Skip to main content
PMC home page
Springer logoLink to Springer
. 2018 Mar 12;55(6):557–568. doi: 10.1007/s00592-018-1124-0

Predictors of treatment response to liraglutide in type 2 diabetes in a real-world setting

N Simioni 1, C Berra 2, M Boemi 3, A C Bossi 4, R Candido 5, G Di Cianni 6, S Frontoni 7, S Genovese 8, P Ponzani 9, V Provenzano 10, G T Russo 11, L Sciangula 12, A Lapolla 13, C Bette 14, M C Rossi 15,; ReaL (NN2211-4118) Study Group*
PMCID: PMC5959971  PMID: 29527621

Abstract

Aims

There is an unmet need among healthcare providers to identify subgroups of patients with type 2 diabetes who are most likely to respond to treatment.

Methods

Data were taken from electronic medical records of participants of an observational, retrospective study in Italy. We used logistic regression models to assess the odds of achieving glycated haemoglobin (HbA1c) reduction ≥ 1.0% point after 12-month treatment with liraglutide (primary endpoint), according to various patient-related factors. RECursive Partitioning and AMalgamation (RECPAM) analysis was used to identify distinct homogeneous patient subgroups with different odds of achieving the primary endpoint.

Results

Data from 1325 patients were included, of which 577 (43.5%) achieved HbA1c reduction ≥ 1.0% point (10.9 mmol/mol) after 12 months. Logistic regression showed that for each additional 1% HbA1c at baseline, the odds of reaching this endpoint were increased 3.5 times (95% CI: 2.90–4.32). By use of RECPAM analysis, five distinct responder subgroups were identified, with baseline HbA1c and diabetes duration as the two splitting variables. Patients in the most poorly controlled subgroup (RECPAM Class 1, mean baseline HbA1c > 9.1% [76 mmol/mol]) had a 28-fold higher odds of reaching the endpoint versus patients in the best-controlled group (mean baseline HbA1c ≤ 7.5% [58 mmol/mol]). Mean HbA1c reduction from baseline was as large as − 2.2% (24 mol/mol) in the former versus − 0.1% (1.1 mmol/mol) in the latter. Mean weight reduction ranged from 2.5 to 4.3 kg across RECPAM subgroups.

Conclusions

Glycaemic response to liraglutide is largely driven by baseline HbA1c levels and, to a lesser extent, by diabetes duration.

Keywords: Liraglutide, Type 2 diabetes, Response to therapy, RECPAM analysis, GLP-1RA

Introduction

Liraglutide is a once-daily human glucagon-like peptide-1 (GLP-1) analogue available for the treatment of type 2 diabetes (T2D), and its efficacy and safety have been demonstrated in the Liraglutide Effect and Action in Diabetes (LEAD) study programme [17]. Liraglutide has also cardioprotective benefits in patients with T2D at increased risk of cardiovascular disease [8]. Liraglutide was approved in the EU in 2009, and data from real-world observational studies have further demonstrated that the benefits of liraglutide on glycated haemoglobin (HbA1c) and body weight loss were consistent with those obtained in the randomised LEAD trials [9]. Long-term studies indicated that the benefits were sustained for up to 3 years [10, 11].

Liraglutide has been demonstrated to have benefits across a diverse spectrum of patients with T2D, but the extent of HbA1c improvement differs within patient groups having different demographics and clinical characteristics [12]. Thus, there is an unmet need to identify subgroups of patients with T2D receiving liraglutide who are most likely to have the greatest response to treatment. This information would help healthcare providers individualise treatment options and assess cost benefits. Patients and healthcare professionals could benefit from a more detailed understanding of factors associated with improved response to liraglutide.

The ReaL study (ClinicalTrials.gov identifier: NCT02255266) was the largest observational study of liraglutide in Italian clinical practice, showing that 43.5% of patients achieved HbA1c reduction ≥ 1% (10.9 mmol/mol) after 12 months of treatment (primary endpoint). This manuscript reports findings from a secondary analysis performed to identify subgroups or classes of patients with T2D who were more likely to have an improved response to liraglutide owing to specific combinations of clinical and socio-demographic characteristics.

Materials and methods

ReaL was an observational, retrospective, longitudinal, multicentre study involving 45 Italian diabetes clinics throughout the country. The design and methods of this real-world study have been previously reported [13]. Briefly, all consecutive patients aged ≥ 18 years diagnosed with T2D and receiving their first prescription of liraglutide in 2011 were eligible for the study. This study was conducted in accordance with the Declaration of Helsinki (last amended by 59th WMA General Assembly, Seoul, October 2013) and the Guidelines for Good Pharmacoepidemiology Practices (ICH-GPP Revision 2, April, 2007). A written informed consent, approved by an independent ethics committee, was signed by all patients before data collection. Data on a range of key clinical variables were obtained from electronic medical records. Information on fasting plasma glucose (FPG), body weight, body mass index (BMI), diabetes duration, presence of diabetes complications, liraglutide treatment, and treatment with other oral antidiabetic drugs (OADs) was extracted at the date of the first liraglutide prescription at baseline in 2011 and after 12 months. The frequency of patients achieving HbA1c reduction ≥ 1% (10.9 mmol/mol) after 12 months’ treatment (primary endpoint) was calculated. This primary endpoint was selected because it represents a mean effect seen in randomised clinical trials of liraglutide and is a strong indicator of effectiveness that is meaningful to both patients and clinicians. It is also in line with the trend in clinical care to individualise specific HbA1c targets. Information on side effects and adverse events was not explored, since it was not available in the electronic medical records in a standardised format.

Statistical analysis

Results are expressed as mean and standard deviation (SD) for continuous variables, and proportion and percentages for categorical measures, respectively. Between-group patient characteristics were compared with a Mann–Whitney U test or Student’s t test (as appropriate) for continuous variables, or a Chi-square test for categorical variables. Univariate logistic regression was used to identify baseline characteristics of patients who achieved the primary endpoint (HbA1c reduction ≥ 1.0% [10.9 mmol/mol] at 12 months), compared with those who did not.

Multivariate logistic regression analysis was performed to identify independent factors associated with the endpoint after adjustment for other variables. Covariates included in the multivariate analysis were age, sex, diabetes duration, baseline HbA1c, FPG, BMI, presence of diabetes complications, treatment at the first prescription of liraglutide (baseline), treatment modality, liraglutide dose, hypertension, dyslipidaemia, and estimated glomerular filtration rate (eGFR) levels. Standardised criteria which were used for diagnosis of hypertension were not established a priori for this study. Data were collected from electronic medical records, but in the Italian national guidelines, hypertension and dyslipidaemia cut-offs are blood pressure (BP) values ≥ 140/90 mmHg and low-density lipoprotein (LDL)-cholesterol ≥ 100 mg/dl, respectively. Covariates used in the multivariate analysis were chosen based on clinical judgment and did not depend on reaching statistical significance in the univariate analysis. Results are shown as odds ratios (ORs) and 95% confidence intervals (CI).

RECursive Partitioning and AMalgamation (RECPAM) analysis, a tree-based statistical method that integrates standard regression and tree-growing techniques, was used to detect potential interactions among the different variables in predicting reduction of at least 1% in HbA1c and identify homogeneous and distinct subgroups of patients with increased likelihood of reaching the endpoint [14]. In diabetes, RECPAM analysis has been previously used to identify: patients with T2D at risk of microalbuminuria [15], factors associated with impaired quality of life in patients using continuous subcutaneous insulin infusion [16], and patients at higher risk of cardiovascular disease [17]. The RECPAM analysis was performed using SAS® (Release 9.4 Cary, NC, USA) and a macro-routine written by F. Pellegrini and updated by M. Scardapane and G. Lucisano. At each partitioning step, the RECPAM method automatically chose the covariate and best binary split to maximise the difference in risk of experiencing the outcome. The algorithm stopped when user-defined stopping rules were met. In this case, each final class was required to have at least 100 patients in total and 30 patients with the target endpoint.

The set of variables tested in the RECPAM analysis was the same tested in the multivariate logistic regression analysis. Continuous variables were not categorised so as to allow the algorithm to choose the natural cut-off points when identifying distinct subgroups of patients. For each subgroup or class, the proportions (%) of patients reaching the endpoint and the likelihood (ORs and 95% CI) to reach the endpoint versus the reference subgroup were obtained. Finally, to detect additional global correlates (i.e. variables playing a role for all patients, irrespective of the interactions detected by RECPAM), a logistic regression model with RECPAM-identified subgroups and all the covariates ruled out by the algorithm was performed. No imputation was used for missing data, and sensitivity analyses were not performed.

Results

A total of 1723 patients were included in the analysis. Baseline characteristics, including diabetes complications and prior treatment regimens, are shown in Table 1. At baseline, most patients were being treated with metformin, either as monotherapy (n = 803, 46.6%) or with sulphonylureas (n = 457, 26.5%). Few patients (n = 100, 5.8%) received insulin. Most patients received liraglutide as an add-on to previous therapies (63.2%), with 33.4% replacing another prior drug with liraglutide, and 3.4% reducing the number of prior therapies. Mean BMI at baseline was 35.6 ± 5.9 kg/m2, with 83.3% of patients considered to have obesity (BMI > 30 kg/m2).

Table 1.

Baseline characteristics of 1723 patients with type 2 diabetes prior to starting liraglutide treatment

Variable Category Value
Age (years) 58.9 ± 9.5
Sex (%) Female 45.1
Diabetes duration (years) 9.6 ± 7.1
HbA1c (% points) 8.3 ± 1.4
(67 ± 15.3 mmol/mol)
Fasting plasma glucose (mg/dL) 171.8 ± 52.2
BMI (kg/m2) 35.6 ± 5.9
Presence of diabetes complications (%)
 Coronary heart disease No 86.9
Yes 13.1
 Stroke No 98.1
Yes 1.9
 Peripheral vascular disease No 93.3
Yes 6.7
 Diabetic retinopathy No 81.5
Yes 18.5
 Sensory-motor neuropathy No 86.5
Yes 13.5
Baseline treatment (%) Metformin 46.6
Other monotherapy 7.6
Metformin + SU 26.5
Other dual 8.6
≥3 OADs 3.7
Insulin ± OADs 7
Liraglutide treatment modality (%) Switch 33.4
Add-on 63.2
Reduce 3.4
Systolic blood pressure (mmHg) 139.3 ± 18.1
Diastolic blood pressure (mmHg) 81.3 ± 10.0
Hypertension (≥ 140/90 mmHg) (%) No 39.8
Yes 60.2
Total cholesterol (mg/dL) 180.8 ± 39.8
HDL-cholesterol (mg/dL) 45.0 ± 10.9
LDL-cholesterol (mg/dL) 102.9 ± 35.3
Dyslipidaemia (%) No 34.4
Yes 65.6
eGFR (%) ≤ 30 mL/min/1.73 m2 0.1
> 30– < 60 mL/min/1.73 m2 11.4
≥ 60– < 90 mL/min/1.73 m2 43.1
≥ 90 mL/min/1.73 m2 45.4
Open in a new tab

Values are mean ± SD or %

Add-on, liraglutide added to prior therapy; BMI, body mass Index; eGFR, estimated glomerular filtration rate (using the Chronic Kidney Disease-Epidemiology Collaboration formula); HbA1c, glycated haemoglobin; HDL, high-density lipoprotein; LDL, low-density lipoprotein; reduce, number of prior OADs was reduced with addition of liraglutide; OAD, oral antidiabetic drug; SU, sulphonylurea; switch, switch to liraglutide from prior therapy

By 12 months (primary endpoint analysis), a total of 194/1723 (11.2%) patients had discontinued liraglutide treatment. For those with a known reason (n = 166), most (n = 75/166) were owing to lack of effectiveness. An additional 35 discontinued due to liraglutide intolerance, 28 owing to gastrointestinal side effects, and 20 discontinued for other reasons. A total of 19 patients were non-adherent to therapy. At 12 months, there were 1325 (76.9%) patients with HbA1c values available at both baseline and 12 months, and 577/1325 (43.5%) reached the primary endpoint (HbA1c reduction ≥ 1.0% [10.9 mmol/mol]).

Patients who reached the endpoint had a shorter mean diabetes duration (9.1 ± 6.9 vs. 10.0 ± 7.0 years, p = 0.04), higher mean HbA1c at baseline (9.0 ± 1.4 [75 ± 15.3 mmol/mol] vs. 7.7 ± 1.0% [61 ± 10.9 mmol/mol], p < 0.0001), higher mean diastolic BP (82.6 ± 10.0 vs. 80.3 ± 9.8 mmHg, p = 0.0002) and higher mean total cholesterol levels (183.1 ± 41.8 vs. 177.2 ± 37.4 mg/dL, p = 0.02) compared to those who failed to reach the primary endpoint. Mean BMI was nearly identical in the two groups (35.6 ± 5.8 vs. 35.5 ± 5.8 kg/m2, p = 0.72), and there were no significant differences in mean high-density lipoprotein (HDL)-cholesterol (p = 0.11) or mean LDL-cholesterol (p = 0.16). There were no significant differences between the two groups in the proportion of patients using antihypertensive or lipid-lowering medications or other diabetes treatments at baseline.

Logistic regression analysis

The odds of achieving the primary endpoint, by patient characteristic, are shown in Table 2. In the univariate analysis, higher HbA1c at baseline was associated with significantly higher odds (OR 2.78; 95% CI [2.43; 3.18]; p < 0.0001). Shorter diabetes duration was associated with a significantly lower odds of reaching the endpoint (OR 0.98; 95% CI [0.97; 1.00]; p = 0.04). Higher diastolic BP (OR 1.02; 95% CI [1.01; 1.04]; p = 0.0002) and higher total cholesterol (OR 1.00; 95% CI [1.00; 1.01]; p = 0.0203) were also associated with significantly increased odds of reaching the endpoint. Other patient characteristics, such as age, sex, BMI, presence of various diabetes complications, dyslipidaemia or eGFR levels, were not significantly associated with odds of reaching the endpoint.

Table 2.

Univariate and multivariate analysis of factors predicting reduction of HbA1c ≥ 1.0% (10.9 mmol/mol) among 1325 patientsa after 12 months of treatment with liraglutide

Variable Category Univariate logistic regression Multivariate logistic regression
Odds ratio (95% CI) p-value Odds ratio (95% CI)b p-value
Age N/A 1.00 (0.99; 1.01) 0.9689 1.02 (1.00; 1.04) 0.02
Diabetes duration (years, continuous) N/A 0.98 (0.97; 1.00) 0.04 0.97 (0.94; 0.99) 0.007
HbA1c (continuous) N/A 2.78 (2.43; 3.18) < 0.0001 3.52 (2.90; 4.27) < 0.0001
BMI kg/m2 (continuous) N/A 1.00 (0.98; 1.02) 0.7207 1.01 (0.98; 1.03) 0.61
Baseline treatment Metformin 1.00c 1.00c N/A
Other monotherapy 1.17 (0.76; 1.80) 0.4651 0.91 (0.52; 1.59) 0.75
Metformin + SU 1.01 (0.77; 1.32) 0.9528 0.50 (0.34; 0.72) 0.0002
Other dual 1.01 (0.67; 1.52) 0.9615 0.59 (0.34; 1.02) 0.06
≥ 3 OADs 1.12 (0.62; 2.02) 0.7025 0.41 (0.19; 0.88) 0.02
Insulin ± OADs 1.00 (0.63; 1.58) 0.9963 0.44 (0.23; 0.85) 0.02
Liraglutide dose 1.8 1.00c 1.00c N/A
1.2 1.43 (1.12; 1.82) 0.0037 1.91 (1.40; 2.61) < 0.0001
Liraglutide treatment modality Switch 1.00c 1.00c N/A
Add-on 1.74 (1.38; 2.20) < 0.0001 1.86 (1.38; 2.51) < 0.0001
Reduce 0.56 (0.26; 1.21) 0.1418 0.62 (0.24; 1.59) 0.32
Sex Female 1.00c
Male 1.09 (0.88; 1.35) 0.4459
Fasting plasma glucose (mg/dL, continuous) N/A 1.01 (1.01; 1.02) < 0.0001
Diabetic retinopathy No 1.00c
Yes 1.17 (0.87; 1.57) 0.2896
Sensory-motor neuropathy No 1.00c
Yes 1.10 (0.79; 1.52) 0.5731
Coronary heart disease No 1.00c
Yes 0.85 (0.62; 1.18) 0.3408
Stroke No 1.00c
Yes 0.82 (0.38; 1.76) 0.6052
Peripheral vascular disease No 1.00c
Yes 0.85 (0.55; 1.32) 0.4702
Blood pressure (mm Hg) ≤ 130/80 1.00c
131–139/81–89 1.25 (0.77; 2.03) 0.3652
≥ 140/90 1.11 (0.86; 1.44) 0.4247
Systolic BP (mm Hg, continuous) N/A 1.00 (1.00; 1.01) 0.5617
Diastolic BP (mm Hg, continuous) N/A 1.02 (1.01; 1.04) 0.0002
Hypertension No 1.00c
Yes 0.91 (0.69; 1.19) 0.4815
Total cholesterol (mg/dL, continuous) N/A 1.00 (1.00; 1.01) 0.0203
HDL-cholesterol (mg/dL, continuous) N/A 1.0 (1.0; 1.0) 0.1091
LDL-cholesterol (mg/dL, continuous) N/A 1.0 (1.0; 1.0) 0.1566
Dyslipidaemia No 1.00c
Yes 0.98 (0.77; 1.24) 0.8573
eGFR > 90 1.00c
61–90 0.97 (0.73; 1.29) 0.8471
31–60 0.63 (0.39; 1.02) 0.0603
0–30 nc nc
Open in a new tab

Add-on, liraglutide added to prior therapy; BMI, body mass index; BP, blood pressure; CI, confidence interval; eGFR, estimated glomerular filtration rate; HbA1c, glycated haemoglobin; LDL, low-density lipoprotein; N/A, not applicable; nc, not calculated; OAD, oral antidiabetic drug; reduce, number of prior OADs was reduced with addition of liraglutide; SU, sulphonylurea; switch, switch to liraglutide from prior therapy

aPatients who had HbA1c data recorded at 12 months

bAdjusted for age, sex, duration of diabetes, baseline HbA1c, FPG, BMI, presence of diabetes complications, hypertension, dyslipidaemia, eGFR levels, treatment scheme at the first prescription of liraglutide, treatment modality, and liraglutide dosage

cReference category

Prior treatment (including insulin) was not significantly associated with reaching the primary endpoint (p > 0.05). However, after adjusting for potential confounding in the multivariate analysis, all prior treatment regimens (except for other dual therapy, p = 0.06) were associated with a significantly lower odds of achieving the endpoint compared with metformin monotherapy (Table 2). Regarding treatment modality, patients who had liraglutide added to their prior therapy had a significantly higher odds of achieving the primary endpoint (OR 1.74 95% CI [1.38; 2.20]; p < 0.0001) compared with patients who switched to liraglutide from their previous therapy. Those results were confirmed in the multivariate analysis.

The proportion of patients using liraglutide at higher doses increased with successive follow-up, with over a third (36.1%) using 1.8 mg at 12 months compared to 5.3% at baseline. Patients using liraglutide 1.2 mg had an increased odds (OR 1.43; 95% CI [1.12; 1.82]; p = 0.0037) of reaching the endpoint compared to those using the highest dose (1.8 mg).

RECPAM analysis

The RECPAM analysis identified five distinct patient subgroups or classes with increasing odds of achieving an HbA1c reduction ≥ 1.0% (10.9 mmol/mol) after 12 months (Fig. 1, Table 3). The proportion of patients reaching the endpoint ranged from 16.3% (reference group) to 83.1%. The splitting variables indicated that baseline HbA1c and, to some extent, diabetes duration were the primary drivers of degree of response to liraglutide, whereas other patient-related factors were not identified as important in discriminating responder subgroups. With patients having baseline HbA1c ≤ 7.5% (58 mmol/mol) considered the reference class (OR = 1.00), the odds of patients in the other classes achieving the endpoint were: Class 4: OR 2.6; 95% CI [1.7; 4.1], patients with HbA1c between 7.5% (58 mmol/mol) and 8.2% (66 mmol/mol), diabetes duration > 5 years; Class 3: OR 6.3; 95% CI [3.8; 10.2], HbA1c between 7.5% (58 mmol/mol) and 8.2% (66 mmol/mol), diabetes duration < 5 years; Class 2: OR 8.5; 95% CI [5.5; 13.1], HbA1c between 8.2% (66 mmol/mol) and 9.1% (76 mmol/mol); and Class 1: OR 28.7; 95% CI [17.8; 46.2], HbA1c > 9.1%.

Fig. 1.

Fig. 1

Open in a new tab

Subgroups of patients with type 2 diabetes with different odds of achieving a HbA1c reduction ≥ 1.0% (10.9 mmo/mol) after 12 months of treatment with liraglutide, identified using RECPAM analysis. The tree-growing algorithm modelled the odds for achieving HbA1c reduction ≥ 1.0%-point using multivariate logistic regression. Splitting variables were automatically selected by the RECPAM routine among the covariates used in the multivariate analysis and are shown between branches. Cut-offs sending patients to the left or right sibling were also automatically chosen by the RECPAM routine and are reported on the relative branches.  %, proportion of patients in subgroup achieving a reduction in HbA1c ≥ 1.0% (10.9 mmol/mol); circles indicate subgroups of patients and squares indicate final RECPAM classes. Numbers inside circles and squares indicate number of patients achieving HbA1c reduction ≥ 1.0% (10.9 mmol/mol). HbA1c, glycated haemoglobin; OR, unadjusted odds ratio (95% confidence interval); RECPAM, RECursive Partitioning and AMalgamation

Table 3.

Clinical characteristics, at baseline and after 12 months of treatment with liraglutide, by RECPAM class

RECPAM classification
Class 1
n = 219		 Class 2
n = 194		 Class 3
n = 106		 Class 4
n = 197		 Class 5
n = 306		 p-value
Splitting variables HbA1c > 9.1%
[76 mmol/mol]		 8.2% < HbA1c ≥ 9.1%
[66 < HbA1c ≥ 76 mmol/mol]		 7.5% < HbA1c ≥ 8.2%
[58 < HbA1c ≥ 66 mmol/mol]
Diabetes duration
≤ 5 years		 7.5% < HbA1c ≥ 8.2%
[58 < HbA1c ≥ 66 mmol/mol]
Diabetes duration
> 5 years		 HbA1c ≤ 7.5%
[58 mmol/mol]
Unadjusted odds of HbA1c being reduced by ≥ 1.0% 28.7
(17.8; 46.2)		 8.5
(5.5; 13.1)		 6.3
(3.8; 10.2)		 2.6
(1.7; 4.1)		 1.00a
Patient characteristic
Baseline HbA1c (%) 10.2 ± 1.0
[88 ± 10.9 mmol/mol]		 8.7 ± 0.3
[72 ± 3.3 mmol/mol]		 7.9 ± 0.2
[63 ± 2.2 mmol/mol]		 7.9 ± 0.2
[63 ± 2.2 mmol/mol]		 7.0 ± 0.5
[53 ± 5.5 mmol/mol]		 < 0.0001
Change in HbA1c (%) − 2.2 ± 1.5
[88 ± 16.4 mmol/mol]		 − 1.0 ± 1.1
[88 ± 12.0 mmol/mol]		 − 0.9 ± 1.0
[88 ± 10.9 mmol/mol]		 − 0.5 ± 0.9
[88 ± 9.8 mmol/mol]		 − 0.1 ± 0.8
[88 ± 8.7 mmol/mol]		 < 0.0001
Baseline FPG (mg/dl) 223.0 ± 56.7 181.5 ± 41.1 157.3 ± 28.9 159.7 ± 33.2 137.5 ± 28.5 < 0.0001
Change in FPG (mg/dl) − 59.1 ± 63.7 − 28.9 ± 49.9 − 20.6 ± 40.3 − 14.4 ± 35.5 − 7.1 ± 33.0 0.0002
Baseline BMI (Kg/m2) 35.6 ± 5.6 35.3 ± 5.6 37.2 ± 6.3 34.1 ± 5.6 35.7 ± 6.2 < 0.0001
Change in BMI (Kg/m2) − 0.9 ± 2.2 − 1.6 ± 2.0 − 1.3 ± 1.9 − 1.1 ± 1.7 − 1.3 ± 2.1 0.02
Baseline weight (Kg) 101.5 ± 18.5 98.3 ± 17.7 103.9 ± 19.1 93.9 ± 17.4 100.2 ± 19.2 < 0.0001
Change in weight (Kg) − 2.5 ± 6.1 − 4.3 ± 5.3 − 3.7 ± 5.2 − 3.1 ± 4.7 − 3.7 ± 5.8 0.03
Age (years) 57.7 ± 9.4 60.7 ± 8.0 56.0 ± 9.1 61.2 ± 9.3 59.2 ± 8.9 < 0.0001
Sex (% male) 57.5 55.2 48.1 52.3 56.9 0.46
Duration diabetes (years) 10.2 ± 6.9 11.2 ± 7.3 2.9 ± 1.5 12.1 ± 6.3 9.1 ± 6.8 < 0.0001
Baseline treatment (%) < 0.0001
Metformin only 34.7 34 71.7 38.6 60.8
Other monotherapy 7.3 7.7 8.5 8.6 7.2
Metformin + SU 35.6 35.6 13.2 31.5 14.4
Other dual therapies 7.3 11.3 3.8 7.6 10.1
≥ 3 OADs 5.5 4.1 1.9 5.6 2.6
Insulin ± OADs 9.6 7.2 0.9 8.1 4.9
Treatment modality (%) 0.34
Switch 31.5 37.6 34.0 36.5 38.2
Add-on 67.1 59.8 65.1 61.4 57.8
Reduction 1.4 2.6 0.9 2.0 3.9
Liraglutide dosage (%) 0.0007
0.6 4.1 4.6 5.7 5.1 7.8
1.2 55.3 50.5 65.1 58.9 66.7
1.8 40.6 44.8 29.2 36.0 25.5
Baseline SBP (mmHg) 142.0 ± 18.4 140.3 ± 16.6 138.0 ± 17.9 140.3 ± 18.7 137.4 ± 16.8 0.09
Change in SBP (mmHg) − 4.2 ± 18.5 − 2.6 ± 16.7 − 4.4 ± 16.0 − 6.3 ± 19.2 − 5.4 ± 17.6 0.57
Baseline DBP (mmHg) 83.5 ± 10.6 81.2 ± 9.4 81.7 ± 10.1 81.0 ± 9.6 80.0 ± 10.0 0.02
Change in DBP (mmHg) − 1.8 ± 11.2 − 0.6 ± 9.6 − 1.0 ± 10.6 − 2.4 ± 11.0 − 1.7 ± 11.1 0.60
Baseline total cholesterol (mg/dl) 187.9 ± 43.6 181.5 ± 36.3 185.2 ± 38.1 175.2 ± 34.9 174.8 ± 38.0 0.007
Change in total cholesterol (mg/dl) − 16.2 ± 40.1 − 9.8 ± 32.3 − 19.9 ± 39.6 − 7.2 ± 34.7 − 7.1 ± 31.0 0.06
Baseline HDL-cholesterol (mg/dl) 42.9 ± 9.5 45.2 ± 11.5 43.5 ± 10.9 46.5 ± 12.0 44.7 ± 10.4 0.07
Change in HDL-cholesterol (mg/dl) 0.6 ± 7.1 1.6 ± 8.3 1.6 ± 7.5 1.8 ± 8.2 0.9 ± 7.9 0.42
Baseline LDL-cholesterol (mg/dl) 104.2 ± 38.8 104.4 ± 30.7 108.5 ± 36.2 96.9 ± 32.1 101.1 ± 32.8 0.13
Change in LDL-cholesterol (mg/dl) − 9.4 ± 35.7 − 10.8 ± 30.9 − 20.4 ± 36.2 − 7.3 ± 31.8 − 8.7 ± 30.6 0.15
Baseline triglycerides (mg/dl) 211.6 ± 120.0 169.6 ± 80.1 182.9 ± 81.8 163.7 ± 77.9 150.8 ± 75.6 <0.0001
Change in triglycerides − 35.4 ± 110.2 − 7.3 ± 85.8 − 16.6 ± 82.2 − 11.4 ± 64.6 − 0.4 ± 60.8 0.002
Baseline albuminuria (mg/l) 73.7 ± 150.3 39.0 ± 92.0 37.2 ± 55.7 40.6 ± 64.9 38.0 ± 84.1 0.07
Change in albuminuria (mg/l) − 20.0 ± 119.2 0.6 ± 58.6 − 1.2 ± 43.3 − 15.2 ± 75.6 − 13.2 ± 89.7 0.91
Baseline eGFR (%) 0.16
0–60 5.5 8.2 2.8 7.6 8.2
61–90 62.1 57.2 68.9 64.5 55.2
> 90 32.4 34.5 28.3 27.9 36.6
Open in a new tab

Values are mean ± SD unless otherwise stated

BMI, body mass index; DBP, diastolic blood pressure; FPG, fasting plasma glucose; HbA1c, glycated haemoglobin; HDL, high-density lipoprotein; LDL, low-density lipoprotein; n, number of subjects in class; OAD, oral antidiabetic drug; RECPAM, RECursive Partitioning and AMalgamation; SBP, systolic blood pressure; SU, sulphonylurea

aReference category for odds ratio

Although all RECPAM classes showed HbA1c reduction, the patient subgroup with the greatest odds of achieving an HbA1c reduction ≥ 1.0% (10.9 mmol/mol) can be described as having the following: mean HbA1c of 10.2% (88 mmol/mol), mean FPG of 223.0 mg/dL, mean diabetes duration of 10.2 years at baseline, metformin treatment ± sulphonylureas at initiation of liraglutide treatment, and liraglutide as an adjunct to prior therapy (versus discontinuation of prior treatment) (Table 3). Each RECPAM class showed a reduction in mean weight, ranging from 2.5 to 4.3 kg, after 12 months’ treatment with liraglutide. There was no obvious relationship between mean HbA1c reduction and mean weight loss. A final logistic model adjusted with other covariates deemed clinically important and with RECPAM classes forced into the model is shown in Table 4. The final logistic model with both the RECPAM classes and the covariates not entering the tree forced in the model (Table 4) showed that additional global variables associated with the likelihood of reaching the endpoint were baseline treatment scheme, liraglutide dosage and treatment modality.

Table 4.

Final logistic modela showing key factors predicting reduction of HbA1c ≥ 1.0% [10.9 mmol/mol] among 1325 patients after 12 months of treatment with liraglutide, with RECPAM classes forced in the model

Factor OR (95% CI) p-value
RECPAM classes
 Class 1 33.69
(18.10–62.74)		 < 0.0001
 Class 2 10.33
(6.23–17.12)		 < 0.0001
 Class 3 5.72
(3.35–9.76)		 < 0.0001
 Class 2 2.89
(1.80–4.65)		 < 0.0001
 Class 5 1.00b
Baseline treatment
 Other monotherapies 0.93
(0.51–1.69)		 0.81
 Metformin + sulphonylurea 0.47
(0.31–0.70)		 0.0002
 Other dual therapies (metformin + TZD, metformin + glinides, SU + TZD) 0.73
(0.40–1.31)		 0.29
 ≥ 3 OADs 0.39
(0.17–0.88)		 0.02
 Insulin ± OADs 0.47
(0.24–0.94)		 0.03
 Metformin only 1.00b
Liraglutide dosage (mg)
 0.6 1.02
(0.49–2.12)		 0.95
 1.2 2.05
(1.45–2.90)		 < 0.0001
 1.8 1.00b
Liraglutide treatment modality
 Add-on to existing treatment 1.79
(1.29–2.50)		 0.0005
 Reduction of no. of drug classes 0.52
(0.17–1.63)		 0.26
 Switch from another drug class 1.00b
Open in a new tab

BMI, body mass index; CI, confidence interval; eGFR, estimated glomerular filtration rate; FPG, fasting plasma glucose; HbA1c, glycated haemoglobin; OAD, oral antidiabetic drug; OR, odds ratio; SU, sulphonylurea; TZD, thiazolidinedione

aModel was adjusted for age, sex, FPG, BMI, presence of diabetes complications, hypertension, dyslipidaemia, and eGFR levels

bReference category

Discussion

This is the first RECPAM analysis to identify distinct groups of patients with T2D who were prescribed liraglutide in routine clinical practice according to their predicted degree of response to liraglutide treatment. These data can improve clinical practice by providing a deeper knowledge of factors influencing liraglutide’s impact on metabolic control. The key message of this analysis is that only baseline HbA1c and to a lesser extent diabetes duration were predictive of liraglutide effectiveness. Furthermore, these results for the first time clarify that HbA1c reduction can exceed 2.0% when baseline levels are > 9.0%. This finding has important clinical and health policy implications for the Italian Drugs Agency (AIFA) regulations, considering that patients with HbA1c ≥ 8.5% are currently excluded from the GLP-1 receptor agonists’ reimbursement policy, which requires HbA1c between 7.5 (58 mmol/mol) and 8.5% (69 mmol/mol) (AIFA regulations).

Different patterns have been reported in clinical trials with regard to dose response with liraglutide. In this study, patients using the 1.2-mg liraglutide dose as maintenance dose were more likely to reach the primary endpoint than those using the higher maintenance dose (1.8 mg). This is likely due to an indication bias because patients struggling to achieve good glycaemic control were up-titrated to the higher dose, but owing to their disease severity, they still did not respond as well as healthier patients who did not require an increased dose. Escalation from the starting liraglutide dose of 0.6–1.2 mg likely occurred earlier after initiation, whereas when escalation to 1.8 mg occurred, it tended to be later in the study.

In line with existing findings [1820], we found that the higher the baseline HbA1c level, the higher the reduction achieved. Multivariate analysis showed that the likelihood of reaching the endpoint increased by 3.5 times for every 1% HbA1c increase at baseline. In addition, by applying the RECPAM analysis, the study showed that the likelihood of reaching the endpoint was 28 times higher with baseline HbA1c > 9.1% as compared to baseline levels < 7.5%. In the EVIDENCE study [21], conducted in France by general practitioners and specialists, on 2029 patients, there was a mean (± SD) HbA1c reduction from baseline of 1.01 ± 1.54% (from 8.46 ± 1.46 to 7.44% ± 1.20; p < 0.0001); after 2 years, 29.9% (95% CI 27.7; 31.2) of patients still had HbA1c ≤ 7.0%; in the cohort treated within specialist care settings (N = 1398), HbA1c reduction was − 0.8%.

In the current study, although there were differences in the degree of liraglutide response, each RECPAM class showed decreases in HbA1c from baseline after 12 months of treatment. As might be expected, a greater proportion of patients with the poorest glycaemic control at baseline achieved the primary endpoint of HbA1c reduction ≥ 1.0% (10.9 mmol/mol) after 12 months, since it would be incrementally more difficult to achieve that degree of absolute HbA1c reduction in patients already at or near glycaemic targets. Nevertheless, these results suggest that there is a distinct subgroup of patients for whom liraglutide treatment can help achieve HbA1c reductions in excess of 2.0% (21.9 mmol/mol), a finding that may have important clinical implications.

The RECPAM algorithm selected only baseline HbA1c and diabetes duration as important splitting variables when creating the responder subgroups or classes. This indicated that other patient variables were less important in determining the degree of response to liraglutide. Although BMI was not selected by the algorithm, this too may be because of the high prevalence of obesity in the sample.

Multivariate logistic regression with RECPAM categories forced into the model further confirmed that liraglutide is best used as an add-on to, rather than replacement for, prior treatment regimens (generally OADs) in T2D (OR 1.79; 95% CI [1.29; 2.50]). This finding is in line with current treatment guidelines [22]. Interestingly, the largest patient subgroup (n = 306, RECPAM Class 5) (Table 3) had comparatively good HbA1c control (≤ 7.5% [58 mmol/mol]), suggesting that there is also a patient subgroup who may initiate liraglutide to pair the glycaemic control to weight loss.

Regarding the role of diabetes duration, a previous study on liraglutide reported a higher efficacy in patients with short diabetes duration [12], while the ReaL study [13] found improvements in metabolic control also in patients with long diabetes duration. RECPAM analysis clarifies that diabetes duration can play a role mainly for patients with HbA1c levels between 7.5 and 8.2%; in particular, one in two patients with diabetes duration ≤ 5 years reached the endpoint, compared to one in three for a diabetes duration > 5 years. The role of BMI and previous therapy as independent predictors emerging in other studies [19, 23] was not confirmed in our study.

A strength of this study was the large sample size. Use of real-world data also makes the findings more generalisable to patient populations seen in regular clinical practice. The observational nature of the study may introduce bias in the selection of patients who were prescribed liraglutide; however, consecutive enrolment of all patients was adopted to minimise this. Since these results reflect the clinical usage of liraglutide in Italy, they may not be generalisable to countries with different usage patterns. As a retrospective study based on electronic medical records, the completeness of information depended on the ability of participating centres to record clinical data. It should be noted that data completeness was judged satisfactory (i.e. 97.2–56.3% complete for the adjustment variables used). Insulin secretion capacity was not evaluated as a potential predictor of HbA1c reduction with liraglutide, although several studies have suggested the usefulness of this parameter in predicting the effectiveness of liraglutide [24, 25]. This would be useful to explore in future studies. We cannot exclude the involvement of other factors, besides HbA1c and partly diabetes duration, in determining HbA1c reduction through liraglutide, but we analysed all factors easily available to diabetologists to guide routine clinical practice.

In conclusion, in this study, glycaemic response to liraglutide was largely driven by baseline HbA1c levels and to a lesser extent by diabetes duration. The clinical benefit seems to be maximised when used as an add-on to prior therapies. All RECPAM classes showed weight loss, which appeared independent of mean HbA1c reduction. RECPAM analyses suggest an urgent need to revise the AIFA criteria for reimbursement due to the finding that HbA1c reduction can exceed 2.0% in people with HbA1c > 9.0%.

Acknowledgements

It is with regret that we announce the death of co-author Dr M. Boemi, to whom this article is dedicated. He participated actively in the drafting and approved the final version of this manuscript. The authors thank Antonio Nicolucci, Michele Sacco and Marco Scardapane (CORESEARCH – Center for Outcomes Research and Clinical Epidemiology, Pescara, Italy) for data management, data analysis, and assistance with manuscript preparation. We thank Cristiano Bette, Margit Kaltoft and Elena Startseva (Novo Nordisk), for their review and input to the manuscript. Medical writing assistance and editorial/submission support were provided by Gary Patronek and Izabel James, of Watermeadow Medical, an Ashfield Company, part of UDG Healthcare plc, funded by Novo Nordisk A/S. This study was funded by Novo Nordisk A/S. The datasets generated during and/or analysed during the current study are available from the corresponding author on reasonable request.

*ReaL Study Group

Expert board and writing committee: Natalino Simioni1, Cesare Berra2, Massimo Boemi3, Antonio Carlo Bossi4, Riccardo Candido5, Graziano Di Cianni6, Simona Frontoni7, Stefano Genovese8, Paola Ponzani9, Vincenzo Provenzano10, Giuseppina Russo11, Luigi Sciangula12, Annunziata Lapolla13, Cristiano Bette14, Maria Chiara Rossi15 on behalf of the ReaL (NN2211-4118) Study Group*

1Presidio Ospedaliero di Cittadella, Cittadella, Padua, Italy, 2Humanitas Research Hospital, Rozzano (MI), Italy, 3IRCCS INRCA, Ancona, Italy, 4Ospedale Treviglio Caravaggio, Treviglio, Italy, 5Ass 1 Triestina, Trieste, Italy, 6Ospedale di Livorno, Livorno, Italy, 7University of Rome Tor Vergata, Rome, Italy, 8Centro Cardiologico Monzino, Milan, Milan, Italy, 9Ospedale La Colletta, ASL3 Genovese, Arenzano, Italy, 10Centro Regionale di Riferimento Diabetologia ed Impianto Microinfusori Sicilia, Partinico, Palermo, Italy, 11University of Messina, Messina, Italy, 12IRCCS Multimedica - Ospedale di Castellanza, Varese, Italy, 13University of Padua, Padua, Italy 14Novo Nordisk Spa, Rome, Italy, 15CORESEARCH – Center for Outcomes Research and Clinical Epidemiology, Pescara, Italy.

Investigators: Riccardo Fornengo, Ospedale Civile Chivasso (Torino); Antonio Carlo Bossi, Ospedale Treviglio (Caravaggio), Fabrizio Querci, Ospedale Pesenti Fenaroli (Alzano Lombardo); Paolo Desenzani, Spedali Civili di Brescia (Montichiari); Luigi Sciangula, Diabetologia Presidio Polispecialistico di Mariano Comense ASST Lariana, Como; Stefano Genovese, IRCCS Multimedica (Milano), Piermarco Piatti, IRCCS (Milano); Enrica Chebat, Ospedale Luigi Sacco (Milano); Cesare Celeste Berra, Humanitas Clinical and Research Center, Rozzano (MI); Paolo Erpoli, Ospedale Sant’Antonio Abate (Milano); Bruno Fattor, Ospedale Generale Regionale (Bolzano), Sandro Inchiostro, Ospedale San Lorenzo (Trento); Alberto Marangoni, Presidio Ospedaliero di Bassano Del Grappa (Vicenza); Loris Confortin, Presidio Ospedaliero Di Castelfranco Veneto (Treviso); Anna Coracina, Presidio Ospedaliero Di Montebelluna (Treviso); Carmela Vinci, Presidio Ospedaliero di San Dona’ Di Piave (Venezia); Natalino Simioni, Presidio Ospedaliero di Cittadella (Padova), Annunziata Lapolla, Complesso Ospedaliero Dei Colli (Padova); Riccardo Candido, ASS 1 Triestina (Trieste); Giuseppe Felace, Ospedale S Giovanni Dei Battuti (Udine); Paola Ponzani, Ospedale La Colletta dii Arenzano (Genova); Marcello Monesi, Ospedale Sant’Anna Di Cona (Ferrara); Francesca Pellicano, Ospedale S Maria Delle Croci (Ravenna); Fabio Baccetti, Ospedale Ss Giacomo e Cristoforo (Massa Carrara); Michele Di Carlo, Ospedale Civile Campo Di Marte (Lucca); Graziano Di Cianni, Ospedale Di Livorno (Livorno); Massimo Boemi, IRCCS INRCA (Ancona); Simona Frontoni, University of Rome Tor Vergata (Roma); Sergio Leotta, Ospedale Sandro Pertini (Roma); Davide Lauro, Policlinico Tor Vergata (Roma); Claudio Ventura, Ospedale Israelitico (Roma); Dario Pitocco, Policlinico A. Gemelli (Roma); Franco Tuccinardi, Ospedale Monsignor Diliegro (Latina); Gaetano Leto, Ospedale Regionale S. Maria Goretti (Latina); Pasquale Alfidi, Ospedale SS Filippo Nicola (Avezzano); Ercole D’Ugo, ASL 2 Lanciano Vasto Chieti (Vasto); Stefania Donatelli, ASL 2 Lanciano Vasto Chieti (Chieti); Ercole Memoli, ASL Avellino (Avellino); Damiano Gullo, Ospedale Nuovo Garibaldi (Catania); Giuseppina Russo, Policlinico G Martino (Messina); Manfredi Rizzo, Policlinico Universita P. Giaccone (Palermo); Vincenzo Provenzano, Ospedale Civile Di Partinico (Palermo); Giuseppe Mattina, ASP Palermo (Palermo); Mario Rizzo, Ospedale Buccheri La Ferla (Palermo).

Other responsible parties: Contract research organisation (CRO) responsible for the submissions to Independent Ethics Committees (IECs), study closure procedures, creation and delivery of study files: TFS People S.r.l - Via Lucrezio Caro 63, 00193, Rome, Italy (Simona Foglietta). CRO responsible for data management: Istituto di Ricerche Farmacologiche Mario Negri - Via Giuseppe La Masa 19, 20156, Milan, Italy (Roberto Latini). CRO responsible for statistical analysis and medical writing: CORESEARCH – Center for Outcomes Research and clinical Epidemiology - S.r.l.Via Tiziano Vecellio 2, 65124, Pescara, Italy (Antonio Nicolucci, Maria Chiara Rossi, Michele Sacco, Marco Scardapane).

Compliance with ethical standards

Conflict of interest

Simioni N: Consulting fees from Novo Nordisk, Lilly, Boehringer Ingelheim and Abbott; member of advisory boards for Novo Nordisk, Lilly and Boehringer Ingelheim; investigator in clinical trials sponsored by Novo Nordisk. Berra C: consulting fees from Novo Nordisk, Lilly, Boehringer Ingelheim, Sanofi, Johnson & Johnson and Bayer; research support from AstraZeneca and Takeda; member of advisory boards for Novo Nordisk, Lilly, Boehringer Ingelheim, AstraZeneca and Sanofi; investigator in clinical trials sponsored by Lilly and Sanofi. Boemi M: member of advisory boards for Lilly, Boehringer Ingelheim and Sanofi; investigator in clinical trials sponsored by Novo Nordisk, Boehringer Ingelheim and Merck SD. Bossi AC: investigator in clinical trials sponsored by Novo Nordisk, Artsana, Lilly, Bayer and Sanofi; consulting fees from AstraZeneca, Roche, Johnson & Johnson and Takeda; research support from Merck SD and Sigma-Tau; member of advisory board for Boehringer Ingelheim. Candido R: investigator in clinical trials sponsored by Novo Nordisk, Lilly and Merck SD; consulting fees from AstraZeneca, Roche and Johnson & Johnson; member of advisory board for Boehringer Ingelheim. Di Cianni G: investigator in clinical trials sponsored by Novo Nordisk, AstraZeneca and Sanofi; member of advisory boards for Lilly and Sanofi. Frontoni S: member of advisory boards for Novo Nordisk, Lilly, AstraZeneca, Johnson & Johnson, Takeda and Sigma-Tau; investigator in clinical trials sponsored by Novo Nordisk and Boehringer Ingelheim. Genovese S: consulting fees from Novo Nordisk, Lilly, Boehringer Ingelheim, AstraZeneca, Merck SD, Sanofi, Johnson & Johnson, Takeda, Abbott Diabetes Care, Bristol Myers & Squibb, Janssen, Lifescan, Menarini and Novartis; member of advisory boards for Novo Nordisk, Boehringer Ingelheim, AstraZeneca, Merck SD, Sanofi, Johnson & Johnson, Takeda, Abbott Diabetes Care, Bruno Farmaceutici, Janssen, Lifescan and Novartis; research support from Novartis; investigator in clinical trials sponsored by Novo Nordisk, Lilly, Boehringer Ingelheim, AstraZeneca, Merck SD, Takeda, Janssen, Novartis and Sanofi. Ponzani P: investigator in clinical trials sponsored by Boehringer Ingelheim, Sanofi, Johnson & Johnson, Bayer and Novartis; member of advisory boards for Novo Nordisk and AstraZeneca. Provenzano V: consulting fees from Novo Nordisk, Lilly, Boehringer Ingelheim, AstraZeneca, Merck SD, Sanofi and Takeda; member of advisory boards for Novo Nordisk, Lilly, Boehringer Ingelheim, AstraZeneca and Sanofi; investigator in clinical trials sponsored by Novo Nordisk, Lilly, Boehringer Ingelheim, AstraZeneca, Merck SD, Sanofi and Roche. Russo GT: investigator in clinical trials sponsored by Lilly, Boehringer Ingelheim, Merck SD, Sanofi and Johnson & Johnson; member of advisory boards for Novo Nordisk, Lilly and Boehringer Ingelheim, member of advisory boards for, and consulting fees from, Novo Nordisk, Lilly and Boehringer Ingelheim. Sciangula L: member of advisory boards for Novo Nordisk, Lilly, AstraZeneca and Johnson & Johnson; consulting fees from Roche; investigator in clinical trials sponsored by Novo Nordisk. Lapolla A: investigator in clinical trials sponsored by Novo Nordisk, Lilly, Boehringer Ingelheim and Sanofi. Bette C: employee of Novo Nordisk SpA (Rome, Italy). Rossi MC: research grant from Novo Nordisk, Sanofi, Dexcom, AstraZeneca, Sigma-Tau, Eli Lilly, Artsana and Medtronic.

Ethical approval

This study was conducted in accordance with the Declaration of Helsinki and the Guidelines for Good Pharmacoepidemiology Practices. According to Italian law (Italian Republic. Determination of the Italian Medicines Agency of March 20, 2008. Official Gazette of the Italian Republic. General Series No. 76; March 31, 2008), prior to study initiation, the protocol, patient informed consent form and patient enrolment procedures were reviewed and approved by an Independent Ethics Committee (IEC). The study protocol was submitted to the Coordinating Centre IEC in advance, then after its official approval, the study documentation was submitted to the local IECs of all participating centres.

Informed consent

Informed consent was obtained from all individual participants included in the study.

Footnotes

M. Boemi: Deceased.

Contributor Information

M. C. Rossi, Phone: +39 0859047114, Email: rossi@coresearch.it

ReaL (NN2211-4118) Study Group*:

Natalino Simioni, Cesare Berra, Massimo Boemi, Antonio Carlo Bossi, Riccardo Candido, Graziano Di Cianni, Simona Frontoni, Stefano Genovese, Paola Ponzani, Vincenzo Provenzano, Giuseppina Russo, Luigi Sciangula, Annunziata Lapolla, Cristiano Bette, and Maria Chiara Rossi

References

  • 1.Victoza® summary of product characteristics (2016)
  • 2.Garber A, Henry R, Ratner R, et al. Liraglutide versus glimepiride monotherapy for type 2 diabetes (LEAD-3 Mono): a randomised, 52-week, phase III, double-blind, parallel-treatment trial. Lancet. 2009;373:473–481. doi: 10.1016/S0140-6736(08)61246-5. [DOI] [PubMed] [Google Scholar]
  • 3.Marre M, Shaw J, Brändle M, et al. Liraglutide, a once-daily human GLP-1 analogue, added to a sulphonylurea over 26 weeks produces greater improvements in glycaemic and weight control compared with adding rosiglitazone or placebo in subjects with Type 2 diabetes (LEAD-1 SU) Diabet Med. 2009;26:268–278. doi: 10.1111/j.1464-5491.2009.02666.x. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 4.Nauck M, Frid A, Hermansen K, et al. Efficacy and safety comparison of liraglutide, glimepiride, and placebo, all in combination with metformin, in type 2 diabetes: the LEAD (liraglutide effect and action in diabetes)-2 study. Diabetes Care. 2009;3:84–90. doi: 10.2337/dc08-1355. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 5.Zinman B, Gerich J, Buse JB, et al. Efficacy and safety of the human GLP-1 analog liraglutide in combination with metformin and TZD in patients with type 2 diabetes mellitus (LEAD-4 Met + TZD) Diabetes Care. 2009;32:1224–1230. doi: 10.2337/dc08-2124. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 6.Russell-Jones D, Vaag A, Schmitz O, et al. Liraglutide vs insulin glargine and placebo in combination with metformin and sulfonylurea therapy in type 2 diabetes mellitus (LEAD-5 met + SU): a randomised controlled trial. Diabetologia. 2009;52:2046–2055. doi: 10.1007/s00125-009-1472-y. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 7.Buse J, Rosenstock J, Sesti G, et al. Liraglutide once a day versus exenatide twice a day for type 2 diabetes: a 26-week randomized, parallel-group, multinational, open-label trial (LEAD-6) Lancet. 2009;374:39–47. doi: 10.1016/S0140-6736(09)60659-0. [DOI] [PubMed] [Google Scholar]
  • 8.Marso SP, Daniels GH, Brown-Frandsen K, et al. Liraglutide and cardiovascular outcomes in type 2 diabetes. N Engl J Med. 2016;375:311–322. doi: 10.1056/NEJMoa1603827. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 9.Ostawal A, Mocevic E, Kragh N, Xu W. Clinical effectiveness of liraglutide in type 2 diabetes treatment in the real-world setting: a systematic literature review. Diabetes Ther. 2016;7:411–438. doi: 10.1007/s13300-016-0180-0. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 10.Ponzani P, Scardapane M, Nicolucci A, Rossi MC. Effectiveness and safety of liraglutide after three years of treatment. Minerva Endocrinol. 2016;41:35–42. [PubMed] [Google Scholar]
  • 11.Rondinelli M, Rossi A, Gandolfi A, et al. Use of liraglutide in the real world and impact at 36 months on metabolic control, weight, lipid profile, blood pressure, heart rate, and renal function. Clin Ther. 2017;39:159–169. doi: 10.1016/j.clinthera.2016.11.001. [DOI] [PubMed] [Google Scholar]
  • 12.Ratner R, Brett J, Khutoryansky N, Aroda VR. Identifying predictors of response to liraglutide in type 2 diabetes using recursive partitioning analysis. Diabetologia. 2012;55(Suppl 1):S332. [Google Scholar]
  • 13.Lapolla A, Berra C, Boemi M, et al. Long-term effectiveness of liraglutide for treatment of type 2 diabetes in a real-life setting: a 24-month, multicenter, non-interventional, retrospective study. Adv Ther. 2017 doi: 10.1007/s12325-017-0652-2. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 14.Ciampi A (1992) Constructing prediction trees from data: the RECPAM approach. In: Proceedings from the Prague 1991 summer school on computational aspects of model choice. Physica-Verlag, Heidelberg, pp 105–152
  • 15.Rossi MC, Nicolucci A, Pellegrini F, et al. Identifying patients with type 2 diabetes at high risk of microalbuminuria: results of the DEMAND (Developing Education on Microalbuminuria for Awareness of reNal and cardiovascular risk in Diabetes) Study. Nephrol Dial Transplant. 2008;23:1278–1284. doi: 10.1093/ndt/gfm798. [DOI] [PubMed] [Google Scholar]
  • 16.Franciosi M, Maione A, Pomili B, et al. Correlates of quality of life in adults with type 1 diabetes treated with continuous subcutaneous insulin injection. Nutr Metab Cardiovasc Dis. 2010;20:7–14. doi: 10.1016/j.numecd.2009.02.012. [DOI] [PubMed] [Google Scholar]
  • 17.Marzona I, Avanzini F, Lucisano G, et al. Are all people with diabetes and cardiovascular risk factors or microvascular complications at very high risk? Findings from the risk and prevention study. Acta Diabetol. 2017;54:123–131. doi: 10.1007/s00592-016-0899-0. [DOI] [PubMed] [Google Scholar]
  • 18.DeFronzo RA, Stonehouse AH, Han J, Wintle ME. Relationship of baseline HbA1c and efficacy of current glucose-lowering therapies: a meta-analysis of randomized clinical trials. Diabet Med. 2010;27:309–317. doi: 10.1111/j.1464-5491.2010.02941.x. [DOI] [PubMed] [Google Scholar]
  • 19.Lapolla A, Frison V, Bettio M, et al. Correlation between baseline characteristics and clinical outcomes in a large population of diabetes patients treated with liraglutide in a real-world setting in Italy. Clin Ther. 2015;37:574–584. doi: 10.1016/j.clinthera.2014.11.015. [DOI] [PubMed] [Google Scholar]
  • 20.Toyoda M, Yokoyama H, Abe K, Nakamura S, Suzuki D. Predictors of response to liraglutide in Japanese type 2 diabetes. Diabetes Res Clin Pract. 2014;106:451–457. doi: 10.1016/j.diabres.2014.09.052. [DOI] [PubMed] [Google Scholar]
  • 21.Gautier JF, Martinez L, Penfornis A, et al. Effectiveness and persistence with liraglutide among patients with type 2 diabetes in routine clinical practice–EVIDENCE: a prospective, 2-year follow-up, observational, post-marketing study. Adv Ther. 2015;32:838–853. doi: 10.1007/s12325-015-0245-x. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 22.American Diabetes Association Standards of medical care in diabetes—2017. Diabetes Care. 2017;40:S1–S138. doi: 10.2337/dc17-S001. [DOI] [PubMed] [Google Scholar]
  • 23.Inoue K, Maeda N, Fujishima Y, et al. Long-term impact of liraglutide, a glucagon-like peptide-1 (GLP-1) analogue, on body weight and glycemic control in Japanese type 2 diabetes: an observational study. Diabetol Metab Syndr. 2014;6:95. doi: 10.1186/1758-5996-6-95. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 24.Kozawa J, Inoue K, Iwamoto R, et al. Liraglutide is effective in type 2 diabetic patients with sustained endogenous insulin-secreting capacity. J Diabetes Invest. 2012;3:294–297. doi: 10.1111/j.2040-1124.2011.00168.x. [DOI] [PMC free article] [PubMed] [Google Scholar]
  • 25.Iwao T, Sakai K, Sata M. Postprandial serum C-peptide is a useful parameter in the prediction of successful switching to liraglutide monotherapy from complex insulin therapy in Japanese patients with type 2 diabetes. J Diabetes Complicat. 2013;27:87–91. doi: 10.1016/j.jdiacomp.2012.07.001. [DOI] [PubMed] [Google Scholar]

Articles from Acta Diabetologica are provided here courtesy of Springer

RESOURCES