Lack of α8 integrin leads to morphological changes in renal mesangial cells, but not in vascular smooth muscle cells

Marek, Ines; Volkert, Gudrun; Jahn, Angelika; Fahlbusch, Fabian; Zürn, Christina; Özcan, Zehra; Goppelt‐Struebe, Margarete; Hilgers, Karl F.; Rascher, Wolfgang; Hartner, Andrea

doi:10.1186/1471-2121-11-102

Cited by 16 publications

(18 citation statements)

References 45 publications

(52 reference statements)

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“…Overexpression of the itga8 did not lead to increases in the expression of matrix components (except for fi bronectin in tubular epithelial cells), but more likely to a downregulation of several matrix molecules. Thus, our results do not argue for an unequivocal profi brotic effect of itga8 expression, neither in mesenchymal nor in epithelial cells, although data from previous experiments (Marek et al, 2010) suggested that the expression of the itga8 might promote a phenotypic change to a more activated mesenchymal phenotype, which is responsible for increased matrix production of cells affected.…”

Section: Discussioncontrasting

confidence: 88%

“…Profi brotic agents like TGF β -1 and angiotensin II are able to induce the expression of the itga8 in different cell types, supporting the notion that α 8 β 1 integrin might exert profi brotic effects (Bouzeghrane et al, 2004;Hartner et al, 1999). Mesangial cells defi cient for the itga8 downregulate the expression of α -smooth muscle actin (a marker of myofi broblast activation) and the profi brotic cytokine CTGF (Marek et al, 2010), further arguing for a contribution of α 8 β 1 90 G. VOLKERT ET AL.…”

Section: Introductionmentioning

confidence: 77%

“…Altogether, loss of the itga8 did not lead to uniform effects in all experiments, but changed the expression of extracellular matrix and its regulators depending on the cell type and on the kind of knock down of the itga8. These fi ndings could at least partly be explained by differences in compensatory mechanisms after itga8 knock down: For example, in α 8 integrin-defi cient mesangial cells, not in α 8 integrin-defi cient vascular smooth-muscle cells or mesangial cells with a transient knock down of the itga8, an increased expression of the α 2 integrin chain is observed, which might account for at least some of the expressional differences detected in these cells (Marek et al, 2010). However, whether the increase in the expression of the α 2 integrin chain in α 8 integrin-defi cient mesangial cells could result in TGF β -1 upregulation, remains unclear, because α 2 integrin-defi cient mice were shown to have increased TGF β -1 expression levels (Girgert et al, 2010).…”

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confidence: 97%

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Contribution of the α8 Integrin Chain to the Expression of Extracellular Matrix Components

Volkert

Jahn

Dinkel

et al. 2014

Cell Communication & Adhesion

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In the kidney, the α 8 integrin chain (itga8) is expressed in mesenchymal cells and is upregulated in fi brotic disease. We hypothesized that itga8 mediates a profi brotic phenotype of renal cells by promoting extracellular matrix and cytokine expression. Genetic itga8 defi ciency caused complex changes in matrix expression patterns in mesangial and smooth-muscle cells, with the only concordant effect in both cell types being a reduction of collagen III expression. Silencing of itga8 with siRNA led to a decline of matrix turnover with repression of matrix metalloproteinases and reduction of matrix production. In contrast, de novo expression of itga8 in tubular epithelial cells resulted in reduced collagen synthesis. Overexpression of itga8 in fi broblasts did not change the expression of matrix molecules or regulators of matrix turnover. Thus, the infl uence of itga8 on the expression of matrix components was not uniform and celltype dependent. Itga8 seems unlikely to exert overall profi brotic effects in renal cells.

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Section: Discussioncontrasting

confidence: 88%

Section: Introductionmentioning

confidence: 77%

mentioning

confidence: 97%

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Contribution of the α8 Integrin Chain to the Expression of Extracellular Matrix Components

Volkert

Jahn

Dinkel

et al. 2014

Cell Communication & Adhesion

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“…They are composed of integrin ␣ (Itg ␣) and integrin ␤ (Itg ␤) subunits, and each Itg ␣␤ combination has its own signaling properties and binding specificity. A number of integrin subunits, such as ␣v, ␣4, ␣5, ␣6, ␤1, ␤3, ␤4, ␤5, ␣6␤1, and ␣␤3, are expressed in SMCs (33)(34)(35). We found that the specific antibodies against ␣v, ␣6, ␤1, ␤3, ␣6␤1, and ␣␤3 significantly blocked PDGF-BBinduced SMC migration, but the antibodies against ␣4, ␣5, ␤4, and ␤5 had no effect on PDGF-BB-induced SMC migration (Fig.…”

Section: Pdgf-bb-induced Cyr61 Has No Feedback Effect On the Activatimentioning

confidence: 72%

The Matricellular Protein Cyr61 Is a Key Mediator of Platelet-derived Growth Factor-induced Cell Migration

Zhang

Feng

et al. 2015

Journal of Biological Chemistry

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Background: PDGF is a potent chemoattractant for cells. Results:The PDGF-induced extracellular matrix component Cyr61 bridges the intracellular PDGF-ERK and JNK signaling pathways with integrin/FAK signaling, leading to cell migration. Conclusion: Cyr61 is a key mediator of PDGF-induced cell migration via the Cyr61-integrin-FAK pathway. Significance: Extracellular Cyr61 convergence with growth factor and integrin/FAK signaling is a new cell migration concept.

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“…Alpha8 integrin ( Itga8 ) is an RGD binding integrin which is expressed on mesangial cells and regulates their biological properties including adhesion, proliferation, migration and apoptosis by interacting with extracellular ligands such as fibronectin, vitronectin or osteopontin [22, 23]. Its role for phagocytosis is not yet known.…”

Section: Introductionmentioning

confidence: 99%

Expression of the Alpha8 Integrin Chain Facilitates Phagocytosis by Renal Mesangial Cells

Marek¹,

Becker²,

Fahlbusch³

et al. 2018

Cell Physiol Biochem

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Background/Aims: Healing of mesangioproliferative glomerulonephritis involves degradation of excess extracellular matrix, resolution of hypercellularity by apoptosis and phagocytosis of apoptotic cells. Integrin receptors participate in the regulation of phagocytosis. In mice deficient for alpha8 integrin (Itga8-/-) healing of glomerulonephritis is delayed. As Itga8 is abundant in mesangial cells (MC) which are non-professional phagocytes, we hypothesized that Itga8 facilitates phagocytosis of apoptotic cells and matrix components by MC. Methods: MC were isolated from wild type (WT) and Itga8-/- mice. Latex beads were coated with matrix components. Apoptosis was induced by cisplatin in macrophages and in DiI-stained MC. After coincubation of latex beads or apoptotic cells with MC, the phagocytosis rate was detected in WT and Itga8-/- MC via fluorescence microscopy and FACS analysis. Results: Itga8-/- MC showed reduced phagocytosis of matrix-coated beads and apoptotic cells compared to WT MC. Reduction of stress fibers was observed in Itga8-/- compared to WT MC. Inhibition of cytoskeletal reorganization by inhibition of Rac1 or ROCK during phagocytosis significantly decreased the rate of phagocytosis by WT MC but not by Itga8-/- MC. Conclusion: The expression of Itga8 facilitates phagocytosis in MC, likely mediated by Itga8-cytoskeleton interactions. An impairment of MC phagocytosis might thus contribute to a delayed glomerular regeneration in Itga8-/- mice.

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Lack of α8 integrin leads to morphological changes in renal mesangial cells, but not in vascular smooth muscle cells

Cited by 16 publications

References 45 publications

Contribution of the α8 Integrin Chain to the Expression of Extracellular Matrix Components

Contribution of the α8 Integrin Chain to the Expression of Extracellular Matrix Components

The Matricellular Protein Cyr61 Is a Key Mediator of Platelet-derived Growth Factor-induced Cell Migration

Expression of the Alpha8 Integrin Chain Facilitates Phagocytosis by Renal Mesangial Cells

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