ZEB1 induces LOXL2-mediated collagen stabilization and deposition in the extracellular matrix to drive lung cancer invasion and metastasis

Peng, David H.; Ungewiss, Christin; Tong, Pan; Byers, Lauren A.; Wang, J.; Canales, Jaime Rodriguez; Villalobos, Pamela; Uraoka, Naohiro; Mino, Barbara; Behrens, Carmen; Wistuba, Ignacio I.; Han, Richard I.; Wanna, C. A.; Fahrenholtz, Monica; Grande‐Allen, K. Jane; Creighton, Chad J.; Gibbons, Don L.

doi:10.1038/onc.2016.358

Cited by 165 publications

(160 citation statements)

References 57 publications

(95 reference statements)

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“…These observations are in line with this study that cell proliferation and migration activity of HCFs are significantly inhibited by interfering with the expression of ZEB1 (Figure A,B), and these findings are according with that miR‐590‐3p suppress cell proliferation and migration of cardiac fibroblasts (Figure C,D) and cancer cells . Furthermore, ZEB1 significantly induces the mRNA expression of Col1A1 and Col3A1 of ECM‐related genes to dive lung cancer invasion and metastasis, and this report is according to our study that the mRNA and protein expressions of Col1A1 and Col3A1 are significantly decreased by interfering with the expression of ZEB1 (Figure C,D). These results demonstrate that ZEB1 promotes the proliferation, differentiation, migration and collagen synthesis of cardiac fibroblasts.…”

Section: Discussionsupporting

confidence: 90%

MiR‐590‐3p regulates proliferation, migration and collagen synthesis of cardiac fibroblast by targeting ZEB1

Yuan

Pan

Wen

et al. 2019

J Cellular Molecular Medi

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Previous studies have implicated the attractive and promising role of miR‐590‐3p to restore the cardiac function following myocardial infarction (MI). However, the molecular mechanisms for how miR‐590‐3p involves in cardiac fibrosis remain largely unexplored. Using human cardiac fibroblasts (HCFs) as the cellular model, luciferase report assay, mutation, EdU assay and transwell migration assay were applied to investigate the biological effects of miR‐590‐3p on the proliferation, differentiation, migration and collagen synthesis of cardiac fibroblasts. We found that miR‐590‐3p significantly suppressed cell proliferation and migration of HCFs. The mRNA and protein expression levels of α‐SMA, Col1A1 and Col3A were significantly decreased by miR‐590‐3p. Moreover, miR‐590‐3p directly targeted at the 3’UTR of ZEB1 to repress the translation of ZEB1. Interfering with the expression of ZEB1 significantly decreased the cell proliferation, migration activity, mRNA and protein expressions of α‐SMA, Col1A1 and Col3A. Furthermore, the expressions of miR‐590‐3p and ZEB1 were identified in infarct area of MI model in pigs. Collectively, miR‐590‐3p suppresses the cell proliferation, differentiation, migration and collagen synthesis of cardiac fibroblasts by targeting ZEB1. These works will provide useful biological information for future studies on potential roles of miR‐590‐3p as the therapeutic target to recover cardiac function following MI.

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Section: Discussionsupporting

confidence: 90%

MiR‐590‐3p regulates proliferation, migration and collagen synthesis of cardiac fibroblast by targeting ZEB1

Yuan

Pan

Wen

et al. 2019

J Cellular Molecular Medi

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“…Next, this step should be performed and the definite mechanism behind need to be explored. LOXL-2 was suggested to be specifically involved in cell adhesion and senescence in earlier study and recently, it was proved as a role in regulating angiogenesis through collagen IV scaffolding [ 43 ] and to participated in the mechanisms in many tumors and carcinoma, like the effect on proliferation of hepatocellular carcinoma, mediating transition and proliferative growth of dormant tumor cells, and drive lung cancer invasion and metastasis [ 44 – 46 ] . However, there was no report of the role of LOXL2 in the pathogenesis of CD or ITB, and we found that LOXL2 distribution was lower in CD patients when compared with ITB, but due to the limited number of samples, we did not validated LOXL2 in a larger sample and the mechanisms warrant further investigation in the future.…”

Section: Discussionmentioning

confidence: 99%

Exploration of Serum Proteomic Profiling and Diagnostic Model That Differentiate Crohn's Disease and Intestinal Tuberculosis

Zhang

Ning

et al. 2016

PLoS ONE

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AimTo explore the diagnostic models of Crohn’s disease (CD), Intestinal tuberculosis (ITB) and the differential diagnostic model between CD and ITB by analyzing serum proteome profiles.MethodsSerum proteome profiles from 30 CD patients, 21 ITB patients and 30 healthy controls (HCs) were analyzed by using weak cationic magnetic beads combined with MALDI-TOF-MS technique to detect the differentially expressed proteins of serum samples. Three groups were made and compared accordingly: group of CD patients and HCs, group of ITB patients and HCs, group of CD patients and ITB patients. Wilcoxon rank sum test was used to screen the ten most differentiated protein peaks (P < 0.05). Genetic algorithm combining with support vector machine (SVM) was utilized to establish the optimal diagnostic models for CD, ITB and the optimal differential diagnostic model between CD and ITB. The predictive effects of these models were evaluated by Leave one out (LOO) cross validation method.ResultsThere were 236 protein peaks differently expressed between group of CD patients and HCs, 305 protein peaks differently expressed between group of ITB patients and HCs, 332 protein peaks differently expressed between group of CD patients and ITB patients. Ten most differentially expressed peaks were screened out between three groups respectively (P < 0.05) to establish diagnostic models and differential diagnostic model. A diagnostic model comprising of four protein peaks (M/Z 4964, 3029, 2833, 2900) can well distinguish CD patients and HCs, with a specificity and sensitivity of 96.7% and 96.7% respectively. A diagnostic model comprising four protein peaks (M/Z 3030, 2105, 2545, 4210) can well distinguish ITB patients and HCs, with a specificity and sensitivity of 93.3% and 95.2% respectively. A differential diagnostic model comprising three potential biomarkers protein peaks (M/Z 4267, 4223, 1541) can well distinguish CD patients and ITB patients, with a specificity and sensitivity of 76.2% and 80.0% respectively. Among the eleven protein peaks from the diagnostic models and differential diagnostic model, two have been successfully purified and identified, Those two peaks were M/Z 2900 from the diagnostic model between CD and HCs and M/Z 1541 from the differential diagnostic model between CD and ITB. M/Z 2900 was identified as appetite peptide, M/Z 1541 was identified as Lysyl oxidase-like 2 (LOXL-2).ConclusionThe differently expressed protein peaks analyzed by serum proteome with weak cationic magnetic beads combined MALDI-TOF-MS technique can effectively distinguish CD patients and HCs, ITB patients and HCs, CD patients and ITB patients. The diagnostic model between CD patients and HCs consisting of four protein peaks (M/Z 4964, 3029, 2833, 2900), the diagnostic model between ITB patients and HCs comprising four protein peaks (M/Z 3030, 2105, 2545, 4210) and the differential diagnostic model between CD patients and ITB patients comprising three protein peaks (M/Z 4267, 4223, 1541) had high specificity and sensitivity and can contribute to diag...

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“…The role of the tumor microenvironment in initiating EMT and metastasis and the role of tumor cell EMT in remodeling the tumor microenvironment can also be further explored (Gibbons et al, 2009; Peng et al, 2016), using appropriate experimental model systems. The molecular profile of a tumor may be influenced by a combination of cancer cell of origin, somatic alterations, and microenvironment.…”

Section: Resultsmentioning

confidence: 99%

Pan‐cancer survey of epithelial–mesenchymal transition markers across the Cancer Genome Atlas

Gibbons

Creighton

2017

Developmental Dynamics

103

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ZEB1 induces LOXL2-mediated collagen stabilization and deposition in the extracellular matrix to drive lung cancer invasion and metastasis

Cited by 165 publications

References 57 publications

MiR‐590‐3p regulates proliferation, migration and collagen synthesis of cardiac fibroblast by targeting ZEB1

MiR‐590‐3p regulates proliferation, migration and collagen synthesis of cardiac fibroblast by targeting ZEB1

Exploration of Serum Proteomic Profiling and Diagnostic Model That Differentiate Crohn's Disease and Intestinal Tuberculosis

Pan‐cancer survey of epithelial–mesenchymal transition markers across the Cancer Genome Atlas

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