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Alternative splicing encodes functional intracellular CD59 isoforms that mediate insulin secretion and are down-regulated in diabetic islets.

Ewelina Golec, Alexander Ekström, Maciej Noga, Muhmmad Omar-Hmeadi, Per-Eric Lund, Bruno O Villoutreix, Ulrika Krus, Katarzyna Wozniak, Olle Korsgren, Erik Renström, Sebastian Barg, Ben C King, Anna M Blom

Proceedings of the National Academy of Sciences of the United States of America 2022 Jun 14


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  • antibodies (1)
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  • glycosylphosphatidylinositol (3)
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    Human pancreatic islets highly express CD59, which is a glycosylphosphatidylinositol (GPI)-anchored cell-surface protein and is required for insulin secretion. How cell-surface CD59 could interact with intracellular exocytotic machinery has so far not been described. We now demonstrate the existence of CD59 splice variants in human pancreatic islets, which have unique C-terminal domains replacing the GPI-anchoring signal sequence. These isoforms are found in the cytosol of β-cells, interact with SNARE proteins VAMP2 and SNAP25, colocalize with insulin granules, and rescue insulin secretion in CD59-knockout (KO) cells. We therefore named these isoforms IRIS-1 and IRIS-2 (Isoforms Rescuing Insulin Secretion 1 and 2). Antibodies raised against each isoform revealed that expression of both IRIS-1 and IRIS-2 is significantly lower in islets isolated from human type 2 diabetes (T2D) patients, as compared to healthy controls. Further, glucotoxicity induced in primary, healthy human islets led to a significant decrease of IRIS-1 expression, suggesting that hyperglycemia (raised glucose levels) and subsequent decreased IRIS-1 expression may contribute to relative insulin deficiency in T2D patients. Similar isoforms were also identified in the mouse CD59B gene, and targeted CRISPR/Cas9-mediated knockout showed that these intracellular isoforms, but not canonical CD59B, are involved in insulin secretion from mouse β-cells. Mouse IRIS-2 is also down-regulated in diabetic db/db mouse islets. These findings establish the endogenous existence of previously undescribed non–GPI-anchored intracellular isoforms of human CD59 and mouse CD59B, which are required for normal insulin secretion.

    Citation

    Ewelina Golec, Alexander Ekström, Maciej Noga, Muhmmad Omar-Hmeadi, Per-Eric Lund, Bruno O Villoutreix, Ulrika Krus, Katarzyna Wozniak, Olle Korsgren, Erik Renström, Sebastian Barg, Ben C King, Anna M Blom. Alternative splicing encodes functional intracellular CD59 isoforms that mediate insulin secretion and are down-regulated in diabetic islets. Proceedings of the National Academy of Sciences of the United States of America. 2022 Jun 14;119(24):e2120083119

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    PMID: 35666870

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