The GK rat model of type 2 diabetes is especially convenient to dissect the pathogenic mechanism necessary for the emergence of overt diabetes because all adult rats obtained in our department (GK/Par colony) to date have stable basal mild hyperglycemia and because overt diabetes is preceded by a period of normoglycemia, ranging from birth to weaning. The purpose of this article is to sum up the information so far available related to the biology of the beta -cell in the GK/Par rat. In terms of beta -cell function, there is no major intrinsic secretory defect in the prediabetic GK/Par beta -cell, and the lack of beta -cell reactivity to glucose (which reflects multiple intracellular abnormalities), as seen during the adult period when the GK/Par rats are overtly diabetic, represents an acquired defect (perhaps glucotoxicity). In terms of beta -cell population, the earliest alteration so far detected in the GK/Par rat targets the size of the beta -cell population. Several convergent data suggest that the permanently reduced beta -cell mass in the GK/Par rat reflects a limitation of beta -cell neogenesis during early fetal life, and it is conceivable that some genes among the set involved in GK diabetes belong to the subset of genes controlling early beta -cell development.
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