Polarity mediates asymmetric trafficking of the Gβ heterotrimeric G-protein subunit GPB-1 in<i>C. elegans</i>embryos

Thyagarajan, Kalyani; Afshar, Katayoun; Gönczy, Pierre

doi:10.1242/dev.063354

Cited by 23 publications

(35 citation statements)

References 43 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In C. elegans, GaÁGDP levels are also modulated by Gbg, since depletion of Gbg results in excess pulling forces, presumably because excess GaÁGDP is available for interaction with GPR-1/2 [44,46]. Intriguingly, intracellular trafficking of the Gb protein GPB-1 is modulated in time and space in C. elegans embryos in a manner consistent with it dictating cortical GPR-1/2 localization [47]. This raises the possibility that intracellular trafficking is crucial for proper spindle positioning, as is the case for other aspects of asymmetric cell division, for instance in Drosophila sensory organ precursor cells [48,49].…”

Section: Cortical Dynein: a Force-generating Motormentioning

confidence: 98%

Mechanisms of spindle positioning: cortical force generators in the limelight

Kotak

Gönczy

2013

Current Opinion in Cell Biology

Self Cite

155

138

View full text Add to dashboard Cite

Correct positioning of the spindle governs placement of the cytokinesis furrow and thus plays a crucial role in the partitioning of fate determinants and the disposition of daughter cells in a tissue. Converging evidence indicates that spindle positioning is often dictated by interactions between the plus-end of astral microtubules that emanate from the spindle poles and an evolutionary conserved cortical machinery that serves to pull on them. At the heart of this machinery lies a ternary complex (LIN-5/GPR-1/2/Ga in Caenorhabditis elegans and NuMA/LGN/Gai in Homo sapiens) that promotes the presence of the motor protein dynein at the cell cortex. In this review, we discuss how the above components contribute to spindle positioning and how the underlying mechanisms are precisely regulated to ensure the proper execution of this crucial process in metazoan organisms IntroductionThe mitotic spindle is a diamond-shaped microtubulebased structure that faithfully segregates sister chromatids during cell division. Several types of microtubules emanate from the spindle poles, including astral microtubules that reach out to the actin rich cortex located beneath the plasma membrane ( Figure 1a). Pulling forces exerted on the plus-end of astral microtubules at the cell cortex are critical for accurately positioning the spindle with respect to cell-intrinsic or cell-extrinsic spatial cues. In turn, correct spindle positioning dictates placement of the cytokinesis furrow and is thus essential for determining the relative size and spatial disposition of the resulting daughter cells [2]. Accurate spindle positioning also ensures that cell fate determinants are appropriately segregated into daughter cells during development and in stem cell lineages [3].What features of the cell cortex allow interactions with astral microtubules to orchestrate spindle positioning? Specialized cortical sites are key. Their importance has been suggested for instance by elegant experiments in Chaetopterus oocytes, in which the meiotic spindle pulled away from its cortical attachment site using a micro-needle returns to that location once released (Figure 1b). Such experiments illustrate the existence of a mechanical link between the spindle and specialized cortical regions [4,5]. Laser microsurgery experiments in Fusarium solani or C. elegans suggested that this link corresponds to astral microtubules connecting the spindle poles with the cell cortex [6,7,8,9,10 ]. Although not the focus of this review, there are instances where pulling forces are exerted along the length of astral microtubules instead of at their plusend located at the cell cortex [11,12,13]. Work in several systems in recent years has increased our understanding of the basic principles governing spindle positioning and identified core molecular players and aspects of their mechanism of action. In this brief review, we will focus on cortically driven spindle positioning in one-cell C. elegans embryos and mammalian cells in culture. In doing so, we will discuss the nature of the t...

show abstract

Section: Cortical Dynein: a Force-generating Motormentioning

confidence: 98%

Mechanisms of spindle positioning: cortical force generators in the limelight

Kotak

Gönczy

2013

Current Opinion in Cell Biology

Self Cite

155

138

View full text Add to dashboard Cite

show abstract

“…First, endocytosis in general affects the actin cytoskeleton and reciprocally, making it challenging to analyze the two processes separately (reviewed by Galletta and Cooper, 2009). Second, inhibiting endocytosis in one-cell C. elegans embryos using a dynamin mutant results in lower levels of cortical GPB-1, thus probably influencing force generation via increased cortical dynein (Thyagarajan et al, 2011). This could explain the clathrin-like centration/rotation phenotype observed upon depletion of the early endosomal protein RAB-5 (Hyenne et al, 2012).…”

Section: Discussionmentioning

confidence: 99%

“…Primary mouse antibodies against α-tubulin (1/300; DM1A, Sigma), GFP (1/100; MAB3580, Millipore) were used together with rabbit antibodies against GPB-1 (1/200; Thyagarajan et al, 2011), LIN-5 (1/300;Nguyen-Ngoc et al, 2007), DHC-1 (1/100; Kotak et al, 2012), PGL-1 (1/300; Kawasaki et al, 1998) or TAC-1 (1/500; Bellanger and Gönczy, 2003). Secondary antibodies were Alexa488-conjugated goat anti-mouse (1:500; Life Technologies, A11001) and Cy3-conjugated goat anti-rabbit (1/1000; Jackson ImmunoResearch, 711-165-152).…”

Section: Antibodies Western Blotting and Indirect Immunofluorescencementioning

confidence: 99%

“…More general cellular processes are also harnessed to modulate forces pulling on centrosomes and spindle poles. Thus, endosomal trafficking of GPB-1 occurs in a cell-cycle-regulated manner, and it has been proposed that trafficking-dependent downregulation of cortical GPB-1 during mitosis is important to allow association of GPR-1/2 with the Gα proteins (Thyagarajan et al, 2011). Moreover, interfering with the actin cytoskeleton during mitosis results in increased pulling forces on the anterior side (Afshar et al, 2010;Berends et al, 2013), although whether this occurs via an impact on ternary complex components, and whether a similar relationship pertains to centration/rotation are unanswered questions.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Clathrin regulates centrosome positioning by promoting acto-myosin cortical tension in C. elegans embryos

Spiró

Thyagarajan

Simone

et al. 2014

Journal of Cell Science

Self Cite

View full text Add to dashboard Cite

Regulation of centrosome and spindle positioning is crucial for spatial cell division control. The one-cell Caenorhabditis elegans embryo has proven attractive for dissecting the mechanisms underlying centrosome and spindle positioning in a metazoan organism. Previous work revealed that these processes rely on an evolutionarily conserved force generator complex located at the cell cortex. This complex anchors the motor protein dynein, thus allowing cortical pulling forces to be exerted on astral microtubules emanating from microtubule organizing centers (MTOCs). Here, we report that the clathrin heavy chain CHC-1 negatively regulates pulling forces acting on centrosomes during interphase and on spindle poles during mitosis in one-cell C. elegans embryos. We establish a similar role for the cytokinesis/apoptosis/ RNA-binding protein CAR-1 and uncover that CAR-1 is needed to maintain proper levels of CHC-1. We demonstrate that CHC-1 is necessary for normal organization of the cortical acto-myosin network and for full cortical tension. Furthermore, we establish that the centrosome positioning phenotype of embryos depleted of CHC-1 is alleviated by stabilizing the acto-myosin network. Conversely, we demonstrate that slight perturbations of the acto-myosin network in otherwise wild-type embryos results in excess centrosome movements resembling those in chc-1(RNAi) embryos. We developed a 2D computational model to simulate cortical rigidity-dependent pulling forces, which recapitulates the experimental data and further demonstrates that excess centrosome movements are produced at medium cortical rigidity values. Overall, our findings lead us to propose that clathrin plays a critical role in centrosome positioning by promoting acto-myosin cortical tension.

show abstract

“…Thus, the asymmetry in Gβγ could contribute to the asymmetry in pulling forces and posterior displacement of the spindle in mitosis. A recent study showed dynamic regulation of cortical GPB-1 levels and trafficking through both early endosomes and recycling endosomes (Thyagarajan et al 2011). In metaphase of the zygote, trafficking rates are higher in the anterior than the posterior, and more GPB-1 remains present in endosomal vesicles in the posterior.…”

Section: The Gα Gtpase Cycle Is Essential For Pulling Force Generationmentioning

confidence: 99%

Polarity Control of Spindle Positioning in the C. elegans Embryo

Fielmich

Heuvel

2015

Cell Polarity 2

View full text Add to dashboard Cite

Cell and tissue polarity guides a large variety of developmental processes, including the choice between symmetric and asymmetric cell division. Asymmetric divisions create cell diversity and are needed for the maintenance of tissue-specific stem cells. Symmetric divisions, on the other hand, promote exponential cell proliferation. Polarized cells often divide symmetrically by cleaving along the axis of polarity. Alternatively, cell cleavage in a plane perpendicular to the polarity axis results in asymmetric division. To control this decision, developmental cues position the mitotic spindle, which instructs the plane of cell cleavage. In animal cells, the positioning of the spindle depends on evolutionarily conserved interactions between a heterotrimeric G-protein alpha subunit, TPR-GoLoco domain protein, and NuMA-related coiled-coil protein. This trimeric complex recruits the dynein microtubule motor and captures astral microtubules at the cortex. The interplay between dynein movement and depolymerizing microtubules generates cortical pulling forces that promote aster movement and spindle positioning. Through mechanisms that are poorly understood, cell polarity and other developmental signals control the microtubule-pulling forces to instruct the orientation and plane of cell division. In this chapter, we review the current understanding of the connection between cell polarity and spindle positioning, with a focus on studies of the early C. elegans embryo. The nematode C. elegans develops through a highly reproducible division pattern and has proven to be a powerful model for studying the regulation and execution of asymmetric cell division.

show abstract

Polarity mediates asymmetric trafficking of the Gβ heterotrimeric G-protein subunit GPB-1 inC. elegansembryos

Cited by 23 publications

References 43 publications

Mechanisms of spindle positioning: cortical force generators in the limelight

Mechanisms of spindle positioning: cortical force generators in the limelight

Clathrin regulates centrosome positioning by promoting acto-myosin cortical tension in C. elegans embryos

Polarity Control of Spindle Positioning in the C. elegans Embryo

Contact Info

Product

Resources

About