Transplantation of Reversibly Immortalized Insulin-Secreting Human Hepatocytes Controls Diabetes in Pancreatectomized Pigs

Author:

Okitsu Teru1,Kobayashi Naoya1,Jun Hee-Sook2,Shin Seungjin2,Kim Su-Jin2,Han Jaeseok2,Kwon Hyokjoon2,Sakaguchi Masakiyo3,Totsugawa Toshinori1,Kohara Michinori4,Westerman Karen A.5,Tanaka Noriaki1,Leboulch Philippe567,Yoon Ji-Won2

Affiliation:

1. Department of Surgery, Okayama University Graduate School of Medicine and Dentistry, Okayama, Japan

2. Laboratory of Viral and Immunopathogenesis of Diabetes, Julia McFarlane Diabetes Research Centre, Faculty of Medicine, The University of Calgary, Calgary, Alberta, Canada

3. Department of Cell Biology, Okayama University Graduate School of Medicine and Dentistry, Okayama, Japan

4. Department of Microbiology and Cell Biology, The Tokyo Metropolitan Institute of Medical Science, Honkomagome, Bukyo-ku, Japan

5. Division of Health Sciences and Technology, Massachusetts Institute of Technology, Cambridge, Massachusetts

6. Genetix Pharmaceuticals, Cambridge, Massachusetts

7. Department of Medicine, Harvard Medical School and Brigham and Women’s Hospital, Boston, Massachusetts

Abstract

Type 1 diabetes results from the destruction of insulin-producing pancreatic β-cells by a β-cell–specific autoimmune process. Although converting other cell types into insulin-producing cells may compensate for the loss of the β-cell mass while evading β-cell–specific T-cell responses, proof-of-principle of this approach in large animal models is lacking. This investigation was initiated to determine whether an insulin-producing human hepatocyte line can control diabetes when transplanted into totally pancreatectomized diabetic pigs. We established a reversibly immortalized human hepatocyte line, YOCK-13, by transferring a human telomerase reverse transcriptase cDNA and a drug-inducible Cre recombinase cassette, followed by cDNA for a modified insulin under the control of the l-type pyruvate kinase (l-PK) promoter. YOCK-13 cells produced small amounts of modified insulin and no detectable endogenous l-PK at low glucose concentrations, whereas they produced large amounts of both modified insulin and l-PK in response to high glucose concentrations. Xenotransplantation of YOCK-13 cells via the portal vein into immunosuppressed, totally pancreatectomized pigs decreased hyperglycemia and prolonged survival without adverse effects such as portal thrombosis, liver necrosis, pulmonary embolism, and tumor development. We suggest that this reversibly immortalized, insulin-secreting human hepatocyte line may overcome the shortage of donor pancreata for islet transplantation into patients with type 1 diabetes.

Publisher

American Diabetes Association

Subject

Endocrinology, Diabetes and Metabolism,Internal Medicine

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