Influence of glycaemic management and BMI on cardiac autonomic

markers in children with type 1 diabetes: a prospective cohort study

 

Ebba Bergdahl1 · Gun Forsander2 · Linda Milkovic3 · Frida Sundberg4 · Frida Dangardt1,5

 

 

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https://link.springer.com/article/10.1007/s00125-025-06592-3

 

 

 

Vol.:(0123456789)Diabetologia

https://doi.org/10.1007/s00125-025-06592-3

 

 

Abstract

Aims/hypothesis

Our aim was to examine the presence of subclinical cardiovascular autonomic neuropathy (CAN) in a

cohort of children with well-regulated type 1 diabetes by measuring baroreceptor sensitivity (BRS), QT variability index

(QTVI) and heart rate variability (HRV).

 

Methods

Forty-five children (aged 6–15.99 years) with a type 1 diabetes duration of ≥5 years, and 37 healthy control children

were included at baseline; and 28 and 18 children, respectively, were included at 2 year follow-up. Cardiac BRS, QTVI and

HRV were measured and anthropometrical data and blood samples were collected from all study participants. Longitudinal

HbA 1c values from 3 months after type 1 diabetes diagnosis and continuous glucose monitoring data from the children with

type 1 diabetes were also collected.

 

Results

Time in normoglycaemia (TING) increased significantly from 42% to 48% between baseline and 2 year follow-up

(p=0.042). No difference in BRS, QTVI or HRV were found between the study groups at baseline or follow-up. Children

with type 1 diabetes with a BMI z score ≥1 showed higher QTVI compared with either lean children with diabetes or healthy

control children. QTVI correlated with type 1 diabetes duration, longitudinal HbA 1c AUC and cystatin C in children with

type 1 diabetes at baseline, and with CV at follow-up. (r=−0.447 p=0.004, r=−0.376 p=0.017, r=−323 p=0.048, and

r=0.568 p=0.01, respectively). There was also a correlation between the increase in TING between the study visits and BRS

at follow-up in children with type 1 diabetes (r=0.524 p=0.031).

 

Conclusions/interpretation

In this well-regulated type 1 diabetes cohort we did not find manifest signs of CAN in children

with type 1 diabetes.

 

These are promising findings and should motivate further to keep striving for normoglycaemia in

paediatric diabetes care. Children with both type 1 diabetes and overweight seem more susceptible to early development of

CAN and might benefit from earlier and more intensive preventive targeting

 

 

Introduction

From the article

Diabetes autonomic neuropathy (DAN) includes disturbances

from the urogenital and gastrointestinal organs, the sudomo-

tor function and cardiovascular autonomic neuropathy

(CAN), the latter of which is the most studied form [1]. CAN

symptoms include tachycardia, orthostatism and exercise

intolerance, and CAN is a known risk factor for cardiovascu-

lar mortality in type 1 diabetes [2].

 

The presence of CAN is

also connected with hypoglycaemia unawareness and severe

hypoglycaemic events in individuals with type 1 diabetes [3].

CAN prevalence in children with type 1 diabetes varies sub-

stantially between different studies, possibly explained by the

lack of a gold-standard evaluation method [4, 5]. The SEARCH

for diabetes in youth study showed a 14.4% prevalence in young

individuals with type 1 diabetes with a mean duration of ill-

ness of 7.9 years, measured as impaired heart rate variability

(HRV) [6], and the DCCT/EDIC study found a CAN preva-

lence of 8.5% 6 years after diagnosis, measured as prolonged RR

interval [7].

 

CAN in children with diabetes has previously been

associated with type 1 diabetes duration, glycaemic manage-

ment [5] and a number of traditional cardiovascular risk factors

such as hypertension and obesity. It is even more pronounced in

young individuals with type 2 diabetes and also in the case of

lower HbA1c levels and shorter duration of illness [8]. Although

data on the prevalence of CAN in children with type 1 diabetes

are inconclusive, studies in adults with type 1 diabetes gener-

ally show a high prevalence of CAN (>30%) [9–11] associated

with type 1 diabetes duration, hypertension and diabetic kidney

disease (DKD) [9, 10, 12]. Hydroxy fatty acids and the tricar-

boxylic acid cycle are also associated with the development of

CAN and may constitute good targets for additional preventive

treatment in the future [13].

 

Hence, trustworthy markers associated with development

of CAN in children with type 1 diabetes are essential to

enable early detection and treatment before development of

manifest CAN [12]. We identify a need for reliable and sensi-

tive methods for early detection of CAN development in chil-

dren with diabetes, both for providing prevalence numbers

to help pathophysiological understanding and for enabling

early preventive treatment of CAN in children with diabetes.

 

Utdrag ur

Discussion

In this prospective cohort study, we used highly sensitive

methods for detection of subclinical CAN in children with

type 1 diabetes with low HbA 1c and no presence of other

traditional cardiovascular risk factors.

 

Children with type 1

diabetes were compared with age- and sex-matched healthy

control children, and we found no differences in BRS, QTVI

or HRV between the study groups at baseline or at 2 year

follow-up, nor any longitudinal changes in either of the study

groups.

 

There was an improvement in TING in children with

diabetes from baseline to follow-up, correlating with higher

BRS at follow-up, and QTVI was higher in children with

diabetes with BMIz ≥1 compared with children both with

and without diabetes and with normal weight. QTVI corre-

lated with type 1 diabetes duration and HbA1cAUC at baseline

and type 1 diabetes duration, cystatin C and age were inde-

pendent determinants for QTVI in children with diabetes in

multivariable regression.

 

Our results, especially the correla-

tions found for QTVI and BRS, as well as the results from

backwards multivariable regression suggest an association

between dysglycaemia and CAN, even in this study cohort

where children with diabetes display comparably low HbA1c

levels, even better lipid profiles than matched healthy control

children, and no other manifest cardiovascular complica-

tions. These quite unique glycaemic and metabolic manage-

ment results possibly explain the findings that there were no

significant differences in any of the measures of subclinical

CAN between children with and without diabetes.

 

 

Conclusion

In type 1 diabetes populations with access to

high technology and improved glycaemic management, data

on chronic complication development are still limited, and

our study adds to this knowledge gap.

 

Encouragingly, we

find no subclinical signs of CAN in this cohort of children

with well-regulated type 1 diabetes with normal weight.

Hence, sustaining low HbA1c and high TIR and TING might

delay or preferably prevent development of CAN. We further

confirm the additional risk of chronic complications that

comes with overweight/obesity in type 1 diabetes, suggest-

ing that intensified cardiovascular preventive focus in this

subgroup might be beneficial. Further studies with larger

study cohorts are essential to confirm our results and to

continue increasing the knowledge behind cardiovascular

complication development in children with well-regulated

type 1 diabetes.

 

Hopefully, this will result in even further

improvement of cardiovascular prevention in children with

diabetes, increasing both life expectancy and quality of life

for people living with type 1 diabetes in the future.

 

 

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