Loss-of-Function Mutation in Thiamine Transporter 1 in a Family With Autosomal Dominant Diabetes

Prapaporn Jungtrakoon; Jun Shirakawa; Patinut Buranasupkajorn; Manoj K Gupta; Dario F De Jesus; Marcus G Pezzolesi; Aussara Panya; Timothy Hastings; Chutima Chanprasert; Christine Mendonca; Rohit N Kulkarni; Alessandro Doria

doi:10.2337/db17-0821

Loss-of-Function Mutation in Thiamine Transporter 1 in a Family With Autosomal Dominant Diabetes

Diabetes. 2019 May;68(5):1084-1093. doi: 10.2337/db17-0821. Epub 2019 Mar 4.

Authors

Prapaporn Jungtrakoon^{1

2

3}, Jun Shirakawa^{1

4}, Patinut Buranasupkajorn^{1

2

5}, Manoj K Gupta^{1

4}, Dario F De Jesus^{1

4}, Marcus G Pezzolesi⁶, Aussara Panya^{1

2

3}, Timothy Hastings², Chutima Chanprasert³, Christine Mendonca², Rohit N Kulkarni^{1

4}, Alessandro Doria^{7

2}

Affiliations

¹ Department of Medicine, Harvard Medical School, Boston, MA.
² Section on Genetics and Epidemiology, Joslin Diabetes Center, Boston, MA.
³ Section on Islet Cell and Regenerative Biology, Joslin Diabetes Center, Boston, MA.
⁴ Division of Molecular Medicine, Research Department, Faculty of Medicine, Siriraj Hospital, Mahidol University, Bangkok, Thailand.
⁵ Division of Hospital and Ambulatory Medicine, Department of Medicine, Faculty of Medicine, Chulalongkorn University, Bangkok, Thailand.
⁶ Division of Nephrology and Hypertension, University of Utah School of Medicine, Salt Lake City, UT.
⁷ Department of Medicine, Harvard Medical School, Boston, MA alessandro.doria@joslin.harvard.edu.

Abstract

Solute Carrier Family 19 Member 2 (SLC19A2) encodes thiamine transporter 1 (THTR1), which facilitates thiamine transport across the cell membrane. SLC19A2 homozygous mutations have been described as a cause of thiamine-responsive megaloblastic anemia (TRMA), an autosomal recessive syndrome characterized by megaloblastic anemia, diabetes, and sensorineural deafness. Here we describe a loss-of-function SLC19A2 mutation (c.A1063C: p.Lys355Gln) in a family with early-onset diabetes and mild TRMA traits transmitted in an autosomal dominant fashion. We show that SLC19A2-deficient β-cells are characterized by impaired thiamine uptake, which is not rescued by overexpression of the p.Lys355Gln mutant protein. We further demonstrate that SLC19A2 deficit causes impaired insulin secretion in conjunction with mitochondrial dysfunction, loss of protection against oxidative stress, and cell cycle arrest. These findings link SLC19A2 mutations to autosomal dominant diabetes and suggest a role of SLC19A2 in β-cell function and survival.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Anemia, Megaloblastic / genetics
Anemia, Megaloblastic / metabolism*
Cell Cycle Checkpoints / genetics
Cell Cycle Checkpoints / physiology
Diabetes Mellitus / genetics
Diabetes Mellitus / metabolism
Humans
Insulin / metabolism
Membrane Transport Proteins / genetics*
Membrane Transport Proteins / metabolism*
Mitochondrial Diseases / genetics
Mitochondrial Diseases / metabolism
Mutation / genetics
Oxidative Stress / genetics
Oxidative Stress / physiology
Thiamine / metabolism

Substances

Insulin
Membrane Transport Proteins
SLC19A2 protein, human
Thiamine

Abstract

Publication types

MeSH terms

Substances

Grants and funding