Introduction
Recent publications of data extracts from population registries have triggered debate about a potential relationship between treatment with insulin glargine (A21Gly,B31Arg,B32Arg human insulin) and an increased incidence of cancer or breast cancer [1‐4]. Here, we fulfil an obligation to report the evidence from randomised clinical trials (RCTs) within the manufacturer’s database.
All RCTs sponsored by sanofi-aventis that compared the use of insulin glargine with another active comparator in either type 1 or type 2 diabetes and had a treatment duration of at least 4 weeks were included in this analysis. These studies included people with either type 1 or type 2 diabetes, and were either part of the initial development plan for the registration of the product (Phase 2 and 3) or conducted after the commercial launch of insulin glargine (Phase 4 studies).
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Methods
As it is obligatory for all sponsored trials routinely to report serious adverse events to the manufacturer, and as the manufacturer has a database of such studies, no literature search was performed. Only RCTs that compared insulin glargine with an active comparator and that had a final clinical study report available for review on 15 May 2009 were included in this analysis.
Studies and ascertainment of malignancy
A thorough review of the sanofi-aventis safety database for the identified studies was performed to assess the incidence of any malignancies that led to reports of serious adverse events during the conduct of the trials. All RCTs of insulin glargine were included. All serious adverse events coded in the Medical Dictionary for Regulatory Activities (MedDRA) System Organ Class of neoplasms—benign, malignant and unspecified—were included in the evaluation [5]. An adverse event is classified as serious if it fulfils the criteria set down by the International Conference on Harmonisation of Technical Requirements for Registration of Pharmaceuticals for Human Use (ICH), that is if it: is life-threatening or results in death; requires inpatient hospitalisation or prolongation of existing hospitalisation; results in persistent or significant disability/incapacity; is a congenital anomaly/birth defect; or is another ‘medically important’ event that may jeopardise the study participant or may require intervention to prevent one of the other outcomes listed in the definition above [6]. The ICH recommends that cancers are characterised as ‘medically important’ adverse events and, therefore, are classified as serious adverse events [6].
All such identified records in the sanofi-aventis pharmacovigilance database were reviewed, by treatment, by the manufacturer’s drug safety personnel with experience of adverse event reporting, and only treatment-emergent neoplasms judged to be malignant were included, independent of treatment group. Each person was counted only once, although separate counts for people and cases are provided if more than one malignancy was reported in the same person. Relative risks and 95% confidence intervals were calculated for insulin glargine relative to the comparator for the total incidence of malignancies and for individual classifications using all identified RCTs in type 1 and type 2 diabetes combined.
Results
The Clintrace sanofi-aventis safety database contains 31 eligible studies. Twelve studies were performed in people with type 1 diabetes and 19 studies in people with type 2 diabetes; most of the studies compared insulin glargine with NPH insulin (20 studies). Nearly all (29) were parallel-group trials (two had a crossover design). Details of these studies are summarised in Table 1. Most studies were open label, 19 were of around 6 months in duration, with six of longer duration, notably the retinopathy study 4016, which had a duration of 5 years [7].
Table 1
Details of the studies included in the analysis
Trial number (reference) | Comparator | Study duration (weeks) | Participants randomised and treated (insulin glargine/control arm) |
|---|---|---|---|
Type 1 diabetes | |||
2002 [15] | NPH | 4 | 168/88 |
2003 [16] | NPH | 4 | 223/110 |
3001 [17] | NPH | 28 | 292/293 |
3003 [18] | NPH | 28 | 174/175 |
3004 [19] | NPH | 28 | 264/270 |
3005 [20] | NPH | 16 | 310/309 |
4003a
| Ultralente | 6–7 | 29/27 |
4005 [21] | NPH | 32 | 26/25 |
4006 [22] | NPH | 32 | 53/52 |
4010 [23] | NPH | 30 | 62/63 |
4030 [24] | NPH or lente | 24 | 85/90 |
4036 [25] | Insulin lispro as CSII | 24 | 26/24 |
Type 2 diabetes | |||
2004 [26] | NPH | 4 | 136/68 |
2006a
| ‘Conventional insulin’ | 4 | 57/57 |
3002 [27] | NPH | 52 | 289/281 |
3006 [28] | NPH | 28 | 259/259 |
3102a
| NPH | 28 | 158/159 |
3502 [29] | OGLDs | 24 | 203/197 |
4001 [30] | NPH | 28 | 464/233 |
4002 [31] | NPH | 24 | 367/389 |
4012 [32] | NPH | 24 | 221/223 |
4013 [33] | NPH | 28 | 231/250 |
4014 [34] | Rosiglitazone | 24 | 105/112 |
NPH | 5 years | 514/503 | |
4020a
| Pioglitazone | 48 | 164/181 |
4021a
| Insulin lispro 25%, insulin lispro protamine 75%, mix | 24 | 113/99 |
4022a
| OGLDs | 48 | 118/130 |
4027 [35] | NPH 30/70 | 28 | 177/187 |
4040 [36] | Insulin lispro | 44 | 205/212 |
4042 [37] | OGLDs and dietary measures | 40 | 103/108 |
6001 [38] | NPH | 36 | 61/49 |
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Overall, 10,880 people were included in the analysis, with 5,657 people randomised to insulin glargine and 5,223 people randomised to the comparator, representing a total follow-up time of 4,711 and 4,524 person-years, respectively. Baseline characteristics of the participants were comparable between treatment groups (Table 2).
Table 2
Participant characteristics in the studies identified for inclusion in the analysis
Trial number | Age (years) | Sex ratio M/F | BMI (kg/m2) | Duration of diabetes (years) | Baseline HbA1c (%) | |||||
|---|---|---|---|---|---|---|---|---|---|---|
Insulin glargine | Comparator | Insulin glargine | Comparator | Insulin glargine | Comparator | Insulin glargine | Comparator | Insulin glargine | Comparator | |
Type 1 diabetes | ||||||||||
2002a
| 37.3 | 37.9 | 51.2/48.8 | 53.4/46.6 | 24.2 | 24.5 | 16.3 | 16.3 | 7.9 | 7.9 |
2003a
| 36.6 | 35.7 | 60.5/39.5 | 61.8/38.2 | 24.0 | 24.0 | 9.5 | 11.0 | 8.0 | 7.8 |
3001 | 39.4 (12.8) | 39.0 (11.7) | 54.8/45.2 | 56.7/43.3 | 24.6 (3.2) | 25.1 (3.3) | 15.9 (11.5) | 15.2 (9.4) | 7.9 (1.2) | 8.0 (1.2) |
3003 | 11.8 (2.5) | 11.5 (2.4) | 55.7/44.3 | 48.0/52.0 | 18.8 (2.8) | 18.9 (2.9) | 5.0 (3.0) | 4.7 (3.1) | 8.5 (1.3) | 8.9 (1.6) |
3004 | 38.2 (12.2) | 38.9 (11.9) | 53.4/46.6 | 47.8/52.2 | 25.6 (4.0) | 25.9 (4.6) | 17.9 (11.7) | 16.9 (10.0) | 7.7 (1.2) | 7.7 (1.1) |
3005 | 38.9 (12.2) | 39.5 (12.2) | 48.7/51.3 | 52.4/ 47.6 | 25.5 (3.4) | 25.7 (3.9) | 18.7 (11.5) | 18.4 (11.8) | 7.6 (1.2) | 7.7 (1.2) |
4003 | 36.4 (9.2) | 37.4 (9.2) | 45.0/55.0 | 26.0/74.0 | 26.3 (3.5) | 25.2 (3.1) | N/A | N/A | N/A | N/A |
4005 | 15.1 (1.7) | 14.5 (1.6) | 46.2/53.8 | 38.5/61.5 | 23.3 (4.1) | 23.0 (3.8) | 6.1 (3.6) | 8.0 (3.3) | 9.4 (1.1) | 9.1 (1.4) |
4006 | 41.1 (13.9) | 41.1 (10.7) | 32.0/68.0 | 41.4/58.6 | 26.5 (2.8) | 25.4 (3.0) | 22.4 (15.1) | 20.8 (11.3) | 8.1 (0.8) | 7.9 (0.8) |
4010 | 41.7 (12.9) | 39.3 (13.9) | 38.7/61.3 | 39.7/60.3 | 27.0 (3.6) | 26.0 (3.9) | 17.9 (10.5) | 17.1 (9.7) | 9.2 (1.1) | 9.7 (1.3) |
4030 | 13.1 (2.4) | 13.3 (2.5) | 45.9/54.1 | 45.6/54.4 | 22.7 (3.8) | 22.7 (5.0) | 5.1 (3.4) | 5.4 (3.7) | 7.8 (0.8) | 8.0 (0.8) |
4036 | 42.4 (9.9) | 37.6 (12.3) | 53.8/46.2 | 54.2/45.8 | 24.3 (1.9) | 23.8 (2.7) | 20.9 (10.6) | 18.5 (8.4) | 7.8 (0.6) | 7.7 (0.7) |
Type 2 diabetes | ||||||||||
2006 | 60.9 (10.8) | 60.5 (9.8) | 59.6/40.4 | 59.6/40.4 | 27.0 (2.9) | 26.3 (3.3) | 13.4 (8.2) | 13.8 (8.6) | 9.3 (1.1) | 9.6 (1.2) |
2004a
| 59.5 | 59.2 | 61/39 | 57.4/42.6 | 27.2 | 27.7 | 9.7 | 9.1 | 9.7 (1.3) | 9.5 (1.4) |
3002 | 59.6 (9.3) | 59.4 (9.1) | 53.3/46.7 | 54.1/45.9 | 29.3 (4.3) | 28.8 (4.3) | 10.2 (6.2) | 10.5 (6.0) | 9.0 (1.2) | 8.9 (1.1) |
3006 | 59.5 (9.7) | 59.2 (9.9) | 57.9/42.1 | 62.2/37.8 | 30.7 (5.0) | 30.4 (5.1) | 13.4 (8.3) | 14.1 (9.0) | 8.6 (1.2) | 8.5 (1.2) |
3102b
| – | – | – | – | – | – | – | – | 9.1 (1.1) | 9.1 (1.0) |
3502 | 56.2 (9.3) | 56.8 (10.0) | 66.5/33.5 | 63.7/36.3 | 31.2 (4.5) | 31.4 (4.6) | 7.7 (5.5) | 8.2 (6.5) | 8.6 (1.1) | 8.5 (1.0) |
8.6 (0.1)c
| 8.6 (0.1)c
| |||||||||
4001 | 60.3 (9.2) | 61.8 (8.5) | 54.9/45.1 | 51.3/48.7 | 28.7 (4.2) | 28.9 (3.9) | 10.2 (7.0) | 9.9 (6.0) | 8.9 (0.8) | 8.9 (0.8) |
4002 | 54.7 (9.5) | 55.6 (8.9) | 55/45 | 56.3/43.7 | 32.5 (4.6) | 32.2 (4.8) | 8.4 (5.6) | 9.0 (5.6) | 8.6 (0.9) | 8.6 (0.9) |
4012 | 55.4 (8.4) | 56.3 (8.4) | 39.4/60.6 | 43.8/56.2 | 24.8 (3.0) | 25.1 (3.1) | 10.3 (6.2) | 10.0 (5.2) | 9.0 (0.9) | 9.1 (0.9) |
4013 | 56.1 (9.9) | 57.1 (9.6) | 42.9/57.1 | 38.0/62.0 | 27.3 (3.7) | 27.2 (4.0) | 10.3 (6.4) | 10.8 (6.4) | 9.0 (1.0) | 9.2 (0.9) |
4014 | 55.9 (10.5) | 55.3 (11.4) | 45.2/54.8 | 58/42 | 34.6 (7.0) | 33.6 (6.3) | 8.5 (5.8) | 8.1 (5.1) | 8.8 (1.0) | 8.7 (1.0) |
4016 | 54.9 (8.8) | 55.3 (8.5) | 54.2/45.8 | 53.6/46.4 | 34.5 (7.2) | 34.1 (7.2) | 10.7 (6.9) | 10.8 (6.7) | 8.4 (1.4) | 8.3 (1.4) |
4020 | 52.5 (11.0) | 51.8 (10.3) | 48/52 | 49.6/50.4 | 33.6 (7.0) | 33.6 (7.3) | 6.4 (4.9) | 5.8 (4.2) | 9.4 (1.2)c
| 9.4 (1.3)c
|
4021 | 54.2 (10.5) | 52.8 (9.8) | 47.8/52.2 | 45.5/54.5 | 33.4 (5.2) | 33.5 (6.2) | 10.1 (7.0) | 8.9 (6.6) | 9.1 (0.9) | 9.0 (0.9) |
4022 | 53.6 (9.7) | 52.1 (10.3) | 47.5/52.5 | 48.5/51.5 | 34.5 (7.0) | 35.2 (7.4) | 7.5 (4.5) | 7.6 (6.0) | 9.0 (1.2) | 9.0 (1.2) |
4027 | 60.9 (8.7) | 60.4 (9.1) | 61.0/39.0 | 57.0/43.0 | 29.5 (3.6) | 29.6 (3.6) | 9.9 (7.3) | 9.9 (6.4) | 8.9 (1.0) | 8.9 (0.9) |
4040 | 60.0 (9.0) | 59.7 (9.0) | 52.5/47.6 | 58.7/41.4 | 29.2 (3.7) | 29.4 (3.5) | 9.0 (6.8) | 8.5 (6.1) | 8.7 (1.0) | 8.7 (1.0) |
4042 | 60.6 (7.7) | 60.7 (8.1) | 55.3/44.7 | 50.0/50.0 | 30.1 (3.5) | 29.8 (3.4) | 10.0 (6.2) | 10.1 (6.9) | 7.6 (0.3) | 7.5 (0.4) |
6001 | 56.1 (9.4) | 57.5 (8.5) | 62/38 | 65/35 | 31.3 (5.3) | 32.1 (5.4) | 8.6 (4.3) | 8.5 (4.8) | 9.1 (1.2) | 9.3 (1.1) |
Overall, there was no difference in the incidence of malignancies between insulin glargine-treated people and the comparator group (Table 3), with 52 cases of malignant cancer documented as a serious treatment-emergent event in 45 people in the insulin glargine group (0.8%) and 48 cases in 46 people in the comparator group (0.9%). Among such malignancies, most occurred in people with type 2 diabetes, with 45 cases in 39 people in the insulin glargine group (1.0%) and 46 cases in 44 people in the comparator group (1.2%).
Table 3
All malignant neoplasms reported in controlled clinical trials comparing insulin glargine with a comparator (participants evaluable for safety)
Trial duration | Insulin glargine | Comparator | ||||
|---|---|---|---|---|---|---|
No. of patients | All malignancies | Breast cancer | No. of patients | All malignancies | Breast cancer | |
No. affected (%) [no. of events] | No. affected (%) [no. of events] | No. affected (%) [no. of events] | No. affected (%) [no. of events] | |||
Type 1 diabetes (12 trials): insulin glargine vs other basal insulin | ||||||
3001 | 292 | 2 (0.7) [2] | 0 | 293 | 0 | 0 |
3004 | 264 | 3 (1.1) [3] | 1 (0.4) [1] | 270 | 0 | 0 |
3005 | 310 | 1 (0.3) [2] | 0 | 309 | 2 (0.6) [2] | 0 |
2002 | 168 | 0 | 0 | 88 | 0 | 0 |
2003 | 223 | 0 | 0 | 110 | 0 | 0 |
3003 | 174 | 0 | 0 | 175 | 0 | 0 |
4003 | 29 | 0 | 0 | 27 | 0 | 0 |
4005 | 26 | 0 | 0 | 25 | 0 | 0 |
4006 | 53 | 0 | 0 | 52 | 0 | 0 |
4010 | 62 | 0 | 0 | 63 | 0 | 0 |
4030 | 85 | 0 | 0 | 90 | 0 | 0 |
4036 | 26 | 0 | 0 | 24 | 0 | 0 |
Total type 1 | 1,712 | 6 (0.4) [7] | 1 (0.1) [1] | 1,526 | 2 (0.1) [2] | 0 |
Type 2 diabetes: insulin glargine vs NPH insulin ≤1 year in duration (ten trials)a
| ||||||
3002 | 289 | 3 (1.0) [3] | 0 | 281 | 7 (2.5) [7] | 1 (0.4) [1] |
3006 | 259 | 6 (2.3) [8] | 0 | 259 | 3 (1.2) [4] | 0 |
3102 | 158 | 1 (0.6) [1] | 0 | 159 | 1 (0.6) [1] | 0 |
4001 | 464 | 3 (0.6) [3] | 0 | 233 | 1 (0.4) [1] | 0 |
4002 | 367 | 0 | 0 | 389 | 1 (0.3) [1] | 1 (0.3) [1] |
2004 | 136 | 0 | 0 | 68 | 0 | 0 |
4012 | 221 | 0 | 0 | 223 | 0 | 0 |
4013 | 231 | 0 | 0 | 250 | 0 | 0 |
4027 | 177 | 0 | 0 | 187 | 0 | 0 |
6001 | 61 | 0 | 0 | 49 | 0 | 0 |
Total | 2,363 | 13 (0.6) [15] | 0 | 2,098 | 13 (0.6) [14] | 2 (0.1) [2] |
Type 2 diabetes: insulin glargine vs NPH insulin >1 year in duration (one trial) | ||||||
4016 | 514 | 20 (3.9) [23] | 3 (0.6) [3] | 503 | 31 (6.2) [32] | 4 (0.8)b
|
Type 2 diabetes: insulin glargine vs oral agents (five trials) | ||||||
3502 | 203 | 1 (0.5) [1] | 0 | 197 | 0 | 0 |
4014 | 105 | 0 | 0 | 112 | 0 | 0 |
4020 | 164 | 0 | 0 | 181 | 0 | 0 |
4022 | 118 | 0 | 0 | 130 | 0 | 0 |
4042 | 103 | 2 (1.9) [2] | 0 | 108 | 0 | 0 |
Total | 693 | 3 (0.4) [3] | 0 | 728 | 0 | 0 |
Type 2 diabetes: insulin glargine vs other insulin than NPH (three trials) | ||||||
2006 | 57 | 1 (1.8) [1] | 0 | 57 | 0 | 0 |
4021 | 113 | 0 | 0 | 99 | 0 | 0 |
4040 | 205 | 2 (1.0) [3] | 0 | 212 | 0 | 0 |
Total | 375 | 3 (0.8) [4] | 0 | 368 | 0 | 0 |
Total type 2 diabetes | 3,945 | 39 (1.0) [45] | 3 (0.1) [3] | 3,697 | 44 (1.2) [46] | 6 (0.2) [6] |
Grand total | 5,657 | 45 (0.8) [52] | 4 (0.1) [4] | 5,223 | 46 (0.9) [48] | 6 (0.1) [6] |
The corresponding RR for malignant cancer with insulin glargine compared with the comparator is 0.90 (95% CI 0.60–1.36).
Four cases of malignant breast cancer were reported in the insulin glargine group (0.1%) and six cases in the control group (0.1%). The RR for breast cancer is 0.62 (95% CI 0.17–2.18).
These data were primarily driven by the findings in the 5 year RCT (study 4016) that compared insulin glargine (n = 514) with NPH insulin (n = 503) in people with type 2 diabetes who were randomised and received treatment [7, 8]. In that study, the overall number of people with neoplasms was similar in the insulin glargine and NPH insulin groups (57 [11.1%] and 62 [12.3%] people, respectively) [8]. When considering only the number of people in the retinopathy study with malignant neoplasms reported as serious treatment-emergent events, the rate was also similar in both groups (insulin glargine vs NPH insulin, 23 cases in 20 people [3.9%] vs 32 cases in 31 people [6.2%]). Finally, the number of people with breast cancer reported as a serious adverse event in that study was similar between the two treatment groups (three [0.6%] vs four [0.8%] cases – there was also an additional fifth case in the NPH insulin group, although this was reported as a non-serious adverse event).
Table 4 summarises the sites of all malignancies in the pooled studies comparing insulin glargine with comparator. The most frequently reported site (insulin glargine vs comparator) included the skin (16 events in 12 people [0.2%] vs seven events in six [0.1%] people, RR 1.85, 95% CI 0.69–4.92), colon and rectum (six [0.1%] vs ten [0.2%], RR 0.55, 95% CI 0.20–1.52), breast (four [0.1%] vs six [0.1%], RR 0.62, 95% CI 0.17–2.18) and gastrointestinal tract (six [0.1%] vs four [0.1%], RR 1.38; 95% CI 0.39–4.90).
Table 4
Location of malignancies in randomised controlled studies of insulin glargine
Classification | No. using insulin glargine (%) [no. of events] | No. in the control group (%) [no. of events] | Relative risk (95% CI) |
|---|---|---|---|
Total number of people | 5,657 (100) [52] | 5,223 (100) [48] | – |
Blood | 2 (0.04) [2] | 1 (0.02) [1] | 1.85 ( 0.17–20.36) |
Vertebral body | 1 (0.02) [1] | 0 | – |
Breast | 4 (0.07) [4] | 6 (0.11) [6] | 0.62 (0.17–2.18) |
Nasal | 1 (0.02) [1] | 0 | – |
Lung | 3 (0.05) [3] | 3 (0.06) [3] | 0.92 (0.19–4.57) |
Gastrointestinal (not otherwise stated) | 6 (0.11) [6] | 4 (0.08) [4] | 1.38 (0.39–4.90) |
Colon and rectum | 6 (0.11) [6] | 10 (0.19) [10] | 0.55 (0.20–1.52) |
Hepatic and biliary | 2 (0.04) [2] | 3 (0.06) [3] | 0.62 (0.10–3.68) |
Pancreas | 3 (0.05) [3] | 3 (0.06) [3]a
| 0.92 (0.19–4.57) |
Renal | 3 (0.05) [3] | 0 | – |
Prostate | 1 (0.02) [1] | 3 (0.06) [3] | 0.31 (0.03–2.96) |
Bladder | 0 | 2 (0.04) [2] | – |
Genitourinary | 3 (0.05) [3] | 4 (0.08) [4] | 0.69 (0.16–3.09) |
Thyroid | 2 (0.04) [2] | 0 | – |
Endocrine | 0 | 1 (0.02) [1] | – |
Neurological | 0 | 2 (0.04) [2] | – |
Skin | 12 (0.21) [16] | 6 (0.11) [7] | 1.85 (0.69–4.92) |
Total number of people with malignanciesb
| 45 (0.80) [52] | 46 (0.88) [48] | 0.90 (0.60–1.36) |
With respect to the type of malignancy, at least two more tumours were reported in the comparator group vs the insulin glargine group for the following classifications: colon and rectum (ten [0.2%] vs six [0.1%]), prostate (three [0.1%] vs one [0.0%]), neurological (two [0.0%] vs zero [0.0%]) and bladder (two [0.0%] vs zero [0.0%]). Conversely, there were nine more cases of skin cancer in the insulin glargine group compared with the comparator group (16 cases in 12 people [0.2%] vs seven cases in six people [0.1%]), including an imbalance of six (0.1%) to one (0.0%) for malignant melanoma. However, in the 5 year Study 4016, the incidence of all melanomas (documented as serious and non-serious adverse events) was not different between treatment groups (three each, with one case in the comparator [NPH insulin] group and two in the insulin glargine group reported as serious adverse events).
Within the sanofi-aventis safety database, in addition to the RCTs, there are 26 completed uncontrolled studies with insulin glargine, involving a total of 68,201 participants with type 1 or type 2 diabetes treated for up to 3 years. The data from these 26 uncontrolled studies represent a total follow-up time of 22,074 person-years for insulin glargine treatment.
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In total, there were 111 cases of malignancy, including nine cases of breast cancer, reported in these studies. The overall cancer rate is estimated to be 5.0 cases per 1,000 person-years (111 out of 22,074 person-years) and the breast cancer rate is estimated to be 82 cases per 100,000 person-years (that is, nine out of 11,027 person-years—the denominator here being the exposure of women in the type 2 diabetes RCTs). In investigator-sponsored trials and product registries (intensified monitoring) for which no enrolment figures are available, the sanofi-aventis safety database contains an additional 75 individuals with malignancies, including nine cases of breast cancer.
Discussion
Based on our analysis of 31 RCTs, insulin glargine was not associated with an increased incidence of cancer, including breast cancer, when compared with the control/comparator group.
The overall incidence of cancer in the trials included in this analysis was lower in people with type 1 diabetes than in those with type 2 diabetes, perhaps because the former were younger and less obese than the people with type 2 diabetes (Table 2), and were exposed for a shorter time. Obesity increases the risk of colon cancer by as much as 1.5- to 2-fold and accounts for up to 35% of the total incidence of colon cancer [9]. In terms of age, the prevalence of cancer increases with increasing age and peaks in people aged 75 years or older [10, 11]. People with type 2 diabetes in this analysis were typically in their mid to late fifties and, thus, the majority were at an age associated with greater risk for cancer compared with the people with type 1 diabetes.
The results presented are based on formal RCTs, which represent level 1—the highest level—of evidence-based study design. Another advantage of the present analysis is that the clinical trials database reviewed here included a large number of people (n = 10,880), allowing the opportunity to identify rarer adverse events. Furthermore, the events were recorded reasonably accurately, as in any RCT, as the monitoring of adverse events followed the rules of good clinical practice and international pharmacovigilance regulations [12]. Finally, our analysis included one long-term 5 year controlled study that showed comparably reassuring findings, with no differences in the incidence of cancers between patients treated with insulin glargine and patients treated with NPH insulin.
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Nevertheless, this analysis must be considered in light of some limitations. The duration of most of the studies was relatively short (mostly 6 months) and does not reflect the lifetime risk for cancer, while only one study was longer than 1 year. Nevertheless, if growth promotion is postulated as the mechanism of any increased cancer risk, it would appear early in the use of any therapeutic entity. None of the RCTs was specifically designed to evaluate the risk of cancer with insulin glargine, although all had mandatory reporting of adverse events, including treatment-emergent neoplasms. Randomised controlled trials may not fully reflect real-life clinical practice; investigators may, for example, be less likely to include people with previous malignancies. People using thiazolidinediones, which have been suggested as protective against breast or pancreatic cancer [13, 14] and linked with increases in bladder cancer, [13] were often not included in the insulin studies, owing to the relative or absolute labelling restrictions in participating countries. Finally, the number of malignancies reported here may differ slightly from the published numbers for each study owing to differences in reporting methods; for example, only cases classified as serious treatment-emergent events were included in this analysis, whereas the original publications may have included cases classified as non-serious or serious. In addition, we only included treatment-emergent cases, whereas some of the publications may have included pre-existing cases.
However, analysis of the 26 uncontrolled trials with insulin glargine shows that the overall cancer rate is estimated to be 5.0 cases per 1,000 person-years. Compared with the age-adjusted incidence rate of 4.63 per 1,000 per year in the USA (based on cases diagnosed in 2002–2006 from 17 geographic areas included in the Surveillance, Epidemiology and End Results [SEER] programme), there was no indication of increased cancer risk in people with diabetes using insulin glargine. However, we acknowledge that under-reporting of cancer events can occur in uncontrolled observational studies, where follow-up with physicians is not always possible and, therefore, these results should be interpreted with caution.
For breast cancer, the incidence rate in women participating in non-interventional trials of insulin glargine may be estimated to be 82 cases per 100,000 person-years. Compared with the incidence rate of 124 per 100,000 women per year in the US SEER database, no safety signal for breast cancer was identified with the use of insulin glargine in these clinical trials.
In conclusion, these data suggest that insulin glargine is not associated with an increased risk of cancer compared with the different comparators (mainly NPH insulin). While the data provide useful reassuring and contributory information regarding the safety of insulin glargine, they underscore the importance of continued long-term follow up of participants in clinical trials.
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Acknowledgements
This analysis was sponsored by sanofi-aventis. Editorial support was provided through the Global Publications Group of sanofi-aventis.
Role of the funding source
The sponsor undertook the review of the pharmacovigilance database, collected and managed the data and undertook the statistical analyses. The corresponding author had full access to the data, and both authors made the decision to submit for publication.
Duality of interest
Institutions connected with P. D. Home receive funding from sanofi-aventis and other insulin analogue manufacturers in regard of his advisory, educational and research activities, including with insulin glargine. P. Lagarenne is an employee of sanofi-aventis.
Open Access
This article is distributed under the terms of the Creative Commons Attribution Noncommercial License which permits any noncommercial use, distribution, and reproduction in any medium, provided the original author(s) and source are credited.
Open AccessThis is an open access article distributed under the terms of the Creative Commons Attribution Noncommercial License (https://creativecommons.org/licenses/by-nc/2.0), which permits any noncommercial use, distribution, and reproduction in any medium, provided the original author(s) and source are credited.