Umesh Dashora,1 Dipesh C Patel,2 Robert Gregory,3 Peter Winocour,4 Ketan Dhatariya,5 Susannah Rowles,6 Andrew Macklin,7 Gerry Rayman,5 Dinesh Nagi,6 on behalf of the ABCD Executive Committee and supported by Diabetes UK
1 Conquest Hospital, Hastings, UK
2 Division of Medicine, University College London, Royal Free Campus, London, UK
3 University Hospitals of Leicester NHS Trust, Leicester, UK
4 ENHIDE, East and North Hertfordshire NHS Trust, Hertfordshire, UK
5 Norfolk and Norwich University Hospitals NHS Foundation Trust, UK
6 Pennine Acute Hospitals NHS Trust, Manchester, UK
7 Dorset County Hospital Foundation Trust, UK
8 Edna Coates Diabetes and Endocrine Unit, Pinderfields Hospital, Wakefield, UK
Address for correspondence: Dr Umesh Dashora
Consultant Physician and Lead, Diabetes and Endocrinology, East Sussex Healthcare NHS Trust, The Ridge, St Leonards on Sea, TN37 7RDTel: +44 (0)1424 755255 E-mail: u.dashora@nhs.net
https://doi.org/10.15277/bjd.2020.265
Dapagliflozin (sodium-glucose co-transporter (SGLT-2) inhibitor) and sotagliflozin (SGLT-1/2 inhibitor) are two of the drugs of the SGLT inhibitor class which have been recommended by the National Institute for Health and Care Excellence (NICE) in people with type 1 diabetes with body mass index ≥27 kg/m2. Dapagliflozin is licensed in the UK for use in the NHS while sotagliflozin may be available in future. These and possibly other SGLT inhibitors may be increasingly used in people with type 1 diabetes as new licences are obtained. These drugs have the potential to improve glycaemic control in people with type 1 diabetes with the added benefit of weight loss, better control of blood pressure and more time in optimal glucose range. However, SGLT inhibitors are associated with a higher incidence of diabetic ketoacidosis without significant hyperglycaemia. The present ABCD/Diabetes UK joint updated position statement is to guide people with type 1 diabetes and clinicians using these drugs to help mitigate this risk and other potential complications. Particularly, caution needs to be exercised in people who are at risk of diabetic ketoacidosis due to low calorie diets, illnesses, injuries, starvation, excessive exercise, excessive alcohol consumption and reduced insulin administration, among other precipitating factors for diabetic ketoacidosis.
Br J Diabetes 2020;20:155-162
Key words: SGLT inhibitors, type 1 diabetes, ketoacidosis, position statement
SGLT inhibitors are an established class of drugs which effectively lower glucose levels in people with type 2 diabetes, with additional cardiac and renal benefits. These drugs reduce blood glucose by preventing renal reabsorption of glucose, a mechanism which is insulin independent but glucose dependent.5 An additional positive effect on lowering blood pressure by natriuresis and weight loss might partly mediate the cardiovascular benefit recently observed in clinical trials in people with type 2 diabetes, although other mechanisms are possible.6–9 Dapagliflozin was the first SGLT-2 inhibitor to be approved for use in Europe in 2011 and in the UK in 2012. NICE has also approved the use of add-on dapagliflozin in people with type 1 diabetes with BMI ≥27kg/m2 when insulin alone is not sufficient to manage their diabetes, as long as their insulin requirement is at least 0.5 units/kg body weight. The medication can be continued as long as it results in sustained reduction in HbA1c of 3 mmol/mol (0.3%) after 6 months.1 There are currently four SGLT-2 inhibitors licensed in the UK: dapagliflozin, canagliflozin empagliflozin and ertugliflozin. Only dapagliflozin has obtained a licence for use in people with type 1 diabetes in the UK. Sotagliflozin is a dual SGLT-1 and 2 inhibitor and has had a favourable NICE technology appraisal guidance but is not yet available in the UK.2 These developments have prompted an update of the previous position statements.10,11 This update is in accordance with the RIGHT statement for practice guidelines.12 The term SGLT has been used when relating to both SGLT-2 and dual SGLT-1/2 inhibitors, whereas SGLT-2 has been used when the intention is to refer to SGLT-2 inhibitors only.
We searched PubMed, Google Scholar, Cinahl and Embase databases with the search words ‘SGLT inhibitors’ AND ‘type 1 diabetes’ and recent meta-analyses from 2020 were included for up-to-date evidence to the information already available in the previous version of the position statement. The evidence and recommendations were shared widely amongst the writing group and consensus was obtained electronically. The views and preferences were sought from people with type 1 diabetes selected from personal contacts and changes were made where appropriate. The limitation of these recommendations is that evidence can change quickly in this area and therefore regular update may be required.
Potential role in type 1 diabetes
Optimal management of type 1 diabetes remains a challenge in the UK. Recent data show that the percentage of people achieving the NICE recommended targets (ie, HbA1c <58 mmol/mol (7.5%), blood pressure <140/80 mmHg, cholesterol <5 mmol/L) is 32.1%, 73.1% and 72.8%, respectively. All three targets combined were achieved in only 20.1% of the people.3,13,14
There are considerable data showing higher cardiovascular15,16 and renal risk17 in people with type 1 diabetes. There is therefore scope for achieving tight glycaemic management with appropriate insulin therapy and any potential adjunct therapy for people with type 1 diabetes that may help improve risk factor and/or cardiovascular and renal outcomes.
Our previous ABCD position statements outline the standards of care for people with type 1 diabetes.18,19 Intensified insulin therapy is often used to manage hyperglycaemia in people with type 1 diabetes on the basis of studies which showed a link between hyperglycaemia and micro and macrovascular complications of diabetes.20 This intensification, however, may increase the risk of hypoglycaemia, weight gain and associated adverse cardiovascular profile.21
Metformin is inexpensive and useful in some people with type 1 diabetes with BMI ≥25 kg/m2, but it does not improve HbA1c in the long term.22,23 Compared with metformin at week 26, SGLT inhibitors like dapagliflozin (5 mg), sotagliflozin (200 mg) and empagliflozin (10 mg) had greater reductions in HbA1c (MD −3 mmol/mol (−0.24%), −3 mmol/mol (−0.23%) and −4 mmol/mol (−0.35%), respectively) and weight.24
GLP-1 analogues and receptor agonists may be helpful in subgroups of people with type 1 diabetes, but the reductions in HbA1c are modest (MD −3 mmol/mol (−0.24%) with liraglutide 1.8 mg) although weight reductions were significant (4.87 kg with liraglutide 1.8 mg), insulin dose reduced, hypoglycaemia reduced but not significantly (OR 0.80) and gastrointestinal adverse events increased significantly (OR nausea 4.70, vomiting 2.50).25,26 Dipeptidyl peptidase-4 (DPP4) inhibitors added to insulin did result in a small but insignificant reduction in HbA1c (1 mmol/mol (0.07%)) and no consistent effect on glucose variability in people with type 1 diabetes.27 By contrast, SGLT inhibitors are oral glucose-lowering drugs with potential as long as they are used appropriately.28,29
Evidence for SGLT inhibitors in type 1 diabetes
There is considerable emerging evidence for use of SGLT inhibitors in people with type 1 diabetes. The initial studies which formed the basis of evidence are summarised in brief in Table 1. Details of subsequent studies are not included in this paper as they have not influenced the position paper. More recent meta-analyses, however, are outlined in the paragraphs below.30–37
In a recent meta-analysis including over 7000 participants and 17 randomised controlled trials (RCTs), SGLT inhibitor therapy significantly reduced HbA1c (4 mmol/mol (0.37%)) and body weight (2.88 kg).38
In another meta-analysis of seven RCTs, lower HbA1c (−3 mmol/mol (−0.28%)), lower insulin dose (MD −0.89) and greater weight loss (−3.03) without any significant difference in hypoglycaemia39 was seen in the sotagliflozin group.
The European Medicines Agency has accepted the application of a marketing authorisation variation for dapagliflozin for use as an oral adjunct treatment to insulin in people with type 1 diabetes.40
In a further RCT from a single centre, 30 people with type 1 diabetes on liraglutide and insulin were put on additional dapagliflozin or placebo.41 In the dapagliflozin group, HbA1c fell by 7 mmol/mol (0.66%) from 7.8% with no change (p<0.01) in the placebo group over 12 weeks.
Adverse effects of SGLT inhibitors
In a systematic review and meta-analysis of seven RCTs including 3,900 participants in comparison to the placebo group, the risk of genital infection (RR 3.22) and DKA (RR 2.66) was higher in the SGLT inhibitor-treated group.42
In another evaluation of the safety of SGLT-2 inhibitors covering 1,653 articles including eight RCTs, compared with placebo, the SGLT-2 inhibitor group was found to have an increased incidence of DKA (OR 4.34), genital infections (OR 3.64), volume depletion (OR 2.10) and diarrhoea (OR 1.64). The risk of diarrhoea was dose-related. There was no increase in the incidence of urinary tract infections, cardiovascular events, renal events, liver injury and fractures.43
In a meta-analysis of 13 RCTs including 7,962 participants, there was a higher risk of DKA (RR 5.04), urinary tract infections (RR 1.2) and genital infections (RR 2.99) but not hypoglycaemia.44
Sotagliflozin meta-analysis of seven RCTs including nearly 3,600 participants showed a higher rate of DKA (RD 0.03) and genital mycotic infections (RD 0.06) but no increase in urinary tract infections compared with placebo.39
People with type 1 diabetes develop DKA in the absence of insulin. Insulin helps reduce glucose but also prevents lipolysis. SGLT inhibitors reduce glucose but have been associated with reports of DKA in people with type 1 diabetes and some people with type 2 diabetes through mechanisms which are not fully understood. The current evidence is presented below.
A study based on the US Food and Drug Administration Adverse Event Reporting System (FAERS) showed that the proportional reporting ratio of DKA in people on SGLT inhibitors was 7.9, was higher for type 1 diabetes and women, in a wide range of age and body weight. Duration of treatment varied and death was reported in 37 individuals (1.54%).45
Peters et al reported a series of case reports of DKA in people taking SGLT inhibitors. Thirteen cases of DKA were observed in nine people. Seven people had type 1 diabetes and two had type 2 diabetes. Four people had repeat episodes.46
A post-hoc re-evaluation of 17,000 participants in a canagliflozin development programme has been reported. Twelve cases of DKA were reported, four (0.07%) in the canagliflozin 100 mg group, six (0.11%) in the canagliflozin 300 mg group and two (0.03%) in the placebo comparator group. Six of the participants (50%) were reported to have either type 1 diabetes or latent autoimmune diabetes of adults (LADA).47
Another study by Perkins et al was an 8-week open-label proof of concept trial using SGLT-2 inhibitors in type 1 diabetes. Two of the 40 participants with type 1 diabetes (5%) had symptomatic ketosis or DKA.48
Putative mechanism of ketogenesis
A small but not insignificant rise in the incidence of DKA in people taking SGLT inhibitors is poorly understood. Several mechanisms have been suggested including excessive dose reduction of insulin, pre-existing propensity to DKA, reduced ketone excretion and shift in substrate metabolism with increased reliance on free fatty acids and ketone bodies rather than glucose and pyruvate.49,50
There is also a possibility that ketogenesis could occur due to the direct action of SGLT inhibitors on human pancreatic alpha cells increasing glucagon secretion.51,52 As the glucose concentration can be closer to target levels, and as the urine ketones may not always be raised in some individuals, the diagnosis of DKA can be delayed or missed.
Effect of insulin dose reduction on ketosis
Insulin deficiency seems to be related to ketoacidosis in people with type 1 diabetes taking SGLT inhibitors. A post-hoc exploratory analysis has shown that ketone formation is increased when insulin dose reduction is >20% compared to when it is <20%.53 Similarly, insulin pump failure and missed insulin doses were the most frequent risk factors in the cases of DKA seen in another study.32 In another small study in people with type 1 diabetes using liraglutide and SGLT-2 inhibitors, two developed DKA. Both participants had a reduction in insulin dose >20% and both events occurred within 48 hours dose titration of dapagliflozin from 5 mg to 10 mg daily.41 In addition, one participant had consumed a large amount of alcohol which is likely to be a factor in the development of euglycaemic ketoacidosis.
Risk of amputations and stroke
The risk of amputations and stroke remains unclear with the available current evidence in people with type 1 or type 2 diabetes. Canagliflozin in people with type 2 diabetes was associated with a higher rate of lower limb amputations mainly at the level of the toe and metatarsals.8 There was a higher rate of fractures in the CANVAS study but not in the CANVAS-R study.8 A recent meta-analysis has confirmed an excess risk of amputations with canagliflozin but not with other SGLT-2 inhibitors.54 In a meta-analysis covering 12 RCTs and 18 observational studies, there was no significant association between SGLT inhibitor exposure and amputations, although there was an increased risk noted in the subgroup analysis with canagliflozin (n=2 RCTs, RR 1.59) but not with other gliflozins.55 Another meta-analysis of five RCTs involving 21,395 participants on SGLT inhibitors has shown no significant increase in the risk of amputation (OR 1.31, NS) with any SGLT inhibitors including canagliflozin. Another trial level meta-analysis of six studies involving 51,713 participants with an event rate of amputation of 2.0% showed no significant association of empagliflozin, dapagliflozin or canagliflozin compared with controls (RR 1.24) including subgroups with or without peripheral artery disease.56 A real-world evidence study looking at lower limb amputation in over 700,000 people in the USA also concluded that there was no increase in the risk of lower limb amputation with canagliflozin compared with other SGLT inhibitors or with non-SGLT inhibitor diabetes drugs in either the overall population or in the subset of people with established cardiovascular disease.57 National advice from European, American and UK professional bodies and regulators is to be cautious with the use of all SGLT inhibitors in people with active foot disease as there may be a possible adverse class effect on foot health.58–62
Numerically, empagliflozin increased but canagliflozin reduced strokes in people with type 2 diabetes, although both were not significant and a subsequent meta-analysis is reassuring.6,8,63,64
Risk during COVID-19
SGLT inhibitors would theoretically be a high-risk strategy given the increased risk of DKA in unwell people with type 1 diabetes infected with COVID-19. However, the potential benefits on heart and kidneys might make them useful in some patients. Further clinical trials will help us in this area.65,66 The risks and benefits of SGLT use should be discussed with the person with diabetes as part of a care planning approach to consider individual circumstances and considerations.
Dapagliflozin is currently licensed and dapagliflozin and sotagliflozin are both recommended as an add-on therapy in people with type 1 diabetes with BMI ≥27 kg/m2 in whom insulin alone is not sufficient to manage their diabetes.
SGLT inhibitors are tolerated well with very few side effects (eg, urinary and genital infections, dehydration and DKA). In general, the rate and prevalence of DKA in people with type 1 diabetes taking SGLT inhibitors is too low to quantify exactly, but may not be insignificant. In people with type 1 diabetes taking SGLT inhibitors, it would make pragmatic sense to anticipate and monitor for possible DKA in situations known to precipitate metabolic decompensation (eg, injury, infections, myocardial infarction, stroke, insulin deficiency, ketogenic diet, surgery, other stressful events and catabolic states). There should be prompts to identify individuals attending Emergency Departments or Medical Admissions Units who are prescribed SGLT inhibitors to warn of the possibility of euglycaemic DKA where the individual may be in diabetic ketoacidosis despite non-elevated glucose levels and low urine ketones. SGLT inhibitors should be stopped in people who are acutely ill or are admitted for elective surgery. SGLT inhibitors should also be discontinued in people who have developed DKA and should not be re-started unless a clear alternative cause of DKA is identified. Insulin doses should not be reduced more than 20% if SGLT inhibitors are added to insulin regimens.
It is recommended that regular monitoring of blood glucose and ketones should be undertaken in people with diabetes taking these drugs to avoid hypoglycaemia as well as ketosis. This Joint ABCD/Diabetes UK position statement will be reviewed following publication of any further evidence and research studies.
Conflict of interest UD reports personal fees from AstraZeneca, during the conduct of the study. SR/GR/RG/AM/DN have nothing to disclose. DCP reports: Commercial: Received fees for lectures and advisory work from AstraZeneca, Boehringer Ingelheim, Eli Lilly, MSD, Napp Pharmaceuticals, Novo Nordisk, Sanofi. Educational Activities: Financial compensation in relation to training of health professionals or planning training packages: I have received conference attendance support from Napp, Novo Nordisk and Sanofi. Expert functions in health care and health guidance processes, e.g. Board member in a development project, member of health board in the municipality: Chair, Association of British Clinical Diabetologists (ABCD) PW reports personal fees from advisory boards for AstraZeneca, Napp, outside the submitted work. KD reports personal fees from Lexicon Pharma/ Sanofi Diabetes, during the conduct of the study.
Funding None.
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