Collagen/β1 integrin signaling up-regulates the ABCC1/MRP-1 transporter in an ERK/MAPK-dependent manner

Azreq, Mohammed Amine El; Naci, Dalila; Aoudjit, Fawzi

doi:10.1091/mbc.e12-02-0132

Cited by 54 publications

(47 citation statements)

References 59 publications

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“…A well-known cellular physiological adaptation contributing to chemoresistance in leukemia is enhanced expression and activity of drug efflux transporters (36). A recent CAM-DR study reported that integrin-␤1 mediated adhesion of Jurkat cells stimulated the expression of the p-glycoprotein transporter MRP1 and decreased intracellular accumulation of doxorubicin (37).…”

Section: Resultsmentioning

confidence: 99%

The Membrane-Proximal KXGFFKR Motif of α-Integrin Mediates Chemoresistance

Liu¹,

Leclair

Yap

et al. 2013

Molecular and Cellular Biology

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Cell adhesion-mediated drug resistance contributes to minimal residual disease and relapse in hematological malignancies. Here, we show that adhesion of Jurkat T-acute lymphoblastic leukemia cells to substrates engaging ␣4␤1-integrin or ␣5␤1-integrin promotes chemoresistance to doxorubicin-induced apoptosis. Reconstituted expression of ␣4␦, a truncated ␣4-integrin with KXGFFKR as the cytoplasmic motif, in ␣4-deficient cells promoted chemoresistance to doxorubicin in a manner independent of ␣4-mediated adhesion. The adhesion-independent chemoresistance did not require ␤1-integrin as the heterodimeric pair, since expression of Tac␦, a monomeric nonintegrin transmembrane protein fused to the juxtamembrane KXGFFKR, was sufficient to reproduce the phenomenon. The requirement for integrin-mediated adhesion in stimulation of Akt phosphorylation and activation was bypassed for cells expressing ␣4␦ and Tac␦. Cells expressing ␣4␦ and Tac␦ exhibited a high influx of extracellular Ca 2؉ , and inhibition of Ca 2؉ channels with verapamil attenuated the adhesion-independent chemoresistance. Tac␦ cells also exhibited greater rates of drug efflux. ␣4␦ and Tac␦ interacted with the Ca 2؉ -binding protein calreticulin, in a manner dependent on the KXGFFKR motif. Adhesion-mediated engagement of ␣4-integrins promoted an increased calreticulin-␣4 association and greater influx of extracellular Ca 2؉ than in nonadherent cells. The ␣-integrin KXGFFKR motif is involved in adhesion-mediated control of chemoresistance in T cells.

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Section: Resultsmentioning

confidence: 99%

The Membrane-Proximal KXGFFKR Motif of α-Integrin Mediates Chemoresistance

Liu¹,

Leclair

Yap

et al. 2013

Molecular and Cellular Biology

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“…The upregulation of genes promoting cell cycle arrest might be explained by mechanisms of derepression invoked as a result of the ablation of β1 integrin, whereas the upregulation of genes supporting cell cycle progression might reflect an attempt to overcome the proliferative defect caused by the loss of β1 integrin signaling. Accordingly, loss of β1 integrin signaling is supported by the observed downregulation of some of the cyclins or cyclin kinases, as well as of MAPK activity, which are known downstream effectors of β1 integrin signaling (Chiang et al, 2011;D'Amico et al, 2000;El Azreq et al, 2012;Saleem et al, 2009;Velling et al, 2004). Also of interest is the downregulation of Ovol2 and Tuba1.…”

Section: Research Article Integrins In Islet Developmentmentioning

confidence: 99%

β1 integrin is a crucial regulator of pancreatic β-cell expansion

et al. 2013

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SUMMARYDevelopment of the endocrine compartment of the pancreas, as represented by the islets of Langerhans, occurs through a series of highly regulated events encompassing branching of the pancreatic epithelium, delamination and differentiation of islet progenitors from ductal domains, followed by expansion and three-dimensional organization into islet clusters. Cellular interactions with the extracellular matrix (ECM) mediated by receptors of the integrin family are postulated to regulate key functions in these processes. Yet, specific events regulated by these receptors in the developing pancreas remain unknown. Here, we show that ablation of the β1 integrin gene in developing pancreatic β-cells reduces their ability to expand during embryonic life, during the first week of postnatal life, and thereafter. Mice lacking β1 integrin in insulin-producing cells exhibit a dramatic reduction of the number of β-cells to only ~18% of wild-type levels. Despite the significant reduction in β-cell mass, these mutant mice are not diabetic. A thorough phenotypic analysis of β-cells lacking β1 integrin revealed a normal expression repertoire of β-cell markers, normal architectural organization within islet clusters, and a normal ultrastructure. Global gene expression analysis revealed that ablation of this ECM receptor in β-cells inhibits the expression of genes regulating cell cycle progression. Collectively, our results demonstrate that β1 integrin receptors function as crucial positive regulators of β-cell expansion.

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“…We did not elucidate the exact mechanism for integrin β 1 -mediated chemoresistance in ELA cells; however, it has been shown that integrin β 1 silencing sensitizes non-small cell lung cancer cells to cisplatin treatment due to a defective activation of the EGFR signaling cascade [94]. Another mechanism mediating cisplatin resistance in ELA cells could involve integrin β 1 -mediated up-regulation of the multidrug resistance-associated protein-1 (MRP-1), as binding of collagen to integrin β 1 has been found to up-regulate expression and activity of MRP-1 in leukemic T-cells [95], and expression of MRP-1 has been correlated to cisplatin resistance of lung cancer cells [96]. Knockdown of integrin β 1 did not affect the sensitivity of ELA cells to gemcitabine, pointing to other resistance mechanisms for this drug.…”

Section: Discussionmentioning

confidence: 99%

Integrin β1, Osmosensing, and Chemoresistance in Mouse Ehrlich Carcinoma Cells

Sørensen

Rasmussen

Broberg

et al. 2015

Cell Physiol Biochem

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Background/Aims:Altered expression of the integrin family of cell adhesion receptors has been associated with initiation, progression, and metastasis of solid tumors as well as in the development of chemoresistance. Here, we investigated the role of integrins, in particular integrin β₁, in cell volume regulation and drug-induced apoptosis in adherent and non-adherent Ehrlich ascites cell lines. Methods:Adhesion phenotypes were verified by colorimetric cell-adhesion-assay. Quantitative real-time PCR and western blot were used to compare expression levels of integrin subunits. Small interfering RNA was used to silence integrin β₁ expression. Regulatory volume decrease (RVD) after cell swelling was studied with calcein-fluorescence-self-quenching and Coulter counter analysis. Taurine efflux was estimated with tracer technique. Caspase assay was used to determine apoptosis. Results:We show that adherent cells have stronger fibronectin binding and a significantly increased expression of integrin α₅, α_v, and β₁ at mRNA and protein level, compared to non-adherent cells. Knockdown of integrin β₁ reduced RVD of the adherent but not of the non-adherent cells. Efflux of taurine was unaffected. In contrast to non-adherent, adherent cells exhibited chemoresistance to chemotherapeutic drugs (cisplatin and gemcitabine). However, knockdown of integrin β₁ promoted cisplatin-induced caspase activity in adherent cells. Conclusion:Our data identifies integrin β₁ as a part of the osmosensing machinery and regulator of cisplatin resistance in adherent Ehrlich cells.

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Collagen/β1 integrin signaling up-regulates the ABCC1/MRP-1 transporter in an ERK/MAPK-dependent manner

Cited by 54 publications

References 59 publications

The Membrane-Proximal KXGFFKR Motif of α-Integrin Mediates Chemoresistance

The Membrane-Proximal KXGFFKR Motif of α-Integrin Mediates Chemoresistance

β1 integrin is a crucial regulator of pancreatic β-cell expansion

Integrin β1, Osmosensing, and Chemoresistance in Mouse Ehrlich Carcinoma Cells

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