&lt;p&gt;miR-939-5p Contributes to the Migration and Invasion of Pancreatic Cancer by Targeting ARHGAP4&lt;/p&gt;

Shen, Yehua; Chen, Gang; Gao, Hongsheng; Li, Ye; Zhuang, Liping; Meng, Zhiqiang; Liu, Luming

doi:10.2147/ott.s227644

Cited by 23 publications

(16 citation statements)

References 38 publications

(51 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…While cell biological studies on the function of ARHGAP4 were rather limited in number, there has been a significant increase of them in recent years. To date, almost all fundamental researches of ARHGAP4 have reported prominent functions in inhibiting cell migration and invasion (Shen et al, 2020;Vogt et al, 2007). Meanwhile, our study must be the first to our knowledge that revealed its molecular mechanism dominated by the SEPT2/9-driven modulation of FAs via its Rho-GAP and SH3 domains.…”

Section: Discussionmentioning

confidence: 75%

ARHGAP4-SEPT2-SEPT9 complex enables both up- and down-modulation of integrin-mediated focal adhesions, cell migration, and invasion

Kang

Matsui

Liu

et al. 2021

MBoC

View full text Add to dashboard Cite

The Rho family of GTPases are inactivated in a cell context-dependent manner by Rho-GTPase-activating proteins (Rho-GAPs), but their signaling mechanisms are poorly understood. Here we demonstrate that ARHGAP4, the Rho-GAPs, forms a complex with SEPT2 and SEPT9 via its Rho-GAP domain and SH3 domain to enable both up- and down-modulation of integrin-mediated focal adhesions (FAs). We show that silencing ARHGAP4 as well as overexpressing its two mutually independent upstream regulators SEPT2 and SEPT9 all induce reorganization of FAs to newly express Integrin Beta 1 and also enhance both cell migration and invasion. Interestingly, even if these cell migration/invasion-associated phenotypic changes are induced upon perturbations to the complex, it does not necessarily cause enhanced clustering of FAs. Instead, its extent depends on whether the microenvironment contains ligands suitable for the upregulated Integrin Beta 1. These results provide novel insights to cell migration, invasion, and microenvironment-dependent phenotypic changes regulated by the newly identified complex.

show abstract

Section: Discussionmentioning

confidence: 75%

ARHGAP4-SEPT2-SEPT9 complex enables both up- and down-modulation of integrin-mediated focal adhesions, cell migration, and invasion

Kang

Matsui

Liu

et al. 2021

MBoC

View full text Add to dashboard Cite

show abstract

“…hsa-miR-939-5p, of potential interest for its role in invasive cancer, is reportedly upregulated in lung adenocarcinomas [43], hepatocellular carcinomas [44,45], ovarian cancer tissue [46] and in the promotion of blood vessel invasion in breast cancer [47]. The recent study by Shen et al [48] shed some light on the role of this hsa-miR-939-5p in PDAC biology and prognosis. By studying human pancreatic cancer tissues and cell lines, the authors demonstrated that high expression levels of this miRNA are associated with a poor prognosis in patients, while promoting in vitro tumor cell migration and invasion by targeting the Rho GTPase, activating protein 4.…”

Section: Discussionmentioning

confidence: 98%

Serum miRNA Profiling for Early PDAC Diagnosis and Prognosis: A Retrospective Study

et al. 2021

View full text Add to dashboard Cite

Background: Tumor stage predicts pancreatic cancer (PDAC) prognosis, but prolonged and short survivals have been described in patients with early-stage tumors. Circulating microRNA (miRNA) are an emerging class of suitable biomarkers for PDAC prognosis. Our aim was to identify whether serum miRNA signatures predict survival of early-stage PDAC. Methods: Serum RNA from archival 15 stage I-III PDAC patients and 4 controls was used for miRNAs expression profile (Agilent microarrays). PDAC patients with comparable age, gender, diabetes, jaundice and surgery were classified according to survival: less than 14 months (7/15 pts, group A) and more than 22 months (8/15 pts, group B). Bioinformatic data analysis was performed by two-class Significance Analysis of Microarray (SAM) algorithm. Binary logistic regression analyses considering PDAC diagnosis and outcome as dependent variables, and ROC analyses were also performed. Results: 2549 human miRNAs were screened out. At SAM, 76 differentially expressed miRNAs were found among controls and PDAC (FDR = 0.4%), the large majority (50/76, 66%) of them being downregulated in PDAC with respect to controls. Six miRNAs were independently correlated with early PDAC, and among these, hsa-miR-6821-5p was associated with the best ROC curve area in distinguishing controls from early PDAC. Among the 71 miRNAs differentially expressed between groups A and B, the most significant were hsa-miR-3135b expressed in group A only, hsa-miR-6126 and hsa-miR-486-5p expressed in group B only. Eight miRNAs were correlated with the presence of lymph-node metastases; among these, hsa-miR-4669 is of potential interest. hsa-miR-4516, increased in PDAC and found as an independent predictor of survival, has among its putative targets a series of gens involved in key pathways of cancer progression and dissemination, such as Wnt and p53 signalling pathways. Conclusions: A series of serum miRNAs was identified as potentially useful for the early diagnosis of PDAC, and for establishing a prognosis.

show abstract

“…Among the 39 PC-specific markers, 15 miRNAs have been reported to serve as PC markers in previous studies. Some of these (miR-155-5p, miR-939-5p, miR-346, miR-3064-5p, miR-661, miR-26a-5p, miR-200b-5p, and miR-218-5p) were found to be differentially expressed in PC tissues [15][16][17][18][19][20]23,24,27,[30][31][32]34,35,[37][38][39]. miR-939-5p, miR-200b-5p, and miR-218-5p were also differentially expressed in PC cell lines.…”

Section: Discussionmentioning

confidence: 99%

Identification of Circulating Serum miRNAs as Novel Biomarkers in Pancreatic Cancer Using a Penalized Algorithm

Lee

Park

et al. 2021

IJMS

View full text Add to dashboard Cite

Pancreatic cancer (PC) is difficult to detect in the early stages; thus, identifying specific and sensitive biomarkers for PC diagnosis is crucial, especially in the case of early-stage tumors. Circulating microRNAs are promising non-invasive biomarkers. Therefore, we aimed to identify non-invasive miRNA biomarkers and build a model for PC diagnosis. For the training model, blood serum samples from 63 PC patients and 63 control subjects were used. We selected 39 miRNA markers using a smoothly clipped absolute deviation-based penalized support vector machine and built a PC diagnosis model. From the double cross-validation, the average test AUC was 0.98. We validated the diagnosis model using independent samples from 25 PC patients and 81 patients with intrahepatic cholangiocarcinoma (ICC) and compared the results with those obtained from the diagnosis using carbohydrate antigen 19-9. For the markers miR-155-5p, miR-4284, miR-346, miR-7145-5p, miR-5100, miR-661, miR-22-3p, miR-4486, let-7b-5p, and miR-4703-5p, we conducted quantitative reverse transcription PCR using samples from 17 independent PC patients, 8 ICC patients, and 8 healthy individuals. Differential expression was observed in samples from PC patients. The diagnosis model based on the identified markers showed high sensitivity and specificity for PC detection and is potentially useful for early PC diagnosis.

show abstract

<p>miR-939-5p Contributes to the Migration and Invasion of Pancreatic Cancer by Targeting ARHGAP4</p>

Cited by 23 publications

References 38 publications

ARHGAP4-SEPT2-SEPT9 complex enables both up- and down-modulation of integrin-mediated focal adhesions, cell migration, and invasion

ARHGAP4-SEPT2-SEPT9 complex enables both up- and down-modulation of integrin-mediated focal adhesions, cell migration, and invasion

Serum miRNA Profiling for Early PDAC Diagnosis and Prognosis: A Retrospective Study

Identification of Circulating Serum miRNAs as Novel Biomarkers in Pancreatic Cancer Using a Penalized Algorithm

Contact Info

Product

Resources

About