Original Contributions

Block in Insulin Release from Column-Perifused Pancreatic β-Cells Induced by Islet Cell Surface Antibodies and Complement

  1. Takahiro Kanatsuna,
  2. Ake Lernmark,
  3. Arthur H Rubenstein and
  4. Donald F Steiner
  1. Departments of Biochemistry and Medicine, the University of Chicago Chicago, Illinois, and the Hagedom Research Laboratory Gentofte, Denmark
  1. Address reprint requests to Dr. Ake Lernmark, Hagedorn Research Laboratory, Niels Steensensvej 6, DK-2820 Gentofte, Denmark.
Diabetes 1981 Mar; 30(3): 231-234. https://doi.org/10.2337/diab.30.3.231

Abstract

Dispersed rat pancreatic islet cells were mixed into a short column of Bio-Gel P-2 polyacrylamide beads and perifused with an antiserum containing islet cell surface antibodies. The release of radioactive chromium from prelabeled cells, as a measure of cell membrane permeability, was not affected by cell surface antibodies alone, but increased dramatically in the presence of complement. While there was an eightfold increase in glucose-stimulated insulin release from β-cells exposed to control serum and complement, insulin release was completely blocked from β-cells exposed to islet-cell-specific antibodies and complement. These findings suggest that islet cell surface antibodies can mediate complement-dependent cytotOXicity.

  • Received April 18, 1980.
  • Revision received September 23, 1980.
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March 1981, 30(3)
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Block in Insulin Release from Column-Perifused Pancreatic β-Cells Induced by Islet Cell Surface Antibodies and Complement
Takahiro Kanatsuna, Ake Lernmark, Arthur H Rubenstein, Donald F Steiner
Diabetes Mar 1981, 30 (3) 231-234; DOI: 10.2337/diab.30.3.231
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