4.7 Article

Molecular composition of the peri-islet basement membrane in NOD mice: a barrier against destructive insulitis

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DIABETOLOGIA
卷 51, 期 9, 页码 1680-1688

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SPRINGER
DOI: 10.1007/s00125-008-1085-x

关键词

autoimmunity; basement membrane; collagen; islets; laminin; matrix; nidogen; NOD; perlecan

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Aims/hypothesis This study examined whether the capsule which encases islets of Langerhans in the NOD mouse pancreas represents a specialised extracellular matrix (ECM) or basement membrane that protects islets from autoimmune attack. Methods Immunofluorescence microscopy using a panel of antibodies to collagens type IV, laminins, nidogens and perlecan was performed to localise matrix components in NOD mouse pancreas before diabetes onset, at onset of diabetes and after clinical diabetes was established (2-8.5 weeks post-onset). Results Perlecan, a heparan sulphate proteoglycan that is characteristic of basement membranes and has not previously been investigated in islets, was localised in the peri-islet capsule and surrounding intra-islet capillaries. Other components present in the peri-islet capsule included laminin chains alpha 2, beta 1 and gamma 1, collagen type IV alpha 1 and alpha 2, and nidogen 1 and 2. Collagen type IV alpha 3-alpha 6 were not detected. These findings confirm that the peri-islet capsule represents a specialised ECM or conventional basement membrane. The islet basement membrane was destroyed in islets where intra-islet infiltration of leucocytes marked the progression from non-destructive to destructive insulitis. No changes in basement membrane composition were observed before leucocyte infiltration. Conclusions/interpretation These findings suggest that the islet basement membrane functions as a physical barrier to leucocyte migration into islets and that degradation of the islet basement membrane marks the onset of destructive autoimmune insulitis and diabetes development in NOD mice. The components of the islet basement membrane that we identified predict that specialised degradative enzymes are likely to function in autoimmune islet damage.

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