Abstract
In 2017, the Korean Diabetes Association (KDA) published a position statement on the use of antihyperglycemic agents for patients with type 2 diabetes mellitus (T2DM). The KDA regularly updates its Clinical Practice Guidelines, but since the last update in 2015, many results from clinical trials have been introduced, and domestic data from studies performed in Korean patients with T2DM have been published. Recently, evidence from large clinical studies assessing cardiovascular outcomes following the use of sodium-glucose cotransporter 2 inhibitors and glucagon-like peptide 1 receptor agonists in patients with T2DM were incorporated into the recommendations. Additionally, new data from clinical trials using dipeptidyl peptidase 4 inhibitors and thiazolidinediones in Korean patients with T2DM were added. Following a systematic review and assessment of recent evidence, the KDA updated and modified its clinical practice recommendations regarding the use of antihyperglycemic agents and revised the treatment algorithm for Korean adult patients with T2DM.
Keywords: Diabetes mellitus, type 2; Hypoglycemic agents; Insulin; Practice guideline
INTRODUCTION
The Clinical Practice Guidelines for type 2 diabetes mellitus (T2DM) provided by the Korean Diabetes Association (KDA) include comprehensive and evidence-based treatment and management guidelines to improve the level of care for adults with T2DM in Korea according to Korean standards. The target users of this guideline are primary care physicians and other healthcare professionals who treat adults with T2DM. Since the first edition was published in 1990, the Clinical Practice Guidelines for adult patients with T2DM have been periodically updated by the Committee of Clinical Practice Guidelines of the KDA [1]. However, since the fifth edition was published in 2015, many results from large clinical trials of antidiabetic drugs have been introduced, and clinical evidence from studies assessing Korean patients with T2DM who use dipeptidyl peptidase 4 (DPP4) inhibitors, glucagon-like peptide 1 receptor agonists (GLP-1RAs), or sodium-glucose cotransporter 2 (SGLT2) inhibitors have accumulated [2,3,4,5]. All novel evidence and results were reviewed to extract recommendations for the treatment of these patients.
The 2017 KDA position statement was written by the Committee of Clinical Practice Guidelines under a formal review process after a systematic and extensive review of articles published from January 1, 2015 to May 31, 2017. The grading system for the scientific evidence was defined by the KDA and modeled after the evidence-grading system of the American Diabetes Association (ADA) with some modifications [6]. Therefore, the level of evidence and strength of the recommendation were not treated as separate entities. The KDA classified recommendation levels into four ratings (A, B, C, and E) according to the quality of evidence (Table 1). If domestic data were limited or evidence was difficult to apply to Korean patients with T2DM, the Committee of Clinical Practice Guidelines made a final decision after intensive discussion. In the absence of qualified supporting evidence, or if the recommendation was based on the consensus of the Expert Committees, a grade E was assigned.
Table 1. Evidence-grading system of the Korean Diabetes Association.
Level of evidence | Description |
---|---|
A | Evidence from well-conducted, generalizable randomized controlled trials that are adequately powered, including |
- Evidence from well-conducted multicenter trials | |
- Evidence from meta-analyses that incorporated quality ratings in the analysis | |
B | Evidence from well-conducted cohort studies |
- Evidence from well-conducted prospective cohort studies or registries | |
- Evidence from well-conducted meta-analyses of cohort studies | |
- Evidence from well-conducted case-control studies | |
C | Evidence from poorly controlled or uncontrolled studies |
- Evidence from randomized controlled studies with some flaws in design, method, or analysis | |
- Evidence from case reports | |
- Evidence from observational studies with potential bias | |
E | Expert consensus |
In this 2017 position statement regarding pharmacological therapies for non-pregnant adult patients with T2DM, the KDA updated the previous recommendations published in 2015. In principle, these recommendations were based on extensive review of scientific evidences; therefore, criteria for the health insurance coverage in Korea were not considered. The treatment algorithm for use of antihyperglycemic agents was also revised. Specifically, the previous algorithm was divided into treatment with non-insulin antihyperglycemic agents and treatment with insulin, whereas the updated 2017 position statement is believed to provide the most recent evidence-based treatment recommendations for adult Korean patients with T2DM.
RECOMMENDATIONS
Oral antihyperglycemic agents and GLP-1RAs for type 2 diabetes mellitus
Principles of initial management after diagnosis of type 2 diabetes mellitus
1. Active lifestyle modification (LSM) and appropriate pharmacotherapy are needed following the initial diagnosis of diabetes [A].
2. An appropriate selection of pharmacotherapies should be made after considering the patient's clinical characteristics and the efficacy, side effects, mechanism of action, risk of hypoglycemia, effect on body weight, patient preference, and combined comorbidity [E].
Principles of treatment with antihyperglycemic agents
1. Metformin is the preferred initial oral antihyperglycemic agent [A].
2. If metformin is contraindicated or intolerable as the initial treatment, then another class of antihyperglycemic agent can be used depending on the clinical situation [E].
3. If monotherapy fails to achieve the glycemic goal, then combination therapy using a second agent with a different mechanism of action should be initiated [A].
4. Dual combination therapy can be used as the initial management strategy depending on the patient [B].
5. Although the maximal dosage of a single oral agent may be prescribed, early initiation of combination therapy is suitable after considering the glucose-lowering efficacy and side effects of the drug [B].
6. When selecting a class of antihyperglycemic agents for combination therapy, the glucose-lowering efficacy, risk of hypoglycemia, body weight gain, and cardiovascular benefits associated with the drugs are preferentially considered [E].
7. The different mechanisms of action, drug interactions, and patient preferences for combination therapy with more than two classes of antihyperglycemic agents should be considered [C].
8. Although insulin therapy is recommended after failed oral combination therapy, changing or adding another class of oral antihyperglycemic agent can be performed [C].
Glycemic control within the target range has beneficial effects for reducing the risk of cardiovascular and/or microvascular complications [7]. The glycemic goal for non-pregnant adult patients with T2DM is ideally a glycosylated hemoglobin (HbA1c) level <6.5%, but this can be tailored to individual circumstances [1,8,9]. Factors to consider when setting a glycemic target goal include age, duration of diabetes, life expectancy, presence of advanced diabetic complications, comorbidities, repeated episodes of hypoglycemia, cognitive dysfunction, and patient preference [1,6,8]. More stringent goals are required for preoperative and postoperative situations, pregnancy, and acute-onset disease. A patient-centered approach is emphasized to successfully achieve the glycemic goal [1,6,8,9,10].
LSM is an essential component of treatment for all patients with T2DM and should be initiated promptly and simultaneously with antidiabetic medications after diagnosis. Patient education within a structured program should be received from a healthcare professional at the time of diagnosis and then followed up with regular reinforcement checks [11,12,13]. For patients with newly diagnosed T2DM, LSM includes medical nutrition therapy, weight control, physical activity, smoking cessation, and avoidance of alcohol should be initiated. Although LSM is a very important component of treatment for T2DM, the administration of antihyperglycemic agents should not be delayed. Pharmacotherapy can be initiated simultaneously and in conjunction with LSM.
T2DM is a chronic metabolic disease with a progressive nature [14]. A gradual decline in β-cell function and progressive increases in insulin resistance lead to a deteriorated glycemic control status and the need for increasingly intensive pharmacotherapies [15]. Therefore, in addition to LSM, a transition from monotherapy to combination therapy with antihyperglycemic agents is usually inevitable. The initiation or add-on to a current therapy of most oral antihyperglycemic agents yields an additional reduction in HbA1c levels of 0.5% to 1.25%, whereas thiazolidinediones (TZDs) and sulfonylureas (SUs) lower HbA1c levels by approximately 1.0% to 1.25% [16].
As an initial therapy for newly diagnosed patients with an HbA1c level ≤7.5%, metformin monotherapy is recommended [17,18,19]. Metformin should not be used in patients with an estimated glomerular filtration rate <30 mL/min/1.73 m2, severe renal or hepatic dysfunction, heart failure, severe infection, or dehydration [6,7,8,9,10]. If metformin is not tolerable or is contraindicated, the alternative choices for monotherapy include DPP4 inhibitors, SGLT2 inhibitors, TZDs, GLP-1RAs, SUs, glinides (meglitinide), α-glucosidase inhibitors (AGIs), and insulin according to patient circumstances (Table 2, Fig. 1). The factors to consider when choosing an antihyperglycemic medication include its efficacy, complementary mechanism of action, risk of hypoglycemia, effect on weight gain, side effects, patient preference, and comorbidities [20,21,22,23]. In the Practical Evidence of Antidiabetic Monotherapy (PEAM) study, the glucose-lowering efficacies of SUs (glimepiride), biguanide (metformin), and TZDs (rosiglitazone) as antidiabetic monotherapies administered for 48 weeks were similar in drug-naive Korean patients with T2DM (decrease in HbA1c levels from 7.8% to 6.9% for glimepiride, P<0.001; from 7.9% to 7.0% for metformin, P<0.001; and from 7.8% to 7.0% for rosiglitazone, P<0.001; P=0.62) [24]. Glimepiride and rosiglitazone significantly increased body weight, while metformin reduced body weight. Symptomatic hypoglycemia was more frequent in the glimepiride group, while diarrhea was more frequent in the metformin group [24].
Table 2. Oral antihyperglycemic agents for patients with type 2 diabetes mellitus used in Korea.
Mechanism and common use | Weight gain | Hypoglycemiaa | HbA1c reduction, %a | Side effects | Caution | |
---|---|---|---|---|---|---|
Biguanide (metformin) | ↓ Hepatic glucose production Start with lower dose and titrate upward slowly |
Neutral or decrease | No | 1.0–2.0 | GI side effects (anorexia, nausea, vomiting, diarrhea, cramping), vitamin B12 deficiency, lactic acidosis (rare) | Contraindication in severe hepatic or renal insufficiency (eGFR <30 mL/min/1.73 m2), severe infection, dehydration, heart failure. Major operation or iodine-contrast use within 48 hours |
Sulfonylurea (gliclazide, glipizide, glimepiride, glibenclamide) | ↑ Insulin secretion from β-cells Before meal |
Yes | Yes | 1.0–2.0 | Severe hepatic or renal insufficiency, secondary failure | |
Meglitinide (repaglinide, nateglinide, mitiglinide) | ↑ Insulin secretion from β-cells, ↓ postprandial hyperglycemia Before each meal |
Yes | Yes | 0.5–1.5 | Severe hepatic or renal insufficiency | |
DPP4 inhibitor (sitagliptin, vildagliptin, saxagliptin, linagliptin, gemigliptin, alogliptin, teneligliptin, anagliptin) | ↑ Postprandial incretin (GLP-1, GIP), ↑ glucose-dependent insulin secretion, ↓ postprandial glucagon secretion, ↓ postprandial hyperglycemia, use regardless of mealtime | No | No | 0.5–1.0 | Angioedema, urticaria Acute pancreatitis Risk for heart failure (saxagliptin, alogliptin) |
Dose titration in severe hepatic or renal insufficiency |
Thiazolidinedione (pioglitazone, lobeglitazone) | ↑ Insulin sensitivity (muscle, adipose tissue), ↓ hepatic glucose production, once daily regardless of mealtime | Yes | No | 0.5–1.4 | Edema, anemia, bone fracture, heart failure | Heart failure, severe hepatic or renal insufficiency |
SGLT2 inhibitor (dapagliflozin, ipragliflozin, empagliflozin) | ↓ Renal glucose reabsorption, ↑ glucosuria Once daily regardless of mealtime |
No | No | 0.5–1.0 | Genitourinary tract infections, polyuria, dehydration, DKA | Old age, heart failure, hypotension, diuretics use, not for severe CKD (eGFR <60 mL/min/1.73 m2) |
α-Glucosidase inhibitor (acarbose, voglibose) | ↓ Upper intestinal glucose absorption, ↓ postprandial hyperglycemia Before each meal |
No | No | 0.5–1.0 | GI side effects (flatulence, diarrhea, bloating) | Severe hepatic or renal insufficiency, chronic inflammatory bowel disease with malabsorption, severe infectionHbA1c |
HbA1c, glycosylated hemoglobin; GI, gastrointestinal; eGFR, estimated glomerular filtration rate; DPP4, dipeptidyl peptidase 4; GLP-1, glucagon-like peptide 1; GIP, gastric inhibitory polypeptide; CKD, chronic kidney disease; SGLT2, sodium-glucose cotransporter 2; DKA, diabetic ketoacidosis.
aMonotherapy.
If the initial HbA1c level of a patient is ≥7.5% or the HbA1c target is not achieved within 3 months initiating monotherapy, dual combination therapy can be considered [6,7,8,9,10,25,26,27,28,29,30]. If the HbA1c target is not achieved within 3 months of initiating dual therapy, a third agent with a complementary mechanism of action can be added for triple combination therapy [31]. Metformin is maintained as background therapy during dual or triple combination therapy. If metformin is not tolerable or is contraindicated, avoid the use of metformin and proceed to the next category in the algorithm (Fig. 1). The reductions in HbA1c values are similar across all drug classes used as monotherapies and metformin-based combinations. Body weight is reduced or maintained with metformin, DPP4 inhibitors, GLP-1RAs, and SGLT2 inhibitors but increased with SUs and TZDs [25,26,27,28,29]. Hypoglycemia is more frequent with SUs [18,19,28,29]. As a monotherapy, DPP4 inhibitors exhibit a lower risk of hypoglycemia, lower risks of side effects and weight gain, and a better glucose-lowering efficacy in Asians compared with other ethnic groups [30]. When added to metformin and SUs, GLP-1RAs are associated with the lowest risk of hypoglycemia (odds ratio, 0.60; 95% confidence interval, 0.39 to 0.94) [19], but gastrointestinal side effects are highest with metformin and GLP-1RAs. SGLT2 inhibitors have greater associations with the potential side effects of urinary tract infection and euglycemic diabetic ketoacidosis [26,32].
If postprandial hyperglycemia occurs, meglitinides, AGIs, DPP4 inhibitors, or GLP-1RAs can be considered [33,34]. The early initiation of combination therapy is preferred over maximizing the dosage of a single agent after considering glucoselowering efficacy and side effects [35,36]. SUs or DPP4 inhibitors are not associated with increased risks of major cardiovascular events in patients with T2DM, irrespective of comparator or background medications [6,37]. However, for patients with longstanding suboptimally controlled T2DM and established atherosclerotic cardiovascular disease, the ADA recommends empagliflozin or liraglutide, because these drugs have been shown to reduce cardiovascular and all-cause mortality rates [6,38,39]. Ongoing studies investigating the cardiovascular benefits of the SGLT2 inhibitors, DPP4 inhibitors, and GLP-1RAs are being conducted [6].
Injections for patients with type 2 diabetes mellitus: insulin and GLP-1RAs
Indications for insulin treatment for patients with type 2 diabetes mellitus
1. Insulin therapy should be initiated if the patient fails to achieve the target glycemic goal despite appropriate treatment with oral antihyperglycemic agents [A].
2. Insulin can be used as an initial treatment at the time of diagnosis of T2DM for patients with metabolic decompensation and/or HbA1c levels >9.0% and/or symptomatic hyperglycemia [E].
3. Initiate insulin therapy in cases of decompensated renal or hepatic insufficiency, myocardial infarction, stroke, acute severe illness, and/or major surgery [B].
Choice of type of insulin treatment
1. A basal insulin regimen or premixed insulin injections (once or twice daily) should be used depending on the patient's circumstances [B].
2. If the glycemic goal is not achieved with a basal insulin or premixed insulin regimen, then a multiple-component insulin regimen should be used [A].
3. A combination therapy of oral antihyperglycemic agents and insulin can be employed depending on the patient's condition [A].
GLP-1RAs
1. A GLP-1RA can be used as monotherapy or combination therapy with oral antihyperglycemic agents or basal insulin [A].
Insulin therapy should be initiated if the patient fails to achieve the target glycemic goal despite the appropriate treatment with oral antihyperglycemic agents. The KDA recommends insulin therapy in two circumstances: as the initial treatment after diagnosis of T2DM and after oral antihyperglycemic agent failure.
Initiation of insulin treatment at the diagnosis of T2DM is recommended if the patient has severe hyperglycemia (HbA1c levels >9.0%) with hyperglycemic symptoms (polyuria, polydipsia, and weight loss) and/or metabolic decompensation [1,6,40]. Insulin therapy should also be considered in patients with decompensated hepatic or renal insufficiency, myocardial infarction, stroke, and/or critical illness, as well as those undergoing major surgery [1,6,41,42].
For patients with T2DM who fail to achieve the glycemic goal following adequate treatment with oral antihyperglycemic agents, insulin injection therapy is the next step [6,7,8,9,19,43,44,45]. Basal insulin alone or in combination with oral antihyperglycemic agents is easy to administer and is the preferred choice. Basal insulin alone, including both intermediate-acting and long-acting analogs, is the most convenient initial insulin regimen. Although the glucose-lowering effects are similar, hypoglycemia occurs less frequently with long-acting basal insulin analogs (insulin glargine or detemir) than with neutral protamine Hagedorn (NPH) insulin (human isophane insulin) [46]. A recently introduced ultra-long-acting insulin, degludec, showed a lower rate of nocturnal hypoglycemia and reduced mean fasting plasma glucose level compared with glargine in patients with T2DM [47,48].
Basal insulin is typically combined with metformin and/or other classes of oral antihyperglycemic agents. The addition of DPP4 inhibitors to a basal insulin regimen results in significant improvements in glycemic control relative to placebo without increasing hypoglycemia or body weight [49,50,51]. Compared with a 25% increase in the insulin dose, the addition of sitagliptin to an insulin-based regimen is more effective at lowering HbA1c levels and is associated with less hypoglycemia and weight gain in Korean patients with uncontrolled T2DM [51]. SGLT2 inhibitors achieve better glycemic control and weight reduction than do DPP4 inhibitors without increasing the risk of hypoglycemia in patients with T2DM inadequately controlled by insulin [52].
The addition of a GLP-1RA to basal insulin or switching to a premixed insulin regimen (once or twice daily) is another option, but this depends on the patient's clinical situation (Table 3) [53]. Premixed insulin products contain a basal component as well as a prandial component (NPH/Regular 70/30, 70/30 aspart mix, 75/25 lispro mix, and 50/50 lispro mix), which provides coverage for both basal and prandial needs in a single injection [6,7,8,9,10]. For patients with T2DM who are unable to achieve glycemic control despite basal insulin titration, the addition of a GLP-1RA to the titrated basal insulin results in HbA1c reductions that are similar to those seen with standard basal-bolus or basal-plus insulin regimens, in conjunction with a lower relative risk of hypoglycemia and a greater decrease in body weight [54,55,56].
Table 3. Glucagon-like peptide 1 receptor agonists for patients with type 2 diabetes mellitus.
Mechanism and common use | Weight gain | Hypoglycemiaa | HbA1c reduction, %a | Side effects | Caution | |
---|---|---|---|---|---|---|
GLP-1 receptor agonist (exenatide, liraglutide, albiglutide, lixisenatide, dulaglutide) | ↑ Glucose-dependent insulin secretion, ↓ postprandial glucagon secretion, ↓ postprandial hyperglycemia, delay gastric emptying, ↑ satiety Once or twice daily or once weekly SC injection |
No | No | 0.6–1.9 | GI side effects (nausea, vomiting, diarrhea) | Acute pancreatitis, C-cell hyperplasia, MEN2/MTC family or past history, severe renal or severe bowel disease |
HbA1c, glycosylated hemoglobin; GLP-1, glucagon-like peptide 1; SC, subcutaneous; GI, gastrointestinal; MEN2, multiple endocrine neoplasia 2; MTC, medullary thyroid cancer.
aMonotherapy.
If glycemic control in patients treated with basal insulin alone or in combination with oral antihyperglycemic agents is not within the target range, treatment intensification via addition of a prandial insulin, such as a rapid-acting insulin analog (lispro, aspart, or glulisine), at the main meal (basal-plus) or at each meal (basal-bolus) is recommended (Table 4, Fig. 2). An insulin intensification strategy might also consist of upward titration of the insulin dose and regimen modification. As prandial insulin, rapid-acting insulin analogs are preferred to regular insulin because of their rapid onset, lower frequency of hypoglycemia, and ease of use (injection before meal) [6,7,8,9,10]. If the HbA1c goal is not reached following the administration of premixed insulin given twice daily, consider switching to a premixed insulin analog (70/30 aspart mix, 75/25 lispro mix, 50/50 lispro mix) given three times daily for intensification. There are no clinically relevant differences in terms of the efficacies of basal-bolus versus premixed insulin regimens for decreasing HbA1c levels in patients with T2DM [53].
Table 4. Properties of different insulins.
Insulin | Action | Maximal effect, hr | Action duration, hr |
---|---|---|---|
Prandial insulin analogs | |||
Rapid-acting analogs | |||
Aspart (NovoRapid) | 10–15 min | 1–1.5 | 3–5 |
Lispro (Humalog) | 10–15 min | 1–2 | 3.5–4.75 |
Glulisine (Apidra) | 10–15 min | 1–1.5 | 3–5 |
Short-acting insulin | |||
Humulin regular | 30 min | 2–3 | 6.5 |
Basal insulin | |||
Intermediate-acting Humulin N | 1–3 hr | 5–8 | Up to 18 |
Long-acting basal analogs | No | ||
Detemir (Levemir) | 90 min | 24 | |
Glargine (Lantus) | 90 min | 24 | |
Degludec (Tresiba) | 60–90 min | >42 | |
Gla-300 (Toujeo) | 6 hr | >36 | |
Mixed insulins | |||
Mixed insulin | |||
NPH/Regular 70/30 | Premixed insulin products contain both a basal and prandial insulin component to cover both basal and prandial glucose levels with a single injection | ||
Aspart 70/30 | |||
Lispro 75/25, 50/50 |
NPH, neutral protamine Hagedorn.
The effects of two insulin-based strategies, glargine once daily and premixed insulin once or twice daily, were compared in subjects with T2DM who did not achieve adequate glycemic control with oral agents. More patients using premixed insulin achieved their target, with less frequent symptomatic hypoglycemia, compared with glargine. Glargine (with or without glulisine) and premix strategies result in similar rates of well-controlled diabetes without hypoglycemia, in that more patients achieve their target HbA1c levels with premixed insulin, whereas overall symptomatic hypoglycemia occurs less frequently with glargine [40,53].
When deciding intensify an insulin regimen, physicians should consider the various advantages and disadvantages of each option, including flexibility, complexity, and the frequency of hypoglycemia. Furthermore, healthcare professionals should provide comprehensive self-care education that includes insulin injection skills, self-monitoring of blood glucose levels, hypoglycemia management, and simple dosage adjustment prior to the initiation of insulin therapy [57].
ACKNOWLEDGMENTS
Financial support for the development of these guidelines was provided by the KDA operating budget; there was no support or involvement from industry sources.
This position statement on antihyperglycemic agent therapy was written by the KDA Committee of Clinical Practice Guidelines. We gratefully acknowledge the following experts who provided a critical review and discussion of this update: Tae-Nyun Kim, Inje University College of Medicine, Busan; Yong-ho Lee, Severance Hospital, Yonsei University College of Medicine, Seoul; Jin-Hwa Kim, Chosun University Hospital, Chosun University College of Medicine, Gwangju; Eun-Gyoung Hong, Hallym University Dongtan Sacred Heart Hospital, Hallym University College of Medicine, Hwaseong; Jaetaek Kim, Chung-Ang University College of Medicine, Seoul; Won-Young Lee, Kangbuk Samsung Hospital, Sungkyunkwan University School of Medicine, Seoul; Bokrye Song, Seoul St. Mary's Hospital, College of Medicine, The Catholic University of Korea, Seoul; Ji Young Kim, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul; Dong Hee Yang, Inje University Ilsan Paik Hospital, Inje University College of Medicine, Goyang; Taeyoung Yang, Taeyoung 21 Hospital, Gwangju; and Hyeongjin Kim, Kim HJ Medical Clinic, Paju, Korea.
Footnotes
This manuscript is simultaneously published in the Diabetes Metabolism Journal and the Korean Journal of Internal Medicine by the Korean Diabetes Association and the Korean Association of Internal Medicine.
CONFLICTS OF INTEREST: No potential conflict of interest relevant to this article was reported.
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