Publications
Most recent paper
DAnkrd49 and Bdbt act via Casein Kinase Iε to regulate planar polarity in Drosophila
May 2020, H Strutt and D Strutt, PLOS Genetics
Read in full on BioRxiv
Abstract
The core planar polarity proteins are essential mediators of tissue morphogenesis, controlling both the polarised production of cellular structures and polarised tissue movements. During development the core proteins promote planar polarisation by becoming asymmetrically localised to opposite cell edges within epithelial tissues, forming intercellular protein complexes that coordinate polarity between adjacent cells.
Here we describe a novel protein complex that regulates the asymmetric localisation of the core proteins in the Drosophila pupal wing. DAnkrd49 (an ankyrin repeat protein) and Bride of Doubletime (Bdbt, a non28 canonical FK506 binding protein family member) physically interact, and regulate each others levels in vivo. Loss of either protein results in a reduction in core protein asymmetry and disruption of the placement of trichomes at the distal edge of pupal wing cells. Post31 translational modifications are thought to be important for the regulation of core protein behaviour and their sorting to opposite cell edges. Consistent with this, we find that loss of DAnkrd49 or Bdbt leads to reduced phosphorylation of the core protein Dishevelled and to decreased Dishevelled levels both at cell junctions and in the cytoplasm. Bdbt has previously been shown to regulate activity of the kinase Discs Overgrown (Dco, also known as Doubletime or Casein Kinase Iε), and Dco itself has been implicated in regulating planar polarity by phosphorylating Dsh as well as the core protein Strabismus.
We demonstrate that DAnkrd49 and Bdbt act as dominant suppressors of Dco activity. These findings support a model whereby Bdbt and DAnkrd49 act together to modulate the activity of Dco during planar polarity establishment.
Selected publications
H Strutt, J Gamage and D Strutt (2019) Reciprocal action of casein kinase Iε on core planar polarity proteins regulates clustering and asymmetric localisation. eLife, 2019(8).
H Strutt, PF Langton, N Pearson, KJ McMillan, D Strutt and PJ Cullen (2019) Retromer controls planar polarity protein levels and asymmetric localisation at intercellular junctions. Current Biology, 29(.), 484–491.e6.
M Ressurreição, S Warrington and D Strutt (2018) Rapid disruption of dishevelled activity uncovers an intercellular role in maintenance of prickle in core planar polarity protein complexes. Cell Reports, 25(6), 1415–1424.e6.
SJ Warrington, H Strutt, KH Fisher and D Strutt (2017) A dual function for prickle in regulating frizzled stability during feedback-dependent amplification of planar polarity. Current Biology, 27(18), 2784–2797.e3.
H Strutt H, J Gamage and D Strutt (2016) Robust Asymmetric Localization of Planar Polarity Proteins Is Associated with Organization into Signalosome-like Domains of Variable Stoichiometry. Cell Reports, 17(10), 2660-2671.
R Hale, AL Brittle, KH Fisher, NAM Monk and D Strutt (2015) Cellular interpretation of the long-range gradient of Four-jointed activity in the Drosophila wing. Elife, 4.
A Brittle, C Thomas and D Strutt (2012) Planar polarity specification through asymmetric subcellular localisation of Fat and Dachsous. Current Biology, 22(10), 907–914.
H Strutt, SJ Warrington and D Strutt (2011) Dynamics of core planar polarity protein turnover and stable assembly into discrete membrane subdomains. Developmental Cell, 20(4), 511–525.
Full list of publications are available on David Strutt's University of Sheffield staff profile.
Planar polarity reviews
Principles of planar polarity in animal development
May 2011, L Goodrich and D Strutt, Development
Read in full on PubMed
Abstract
Planar polarity describes the coordinated polarisation of cells or structures in the plane of a tissue. The patterning mechanisms that underlie planar polarity are well characterised in Drosophila, where many events are regulated by two pathways: the 'core' planar polarity complex and the Fat/Dachsous system. Components of both pathways also function in vertebrates and are implicated in diverse morphogenetic processes, some of which self-evidently involve planar polarisation and some of which do not. Here, we review the molecular mechanisms and cellular consequences of planar polarisation in diverse contexts, seeking to identify the common principles across the animal kingdom.
Planar polarity from flies to vertebrates
Febuary 2014, M Fanto and H McNeill, Journal of Cell Science
Read in full on PubMed
Abstract
Planar cell polarity (PCP) has been demonstrated in the epithelium of organisms from flies to humans. Recent research has revealed that the planar organization of cells requires a conserved set of genes, known as the PCP genes. Tbe PCP proteins Frizzled (Fz) and Dishevelled (Dsh) function as key players in PCP signalling. Although Fz and Dsh are also involved in Wingless (Wg)/Wnt signalling, these proteins have independent functions in a non-canonical pathway dedicated to PCP. Reorganisation of the cell surface and cytoskeleton is required, and recent work has focused on how cell adhesion molecules (such as Fat, Dachsous and Flamingo) function in this process.
Methods for studying planar cell polarity
June 2014, J Olofsson and JD Axelrod, Methods
Read in full on PubMed
Abstract
Planar cell polarity (PCP) is the polarity of epithelial cells in the plane orthogonal to the apical-basal axis, and is controlled by a partially defined signaling system. PCP related signaling also plays roles in cell migration, tissue re-organization and stem cell differentiation during embryonic development, and later, in regeneration and repair. Aberrant signaling has been linked to a broad range of pathophysiologies including cancer, developmental defects, and neurological disorders. The deepest mechanistic insights have come from studies of PCP in Drosophila.
In this chapter we review tools and methods to study PCP signaling in Drosophila epithelia, where it was found to involve asymmetric protein localization that is coordinated between adjacent cells. Such signaling has been most extensively studied in wing, eye, and abdomen, but also in other tissues such as leg and notum.
In the adult fly, PCP is manifested in the coordinated direction of hairs and bristles, as well as the organization of ommatidia in the eye. The polarity of these structures is preceded by asymmetric localization of PCP signaling proteins at the apical junctions of epithelial cells. Based on genetic and molecular criteria, the proteins that govern PCP can be divided into distinct modules, including the core module, the Fat/Dachsous/Four-jointed (Fat/Ds/Fj) module (often referred to as the 'global' module) as well as tissue specific effector modules. Different tissues and tissue regions differ in their sensitivity to disturbances in the various modules of the PCP signaling system, leading to controversies about the interactions among the modules, and emphasizing the value of studying PCP in multiple contexts.
Here, we review methods including those generally applicable, as well as some that are selectively useful for analyses of PCP in eye (including eye discs), wing (including wing discs), pupal and adult abdomen, and the cuticle of larvae and embryos.
The cell biology of planar cell polarity
October 2014, D Devenport, Journal of Cell Biology
Read in full on PubMed
Abstract
Planar cell polarity (PCP) refers to the coordinated alignment of cell polarity across the tissue plane. Key to the establishment of PCP is asymmetric partitioning of cortical PCP components and intercellular communication to coordinate polarity between neighboring cells.
Recent progress has been made toward understanding how protein transport, endocytosis, and intercellular interactions contribute to asymmetric PCP protein localisation. Additionally, the functions of gradients and mechanical forces as global cues that bias PCP orientation are beginning to be elucidated. Together, these findings are shedding light on how global cues integrate with local cell interactions to organise cellular polarity at the tissue level.
Mechanisms of planar cell polarity establishment in Drosophila
November 2014, JM Carvajal-Gonzalez and M Mlodzik, F1000Prime Rep
Read in full on PubMed
Abstract
Correct patterning and polarization of epithelial and mesenchymal cells are essential for morphogenesis and function of all organs and organisms. Epithelial cells are generally polarized in two axes: (a) the ubiquitous apical-basal axis and (b) polarity within the plane of the epithelium. The latter is generally referred to as planar cell polarity (PCP) and also is found in several contexts of mesenchymal cell patterning.
In Drosophila, all adult structures display PCP features, and two conserved molecular systems (the Fat [Ft]/Dachsous [Ds] system and the Frizzled [Fz]/PCP pathway) that regulate this process have been identified. Although significant progress has been made in dissecting aspects of PCP signaling within cells, much remains to be discovered about the mechanisms of long-range and local PCP cell-cell interactions. Here, we discuss the current models based on Drosophila studies and incorporate recent insights into this long-standing cell and developmental biology problem.