Global Gene Expression Analysis in an in vitro Fibroblast Model of Idiopathic Pulmonary Fibrosis Reveals Potential Role for CXCL14/CXCR4

Rodríguez, L. Raposo; Emblom-Callahan, Margaret C.; Chhina, Mantej K.; Bui, Sarah; Aljeburry, Bilal; Tran, Luc H.; Novak, Rebecca; Lemma, M.; Nathan, Steven D.; Grant, Geraldine M.

doi:10.1038/s41598-018-21889-7

Cited by 32 publications

(35 citation statements)

References 60 publications

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“…We speculate that a recapitulation of this morphology may promote degenerative human NP cells to assume a more juvenile phenotype. Our data suggests that VP treatment is able to support morphological changes, which shows association with a transition in degenerative NP cells to decrease expression of the fibroblastic markers CTGF, ACTA2, S100A4, and DDR2 87‐98 . and increase expression of known markers of NP and notochordal phenotype KRT19, LAMA1, and KLF6, NOG, and THBS2 14,19,60‐62 .…”

Section: Discussionmentioning

confidence: 64%

“…Our data suggests that VP treatment is able to support morphological changes, which shows association with a transition in degenerative NP cells to decrease expression of the fibroblastic markers CTGF, ACTA2, S100A4, and DDR2. [87][88][89][90][91][92][93][94][95][96][97][98] and increase expression of known markers of NP and notochordal phenotype KRT19, LAMA1, and KLF6, NOG, and THBS2. 14,19,[60][61][62] It should be noted, though, that these VP-induced effects may be unable to completely shift cells toward profiles consistent with juvenile NP, as previously specified markers, such as CDH2 and BASP1, were downregulated at all three time points.…”

Section: Upregulated Gene Setsmentioning

confidence: 99%

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Verteporfin treatment controls morphology, phenotype, and global gene expression for cells of the human nucleus pulposus

et al. 2020

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Cells of the nucleus pulposus (NP) are essential contributors to extracellular matrix synthesis and function of the intervertebral disc. With age and degeneration, the NP becomes stiffer and more dehydrated, which is associated with a loss of phenotype and biosynthetic function for its resident NP cells. Also, with aging, the NP cell undergoes substantial morphological changes from a rounded shape with pronounced vacuoles in the neonate and juvenile, to one that is more flattened and spread with a loss of vacuoles. Here, we make use of the clinically relevant pharmacological treatment verteporfin (VP), previously identified as a disruptor of yes-associated protein-TEA domain family member-binding domain (TEAD) signaling, to promote morphological changes in adult human NP cells in order to study variations in gene expression related to differences in cell shape. Treatment of adult, degenerative human NP cells with VP caused a shift in morphology from a spread, fibroblastic-like shape to a rounded, clustered morphology with decreased transcriptional activity of TEAD and serum-response factor. These changes were accompanied by an increased expression of vacuoles, NP-specific gene markers, and biosynthetic activity. The contemporaneous observation of VP-induced

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Section: Discussionmentioning

confidence: 64%

Section: Upregulated Gene Setsmentioning

confidence: 99%

Verteporfin treatment controls morphology, phenotype, and global gene expression for cells of the human nucleus pulposus

et al. 2020

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“…Our data have now shown that C2 cells can induce the expression of ACTA2 in PF and that this effect is likely to be mediated by means of miR‐27a downregulation. It is known that normal fibroblasts can adapt to in vitro culture systems by promoting markers typically associated with fibroblast activation such as ACTA2 [46], which could explain the weak positive signal for ACTA2 in our control groups. Nevertheless, our results showed a marked increase in ACTA2 fluorescent signals and mRNA upregulation in coculture and transfection experiments.…”

Section: Discussionmentioning

confidence: 88%

Deregulation of miR‐27a may contribute to canine fibroblast activation after coculture with a mast cell tumour cell line

et al. 2020

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The tumour microenvironment comprises a diverse range of cells, including fibroblasts, immune cells and endothelial cells, along with extracellular matrix. In particular, fibroblasts are of significant interest as these cells are reprogrammed during tumorigenesis to become cancer‐associated fibroblasts (CAFs), which in turn support cancer cell growth. MicroRNAs (miRNAs) have been shown to be involved in this intercellular crosstalk in humans. To assess whether miRNAs are also involved in the activation of fibroblasts in dogs, we cocultured primary canine skin fibroblasts with the canine mast cell tumour cell line C2 directly or with C2‐derived exosomes, and measured differential abundance of selected miRNAs. Expression of the CAF markers alpha‐smooth muscle actin (ACTA2) and stanniocalcin 1 confirmed the activation of our fibroblasts after coculture. We show that fibroblasts displayed significant downregulation of miR‐27a and let‐7 family members. These changes correlated with significant upregulation of predicted target mRNAs. Furthermore, RNA interference knockdown of miR‐27a revealed that cyclin G1 (CCNG1) exhibited negative correlation at the mRNA and protein level, suggesting that CCNG1 is a target of miR‐27a in canine fibroblasts and involved in their activation. Importantly, miR‐27a knockdown itself resulted in fibroblast activation, as demonstrated by the formation of ACTA2 filaments. In addition, interleukin‐6 (IL‐6) was strongly induced in our fibroblasts when cocultured, indicating potential reciprocal signalling. Taken together, our findings are consistent with canine fibroblasts being reprogrammed into CAFs to further support cancer development and that downregulation of miR‐27a may play an important role in the tumour–microenvironment crosstalk.

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“…The gathered data showed that poly P suppresses intestinal inflammation and fibrosis through downregulating of the expression of inflammation- and fibrosis-associated molecules in the intestinal epithelium [ 44 , 92 ]. Furthermore, it had been published that the CXCL14/CXCR4 chemokine axis is involved in the progression and/or activation of fibroblasts during initiation of pulmonary fibrosis in the lung [ 93 ]. In tunr, one therapeutic starting treatment could be the application of 2-aminopurine [ 94 ].…”

Section: Discussionmentioning

confidence: 99%

Polyphosphate Reverses the Toxicity of the Quasi-Enzyme Bleomycin on Alveolar Endothelial Lung Cells In Vitro

Müller

Neufurth

Wang

et al. 2021

Cancers

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The anti-cancer antitumor antibiotic bleomycin(s) (BLM) induces athyminic sites in DNA after its activation, a process that results in strand splitting. Here, using A549 human lung cells or BEAS-2B cells lunc cells, we show that the cell toxicity of BLM can be suppressed by addition of inorganic polyphosphate (polyP), a physiological polymer that accumulates and is released from platelets. BLM at a concentration of 20 µg ml−1 causes a decrease in cell viability (by ~70%), accompanied by an increased DNA damage and chromatin expansion (by amazingly 6-fold). Importantly, the BLM-caused effects on cell growth and DNA integrity are substantially suppressed by polyP. In parallel, the enlargement of the nuclei/chromatin in BLM-treated cells (diameter, 20–25 µm) is normalized to ~12 µm after co-incubation of the cells with BLM and polyP. A sequential application of the drugs (BLM for 3 days, followed by an exposure to polyP) does not cause this normalization. During co-incubation of BLM with polyP the gene for the BLM hydrolase is upregulated. It is concluded that by upregulating this enzyme polyP prevents the toxic side effects of BLM. These data might also contribute to an application of BLM in COVID-19 patients, since polyP inhibits binding of SARS-CoV-2 to cellular ACE2.

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Global Gene Expression Analysis in an in vitro Fibroblast Model of Idiopathic Pulmonary Fibrosis Reveals Potential Role for CXCL14/CXCR4

Cited by 32 publications

References 60 publications

Verteporfin treatment controls morphology, phenotype, and global gene expression for cells of the human nucleus pulposus

Verteporfin treatment controls morphology, phenotype, and global gene expression for cells of the human nucleus pulposus

Deregulation of miR‐27a may contribute to canine fibroblast activation after coculture with a mast cell tumour cell line

Polyphosphate Reverses the Toxicity of the Quasi-Enzyme Bleomycin on Alveolar Endothelial Lung Cells In Vitro

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