AI Article Synopsis

  • Hyperglycaemia in Type 1 diabetes (T1D) is mainly due to a lack of insulin, but insulin resistance (IR) can also worsen blood sugar instability and lead to long-term heart issues.
  • A study examined blood samples from 28 children with T1D to identify how certain metabolites relate to blood sugar control and IR, using statistical analyses to find significant correlations.
  • Results indicated that incomplete fat oxidation and the way fats and amino acids are metabolized are linked to blood sugar control and insulin dosage in young children with T1D.

Article Abstract

Objective: Hyperglycaemia in Type 1 diabetes (T1D) results from an absolute insulin deficiency. However, insulin resistance (IR) may exacerbate glycaemic instability in T1D and contribute to long-term cardiovascular complications. We previously showed that IR in teenagers with obesity is associated with sex-dependent derangements in the catabolism of branched-chain amino acids (BCAA) and fatty acids. Here we hypothesized that byproducts of BCAA and fatty acid metabolism may serve as biomarkers or determinants of glycaemic control and IR in prepubertal or early pubertal children with T1D.

Methods: Metabolites, hormones and cytokines from fasting blood samples were analysed in 28 children (15 females, 13 males; age 6-11 years) with T1D. Principal components analysis (PCA) and multiple linear regression models were used to correlate metabolites of interest with glycaemic control, total daily insulin dose (TDD, units/kg/d), adiponectin and the triglyceride (TG) to high-density lipoprotein (HDL) ratio.

Results: Males and females were comparable in age, BMI-z, insulin sensitivity, glycaemic control, inflammatory markers, BCAAs and C2/C3/C5-acylcarnitines. The majority of components retained in PCA were related to fatty acid oxidation (FAO) and BCAA catabolism. HbA1c correlated positively with Factor 2 (acylcarnitines, incomplete FAO) and Factor 9 (fasting glucose). TDD correlated negatively with C3 and C5 and Factor 10 (BCAA catabolism) and positively with the ratio of C2 to C3 + C5 and Factor 9 (fasting glucose).

Conclusions: These findings suggest that glucose intolerance in prepubertal or early pubertal children with T1D is accompanied by incomplete FAO while TDD is associated with preferential catabolism of fats relative to amino acids.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10638627PMC
http://dx.doi.org/10.1002/edm2.448DOI Listing

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