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      The morphological and functional diversity of apical microvilli

      1 , 1 , 2 , 1 , 3 , 4 , 5
      Journal of Anatomy
      Wiley

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          Cellular signalling by primary cilia in development, organ function and disease

          Primary cilia project in a single copy from the surface of most vertebrate cell types; they detect and transmit extracellular cues to regulate diverse cellular processes during development and to maintain tissue homeostasis. The sensory capacity of primary cilia relies on the coordinated trafficking and temporal localization of specific receptors and associated signal transduction modules in the cilium. The canonical hedgehog (HH) pathway, for example, is a bona fide ciliary signalling system that regulates cell fate and self-renewal in development and tissue homeostasis. Specific receptors and associated signal transduction proteins can also localize to primary cilia in a cell type-dependent manner; available evidence suggests that the ciliary constellation of these proteins can temporally change to allow the cell to adapt to specific developmental and homeostatic cues. Consistent with important roles for primary cilia in signalling, mutations that lead to their dysfunction underlie a pleiotropic group of diseases and syndromic disorders termed ciliopathies, which affect many different tissues and organs of the body. In this review we highlight central mechanisms by which primary cilia coordinate HH, G-protein-coupled receptor, WNT, receptor tyrosine kinase and TGFβ/BMP signalling, and illustrate how defects in the balanced output of ciliary signalling events are coupled to developmental disorders and disease progression.
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            Stem cells, self-renewal, and differentiation in the intestinal epithelium.

            The mammalian intestine is covered by a single layer of epithelial cells that is renewed every 4-5 days. This high cell turnover makes it a very attractive and comprehensive adult organ system for the study of cell proliferation and differentiation. The intestine is composed of proliferative crypts, which contain intestinal stem cells, and villi, which contain differentiated specialized cell types. Through the recent identification of Lgr5, an intestinal stem cell marker, it is now possible to visualize stem cells and study their behavior and differentiation in a much broader context. In this review we describe the identification of intestinal stem cells. We also discuss genetic studies that have helped to elucidate those signals important for progenitor cells to differentiate into one of the specialized intestinal epithelial cell types. These studies describe a genetic hierarchy responsible for cell fate commitment in normal gut physiology. Where relevant we also mention aberrant deregulation of these molecular pathways that results in colon cancer.
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              The Actin Cytoskeleton and Actin-Based Motility

              The actin cytoskeleton—a collection of actin filaments with their accessory and regulatory proteins—is the primary force-generating machinery in the cell. It can produce pushing (protrusive) forces through coordinated polymerization of multiple actin filaments or pulling (contractile) forces through sliding actin filaments along bipolar filaments of myosin II. Both force types are particularly important for whole-cell migration, but they also define and change the cell shape and mechanical properties of the cell surface, drive the intracellular motility and morphogenesis of membrane organelles, and allow cells to form adhesions with each other and with the extracellular matrix.
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                Author and article information

                Contributors
                (View ORCID Profile)
                (View ORCID Profile)
                Journal
                Journal of Anatomy
                Journal of Anatomy
                Wiley
                0021-8782
                1469-7580
                March 2023
                October 25 2022
                March 2023
                : 242
                : 3
                : 327-353
                Affiliations
                [1 ]Department of Cell Biology, Faculty of Medicine and Dentistry University of Alberta Edmonton Alberta Canada
                [2 ]Department of Biology University of New Brunswick Fredericton New Brunswick Canada
                [3 ]Division of Anatomy, Department of Surgery, Faculty of Medicine and Dentistry University of Alberta Edmonton Alberta Canada
                [4 ]Department of Medical Genetics, Faculty of Medicine and Dentistry University of Alberta Edmonton Alberta Canada
                [5 ]Women and Children's Health Research Institute University of Alberta Edmonton Alberta Canada
                Article
                10.1111/joa.13781
                36281951
                32ab2cf6-5cf1-4a16-8e7f-9e00ad2dc862
                © 2023

                http://onlinelibrary.wiley.com/termsAndConditions#vor

                http://doi.wiley.com/10.1002/tdm_license_1.1

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