cancer is one of the most common gynecological malignancies. However,studies 25 on the expression and molecular mechanism of miR-205 and miR-141 in CC are insufficient 26 recently. Expression profile microarray with 21329 Oligo DNA were used to detect the 27 expression of mRNAs in miR-205 up-regulated or miR-141 down-regulated HeLa and SiHa 28 cells and mRNAs in normal HeLa and SiHa cells. Gene Ontology (GO), Kyoto Encyclopedia 29 of Genes and Genomes (KEGG) pathway were performed to assess the potential pathways 30 of miR-205 in SiHa cell.Compared with normal HeLa cell, there were 38 differentially 31 expressed genes (DEGs) in miR-205 up-regulated HeLa cell. Nine were up-regulation genes 32 and 29 were down-regulation genes. There were 23 DEGs in miR-141 down-regulated HeLa 33 cell. One was up-regulated and 22 were down-regulated. Compared with normal SiHa cell, 34 there were 128 DEGs in miR-205 up-regulated SiHa cell. One hundred and three were up-35 regulation genes and 25 were down-regulation genes. There were 80 DEGs in miR-141 36 down-regulated SiHa cell. Forty two were up-regulation genes and 28 were down-regulation 37 genes. For miR-205 up-regulated SiHa cell, GO outcome showed that "ubiquitin-protein 38 ligase activity", "MAP kinase phosphatase activity", were the most enriched terms (P < 0.05). 39 And in KEGG analysis, "Cell cycle" was notably enriched, and Smad4 in this pathway was 40 up-regulated (P < 0.05). Expression profile microarray technology can effectively screen out 41 DEGs in cervical cancer cells after up-regulating miR-205 or down-regulating miR-141. 42 Which may enable us to understand the pathogenesis and lay an important foundation for 43 the prevention and treatment of cervical cancer. 44 Keywords: Gene expression profiling, cervical cancer, miRNA. 45 Introduction 3 46 Cervical cancer is one of the most common gynecological malignancies and the fourth 47 leading cause of cancer-related death worldwide. There were 527,600 new cases of cervical 48 cancer and 265,700 deaths worldwide in 2012.(1) It is the most common cancer of women in 49 many low-income countries.(2) Persistent infection of human papillomavirus (HPV) type 16 50 and 18 are the major risk factors for cervical cancer. In HPV high-risk cervical cancer cases, 51 HPV16 and 18 phenotypes account for 70%.(3) After HPV DNA integrated into the host DNA, 52 E6 and E7 genes are expressed. E6 induces the degradation of p53, stimulates telomerase 53 activity, and induces centrosome distortion and instability of the chromosome.(4) The binding 54 of E7 protein with human pRb and E2F transcription factor mediates cell transformation, 55 leading to the separation of pRb and E2F transcription factor and making cells enter S phase 56 of cell cycle early.(5) The occurrence of cervical cancer is a multi-factor, multi-stage and 57 multi-gene proce...

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“…Beyond KRAS mutations, the mutation or loss of key tumor suppressor genes like CDKN2a (a.k.a. p16), p53 and SMAD4 are also common in PDAC . Their loss increases cell cycle rates (thru CDKN2a loss) and increases resistance to apoptosis and KRAS G12D induced senescence ( via p53 loss) .…”

Section: Oncogenes and Polyamine Metabolismmentioning

confidence: 99%

“…p16), p53 and SMAD4 are also common in PDAC. 57 Their loss increases cell cycle rates (thru CDKN2a loss) and increases resistance to apoptosis and KRAS G12D induced senescence (via p53 loss). 58 These genes also have connections to polyamine metabolism.…”

Section: Oncogenes and Polyamine Metabolismmentioning

confidence: 99%

An overview of polyamine metabolism in pancreatic ductal adenocarcinoma

Phanstiel

2017

Intl Journal of Cancer

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Pancreatic ductal adenocarcinoma (PDAC) is one of the deadliest major cancers, with a five year survival rate of less than 8%. With current therapies only giving rise to modest life extension, new approaches are desperately needed. Even though targeting polyamine metabolism is a proven anticancer strategy, there are no reports, which thoroughly survey the literature describing the role of polyamine biosynthesis and transport in PDAC. This review seeks to fill this void by describing what is currently known about polyamine metabolism in PDAC and identifies new targets and opportunities to treat this disease. Due to the pleiotropic effects that polyamines play in cells, this review covers diverse areas ranging from polyamine metabolism (biosynthesis, catabolism and transport), as well as the potential role of polyamines in desmoplasia, autophagy and immune privilege. Understanding these diverse roles provides the opportunity to design new therapies to treat this deadly cancer via polyamine depletion.

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The TGF-β/Smad4 Signaling Pathway in Pancreatic Carcinogenesis and Its Clinical Significance

Cited by 140 publications

References 92 publications

Tumour‐derived transforming growth factor‐β signalling contributes to fibrosis in patients with cancer cachexia

Tumour‐derived transforming growth factor‐β signalling contributes to fibrosis in patients with cancer cachexia

Microarray screening of differentially expressed genes after up-regulating miR-205 or down-regulating miR-141 in cervical cancer cells

An overview of polyamine metabolism in pancreatic ductal adenocarcinoma

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