Abstract
BackgroundType 1 diabetes mellitus is characterized by an inability to produce insulin endogenously. Based on a series of histopathology studies of patients with recent onset of the disease, it is commonly stated that the onset of clinical symptoms corresponds to an 80-95% reduction in beta cell mass. Motivated by the clinical importance of the degree of beta cell destruction at onset, a meta-analysis was used to determine the validity of this common wisdom.Methods and FindingsThe histopathology results identifying insulin containing islets in patients younger than 20 years of age were extracted from three different studies. The results for 105 patients were stratified by duration of diabetic symptoms and age at onset. Linear regression and a non-parametric bootstrap approach were used to determine the dependence of residual beta cell mass to age at onset. The percentage reduction in beta cell mass was highly correlated (p<0.001) with the age of onset with the greatest reduction in beta cell mass in the youngest patients. As this trend had not been previously observed, an alternative physiology-based model is proposed that captures this age-dependence.ConclusionsThe severity in beta cell reduction at onset decreased with age where, on average, a 40% reduction in beta cell mass was sufficient to precipitate clinical symptoms at 20 years of age. The observed trend was consistent with a physiology-based model where the threshold for onset is based upon a dynamic balance between insulin-production capacity, which is proportional to beta cell mass, and insulin demand, which is proportional to body weight.
Highlights
Type 1 diabetes mellitus is characterized by an impaired ability to produce insulin due to the progressive and selective destruction of beta cells in the pancreatic islets of Langerhans [1]
The ‘‘excess’’ beta cell mass corresponds to the reduction in beta cell mass that is required before hyperglycemia occurs. This relationship is derived from a dynamic mole balance between the source of insulin, which is proportional to beta cell mass (BCMTotal(t)), and sinks for insulin, which are proportional to body weight (BWt(t)) [25]
The fundamental characteristic of Type 1 diabetes mellitus is the loss of endogenous insulin production
Summary
Type 1 diabetes mellitus is characterized by an impaired ability to produce insulin due to the progressive and selective destruction of beta cells in the pancreatic islets of Langerhans [1]. Any effort to prolong endogenous insulin production may have a significant impact on the long-term quality of life for patients with Type 1 diabetes mellitus. Clinical management of this disease faces two significant challenges: the increase in incidence of Type 1 diabetes mellitus across the globe [6,7] and the lack of a cure. The percentage reduction in beta cell mass was highly correlated (p,0.001) with the age of onset with the greatest reduction in beta cell mass in the youngest patients As this trend had not been previously observed, an alternative physiology-based model is proposed that captures this age-dependence. The observed trend was consistent with a physiology-based model where the threshold for onset is based upon a dynamic balance between insulin-production capacity, which is proportional to beta cell mass, and insulin demand, which is proportional to body weight
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