Persistent glucose production during glucose infusion in the neonate.

Cowett, Richard M.; Oh, William; Schwartz, Robert

doi:10.1172/jci110791

Cited by 143 publications

(87 citation statements)

References 28 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…mg/kg/min in unfasted adults [79], EGP is higher at ~ 4 mg/kg/min in fasted adults [79]) and is also unsuppressed at higher BG and/or glucose infusion rate in premature infants [80]. Infants born less than 27 weeks gestation lack glycogen stores, so intravenous/frequent exogenous nutrition is required to meet energy needs.…”

Section: Discussionmentioning

confidence: 99%

Insulin kinetics and the Neonatal Intensive Care Insulin–Nutrition–Glucose (NICING) model

Dickson

Pretty

Alsweiler

et al. 2017

Mathematical Biosciences

View full text Add to dashboard Cite

Background: Models of human glucose-insulin physiology have been developed for a range of uses, with similarly different levels of complexity and accuracy. STAR (Stochastic Targeted) is a modelbased approach to glycaemic control. Elevated blood glucose concentrations (hyperglycaemia) are a common complication of stress and prematurity in very premature infants, and have been associated with worsened outcomes and higher mortality. This research identifies and validates the model parameters for model-based glycaemic control in neonatal intensive care.

show abstract

Section: Discussionmentioning

confidence: 99%

Insulin kinetics and the Neonatal Intensive Care Insulin–Nutrition–Glucose (NICING) model

Dickson

Pretty

Alsweiler

et al. 2017

Mathematical Biosciences

View full text Add to dashboard Cite

show abstract

“…Age is generally considered an important determinant of EGP: glucose requirements in pre-term infants are approximately 44 lmol ⁄ kg ⁄ min (Van Kempen et al 2003), glucose production in term infants is approximately 33 lmol ⁄ kg ⁄ min and ranges between 27 and 43 lmol ⁄ kg ⁄ min in 1-month to 6-year-old children. Thereafter EGP decreases with age to 20 lmol ⁄ kg ⁄ min at the age of 8-10 years and 13 lmol ⁄ kg ⁄ min in adolescents (Bier et al 1977;Cowett et al 1983;Kalhan et al 1986;Haymond & Sunehag 1999;Sunehag et al 2001). Glucose production in children between 2.5 and 3.9 years with idiopathic ketotic hypoglycaemia ranged between 31.2 and 39.6 lmol ⁄ kg ⁄ min after an overnight fast (Huidekoper et al 2007).…”

Section: Discussionmentioning

confidence: 99%

Very young children with uncomplicated falciparum malaria have higher risk of hypoglycaemia: a study from Suriname

Zijlmans

Kempen

Ackermans

et al. 2008

Tropical Med Int Health

View full text Add to dashboard Cite

Summaryobjective To measure glucose kinetics and the influence of age, nutritional status and fasting duration in children with uncomplicated falciparum malaria (UFM) under the age of 5 years. results Plasma glucose concentration was lower in the group of very young children than in the older children (P = 0.028). There were no differences in EGP and GNG between the groups. Overall GNG contributed 56% (median, range 17-87%) to EGP, with no differences between the groups (P = 0.240).Glucose clearance was lower in the older children (P = 0.026). Glucose concentration did not differ between children with weight for length ⁄ height less than )1.3 SD and children with weight for length ⁄ height greater than )1.3 SD (P = 0.266). Plasma glucose concentration was not predicted by fasting duration (P = 0.762).conclusions Our data suggest a higher risk of hypoglycaemia in very young children with uncomplicated malaria as plasma glucose concentration was lower in this study group. Since this could not be attributed to an impaired EGP, and because glucose clearance was lower in the older children, we presume that older children were better capable of reducing glucose utilization during fasting. Studies on glucose kinetics are feasible in very young children with malaria and give more insight in the pathophysiology of hypoglycaemia.

show abstract

“…The known mechanisms responsible for hyperglycaemia specific to extremely premature infants are related to their reduced ability to produce insulin [11]; defective beta-cell processing of pro-insulin (which is 10-16 times less active than insulin) to insulin [12]; an inability to suppress hepatic glucose production in response to glucose infusion [13]; and, finally, a decreased uptake of glucose secondary to a limited mass of insulin-sensitivity tissues (e.g. : muscle and adipose tissue) [14].…”

Section: Introductionmentioning

confidence: 99%

Development of blood glucose control for extremely premature infants

Compte

Chase

Lynn

et al. 2011

Computer Methods and Programs in Biomedicine

View full text Add to dashboard Cite

Abstract:Extremely premature neonates often experience hyperglycaemia, which has been linked to increased mortality and worsened outcomes. Insulin therapy can assist in controlling blood glucose levels and promoting needed growth. This study presents the development of a model-based stochastic targeted controller designed to adapt insulin infusion rates to match the unique and changing metabolic state and control parameters of the neonate. Long-term usage of targeted BG control requires successfully forecasting variations in neonatal metabolic state, accounting for differences in clinical practices between units, and demonstrating robustness to errors that can occur in everyday clinical usage. Simulation studies were used to evaluate controller ability to target several common BG ranges and evaluate controller sensitivity to missed BG measurements and delays in control interventions on a virtual patient cohort of 25 infants developed from retrospective data. Initial clinical pilot trials indicated model performance matched expected performance from simulations. Stochastic targeted glucose control developed using validated patient-specific virtual trials can yield effective protocols for this cohort. Long-term trials show fundamental success, however clinical interface design appears as a critical factor to ensuring good compliance and thus good control.3

show abstract

Persistent glucose production during glucose infusion in the neonate.

Cited by 143 publications

References 28 publications

Insulin kinetics and the Neonatal Intensive Care Insulin–Nutrition–Glucose (NICING) model

Insulin kinetics and the Neonatal Intensive Care Insulin–Nutrition–Glucose (NICING) model

Very young children with uncomplicated falciparum malaria have higher risk of hypoglycaemia: a study from Suriname

Development of blood glucose control for extremely premature infants

Contact Info

Product

Resources

About