Metformin improves glycemic variability in adults with type 1 diabetes mellitus: an open-label randomized control trial

in Endocrine Connections
Authors:
Xiuzhen Zhang Department of Endocrinology and Metabolism, Shenzhen People’s hospital, The Second Clinical Medical College, Jinan University, Shenzhen, Guangdong, China

Search for other papers by Xiuzhen Zhang in
Current site
Google Scholar
PubMed
Close
https://orcid.org/0000-0002-2246-5592
,
Dan Xu Department of Endocrinology and Metabolism, Shenzhen People’s hospital, The Second Clinical Medical College, Jinan University, Shenzhen, Guangdong, China

Search for other papers by Dan Xu in
Current site
Google Scholar
PubMed
Close
,
Ping Xu Department of Endocrinology and Metabolism, Shenzhen People’s hospital, The Second Clinical Medical College, Jinan University, Shenzhen, Guangdong, China

Search for other papers by Ping Xu in
Current site
Google Scholar
PubMed
Close
,
Shufen Yang Department of Endocrinology and Metabolism, Shenzhen People’s hospital, The Second Clinical Medical College, Jinan University, Shenzhen, Guangdong, China

Search for other papers by Shufen Yang in
Current site
Google Scholar
PubMed
Close
,
Qingmei Zhang Department of Endocrinology and Metabolism, Shenzhen People’s hospital, The Second Clinical Medical College, Jinan University, Shenzhen, Guangdong, China

Search for other papers by Qingmei Zhang in
Current site
Google Scholar
PubMed
Close
,
Yan Wu Department of Endocrinology and Metabolism, Shenzhen People’s hospital, The Second Clinical Medical College, Jinan University, Shenzhen, Guangdong, China

Search for other papers by Yan Wu in
Current site
Google Scholar
PubMed
Close
, and
Fengyi Yuan Department of Endocrinology and Metabolism, Shenzhen People’s hospital, The Second Clinical Medical College, Jinan University, Shenzhen, Guangdong, China

Search for other papers by Fengyi Yuan in
Current site
Google Scholar
PubMed
Close

Correspondence should be addressed to F Yuan: 521jane@outlook.com
Open access

Sign up for journal news

Introduction

Metformin has been demonstrated to enhance cardioprotective benefits in type 1 diabetes (T1DM). Although glycemic variability (GV) is associated with increased risk of CVD in diabetes, there is a scarcity of research evaluating the effect of metformin on GV in T1DM.

Objectives

In the present study, the effects of adjuvant metformin therapy on GV and metabolic control in T1DM were explored.

Patients and methods

A total of 65 adults with T1DM were enrolled and subjected to physical examination, fasting laboratory tests, and continuous glucose monitoring, and subsequently randomized 1:1 to 3 months of 1000–2000 mg metformin daily add-on insulin (MET group, n = 34) or insulin (non-MET group, n = 31). After, baseline measurements were repeated.

Results

The mean amplitude of glycemic excursions was substantially reduced in MET group, compared with non-MET group (–1.58 (–3.35, 0.31) mmol/L vs 1.36 (–1.12, 2.24) mmol/L, P = 0.004). In parallel, the largest amplitude of glycemic excursions (–2.83 (–5.47, –0.06) mmol/L vs 0.45 (–1.29, 4.48) mmol/L, P = 0.004), the s.d. of blood glucose (–0.85 (–1.51, 0.01) mmol/L vs –0.14 (–0.68, 1.21) mmol/L, P = 0.015), and the coefficient of variation (–6.66 (–15.00, 1.50)% vs –1.60 (–6.28, 11.71)%, P = 0.012) all demonstrated improvement in the MET group, compared with the non-MET group. Significant reduction in insulin dose, BMI, and body weight was observed in patients in MET, not those in non-MET group.

Conclusion

Additional metformin therapy improved GV in adults with T1DM, as well as improving body composition and reducing insulin requirement. Hence, metformin as an adjunctive therapy has potential prospects in reducing the CVD risk in patients with T1DM in the long term.

Abstract

Introduction

Metformin has been demonstrated to enhance cardioprotective benefits in type 1 diabetes (T1DM). Although glycemic variability (GV) is associated with increased risk of CVD in diabetes, there is a scarcity of research evaluating the effect of metformin on GV in T1DM.

Objectives

In the present study, the effects of adjuvant metformin therapy on GV and metabolic control in T1DM were explored.

Patients and methods

A total of 65 adults with T1DM were enrolled and subjected to physical examination, fasting laboratory tests, and continuous glucose monitoring, and subsequently randomized 1:1 to 3 months of 1000–2000 mg metformin daily add-on insulin (MET group, n = 34) or insulin (non-MET group, n = 31). After, baseline measurements were repeated.

Results

The mean amplitude of glycemic excursions was substantially reduced in MET group, compared with non-MET group (–1.58 (–3.35, 0.31) mmol/L vs 1.36 (–1.12, 2.24) mmol/L, P = 0.004). In parallel, the largest amplitude of glycemic excursions (–2.83 (–5.47, –0.06) mmol/L vs 0.45 (–1.29, 4.48) mmol/L, P = 0.004), the s.d. of blood glucose (–0.85 (–1.51, 0.01) mmol/L vs –0.14 (–0.68, 1.21) mmol/L, P = 0.015), and the coefficient of variation (–6.66 (–15.00, 1.50)% vs –1.60 (–6.28, 11.71)%, P = 0.012) all demonstrated improvement in the MET group, compared with the non-MET group. Significant reduction in insulin dose, BMI, and body weight was observed in patients in MET, not those in non-MET group.

Conclusion

Additional metformin therapy improved GV in adults with T1DM, as well as improving body composition and reducing insulin requirement. Hence, metformin as an adjunctive therapy has potential prospects in reducing the CVD risk in patients with T1DM in the long term.

Introduction

Amongst the background of the rising incidence of type 1 diabetes mellitus (T1DM) across the globe, public concern has reached a new high (1). Despite progress in diabetes care, as the leading cause of mortality in T1DM (2), cardiovascular disease (CVD) contributes to a two- to four-times higher death rate in patients with T1DM, compared with the general population (3, 4). Diabetes Control and Complications Trials (DCCT) have exhibited that intensive insulin therapy attenuated atherosclerosis in T1DM patients, which was primarily ascribed to the reduction in hemoglobin A1c (HbA1c) level (5). As the standard metric of glycemic control, the HbA1c level is ideally maintained as close to normal as possible for the purpose of reducing the incidence rate of long-term diabetic complications (6). However, the titration of increased insulin dosage is usually accompanied by weight gain and glycemic variability (GV). Further, with the increasing prevalence of obesity and overweight in patients with T1DM (7, 8), insulin resistance (IR) considered to increase the CVD risk has become prominent in these individuals (9, 10). Moreover, a culmination of evidence proposes that GV is integral in predicting adverse clinical outcomes in patients with diabetes, including hypoglycemia, diabetic complications as well as mortality (11), emerging as one of the core treatment targets of potential therapeutic strategies. High GV is an independent risk factor of CVD and could lead to further complications than constant hyperglycemia (12). For this reason, novel approaches to flattening glucose fluctuations that will reduce the risk of CVD in T1DM are in dire need.

For over five decades, metformin is an oral antihyperglycemic drug that has been used extensively in the treatment of type 2 diabetes (T2DM). Prior research has reported that metformin achieved glycemic control by lowering hepatic glucose output, increasing the glucose uptake in muscle, and decreasing the intestinal carbohydrates absorption rate, as well as improving insulin sensitivity (13, 14). The UK Prospective Diabetes Study (UKPDS) revealed that metformin reduced the CVD risk in patients with T2DM (15). Metformin is recommended by only a few guidelines for overweight/obese T1DM patients, and the role thereof in adjuvant therapy for T1DM has drawn increasing concern in recent years. Aside from the reduction in the daily insulin dose and body weight, direct improvements in insulin sensitivity and carotid intima-media thickness (cIMT) were also detected in T1DM patients after additional metformin therapy, indicating that this therapeutic strategy can form potential CVD risk protection (16, 17, 18).

On the basis of present knowledge, whether metformin as adjuvant therapy could help reduce GV in patients with T1DM has not yet been illustrated. Therefore, the present 3-month randomized control trial was conducted in accordance with the following objectives: to evaluate the effect of additional metformin in insulin treatment on the primary outcome of GV and HbA1c, in addition to other parameters of glycemic control and anthropometric indexes.

Methods and patients

The present trial was a 3-month open-label, randomized, controlled clinical trial. Subjects with T1DM were consecutively recruited between July 2017 and July 2019 at the outpatient clinic of the Department of Endocrinology and Metabolism of the Shenzhen People’s hospital (The Second Clinical Medical College, Jinan University). This trial was registered at clinicaltrials.gov (NCT03590262) and conducted in accordance with the Declaration of Helsinki and the International Conference of Harmonization-Good Clinical Practice. The study protocol was approved by the Ethics Committee of the hospital, and written informed consent was obtained from each participant. The inclusion criteria included age range of 18 to 75 years, T1DM (positive for ≥1 diabetes mellitus-associated autoantibody), and treated with continuous s.c. insulin infusion or multiple daily injections at a stable regimen, with self-monitoring of blood glucose (SMBG) at least three times per day for at least 1 month is required prior to participation in the study. The exclusion criteria consisted of resting blood pressure (BP) > 140/90 mmHg, smoking, medications affecting insulin sensitivity (steroids, immunosuppressants, noninsulin antidiabetic agents), history of CVD, hypertension, renal failure defined as glomerular filtration rate < 45 mL/min/1.73 m2, diabetic ketoacidosis or severe illness within 30 days, inability to tolerate ≥ 500 mg metformin twice per day and pregnancy. The same diet and physical activity instructions were given by the same dietician and diabetic educator to all patients before randomization, and compliance was reinforced at each follow-up.

Study design

After preliminary screening, 65 eligible participants were recruited and randomized by a ratio of 1:1 into a group receiving 1000–2000 mg metformin daily add-on insulin therapy (MET, n = 34) or a group receiving insulin treatment only (non-MET, n = 31), with the trial lasting 3 months. The mean metformin dose was 1500 mg/day (range, 1000–2000 mg/day), which was adjusted pursuant to the patient’s drug tolerance, while the insulin dosage was adjusted predicated on SMBG. All participants were subjected to a comprehensive evaluation at baseline and a 3-month follow-up visit, including physical examination (BP, weight, height), data concerning lifestyle (physical activity and eating habit), frequency of hypoglycemia, and the daily insulin regimen.

Laboratory measurements

Blood analyses that included serum glucose, total cholesterol (TC), triglyceride (TG), high-density lipoprotein-cholesterol (HDL-C), low-density lipoprotein-cholesterol (LDL-C) were performed at the central laboratory of the hospital by using a biochemical analyzer (Modular Analytics, Roche).These parameters were investigated in all participants at fasting during the first visit and subsequently repeated after completion of the 3-month follow-up.

CGM measurements and parameter calculation

Glucose levels were continuously monitored in all participants by professional retrospective CGM (iPro™2, Medtronic Minimed Inc., Northridge, CA, USA) for 5 days at baseline and the end of the 3-month intervention. All participants were required to do pre-prandial SMBG four times a day (before breakfast, lunch, dinner, and before bedtime) with a glucometer (Accu-Chek Mobile, Roche Diagnostics) for calibrating the CGM. The accuracy of the glucometer was calibrated by fasting blood glucose levels tested in the central laboratory, and the deviation was less than 15%. Consecutive 72-h calibrated glucose profiles of each participant at baseline and after the 3-month intervention were recorded for further statistical analysis. CGM data from iPro™2 sensor were downloaded via Carelink iPro for analysis.

Parameters of GV were calculated, such as the s.d. of blood glucose (SDBG), mean amplitude of glucose excursions (MAGE), largest amplitude of glycemic excursions (LAGE), coefficient of variation (CV), and mean of daily differences (MODD). The time in range (TIR, glucose range of 3.9–10.0 mmol/L during a 24-h period) and mean sensor glucose (MSG) were also calculated from the CGM data.

Outcomes

The primary outcomes were changes in MAGE and HbA1c from baseline to 3 months, while the secondary outcomes were changes in SD, LAGE, CV, MODD, TIR, BMI, BP, lipid profiles, and the daily insulin dose at the 3-month follow-up, compared with baseline. Safety data include the incidence of all symptomatic or biochemically proven hypoglycemic episodes (<2.8 mmol/L) and medication adverse events.

Power calculations and statistical analyses

Owing to being a pilot study, the sample size was estimated pursuant to the feasibility of conducting the study, with a convenience sample size of 70 ultimately being adopted. Descriptive statistics were employed to summarize baseline characteristics as mean ± s.d. for normally distributed data and as median (interquartile range (IQR)) for non-normally distributed data. Variables were checked for the distributional assumption of normality with normal plots, in addition to Kolmogorov–Smirnov and Shapiro–Wilks tests, and categorical variables were expressed as percentages. In the univariate comparisons between the MET and the non-MET, categorical variables were compared by chi-squared tests, while continuous variables were compared by t-tests or Wilcoxon–Mann–Whitney tests as appropriate. A P-value of < 0.05 (two-tailed) was considered statistically significant. All statistical analyses were conducted by utilizing the Statistical Package for the Social Sciences (version 23.0; SPSS Inc.).

Results

A total of 70 patients participated, with 5 of them being ineligible or lost to follow-up. Among the 65 eligible randomized participants, 3 participants (2 in the MET group, and 1 in the Non-MET group) did not complete the study protocol. Figure 1 exhibits the diagram depicting the randomization and follow-up visit sample sizes, while baseline clinical characteristics of the participants are summarized in Table 1. The mean age of participants was 31 ± 10 years old, and the median duration of diabetes was 8 years (interquartile range, 2–15 years). The mean daily insulin dose was 0.63 ± 0.09 U/kg of body weight, and BMI was 23.0 ± 1.8 kg/m2. The baseline characteristics of patients with T1DM randomized into two groups that finished the study are presented in Table 1. There were no major differences in sex, age, duration of diabetes, BMI, or parameters of metabolic control (HbA1c value, lipid profiles) between the two groups at baseline. Further, no substantial differences in the CGM parameters, such as MAGE, LAGE, SDBG, MODD, CV, TIR, or MSG were found between the two groups at baseline.

Figure 1
Figure 1

The diagram of clinical trials in participants with type 1 diabetes mellitus. f/u, follow-up.

Citation: Endocrine Connections 10, 9; 10.1530/EC-21-0146

Table 1

Baseline clinical characteristics of patients. A total of 65 eligible randomized participants (metformin group (MET), n = 34; non-metformin group (non-MET), n = 31), 32 patients in the MET, and 30 in the non-MET completed the study protocol. Normally distributed quantitative variables are presented as the mean ± s.d., and nonnormally distributed quantitative variables are presented as the median (interquartile range, IQR).

Variable Total MET Non-MET P-value
Sex, female/male, n (%) 36 (55)/29 (45) 18 (56)/14 (44) 18 (60)/12 (40) 0.767
Age (years) 31 ± 10 31 ± 10 32 ± 11 0.583
Diabetes duration (year) 8 (2, 15) 8 (2, 12) 9 (3, 20) 0.237
Body weight (kg) 62.4 ± 7.5 62.6 ± 7.6 62.2 ± 7.6 0.814
Daily insulin dose (U/kg of body weight) 0.63 ± 0.09 0.62 ± 0.07 0.64 ± 0.10 0.315
BMI (kg/m2) 23.0 ± 1.8 23.0 ± 1.8 22.9 ± 1.8 0.917
TG (mmol/L) 1.98 ± 0.62 2.11 ± 0.61 1.83 ± 0.60 0.066
TC (mmol/L) 5.19 ± 0.78 5.24 ± 0.64 5.13 ± 0.91 0.574
HDL-C (mmol/L) 1.09 ± 0.19 1.12 ± 0.19 1.05 ± 0.18 0.159
LDL-C (mmol/L) 3.16 ± 0.68 3.20 ± 0.55 3.12 ± 0.80 0.652
SBP (mmHg) 117 ± 10 117 ± 10 117 ± 9 0.789
DBP (mmHg) 74 ± 7 72 ± 7 75 ± 8 0.210
HbA1c (%) 8.1 ± 0.9 8.2 ± 0.8 8.0 ± 0.9 0.246
Creatinine (μmol/L) 61.3 ± 14.8 64.0 ± 16.6 58.4 ± 12.4 0.137
eGFR (mL/min/1.73 m2) 115.3 ± 15.7 112.6 ± 18.4 118.1 ± 11.9 0.172
MAGE (mmol/L) 5.63 (3.58, 7.97) 6.03 (3.82, 8.24) 5.35 (2.95, 7.23) 0.058
LAGE (mmol/L) 10.49 (7.22, 14.71) 10.94 (9.27, 14.77) 8.96 (5.81, 14.87) 0.128
SDBG (mmol/L) 2.78 (1.65, 3.53) 2.87 (1.80, 3.59) 2.51 (1.30, 3.53) 0.121
MODD (mmol/L) 2.83 (2.31, 3.60) 2.80 (2.27, 3.49) 2.94 (2.40, 3.63) 0.827
CV (%) 26.87 (17.36, 33.70) 30.54 (18.64, 34.96) 25.03 (14.62, 32.82) 0.220
TIR (%) 53.27 (35.76, 64.89) 51.91 (29.23, 59.07) 53.27 (35.94, 68.45) 0.379
MSG (mmol/L) 10.22 (9.16, 11.19) 10.36 (9.49, 11.48) 10.06 (8.92, 10.83) 0.254

CV, coefficient of variation; DBP, diastolic blood pressure; eGFR, estimated glomerular filtration rate; HbA1c, hemoglobin A1c; HDL-C, high-density lipoprotein cholesterol; LAGE, largest amplitude of glycemic excursions; LDL-C, low-density lipoprotein cholesterol; MAGE, mean amplitude of glucose excursions; MODD, mean of daily differences; MSG, mean sensor glucose; SBP, systolic blood pressure; SDBG, standard deviation of blood glucose; TC, total cholesterol; TG, total triglyceride; TIR, time in range.

Effect of metformin on glycemic end points

The results of the 3-month treatments in MET and non-MET for the investigated variables are revealed in Table 2. The primary outcome of MAGE demonstrated significant improvement in the MET group, as against the non-MET group (–1.58 (–3.35, 0.31) mmol/L vs 1.36 (–1.12, 2.24) mmol/L, P = 0.004). Additionally, SDBG (–0.85 (–1.51, 0.01) mmol/L vs –0.14 (–0.68, 1.21) mmol/L, P = 0.015), LAGE (–2.83 (–5.47, –0.06) mmol/L vs 0.45 (–1.29, 4.48) mmol/L, P = 0.004), and CV (–6.66 (–15.00, 1.50) % vs –1.60 (–6.28, 11.71) %, P = 0.012) all exhibited improvement in the MET group, compared with the non-MET group. MSG was reduced (–0.23 (–0.46, 0.30) mmol/L vs 0.22 (–0.24, 0.60) mmol/L, P = 0.043) with additional metformin. No significant difference in HbA1c (0.00 (–0.20, 0.10)% vs 0.05 (–0.20, 0.20)%, P = 0.182) between the MET group and the non-MET group. In parallel, changes in TIR displayed no major difference between the two groups.

Table 2

The changes in glycemic variability and glycemic control between the MET group and the non-MET group after 3-month intervention. Variables are expressed as the median (interquartile range, IQR).

MET (n = 32) Non-MET (n = 30) P-Value
Glycemic variability
 ΔMAGE (mmol/L) –1.58 (–3.35, 0.31) 1.36 (–1.12, 2.24) 0.004
 ΔSDBG (mmol/L) –0.85 (–1.51, 0.01) –0.14 (–0.68, 1.21) 0.015
 ΔLAGE (mmol/L) –2.83 (–5.47, –0.06) 0.45 (–1.29, 4.48) 0.004
 ΔCV (%) –6.66 (–15.00, 1.50) −1.60 (–6.28, 11.71) 0.012
 ΔMODD (mmol/L) –0.10 (–1.08, 0.42) –0.31 (–1.40, 1.55) 0.833
Glycemic control
 ΔTIR (%) –2.28 (–8.60, 3.67) 0.00 (–14.32, 6.69) 1.000
 ΔMSG (mmol/L) –0.23 (–0.46, 0.30) 0.22 (–0.24, 0.60) 0.043
 ΔHBA1c (%) 0.00 (–0.20, 0.10) 0.05 (–0.20, 0.20) 0.182

Delta (Δ)value = 3-month value – baseline value.

CV, coefficient of variation; HBA1c, hemoglobin A1cLAGE, largest amplitude of glycemic excursions; MAGE, mean amplitude of glucose excursions; MODD, mean of daily differences; MSG, mean sensor glucose; SDBG, standard deviation of blood glucose; TIR, time in range.

Subgroup analysis of glycemic variability and glycemic control in the MET group

The patients in the MET group were further divided into two subgroups on the basis of the median of baseline BMI (23.2 kg/m2), FPG (8.6 mmol/L), and HbA1c (8.2%), respectively (Table 3). The patients with a higher BMI presented greater reduction in MAGE (–2.97 (–4.42, –0.11) mmol/L vs –0.1 (–3.61, 0.97) mmol/L, P = 0.013) and CV (–11.26 (–16.36, –1.15)% vs –1.81(–11.87, 9.00)%, P = 0.049) as against those with a lower BMI. Yet, the changes in SDBG, LAGE, MODD, TIR, MSG, and HbA1c were not especially different between the two subgroups. No significant difference in the changes of GV and glycemic control was found between patients with different levels of FPG or HbA1c at baseline.

Table 3

Subgroup analysis of glycemic variability and glycemic control in the metformin group. Data are the median (interquartile range, IQR).

subgroups n ΔMAGE (mmol/L) ΔCV (%) ΔSDBG (mmol/L) ΔLAGE (mmol/L) ΔMODD (mmol/L) ΔTIR (%) ΔMSG (mmol/L) ΔHBA1c (%)
BMI (kg/m2) <23.2 21.3 ± 1.1 14 –0.11 (–3.61, 0.97)a –1.81 (–11.87, 9.00)a –0.23 (–1.36, 1.01) –0.78 (–3.61, 0.97) –0.28 (–1.72, 1.25) –2.42 (–9.69, 5.96) –0.21 (–0.49, 0.34) –0.05 (–0.30, 0.30)
≥23.2 24.3 ± 0.9 18 –2.97 (–4.42, –0.11)a –11.26 (–16.36, –1.15)a –1.15 (–1.63, –0.36) –3.44 (–8.13, –0.26) 0.02 (–1.05, 0.31) –1.47 (–9.31, 3.82) –2.97 (–0.46, 0.20) 0.00 (–0.50, 0.30)
FPG (mmol/L) <8.6 7.7 ± 0.7 12 –1.58 (–3.41, 0.32) –3.69 (–12.47, 1.40) –0.60 (–1.21, –0.07) –1.55 (–3.88, 2.47) 0.22 (–0.28, 0.84) –1.91 (–8.22, 7.74) –0.21 (–0.42, 0.03) 0.00 (–0.10, 0.10)
≥8.6 9.1 ± 0.4 20 –1.52 (–3.35, 0.31) –9.70 (–16.19, 3.08) –1.01 (–1.70, 0.29) –2.99 (–5.97, –0.42) –0.88 (–1.72, 0.26) –2.28 (–11.93, 3.28) –0.25 (–0.54, 0.33) –0.05 (–0.30, 0.10)
HbA1c (%) <8.2 7.6 ± 0.4 16 –2.21 (–3.63, 1.19) –11.21 (–15.32, 8.12) –1.01 (–1.42, 0.22) –2.83 (–7.61, 2.47) –0.17 (–1.02, 0.80) –5.21 (–12.34, 7.39) –0.15 (–0.42, 0.33) 0.00 (–0.28, 0.10)
≥8.2 8.9 ± 0.5 16 –0.68 (–2.88, 0.13) –3.56 (–15.00, 1.50) –0.72 (–1.58, 0.01) –1.95 (–4.97, –0.25) –0.10 (–2.16, 0.42) –1.37 (–8.05, 3.24) –0.26 (–0.50, 0.19) –0.10 (–0.20, 0.10)

aP<0.05 compared within subgroups.

FPG, fasting plasma glucose; HbA1c, glycated hemoglobin A1c.

Effect of metformin on insulin requirement and markers of body composition

Significant reduction in daily insulin dose per body weight (–0.02 ± 0.01 U/kg of body weight vs 0.00 ± 0.02 U/kg of body weight, P < 0.001; Fig. 2A and Table 4) was identified in the MET group as against the non-MET group. Both body weight (–0.4 ± 0.6 kg vs 0.2 ± 0.5 kg , P < 0.001; Fig. 2B and Table 4) and BMI (–0.2 ± 0.2 kg/m2 vs 0.1 ± 0.2 kg/m2, P < 0.001; Fig. 2C and Table 4) were substantially reduced in the MET group compared with the non-MET group after the 3-month intervention.

Figure 2
Figure 2

Metformin reduced insulin requirement and improved body composition in patients with type 1 diabetes mellitus. (A) Change in daily insulin dose (U per kg of body weight) in response to MET group vs non-MET group. (B) Change in bodyweight (kilograms) in response to MET group vs non-MET group. (C) Change in BMI (kilograms per meter squared) in response to MET group vs non-MET group. Significant reductions in daily insulin dose, body weight as well as BMI were observed in the patients in the MET group, and the changes were significantly different in comparison with those in non-MET group.

Citation: Endocrine Connections 10, 9; 10.1530/EC-21-0146

Table 4

The changes in lipid profiles and other parameters between the MET group and the non-MET group after 3-month intervention.

MET (n = 32) Non-MET (n = 30) P-Value
ΔTG (mmol/L) –0.23 ± 0.62 –0.13 ± 0.55 0.520
ΔTC (mmol/L) 0.03 ± 0.15 0.04 ± 0.24 0.899
ΔHDL-C (mmol/L) 0.11 ± 0.22 0.07 ± 0.21 0.473
ΔLDL-C (mmol/L) 0.00 ± 0.39 0.07 ± 0.35 0.448
ΔBody weight (kg) –0.4 ± 0.6 0.2 ± 0.5 <0.001
ΔBMI –0.2 ± 0.2 0.1 ± 0.2 <0.001
ΔDaily insulin dose (U/kg of body weight) –0.02 ± 0.01 0.00 ± 0.02 <0.001
ΔSBP –1 ± 9 0 ± 9 0.665
ΔDBP 1 ± 7 –1 ± 8 0.369

DBP, diastolic blood pressure; HDL-C, high-density lipoprotein cholesterol; LDL-C, low-density lipoprotein cholesterol; SBP, systolic blood pressure; TC, total cholesterol; TG, total triglyceride.

Effect of metformin on other traditional CVD risk factors

The adjuvant metformin therapy resulted in no notable change of lipids profile (TG, TC, HDL-c, and LDL-c), systolic BP, and diastolic BP between the two groups (Table 4).

Safety data

Among the 65 randomized participants, only 3 participants (4.6%) failed to complete the study protocol. There were no severe adverse events, with only minor gastrointestinal side effects (nausea, flatulence, reduced appetite, diarrhea) being reported in 8 participants in the MET group (23.5%). This led to de-escalation in the metformin dose in 4 participants (11.8%), while for the other 4 patients, these symptoms spontaneously resolved within 7 days. Hence, all participants tolerated at least 1000 mg metformin per day. Hypoglycemia events were recorded in 4 subjects with MET and 3 subjects with non-MET, and no severe hypoglycemia events were identified during the whole study. No major changes in serum creatinine, alanine aminotransferase, aspartate aminotransferase were observed between the two groups (data not shown).

Discussion

In the present randomized, open-label, controlled trial, a slight decline in the HbA1c level in the MET group was observed, in contrast to the rising trend in the non-MET group. However, there was no significant difference in these changes between the two groups.

In recent years, a profusion of attempts has been made to assist T1DM patients in achieving near-normal glycemic control, including advancement in diabetes management through the development of insulin analogs, insulin infusion devices, as well as glucose monitoring systems. Despite these attempts, the current situation is far from satisfactory (19, 20, 21). Previous clinical studies and meta-analyses have reported that metformin, as an adjuvant therapy to T1DM, has minimal benefits for glycemic control (7, 16, 18, 22, 23). Conversely, new evidence has revealed modest improvements in the HbA1c level of T1DM patients with adjuvant metformin therapy. One meta-analysis highlighted that metformin reduced the HbA1c level by 0.26% in T1DM (24). These discrepancies may be attributed to different study durations with a 3-month cutoff point, implying that the reduction in the HbA1c level caused by metformin could not sustain over time (24). Moreover, a study of T1DM patients under real-world conditions reported that the HbA1c level decreased after a 1-year follow-up owing to scheduled follow-up visits rather than additional metformin treatment (25).

For further evaluation, TIR, which generally describes the percent of time spent within the target glucose range (3.9–10 mmol/L), was also calculated from the CGM data. Yet, no notable difference was observed in TIR before and after the 3-month treatment between the two groups. Emerging as one of the central metrics of glycemic control, TIR has a close association with vascular complications of diabetes (26, 27). Although a goal of >70% TIR was recommended by recent consensus statements for people with diabetes (28), the baseline TIR of T1DM patients in the present study was considerably below target and was seemingly not improved by the adjuvant metformin therapy.

Tough robust data have suggested that HbA1c and TIR are important predictors of CVD risk in patients with diabetes (6, 26, 27, 28, 29), but these metrics can only reflect the average glucose levels over a period of time. Further metrics are required to understand glycemic control in the entirety thereof, particularly those reflecting glucose fluctuations, such as hypoglycemia. Notably, hypoglycemia is a crucial barrier for patients with T1DM to achieve near-normal glycemic control (19, 21). Reports have indicated that T1DM patients with HbA1c levels of <7.0 or >7.5% suffered more frequent severe hypoglycemia than those with HbA1c levels of 7.0 to 7.5% (21). GV, meanwhile, reflects the glucose homeostasis over a given interval of time and has become prominent as another vital metric for assessing glycemic control in clinical practice. Further, GV supposedly contributes more to the onset of diabetic cardiovascular complications than persistent hyperglycemia. Prior research has demonstrated that acute glycemic fluctuations could lead to CVD through oxidative stress and nuclear factor-κB activation (30, 31). Moreover, a positive association between intermittent high blood glucose exposure, endothelial dysfunction, and damage has already been illustrated (32), while flattening GV has been reported to mitigate IR and reduce cIMT, a surrogate of CVD, in patients with T2DM (33). As against T2DM, GV notably has a more robust impact on diabetes complications in T1DM, most likely being attributed to the marked islet cell secretory dysfunction in the latter group (12).

As previously mentioned, the effect of metformin on HbA1c levels has been fully explored in patients with T1DM, while studies focusing on the aspect of GV are scarce. The other primary finding of the present study was that, in patients with T1DM, adjuvant metformin therapy reduced MAGE, together with other metrics of GV (SDBG, LAGE, and CV). Similar reductions in MAGE and SD were also detected by Fei Gao et al. in patients with T2DM by employing metformin add-on insulin therapy (34). Various metrics have been introduced to describe GV over the years, yet no consensus has been reached on the most appropriate characterization thereof. Introduced by Service et al. as the 'gold standard' for the evaluation of the intra-day GV, MAGE centers on major glycemic excursions rather than minor ones (35). Dasari et al. reported that MAGE was closely linked with oxidative stress markers (36). Further, a meta-analysis conducted by Pu et al. revealed that a higher MAGE was associated with a higher risk of major adverse cardiovascular events (MACEs) in individuals, whether with or without diabetes (37). However, no significant changes in MODD, which estimates between-day GV (38), were identified between the two groups in the present study. Since only 72 h of CGM data were collected for quantification of GV in the present study, a longer CGM time might be required for the further evaluation of this metric.

Thus, the hypothesis in the present study is that metformin add-on insulin therapy could reduce glycemic fluctuation in T1DM to some extent, which may serve as one of the mechanisms of alleviating endothelium damage and enhance cardioprotective benefits. This hypothesis needs to be verified by prospective studies.

The final finding of the present study was that additional metformin decreased BMI and body weight by 0.2 kg/m2 and 0.4 kg, respectively. Bjornstad P et al. reported similar results in youth with T1DM (16), and even further reduction in BMI was detected by Agnieszka Z et al. in adults with T1DM, in addition to excess body fat (17). Moreover, adjuvant metformin therapy also reduced the insulin requirement in the present study. Lund et al. correspondingly identified a sustained reduction in weight and insulin dosage in T1DM patients over a 1-year treatment with metformin (39). All of the aforementioned research has indicated that additional metformin improved metabolic control while reducing IR in patients with T1DM. Be that as it may, in the present study, no improvement was observed in other cardiovascular risk factors, such as lipid profiles and blood pressure, in the MET group. These results align well with previous research on youth with T1DM (16). In contrast, conflicting conclusions were reported by Liu et al. who found improvement in partial lipid profiles and diastolic blood pressure in T1DM patients with additional metformin (24).

According to the previous literature, metformin supposedly increases the risk of gastrointestinal adverse effects and may induce more hypoglycemia events in patients with T1DM (24, 40). In the present study, no severe adverse events were observed, and only four participants (11.8%) in the metformin group had the insulin dose thereof down escalated due to gastrointestinal side effects. Further, all patients tolerated at least 1000 mg metformin per day during the whole study, and metformin did not increase the incidence of hypoglycemia.

There are several significant strengths and limitations of the present study. First, this carefully designed, well-conducted clinical study is the first study to explore the effects of additional metformin on the GV in adults with T1DM. Secondly, both normal-weight and overweight/obese patients with T1DM were included, allowing further subgroup analysis in patients with different BMI levels. Thirdly, the patients in both groups demonstrated relatively well adherence to CGM and had high visit attendance. The limitations in our study include the fact that the open-label design thereof may lead to a degree of bias. Moreover, CGM data were collected for 72 h, while a recommendation of 2–4 weeks of data collection has been proposed by current guidelines in clinical practice (28, 41). This is because prolonging the duration of CGM could minimize the statistical bias of GV and TIR on the individual level. Additionally, the effect of individual diet and exercise deviations on GV could not be wholly excluded. The bias was minimized by reinforcing the guidance for diet and physical activity at each visit and urging the patients to maintain the same diet and physical activity during the CGM period.

Conclusions

Additional metformin therapy for 3 months reduced blood glucose fluctuation in adults with T1DM, particularly in those with higher BMI. Further, metformin improved the body composition and reduced the insulin requirement, indicating the reduction in insulin resistance in patients with T1DM. No severe adverse events or hypoglycemia was induced by additional metformin. To conclude, metformin as an adjunctive therapy has potential prospects in the management of CVD risk in T1DM in the long term, which needs to be further elucidated in outcome trials.

Declaration of interest

The authors declare that there is no conflict of interest that could be perceived as prejudicing the impartiality of the research reported.

Funding

This research did not receive any specific grant from any funding agency in the public, commercial or not-for-profit sector.

Author contribution statement

X Z conceived the study and wrote the paper. X Z and F Y contributed to the design of the research. All authors were involved in data collection. D X, P X, and S Y analyzed the data. Q Z and W Y revised the manuscript. X Z and F Y are the guarantors of this work. All authors edited and approved the final version of the manuscript.

Acknowledgements

The authors thank all of the patients who participated in this study. The authors also thank the colleagues who devoted their efforts to this study, including dietician, diabetic educators, nurses, and technicians.

References

  • 1

    Mayer-Davis EJ, Dabelea D, Lawrence JM. Incidence trends of Type 1 and Type 2 diabetes among youths, 2002–2012. New England Journal of Medicine 2017 377 301. (https://doi.org/10.1056/NEJMc1706291)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 2

    Rawshani A, Rawshani A, Franzen S, Eliasson B, Svensson AM, Miftaraj M, McGuire DK, Sattar N, Rosengren A, Gudbjornsdottir S. Mortality and cardiovascular disease in Type 1 and Type 2 diabetes. New England Journal of Medicine 2017 376 14071418. (https://doi.org/10.1056/NEJMoa1608664)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 3

    Livingstone SJ, Looker HC, Hothersall EJ, Wild SH, Lindsay RS, Chalmers J, Cleland S, Leese GP, McKnight J & Morris AD et al. Risk of cardiovascular disease and total mortality in adults with type 1 diabetes: scottish registry linkage study. PLoS Medicine 2012 9 e1001321. (https://doi.org/10.1371/journal.pmed.1001321)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 4

    Livingstone SJ, Levin D, Looker HC, Lindsay RS, Wild SH, Joss N, Leese G, Leslie P, McCrimmon RJ & Metcalfe W et al. Estimated life expectancy in a Scottish cohort with type 1 diabetes, 2008–2010. JAMA 2015 313 3744. (https://doi.org/10.1001/jama.2014.16425)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 5

    Cleary PA, Orchard TJ, Genuth S, Wong ND, Detrano R, Backlund JY, Zinman B, Jacobson A, Sun W & Lachin JM et al. The effect of intensive glycemic treatment on coronary artery calcification in type 1 diabetic participants of the Diabetes Control and Complications Trial/Epidemiology of Diabetes Interventions and Complications (DCCT/EDIC) Study. Diabetes 2006 55 35563565. (https://doi.org/10.2337/db06-0653)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 6

    Diabetes Control and Complications Trial Research Group, Nathan DM, Genuth S, Lachin J, Cleary P, Crofford O, Davis M, Rand L, Siebert C. The effect of intensive treatment of diabetes on the development and progression of long-term complications in insulin-dependent diabetes mellitus. New England Journal of Medicine 1993 329 977986. (https://doi.org/10.1056/NEJM199309303291401)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 7

    Bloomgarden Z, Ning G. Type 2 treatments for type 1 diabetes. Journal of Diabetes 2016 8 599601. (https://doi.org/10.1111/1753-0407.12430)

  • 8

    Chillaron JJ, Flores Le-Roux JA, Benaiges D, Pedro-Botet J. Type 1 diabetes, metabolic syndrome and cardiovascular risk. Metabolism: Clinical and Experimental 2014 63 181187. (https://doi.org/10.1016/j.metabol.2013.10.002)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 9

    Nadeau KJ, Regensteiner JG, Bauer TA, Brown MS, Dorosz JL, Hull A, Zeitler P, Draznin B, Reusch JE. Insulin resistance in adolescents with type 1 diabetes and its relationship to cardiovascular function. Journal of Clinical Endocrinology and Metabolism 2010 95 513521. (https://doi.org/10.1210/jc.2009-1756)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 10

    Schauer IE, Snell-Bergeon JK, Bergman BC, Maahs DM, Kretowski A, Eckel RH, Rewers M. Insulin resistance, defective insulin-mediated fatty acid suppression, and coronary artery calcification in subjects with and without type 1 diabetes: the CACTI study. Diabetes 2011 60 306314. (https://doi.org/10.2337/db10-0328)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 11

    Zhou Z, Sun B, Huang S, Zhu C, Bian M. Glycemic variability: adverse clinical outcomes and how to improve it? Cardiovascular Diabetology 2020 19 102. (https://doi.org/10.1186/s12933-020-01085-6)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 12

    Ceriello A, Ihnat MA. ‘Glycaemic variability’: a new therapeutic challenge in diabetes and the critical care setting. Diabetic Medicine 2010 27 862867. (https://doi.org/10.1111/j.1464-5491.2010.02967.x)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 13

    Klip A, Leiter LA. Cellular mechanism of action of metformin. Diabetes Care 1990 13 696704. (https://doi.org/10.2337/diacare.13.6.696)

  • 14

    Cusi K, Consoli A, DeFronzo RA. Metabolic effects of metformin on glucose and lactate metabolism in noninsulin-dependent diabetes mellitus. Journal of Clinical Endocrinology and Metabolism 1996 81 40594067. (https://doi.org/10.1210/jcem.81.11.8923861)+

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 15

    UK Prospective Diabetes Study Group. Effect of intensive blood-glucose control with metformin on complications in overweight patients with type 2 diabetes (UKPDS 34). Lancet 1998 352 854865. (https://doi.org/10.1016/S0140-6736(9807037-8)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 16

    Bjornstad P, Schafer M, Truong U, Cree-Green M, Pyle L, Baumgartner A, Garcia Reyes Y, Maniatis A, Nayak S & Wadwa RP et al. Metformin improves insulin sensitivity and vascular health in youth with type 1 diabetes mellitus. Circulation 2018 138 28952907. (https://doi.org/10.1161/CIRCULATIONAHA.118.035525)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 17

    Zawada A, Naskret D, Burchardt P, Niedzwiecki P, Pilacinski S, Wierusz-Wysocka B, Grzymislawski M, Zozulinska-Ziolkiewicz D. Metformin added to intensive insulin therapy improves metabolic control in patients with type 1 diabetes and excess body fat. Polish Archives of Internal Medicine 2018 128 294300. (https://doi.org/10.20452/pamw.4241)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 18

    Petrie JR, Chaturvedi N, Ford I, Brouwers MCGJ, Greenlaw N, Tillin T, Hramiak I, Hughes AD, Jenkins AJ & Klein BEK et al. Cardiovascular and metabolic effects of metformin in patients with type 1 diabetes (REMOVAL): a double-blind, randomised, placebo-controlled trial. Lancet: Diabetes and Endocrinology 2017 5 597609. (https://doi.org/10.1016/S2213-8587(1730194-8)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 19

    Simmons JH, Chen V, Miller KM, McGill JB, Bergenstal RM, Goland RS, Harlan DM, Largay JF, Massaro EM & Beck RW et al. Differences in the management of type 1 diabetes among adults under excellent control compared with those under poor control in the T1D exchange clinic registry. Diabetes Care 2013 36 35733577. (https://doi.org/10.2337/dc12-2643)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 20

    Haller MJ, Silverstein JH. In pursuit of lower A1c. Journal of Pediatrics 2009 155 161162. (https://doi.org/10.1016/j.jpeds.2009.03.006)

  • 21

    Weinstock RS, Xing D, Maahs DM, Michels A, Rickels MR, Peters AL, Bergenstal RM, Harris B, Dubose SN & Miller KM et al. Severe hypoglycemia and diabetic ketoacidosis in adults with type 1 diabetes: results from the T1D exchange clinic registry. Journal of Clinical Endocrinology and Metabolism 2013 98 34113419. (https://doi.org/10.1210/jc.2013-1589)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 22

    Liu C, Wu D, Zheng X, Li P, Li L. Efficacy and safety of metformin for patients with type 1 diabetes mellitus: a meta-analysis. Diabetes Technology and Therapeutics 2015 17 142148. (https://doi.org/10.1089/dia.2014.0190)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 23

    Libman IM, Miller KM, DiMeglio LA, Bethin KE, Katz ML, Shah A, Simmons JH, Haller MJ, Raman S & Tamborlane WV et al. Effect of metformin added to insulin on glycemic control among overweight/obese adolescents with type 1 diabetes: a randomized clinical trial. JAMA 2015 314 22412250. (https://doi.org/10.1001/jama.2015.16174)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 24

    Liu YS, Chen CN, Chen ZG, Peng Y, Lin XP, Xu LL. Vascular and metabolic effects of metformin added to insulin therapy in patients with type 1 diabetes: a systematic review and meta-analysis. Diabetes/Metabolism Research and Reviews 2020 36 e3334. (https://doi.org/10.1002/dmrr.3334)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 25

    Qiu L, Ling P, Yang D, Luo S, Zheng X, Liang H, Yuan Y, Liang G, Xu W & Yao B et al. Current status of metformin in addition to insulin therapy in adult patients with type 1 diabetes mellitus: an analysis from the Guangdong type 1 diabetes mellitus translational medicine study. Journal of Diabetes 2020 12 754760. (https://doi.org/10.1111/1753-0407.13025)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 26

    Yoo JH, Choi MS, Ahn J, Park SW, Kim Y, Hur KY, Jin SM, Kim G, Kim JH. Association between continuous glucose monitoring-derived time in range, other core metrics, and albuminuria in type 2 diabetes. Diabetes Technology and Therapeutics 2020 22 768776. (https://doi.org/10.1089/dia.2019.0499)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 27

    Beck RW, Bergenstal RM, Riddlesworth TD, Kollman C, Li Z, Brown AS, Close KL. Validation of time in range as an outcome measure for diabetes clinical trials. Diabetes Care 2019 42 400405. (https://doi.org/10.2337/dc18-1444)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 28

    Danne T, Nimri R, Battelino T, Bergenstal RM, Close KL, DeVries JH, Garg S, Heinemann L, Hirsch I & Amiel SA et al. International consensus on use of continuous glucose monitoring. Diabetes Care 2017 40 16311640. (https://doi.org/10.2337/dc17-1600)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 29

    UK Prospective Diabetes Study Group. Intensive blood-glucose control with sulphonylureas or insulin compared with conventional treatment and risk of complications in patients with type 2 diabetes (UKPDS 33). Lancet 1998 352 837853. (https://doi.org/10.1016/S0140-6736(9807019-6)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 30

    Zhang W, Zhao S, Li Y, Peng G, Han P. Acute blood glucose fluctuation induces myocardial apoptosis through oxidative stress and nuclear factor-kB activation. Cardiology 2013 124 1117. (https://doi.org/10.1159/000345436)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 31

    Saisho Y Glycemic variability and oxidative stress: a link between diabetes and cardiovascular disease? International Journal of Molecular Sciences 2014 15 1838118406. (https://doi.org/10.3390/ijms151018381)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 32

    Nusca A, Tuccinardi D, Albano M, Cavallaro C, Ricottini E, Manfrini S, Pozzilli P, Di Sciascio G. Glycemic variability in the development of cardiovascular complications in diabetes. Diabetes/Metabolism Research and Reviews 2018 34 e3047. (https://doi.org/10.1002/dmrr.3047)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 33

    Liang S, Yin H, Wei C, Xie L, He H, Liu X. Glucose variability for cardiovascular risk factors in type 2 diabetes: a meta-analysis. Journal of Diabetes and Metabolic Disorders 2017 16 45. (https://doi.org/10.1186/s40200-017-0323-5)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 34

    Gao F, Ma X, Peng J, Lu J, Lu W, Zhu W, Bao Y, Vigersky RA, Jia W, Zhou J. The effect of acarbose on glycemic variability in patients with type 2 diabetes mellitus using premixed insulin compared to metformin (AIM): an open-label randomized trial. Diabetes Technology and Therapeutics 2020 22 256264. (https://doi.org/10.1089/dia.2019.0290)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 35

    Service FJ, Molnar GD, Rosevear JW, Ackerman E, Gatewood LC, Taylor WF. Mean amplitude of glycemic excursions, a measure of diabetic instability. Diabetes 1970 19 644655. (https://doi.org/10.2337/diab.19.9.644)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 36

    Dasari PS, Gandomani BS, Teague AM, Pitale A, Otto M, Short KR. Glycemic variability is associated with markers of vascular stress in adolescents. Journal of Pediatrics 2016 172 47.e4255.e42.(https://doi.org/10.1016/j.jpeds.2016.01.065)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 37

    Pu Z, Lai L, Yang X, Wang Y, Dong P, Wang D, Xie Y, Han Z. Acute glycemic variability on admission predicts the prognosis in hospitalized patients with coronary artery disease: a meta-analysis. Endocrine 2020 67 526534. (https://doi.org/10.1007/s12020-019-02150-1)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 38

    Molnar GD, Taylor WF, Ho MM. Day-to-day variation of continuously monitored glycaemia: a further measure of diabetic instability. Diabetologia 1972 8 342348. (https://doi.org/10.1007/BF01218495)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 39

    Lund SS, Tarnow L, Astrup AS, Hovind P, Jacobsen PK, Alibegovic AC, Parving I, Pietraszek L, Frandsen M & Rossing P et al. Effect of adjunct metformin treatment in patients with type-1 diabetes and persistent inadequate glycaemic control: a randomized study. PLoS ONE 2008 3 e3363. (https://doi.org/10.1371/journal.pone.0003363)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 40

    Priya G, Kalra S. A review of insulin resistance in type 1 diabetes: is there a place for adjunctive metformin? Diabetes Therapy 2018 9 349361. (https://doi.org/10.1007/s13300-017-0333-9)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 41

    Battelino T, Danne T, Bergenstal RM, Amiel SA, Beck R, Biester T, Bosi E, Buckingham BA, Cefalu WT & Close KL et al. Clinical targets for continuous glucose monitoring data interpretation: recommendations From the international consensus on time in range. Diabetes Care 2019 42 15931603. (https://doi.org/10.2337/dci19-0028)

    • PubMed
    • Search Google Scholar
    • Export Citation

 

  • Collapse
  • Expand
  • Figure 1

    The diagram of clinical trials in participants with type 1 diabetes mellitus. f/u, follow-up.

  • Figure 2

    Metformin reduced insulin requirement and improved body composition in patients with type 1 diabetes mellitus. (A) Change in daily insulin dose (U per kg of body weight) in response to MET group vs non-MET group. (B) Change in bodyweight (kilograms) in response to MET group vs non-MET group. (C) Change in BMI (kilograms per meter squared) in response to MET group vs non-MET group. Significant reductions in daily insulin dose, body weight as well as BMI were observed in the patients in the MET group, and the changes were significantly different in comparison with those in non-MET group.

  • 1

    Mayer-Davis EJ, Dabelea D, Lawrence JM. Incidence trends of Type 1 and Type 2 diabetes among youths, 2002–2012. New England Journal of Medicine 2017 377 301. (https://doi.org/10.1056/NEJMc1706291)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 2

    Rawshani A, Rawshani A, Franzen S, Eliasson B, Svensson AM, Miftaraj M, McGuire DK, Sattar N, Rosengren A, Gudbjornsdottir S. Mortality and cardiovascular disease in Type 1 and Type 2 diabetes. New England Journal of Medicine 2017 376 14071418. (https://doi.org/10.1056/NEJMoa1608664)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 3

    Livingstone SJ, Looker HC, Hothersall EJ, Wild SH, Lindsay RS, Chalmers J, Cleland S, Leese GP, McKnight J & Morris AD et al. Risk of cardiovascular disease and total mortality in adults with type 1 diabetes: scottish registry linkage study. PLoS Medicine 2012 9 e1001321. (https://doi.org/10.1371/journal.pmed.1001321)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 4

    Livingstone SJ, Levin D, Looker HC, Lindsay RS, Wild SH, Joss N, Leese G, Leslie P, McCrimmon RJ & Metcalfe W et al. Estimated life expectancy in a Scottish cohort with type 1 diabetes, 2008–2010. JAMA 2015 313 3744. (https://doi.org/10.1001/jama.2014.16425)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 5

    Cleary PA, Orchard TJ, Genuth S, Wong ND, Detrano R, Backlund JY, Zinman B, Jacobson A, Sun W & Lachin JM et al. The effect of intensive glycemic treatment on coronary artery calcification in type 1 diabetic participants of the Diabetes Control and Complications Trial/Epidemiology of Diabetes Interventions and Complications (DCCT/EDIC) Study. Diabetes 2006 55 35563565. (https://doi.org/10.2337/db06-0653)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 6

    Diabetes Control and Complications Trial Research Group, Nathan DM, Genuth S, Lachin J, Cleary P, Crofford O, Davis M, Rand L, Siebert C. The effect of intensive treatment of diabetes on the development and progression of long-term complications in insulin-dependent diabetes mellitus. New England Journal of Medicine 1993 329 977986. (https://doi.org/10.1056/NEJM199309303291401)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 7

    Bloomgarden Z, Ning G. Type 2 treatments for type 1 diabetes. Journal of Diabetes 2016 8 599601. (https://doi.org/10.1111/1753-0407.12430)

  • 8

    Chillaron JJ, Flores Le-Roux JA, Benaiges D, Pedro-Botet J. Type 1 diabetes, metabolic syndrome and cardiovascular risk. Metabolism: Clinical and Experimental 2014 63 181187. (https://doi.org/10.1016/j.metabol.2013.10.002)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 9

    Nadeau KJ, Regensteiner JG, Bauer TA, Brown MS, Dorosz JL, Hull A, Zeitler P, Draznin B, Reusch JE. Insulin resistance in adolescents with type 1 diabetes and its relationship to cardiovascular function. Journal of Clinical Endocrinology and Metabolism 2010 95 513521. (https://doi.org/10.1210/jc.2009-1756)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 10

    Schauer IE, Snell-Bergeon JK, Bergman BC, Maahs DM, Kretowski A, Eckel RH, Rewers M. Insulin resistance, defective insulin-mediated fatty acid suppression, and coronary artery calcification in subjects with and without type 1 diabetes: the CACTI study. Diabetes 2011 60 306314. (https://doi.org/10.2337/db10-0328)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 11

    Zhou Z, Sun B, Huang S, Zhu C, Bian M. Glycemic variability: adverse clinical outcomes and how to improve it? Cardiovascular Diabetology 2020 19 102. (https://doi.org/10.1186/s12933-020-01085-6)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 12

    Ceriello A, Ihnat MA. ‘Glycaemic variability’: a new therapeutic challenge in diabetes and the critical care setting. Diabetic Medicine 2010 27 862867. (https://doi.org/10.1111/j.1464-5491.2010.02967.x)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 13

    Klip A, Leiter LA. Cellular mechanism of action of metformin. Diabetes Care 1990 13 696704. (https://doi.org/10.2337/diacare.13.6.696)

  • 14

    Cusi K, Consoli A, DeFronzo RA. Metabolic effects of metformin on glucose and lactate metabolism in noninsulin-dependent diabetes mellitus. Journal of Clinical Endocrinology and Metabolism 1996 81 40594067. (https://doi.org/10.1210/jcem.81.11.8923861)+

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 15

    UK Prospective Diabetes Study Group. Effect of intensive blood-glucose control with metformin on complications in overweight patients with type 2 diabetes (UKPDS 34). Lancet 1998 352 854865. (https://doi.org/10.1016/S0140-6736(9807037-8)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 16

    Bjornstad P, Schafer M, Truong U, Cree-Green M, Pyle L, Baumgartner A, Garcia Reyes Y, Maniatis A, Nayak S & Wadwa RP et al. Metformin improves insulin sensitivity and vascular health in youth with type 1 diabetes mellitus. Circulation 2018 138 28952907. (https://doi.org/10.1161/CIRCULATIONAHA.118.035525)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 17

    Zawada A, Naskret D, Burchardt P, Niedzwiecki P, Pilacinski S, Wierusz-Wysocka B, Grzymislawski M, Zozulinska-Ziolkiewicz D. Metformin added to intensive insulin therapy improves metabolic control in patients with type 1 diabetes and excess body fat. Polish Archives of Internal Medicine 2018 128 294300. (https://doi.org/10.20452/pamw.4241)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 18

    Petrie JR, Chaturvedi N, Ford I, Brouwers MCGJ, Greenlaw N, Tillin T, Hramiak I, Hughes AD, Jenkins AJ & Klein BEK et al. Cardiovascular and metabolic effects of metformin in patients with type 1 diabetes (REMOVAL): a double-blind, randomised, placebo-controlled trial. Lancet: Diabetes and Endocrinology 2017 5 597609. (https://doi.org/10.1016/S2213-8587(1730194-8)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 19

    Simmons JH, Chen V, Miller KM, McGill JB, Bergenstal RM, Goland RS, Harlan DM, Largay JF, Massaro EM & Beck RW et al. Differences in the management of type 1 diabetes among adults under excellent control compared with those under poor control in the T1D exchange clinic registry. Diabetes Care 2013 36 35733577. (https://doi.org/10.2337/dc12-2643)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 20

    Haller MJ, Silverstein JH. In pursuit of lower A1c. Journal of Pediatrics 2009 155 161162. (https://doi.org/10.1016/j.jpeds.2009.03.006)

  • 21

    Weinstock RS, Xing D, Maahs DM, Michels A, Rickels MR, Peters AL, Bergenstal RM, Harris B, Dubose SN & Miller KM et al. Severe hypoglycemia and diabetic ketoacidosis in adults with type 1 diabetes: results from the T1D exchange clinic registry. Journal of Clinical Endocrinology and Metabolism 2013 98 34113419. (https://doi.org/10.1210/jc.2013-1589)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 22

    Liu C, Wu D, Zheng X, Li P, Li L. Efficacy and safety of metformin for patients with type 1 diabetes mellitus: a meta-analysis. Diabetes Technology and Therapeutics 2015 17 142148. (https://doi.org/10.1089/dia.2014.0190)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 23

    Libman IM, Miller KM, DiMeglio LA, Bethin KE, Katz ML, Shah A, Simmons JH, Haller MJ, Raman S & Tamborlane WV et al. Effect of metformin added to insulin on glycemic control among overweight/obese adolescents with type 1 diabetes: a randomized clinical trial. JAMA 2015 314 22412250. (https://doi.org/10.1001/jama.2015.16174)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 24

    Liu YS, Chen CN, Chen ZG, Peng Y, Lin XP, Xu LL. Vascular and metabolic effects of metformin added to insulin therapy in patients with type 1 diabetes: a systematic review and meta-analysis. Diabetes/Metabolism Research and Reviews 2020 36 e3334. (https://doi.org/10.1002/dmrr.3334)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 25

    Qiu L, Ling P, Yang D, Luo S, Zheng X, Liang H, Yuan Y, Liang G, Xu W & Yao B et al. Current status of metformin in addition to insulin therapy in adult patients with type 1 diabetes mellitus: an analysis from the Guangdong type 1 diabetes mellitus translational medicine study. Journal of Diabetes 2020 12 754760. (https://doi.org/10.1111/1753-0407.13025)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 26

    Yoo JH, Choi MS, Ahn J, Park SW, Kim Y, Hur KY, Jin SM, Kim G, Kim JH. Association between continuous glucose monitoring-derived time in range, other core metrics, and albuminuria in type 2 diabetes. Diabetes Technology and Therapeutics 2020 22 768776. (https://doi.org/10.1089/dia.2019.0499)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 27

    Beck RW, Bergenstal RM, Riddlesworth TD, Kollman C, Li Z, Brown AS, Close KL. Validation of time in range as an outcome measure for diabetes clinical trials. Diabetes Care 2019 42 400405. (https://doi.org/10.2337/dc18-1444)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 28

    Danne T, Nimri R, Battelino T, Bergenstal RM, Close KL, DeVries JH, Garg S, Heinemann L, Hirsch I & Amiel SA et al. International consensus on use of continuous glucose monitoring. Diabetes Care 2017 40 16311640. (https://doi.org/10.2337/dc17-1600)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 29

    UK Prospective Diabetes Study Group. Intensive blood-glucose control with sulphonylureas or insulin compared with conventional treatment and risk of complications in patients with type 2 diabetes (UKPDS 33). Lancet 1998 352 837853. (https://doi.org/10.1016/S0140-6736(9807019-6)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 30

    Zhang W, Zhao S, Li Y, Peng G, Han P. Acute blood glucose fluctuation induces myocardial apoptosis through oxidative stress and nuclear factor-kB activation. Cardiology 2013 124 1117. (https://doi.org/10.1159/000345436)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 31

    Saisho Y Glycemic variability and oxidative stress: a link between diabetes and cardiovascular disease? International Journal of Molecular Sciences 2014 15 1838118406. (https://doi.org/10.3390/ijms151018381)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 32

    Nusca A, Tuccinardi D, Albano M, Cavallaro C, Ricottini E, Manfrini S, Pozzilli P, Di Sciascio G. Glycemic variability in the development of cardiovascular complications in diabetes. Diabetes/Metabolism Research and Reviews 2018 34 e3047. (https://doi.org/10.1002/dmrr.3047)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 33

    Liang S, Yin H, Wei C, Xie L, He H, Liu X. Glucose variability for cardiovascular risk factors in type 2 diabetes: a meta-analysis. Journal of Diabetes and Metabolic Disorders 2017 16 45. (https://doi.org/10.1186/s40200-017-0323-5)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 34

    Gao F, Ma X, Peng J, Lu J, Lu W, Zhu W, Bao Y, Vigersky RA, Jia W, Zhou J. The effect of acarbose on glycemic variability in patients with type 2 diabetes mellitus using premixed insulin compared to metformin (AIM): an open-label randomized trial. Diabetes Technology and Therapeutics 2020 22 256264. (https://doi.org/10.1089/dia.2019.0290)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 35

    Service FJ, Molnar GD, Rosevear JW, Ackerman E, Gatewood LC, Taylor WF. Mean amplitude of glycemic excursions, a measure of diabetic instability. Diabetes 1970 19 644655. (https://doi.org/10.2337/diab.19.9.644)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 36

    Dasari PS, Gandomani BS, Teague AM, Pitale A, Otto M, Short KR. Glycemic variability is associated with markers of vascular stress in adolescents. Journal of Pediatrics 2016 172 47.e4255.e42.(https://doi.org/10.1016/j.jpeds.2016.01.065)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 37

    Pu Z, Lai L, Yang X, Wang Y, Dong P, Wang D, Xie Y, Han Z. Acute glycemic variability on admission predicts the prognosis in hospitalized patients with coronary artery disease: a meta-analysis. Endocrine 2020 67 526534. (https://doi.org/10.1007/s12020-019-02150-1)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 38

    Molnar GD, Taylor WF, Ho MM. Day-to-day variation of continuously monitored glycaemia: a further measure of diabetic instability. Diabetologia 1972 8 342348. (https://doi.org/10.1007/BF01218495)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 39

    Lund SS, Tarnow L, Astrup AS, Hovind P, Jacobsen PK, Alibegovic AC, Parving I, Pietraszek L, Frandsen M & Rossing P et al. Effect of adjunct metformin treatment in patients with type-1 diabetes and persistent inadequate glycaemic control: a randomized study. PLoS ONE 2008 3 e3363. (https://doi.org/10.1371/journal.pone.0003363)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 40

    Priya G, Kalra S. A review of insulin resistance in type 1 diabetes: is there a place for adjunctive metformin? Diabetes Therapy 2018 9 349361. (https://doi.org/10.1007/s13300-017-0333-9)

    • PubMed
    • Search Google Scholar
    • Export Citation
  • 41

    Battelino T, Danne T, Bergenstal RM, Amiel SA, Beck R, Biester T, Bosi E, Buckingham BA, Cefalu WT & Close KL et al. Clinical targets for continuous glucose monitoring data interpretation: recommendations From the international consensus on time in range. Diabetes Care 2019 42 15931603. (https://doi.org/10.2337/dci19-0028)

    • PubMed
    • Search Google Scholar
    • Export Citation