T cells use sophisticated shape dynamics (morphodynamics) to migrate towards and neutralize infected and cancerous cells. However, there is limited quantitative understanding of the migration process in three-dimensional extracellular matrices (ECMs) and across timescales. Here, we leveraged recent advances in lattice light-sheet microscopy to quantitatively explore the three-dimensional morphodynamics of migrating T cells at high spatio-temporal resolution. We first developed a new shape descriptor based on spherical harmonics, incorporating key polarization information of the uropod. We found that the shape space of T cells is low-dimensional. At the behavioural level, run-and-stop migration modes emerge at approximately 150 s, and we mapped the morphodynamic composition of each mode using multiscale wavelet analysis, finding 'stereotyped' motifs. Focusing on the run mode, we found morphodynamics oscillating periodically (every approx. 100 s) that can be broken down into a biphasic process: front-widening with retraction of the uropod, followed by a rearward surface motion and forward extension, where intercalation with the ECM in both of these steps likely facilitates forward motion. Further application of these methods may enable the comparison of T cell migration across different conditions (e.g. differentiation, activation, tissues and drug treatments) and improve the precision of immunotherapeutic development.
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http://dx.doi.org/10.1098/rsif.2022.0081 | DOI Listing |
Methods Mol Biol
December 2024
Department of Chromosome Science, National Institute of Genetics, Shizuoka, Japan.
The bipolar shape of the microtubule-based spindle is a pivotal morphological phenotype for accurate chromosome segregation during cell division. However, existing descriptions of spindle morphogenesis remain largely qualitative. Here, we introduce a method that provides a quantitative description of the morphological growth dynamics of spindles using Xenopus egg cytoplasmic extract and a computational image analysis pipeline.
View Article and Find Full Text PDFProc Natl Acad Sci U S A
November 2024
Van der Waals-Zeeman Institute, Institute of Physics, University of Amsterdam, Amsterdam 1098XH, The Netherlands.
Photosynthetic algae play a significant role in oceanic carbon capture. However, their performance is constantly challenged by fluctuations in environmental light conditions. While phototaxis is a common strategy to cope with such fluctuations, nonmotile species must adopt alternative mechanisms to avoid light-induced damage.
View Article and Find Full Text PDFTissue Cell
December 2024
Department of Toxicology, Ch. Charan Singh University Meerut, 250 004, India. Electronic address:
Aims: Present study demonstrates dose and time dependent effects of NiONPs (<30 nm) on the ovaries of Wistar rat.
Methods: Female rats were gavaged NiONPs or NiOMPs (5 mg/kg b.w.
bioRxiv
October 2024
Department of Cell Biology, School of Medicine, Johns Hopkins University.
Motility is a hallmark of life's dynamic processes, enabling cells to actively chase prey, repair wounds, and shape organs. Recreating these intricate behaviors using well-defined molecules remains a major challenge at the intersection of biology, physics, and molecular engineering. Although the polymerization force of the actin cytoskeleton is characterized as a primary driver of cell motility, recapitulating this process in protocellular systems has proven elusive.
View Article and Find Full Text PDFPlant Cell Physiol
December 2024
Faculty of Science, Hokkaido University, Kita-ku N10-W8, Sapporo, 060-0810 Japan.
Ubiquitination is a reversible post-translational modification involving the attachment of ubiquitin, a 76-amino acid protein conserved among eukaryotes. The protein 'ubiquitin' was named after it was found to be ubiquitously expressed in cells. Ubiquitination was first identified as a post-translational modification that mediates energy-consuming protein degradation by the proteasome.
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