Interphase microtubule organization is critical for cell function and tissue architecture. In general, physical mechanisms are sufficient to drive microtubule organization in single cells, whereas cells within tissues are thought to utilize signalling mechanisms. By improving the imaging and quantitation of microtubule alignment within developing Drosophila embryos, here we demonstrate that microtubule alignment underneath the apical surface of epithelial cells follows cell shape. During development, epidermal cell elongation and microtubule alignment occur simultaneously, but by perturbing cell shape, we discover that microtubule organization responds to cell shape, rather than the converse. A simple set of microtubule behaviour rules is sufficient for a computer model to mimic the observed responses to changes in cell surface geometry. Moreover, we show that microtubules colliding with cell boundaries zip-up or depolymerize in an angle-dependent manner, as predicted by the model. Finally, we show microtubule alignment responds to cell shape in diverse epithelia.
An effective boundary condition is derived for the top of the troposphere, based on a wave radiation condition at the tropopause. This boundary condition, which can be formulated as a pseudodifferential equation, leads to new vertical dissipative modes. These modes can be computed explicitly in the classical setup of a hydrostatic, nonrotating atmosphere with a piecewise constant Brunt-V€ ais€ al€ a frequency.In the limit of an infinitely strongly stratified stratosphere, these modes lose their dissipative nature and become the regular baroclinic tropospheric modes under the rigid-lid approximation. For realistic values of the stratification, the decay time scales of the first few modes for mesoscale disturbances range from an hour to a week, suggesting that the time scale for some atmospheric phenomena may be set up by the rate of energy loss through upward-propagating waves.Corresponding author address: Lyubov Chumakova, MIT 2-376,
Robustness of biological systems is crucial for their survival, however, for many systems its origin is an open question. Here we analyze one sub-cellular level system, the microtubule cytoskeleton. Microtubules self-organize into a network, along which cellular components are delivered to their biologically relevant locations. While the dynamics of individual microtubules is sensitive to the organism's environment and genetics, a similar sensitivity of the overall network would result in pathologies. Our large-scale stochastic simulations show that the self-organization of microtubule networks is robust in a wide parameter range in individual cells. We confirm this robustness in vivo on the tissue-scale using genetic manipulations of Drosophila epithelial cells. Finally, our minimal mathematical model shows that the origin of robustness is the separation of time-scales in microtubule dynamics rates. Altogether, we demonstrate that the tissue-scale self-organization of a microtubule network depends only on cell geometry and the distribution of the microtubule minus-ends.
Robustness of biological systems is crucial for their survival, however, for many systems its origin is an open question. Here we analyze one sub-cellular level system, the microtubule cytoskeleton. Microtubules self-organize into a network, along which cellular components are delivered to their biologically relevant locations. While individual microtubule are highly dynamic with their dynamics depends on the organism environment and genetics, network sensitivity to this dynamics would result in pathologies. Combining mathematical modelling with genetic manipulations in Drosophila, we show that the microtubule self-organization indeed does not depend on dynamics of individual microtubules, and thus is robust on the tissue level. We demonstrate the origin of this robustness via a mathematical model, suggesting this being a generic mechanism.
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