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Polycystins and intercellular mechanotransduction: A precise dosage of polycystin 2 is necessary for alpha-actinin reinforcement of junctions upon mechanical stimulation

Author(s)
Bhoonderowa, LaxsoomeeHameurlaine, FatimaArbabian, AtousaFaqir, FahimaAmblard, FrancoisCoscoy, Sylvie
Issued Date
2016-10
DOI
10.1016/j.yexcr.2016.08.021
URI
https://scholarworks.unist.ac.kr/handle/201301/31029
Fulltext
https://www.sciencedirect.com/science/article/pii/S0014482716302609?via%3Dihub
Citation
EXPERIMENTAL CELL RESEARCH, v.348, no.1, pp.23 - 35
Abstract
Polycystins 1 and 2, which are mutated in Autosomal Polycystic Kidney Disease, are involved in mechanotransduction through various mechanisms. In renal cells, polycystins not only have an important mechanotransductive role in primary cilia but are also present in intercellular contacts but their role there remains unclear. Here, we address the hypothesis that polycystins are involved in mechanotransduction via intercellular junctions, which would be expected to have consequences on tissue organization. We focused on the role of polycystin 2, which could be involved in mechanical organization at junctions either by its channel activity or by the direct recruitment of cytoskeleton components such as the F-actin cross-linker a-actinin. After mechanical stimulation of intercellular junctions in MDCK renal epithelial cells, a-actinin is rapidly recruited but this is inhibited upon overexpression of PC2 or the D509V mutant that lacks channel activity, and is also decreased upon PC2 silencing. This suggests that a precise dosage of PC2 is necessary for an adequate mechanosensitive alpha-actinin recruitment at junctions. At the multicellular level, a change in PC2 expression was associated with changes in velocity in confluent epithelia and during wound healing together with a loss of orientation. This study suggests that the mechanosensitive regulation of cytoskeleton by polycystins in intercellular contacts may be important in the context of ADPKD.
Publisher
ELSEVIER INC
ISSN
0014-4827
Keyword (Author)
PolycystinAlpha-actininCytoskeletonMechanotransductionCell junctionEpithelial cellsIon channel
Keyword
E-CADHERINKIDNEY-DISEASEFOCAL ADHESIONSSTRESS FIBERSCELL MOTILITYPRIMARY CILIAMDCK CELLSCATENINRECRUITMENTBINDING

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