Insulin and Glucagon Responses to Provocation with Glucose and Arginine in Prepubertal Children with Thalassemia Major Before and After Long-term Blood Transfusion

doi:10.1093/tropej/42.5.291

Journal of Tropical Pediatrics 1996 42(5):291-296; doi:10.1093/tropej/42.5.291
© 1996 by Oxford University Press

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Insulin and Glucagon Responses to Provocation with Glucose and Arginine in Prepubertal Children with Thalassemia Major Before and After Long-term Blood Transfusion

Ashraf T. Soliman, MD^*^,, Nagwa El Banna, MD^**, Issa AlSalmi, MB Ch B^** and Maurice Asfour, MD^**

^*Department of Pediatrics, University of Alexandria Alexandria, Egypt
^**Department of Endocrinology, Royal Hospital Muscat, Oman

Correspondence: Dr Ashraf T. Soliman, Pediatric Endocrinology, Royal Hospital, P.O. Box 2331, Seeb, Muscat, Code 111, Oman

Hypertransfusion therapy has dramatically increased the durationand quality of life in patients with B-thalassemia major; however,it leads to chronic iron overload, and is frequently complicatedby the development of diabetes mellitus or impaired glucosetolerance. To determine the early effect of iron overload onthe endocrine pancreatic function, we studied glucose, insulin,and glucagon responses to oral load of glucose and to arginineprovocation in 15 children with B-thalassemia major, beforeand after (3.1±0.6 years) high-transfusion and iron chelationand compared them with 15 age matched normal controls. In addition,we evaluated growth hormone (GH) responses to oral clonidineand measured the circulating insulin-like growth factor-I concentrationin thalassemic children on long-term transfusion and controls.After long-term high-transfusion, thalassemic children had significantlydecreased serum insulin concentrations and low insulin/glucoseratios at 60 and 120 min after an oral glucose load (1.75 g/kg)in comparison with values before therapy and those for controls.None of the thalassemic children had glucose intolerance afterthis period of frequent blood transfusion; however, their serumglucose levels at 60 and 120 min after the oral glucose loadwere significantly higher compared to control children. Thirtyminutes after starting arginine infusion, serum insulin concentrationwas significantly lower in thalassemic children compared tobefore therapy. Basal and arginine-stimulated glucagon secretionswere significantly elevated in thalassemic children on long-termblood transfusion with significantly low serum insulin/glucagonratios. In addition, the high basal serum glucagon concentrationswere not suppressed after the oral glucose load. Despite hyperglucagonaemiain all thalassemic children, their blood glucose dropped appropriatelybelow 50 per cent of the fasting glucose level after an intravenousinsulin dose (0.1 U/kg) ruling out any significant insulin-resistance.GH responses to clonidine provocation were subnormal in thalassemicchildren after long-term blood transfusion compared to controls.In summary, thalassemic children on long-term blood transfusionand iron chelation have progressive and early loss of B-cellmass, manifested by decreased insulin release in response tosecretagogues, before the development of significant insulinresistance or impairment of glucose tolerance.

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