Collection articles

The Collection contains recently-published Reviews from Nature, Nature Cell Biology and Nature Reviews Molecular Cell Biology. These articles are available free until 31 December 2008.

  • Review

    • The many faces of actin: matching assembly factors with cellular structures

      Ekta Seth Chhabra & Henry N. Higgs

      Nature Cell Biology 95, 1110-1121 (2007)

      Actin filaments are major components of at least 15 distinct structures in metazoan cells. These filaments assemble from a common pool of actin monomers, but do so at different times and places, and in response to different stimuli. All of these structures require actin-filament assembly factors. To date, many assembly factors have been identified, including Arp2/3 complex, multiple formin isoforms and spire. Now, a major task is to figure out which factors assemble which actin-based structures. Here, we focus on structures at the plasma membrane, including both sheet-like protrusive structures (such as lamellipodia and ruffles) and finger-like protrusions (such as filopodia and microvilli). Insights gained from studies of adherens junctions and the immunological synapse are also considered.

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    Review

    • Intermediate filaments: from cell architecture to nanomechanics

      Harald Herrmann, Harald Bär, Laurent Kreplak, Sergei V. Strelkov & Ueli Aebi

      Nature Reviews Molecular Cell Biology 8, 562-573 (2007)

      Intermediate filaments (IFs) constitute a major structural element of animal cells. They build two distinct systems, one in the nucleus and one in the cytoplasm. In both cases, their major function is assumed to be that of a mechanical stress absorber and an integrating device for the entire cytoskeleton. In line with this, recent disease mutations in human IF proteins indicate that the nanomechanical properties of cell-type-specific IFs are central to the pathogenesis of diseases as diverse as muscular dystrophy and premature ageing. However, the analysis of these various diseases suggests that IFs also have an important role in cell-type-specific physiological functions.

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    Insight

    • Dynamics and mechanics of the microtubule plus end

      Joe Howard & Anthony A. Hyman

      Nature 422, 753-758 (17 April 2003); doi:10.1038/nature01600

      An important function of microtubules is to move cellular structures such as chromosomes, mitotic spindles and other organelles around inside cells. This is achieved by attaching the ends of microtubules to cellular structures; as the microtubules grow and shrink, the structures are pushed or pulled around the cell. How do the ends of microtubules couple to cellular structures, and how does this coupling regulate the stability and distribution of the microtubules? It is now clear that there are at least three properties of a microtubule end: it has alternate structures; it has a biochemical transition defined by GTP hydrolysis; and it forms a distinct target for the binding of specific proteins. These different properties can be unified by thinking of the microtubule as a molecular machine, which switches between growing and shrinking modes. Each mode is associated with a specific end structure on which end-binding proteins can assemble to modulate dynamics and couple the dynamic properties of microtubules to the movement of cellular structures.


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