Metabolic and genomic dissection of diabetes in the Cohen rat

Author:

Yagil Chana1,Barkalifa Ronit1,Sapojnikov Marina1,Wechsler Alexander1,Ben-Dor David2,Weksler-Zangen Sarah3,Kaiser Nurit4,Raz Itamar3,Yagil Yoram1

Affiliation:

1. Laboratory for Molecular Medicine and Israeli Rat Genome Center, Ben-Gurion University Barzilai Medical Center Campus, Ashkelon

2. Department of Pathology, Faculty of Health Sciences, Ben-Gurion University Barzilai Medical Center Campus, Ashkelon

3. Diabetes Unit, Hadassah-Hebrew University Medical Center, Jerusalem, Israel

4. Endocrinology and Metabolism Service, Hadassah-Hebrew University Medical Center, Jerusalem, Israel

Abstract

We investigated the metabolic and genetic basis of diabetes in the Cohen Diabetic rat, a model of diet-induced diabetes, as a means to identify the molecular mechanisms involved. By altering individual components in the diabetogenic diet, we established that the dietary susceptibility that leads to the development of diabetes in this model is directly related to the high casein and low copper content in chow. The development of diabetes is accompanied by depletion of the acini from the exocrine pancreas and replacement with fat cells, while the appearance of the islets of Langerhans remains intact. With reversion back from diabetogenic to regular diet, the diabetic phenotype disappears but the histological changes in the exocrine pancreas prevail. Using positional cloning, we detected a major quantitative trait locus (QTL) on rat chromosome 4 with a chromosomal span of 4.9 cM, and two additional loci on chromosomes 7 and X. A screen for genes within that QTL in the rat and in the syntenic regions in mouse and man revealed only 23 candidate genes. Notable among these genes is Ica1, which has been causally associated with diabetes and bovine casein. We conclude that the development of diabetes in our model is dependent upon high casein and low copper in diet, that it is accompanied by histomorphological changes in the exocrine but not endocrine pancreas, that it is reversible, and that it is associated with a major QTL on chromosome 4 in which we detected Ica1, a high priority candidate gene.

Publisher

American Physiological Society

Subject

Genetics,Physiology

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