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Diabetes mellitus

Last updated: May 14, 2025

Summarytoggle arrow icon

Diabetes mellitus (DM) describes a group of metabolic diseases that are characterized by chronic hyperglycemia. Type 1 diabetes mellitus (T1DM) is caused by an autoimmune response that triggers the destruction of insulin-producing beta cells in the pancreas and results in an absolute insulin deficiency. It often develops during childhood, manifesting with an acute onset (e.g., diabetic ketoacidosis). Type 2 diabetes mellitus (T2DM) is much more common, has a strong genetic component, and is associated with obesity and a sedentary lifestyle. T2DM is characterized by insulin resistance and impaired insulin secretion due to pancreatic beta-cell dysfunction, resulting in relative insulin deficiency. This type of diabetes usually remains undiagnosed for many years. Testing for hyperglycemia is recommended for patients with classic symptoms of diabetes mellitus, and screening is recommended for asymptomatic patients who are at high risk of prediabetes or diabetes (e.g., patients with obesity and additional risk factors). The diagnosis is made based on blood glucose or HbA1c levels. The main goal of treatment is blood glucose control tailored to glycemic targets while avoiding hypoglycemia. Diabetes care should be comprehensive and patient-centered and should include monitoring and management of ASCVD risk factors, microvascular complications (e.g., diabetic retinopathy, diabetic nephropathy, diabetic neuropathy), and macrovascular complications (e.g., coronary artery disease, stroke, peripheral artery disease). Management should also include general lifestyle modifications (e.g., smoking cessation, exercise, nutritional support) and pharmacological treatment (e.g., antihyperglycemics, statins, ACE inhibitors or angiotensin receptor blockers, and aspirin). The management of diabetes in children is largely similar to adults, except that certain medications (sulfonylureas, dipeptidyl peptidase-4 inhibitors, SGLT-2 inhibitors, and thiazolidinediones) are not approved for use in this age group.

See also “Diabetes in pregnancy,” “Insulin,” and “Hyperglycemic crises.”

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Overviewtoggle arrow icon

Type 1 vs Type 2 diabetes mellitus
Features Type 1 DM Type 2 DM [1]
Genetics
  • Negative HLA association
  • Strong familial predisposition [3]
  • Polygenic
Pathogenesis
Association with obesity
  • No
  • Yes
Onset
  • Childhood onset typically < 20 years but can occur at any age
  • Peaks at age 4–6 years and 10–14 years
  • Gradual; usually at age > 40 years
C-peptide (insulin)
  • Decreased or absent
  • Initially elevated, decreased in advanced stage
Glucose intolerance
  • Severe
  • Mild to moderate
Insulin sensitivity
  • High
  • Low
Risk of ketoacidosis
  • High
  • Low
β-cells in the islets
  • Decreased

Classic symptoms (i.e., polyuria, polydipsia, polyphagia, weight loss)

  • Common
  • Sometimes
Histology
  • Amyloidpolypeptide (IAPP) deposits in islets
Treatment
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Epidemiologytoggle arrow icon

Type 1 DM

  • Prevalence [4]
    • ∼ 1.6 million in the US
    • ∼ 5–10% of all patients with diabetes
  • Age [4]
    • Childhood onset typically < 20 years but can occur at any age
    • Peaks at age 4–6 years and 10–14 years
  • Race: highest prevalence in non-Hispanic White individuals [5]

Type 2 DM

  • Prevalence [4]
    • ∼ 10.5% of adult population in the US
    • Near 34 million individuals in the US have diabetes with 7.3 million being undiagnosed.
  • Incidence: ∼ 6.7 per 1,000 among the US adults [4]
  • Age
    • Adult onset typically > 40 years [5]
    • Mean age of onset is decreasing
  • Gender: > [4]
  • Race: highest prevalence in Native Americans, Hispanics, African Americans, and Asian non-Hispanic Americans [4]

Epidemiological data refers to the US, unless otherwise specified.

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Etiologytoggle arrow icon

Type 1 DM [6][7]

“If you buy 4 DiaMonds and only pay for 3, you get 1 for free:” DR4 and DR3 are associated with Diabetes Mellitus type 1.

Type 2 DM [8][9][10]

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Classificationtoggle arrow icon

Classification according to the WHO and American Diabetes Association (ADA) [10][15]

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Pathophysiologytoggle arrow icon

Normal insulin physiology [16]

Type 1 diabetes [6]

Type 2 diabetes

Mechanisms [5]

Progression [1]

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Clinical featurestoggle arrow icon

Clinical features of diabetes mellitus

Type 1 DM Type 2 DM [1]
Onset
  • Often sudden
  • Diabetic ketoacidosis (DKA) is the first manifestation in 25–50% of cases. [10]
  • Children may present with acute illness and classic symptoms.
  • Typically gradual
  • The majority of patients are asymptomatic.
  • Some patients may present with a hyperglycemic crisis.
    • Elderly patients especially may present in a hyperglycemic hyperosmolar state. [20]
    • Occasionally, patients with T2DM present with DKA , which mostly affects Black and Hispanic individuals. [21]
  • Symptoms of complications may be the first clinical sign of disease.
Clinical features
  • A thin appearance is typical for patients with T1DM.

Diabetes mellitus should be suspected in patients with recurrent cellulitis, candidiasis, dermatophyte infections, gangrene, pneumonia (particularly tuberculosis reactivation), influenza, genitourinary infections (UTIs), osteomyelitis, and/or vascular dementia.

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Screeningtoggle arrow icon

See “Hyperglycemia tests” for recommended screening methods.

Indications for diabetes screening [10]

The indications listed below are consistent with the 2025 ADA guidelines. The USPSTF recommends screening in adults aged 35–70 years with overweight or obesity. [10][24][25]

If results are normal, repeat testing in asymptomatic patients at least every three years. Patients with prediabetes should be tested annually. Patients with a history of gestational diabetes should be tested every 1–3 years. [10]

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Diagnosistoggle arrow icon

Diagnostic criteria for diabetes mellitus [10]

The following tests may be performed in combination for screening and/or diagnosis. If two separate blood samples are used, the second should be obtained soon after the first.

Hyperglycemia tests [10]

Blood glucose tests

  • Random blood glucose: blood glucose measured at any time irrespective of recent meals
  • Fasting plasma glucose (FPG): blood glucose measured after > 8 hours of fasting
    • Inexpensive and widely available
    • Should not be used to diagnose diabetes in hospitalized patients or in patients with critical illness
  • Oral glucose tolerance test (OGTT) [26]
    • Most sensitive test
    • Less convenient and more expensive than other tests
    • One-step OGTT: measurement of fasting plasma glucose and blood glucose 2 hours after the consumption of 75 g of glucose
    • Two-step OGTT: used in diagnosis of gestational diabetes
      • Nonfasting patients are given 50 g of glucose and blood glucose is measured after 1 hour.
      • If values at 1 hour are ≥ 130–140 mg/dL , measure fasting plasma glucose and blood glucose 1, 2, and 3 hours after the consumption of 100 g of glucose.
      • For interpretation of results, see “Diagnosis of gestational diabetes.”

Hemoglobin A1C (HbA1c or A1C)

Significant discrepancy between HbA1c and glucose measurements warrants investigation of the underlying cause (e.g., sickle cell trait).

Interpretation of hyperglycemia tests [10]
FPG 2-hour glucose value after one-step OGTT HbA1c
Diabetes mellitus ≥ 126 mg/dL (≥ 7.0 mmol/L) ≥ 200 mg/dL (≥ 11.1 mmol/L) ≥ 6.5%
Prediabetes 100–125 mg/dL (5.6–6.9 mmol/L) = impaired fasting glucose 140–199 mg/dL (7.8–11.0 mmol/L) = impaired glucose tolerance 5.7–6.4%
Normal < 100 mg/dL (< 5.6 mmol/L) < 140 mg/dL (< 7.8 mmol/L) < 5.7%

Additional recommended studies [29]

Perform in all patients as part of the initial diagnostic workup and reassess at least annually.

Additional optional studies

These tests are not routinely indicated or required to establish a diagnosis.

Screening for T1DM with autoantibodies is not routinely recommended but can be considered in patients with presymptomatic T1DM and increased genetic risk (e.g., first-degree relatives with T1DM). [10]

Consider specialist consultation if the differentiation between T2DM and T1DM is unclear.

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Differential diagnosestoggle arrow icon

The differential diagnoses listed here are not exhaustive.

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Managementtoggle arrow icon

General principles [29][34]

Diabetes care should be patient-centered and comprehensive and include lifestyle modifications and assessment of psychosocial health. Consider social determinants of health and formulate a treatment plan together with the patient.

The goals of diabetes management include eliminating symptoms of hyperglycemia, reducing or eliminating complications, and enabling as healthy a lifestyle as possible. [25]

Physical exercise reduces blood glucose and increases insulin sensitivity.

Lifestyle modifications [34]

Lifestyle recommendations for patients with diabetes mellitus [34]
Physical activity
  • Recommend regular exercise.
    • 75–180 minutes of aerobic exercise spread over ≥ 3 days per week
    • 2–3 sessions of resistance exercise per week
  • Recommend reducing sedentary time and increasing nonsedentary activities.
Balanced diet and nutrition
  • Refer to a registered nutritionist.
  • Individualize dietary recommendations taking into account the patient’s health status, preferences, and cultural background.
  • General recommendations include:
    • A high-fiber diet
    • Eating nonstarchy vegetables, whole foods
    • Avoiding refined sugar and grains
Weight management [38]
Other
  • Recommend smoking cessation for all patients; offer counseling if necessary. [39]
  • Advise against recreational cannabis in patients with T1DM or those risk for diabetic ketoacidosis. [34]
  • Alcohol consumption should be: [34]
    • Limited to a moderate intake
    • Consumed with food to avoid hypoglycemia, with glucose monitored after consumption
  • Provide psychosocial screening for patients and caregivers. [34]

Glycemic targets in diabetes [40][41]

  • Consider the following patient factors when setting a glycemic target:
    • Risk of hypoglycemia or other adverse effects
    • Presence of vascular complications and comorbidities
    • Patient preferences and resources
    • Disease duration
    • Life expectancy
  • Re-evaluate glycemic targets continuously and adjust if necessary.
Common glycemic targets [40]
HbA1c

< 7%: suitable for most patients [40][41]

Preprandial capillary glucose

80–130 mg/dL (4.4–7.2 mmol/L)

Peak postprandial capillary glucose

< 180 mg/dL (< 10.0 mmol/L)

Continuous glucose monitor

> 70% time in goal range (e.g., 70–180 mg/dL)

Glycemic targets should be individualized. A target of HbA1c < 7% is usually suitable for most nonpregnant adults. [40]

Assess for past hypoglycemic episodes or risk of hypoglycemia regularly and adjust glycemic goals accordingly. Hypoglycemia is one of the major limitations to adequate glycemic control. [40]In patients that meet preprandial glucose targets, HbA1c above target may be due to postprandial hyperglycemia, requiring prandial insulin dose adjustments.

Glycemic monitoring for diabetes [40][42]

HbA1c monitoring

HbA1c is measured at fixed intervals.

Fructosamine or continuous glucose monitoring may be used as alternatives to HbA1c if needed.

Home glucose monitoring

Glucose levels can be used to evaluate treatment and prevent hypoglycemia and hyperglycemia, especially in patients using insulin.

  • Self-monitoring of blood glucose: at fixed times or as needed
    • Indication: insulin therapy (particularly for intensive regimens)
    • Consider for any patient to assess for hypoglycemia or the impact of diet and/or exercise.
  • Continuous glucose monitoring: Interstitial glucose levels are measured continuously or intermittently using a subcutaneous device. [42]
    • Improves glycemic monitoring, which reduces the risk of hypoglycemia
    • Early use is recommended for adults with T1DM (can be used in combination with an insulin pump).
    • Advised for use in patients with diabetes on any form of insulin therapy
    • Consider in:
      • Patients with T2DM on noninsulin glucose-lowering drugs
      • Patients not meeting HbA1c targets

Hypoglycemia

  • Assess for episodes of hypoglycemia (symptomatic or asymptomatic) at every follow-up visit.
  • Prescribe glucagon for individuals taking insulin or at high-risk for hypoglycemic events
  • In patients with at least one clinically significant hypoglycemia event or asymptomatic hypoglycemia:
    • Check for possible contributors (e.g., medication interaction or errors).
    • Consider relaxing the glycemic targets and adjusting management.

Reassess and adjust treatment at regular intervals (e.g., every 3–6 months).

Early morning hyperglycemia

  • Early morning hyperglycemia may be caused by:
    • Dawn phenomenon
      • A physiological increase of growth hormone levels in the early morning hours stimulates hepatic gluconeogenesis and leads to a subsequent increase in insulin demand that cannot be met in insulin-dependent patients, resulting in elevated blood glucose levels.
      • Consider measurement of nocturnal blood glucose levels before initiating insulin therapy.
      • Long-acting insulin dose may be given later or increased under careful glycemic control.
    • Somogyi effect (widely taught but unproven hypothesis)
      • Description: Nocturnal hypoglycemia due to evening insulin injection triggers a counterregulatory secretion of hormones , leading to elevated blood glucose levels in the morning.
      • There is no evidence to support the existence of this effect. [43][44][45]

Do not assume that early morning hyperglycemia is due to nocturnal hypoglycemia. It is more likely caused by nocturnal hyperglycemia with or without hypoinsulinemia and/or early morning secretion of counterregulatory hormones (e.g., cortisol). [43][44][45]

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Glycemic treatmenttoggle arrow icon

This section outlines the approach to pharmacological treatment of diabetes mellitus.

Type 1 diabetes mellitus

Insulin replacement therapy [46]

Educate patients on calculating insulin requirements throughout the day based on activities and meals. [46]

Other treatment strategies [46]

Type 2 diabetes mellitus

Approach [46]

Noninsulin diabetes medications

Noninsulin diabetes medications [46]
Drug class

Examples

Important considerations
Biguanides
Dipeptidyl peptidase-4 inhibitor
SGLT-2 inhibitors
GLP-1 receptor agonists
  • Recommend in patients with [46]
  • Beneficial for patients who need to lose or maintain their weight
Sulfonylureas
Thiazolidinedione

Oral monotherapy usually lowers HbA1c levels by ∼ 1%. Every noninsulin drug added to metformin will lower the HbA1c by an additional 0.7–1.0%. [46]

Beware of drug interactions and drug incompatibilities; combining sulfonylureas with insulin increases the risk for hypoglycemia. [50]

Many oral diabetes medications should be avoided in patients undergoing surgery or experiencing severe illness; consider insulin therapy instead.

Indications for insulin therapy in T2DM [46]

Approach to insulin treatment in T2DM [46]

Include GLP-1 receptor agonists in the treatment strategy prior to starting insulin therapy in patients with T2DM, unless they are inappropriate or insulin therapy is preferred.

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Screening for complications of diabetestoggle arrow icon

Screening for microvascular complications of diabetes

Screening for macrovascular complications of diabetes [36]

  • Check BP at every clinic appointment and encourage patients with elevated BP to measure blood pressure at home.
  • Obtain a lipid panel at the time of diabetes diagnosis and repeat every 5 years for patients < 40 years.
  • Screening for cardiovascular disease is not recommended for asymptomatic individuals. [36]
  • Consider screening asymptomatic individuals for cardiovascular disease on a case-by-case basis:
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T2DM (outpatient management)

Assessment: This is a @AGE@-year-old @SEX@ with T2DM diagnosed in [**year] presenting for routine management.

–Current glycemic control: [HbA1c **%, fasting glucose mg/dL]

–Symptoms: [**asymptomatic, polyuria, polydipsia, fatigue]

–Complications: [**none, neuropathy, nephropathy, retinopathy]

–Comorbidities: [**hypertension, dyslipidemia, obesity]

Plan

Glycemic management

–Target HbA1c: < [**%]

–Nutrition counseling

–≥ 150 minutes of moderate-intensity aerobic activity per week

Current medications

Metformin [** mg **FREQUENCY]

GLP-1 receptor agonist: [**liraglutide or semaglutide] for cardiovascular benefit, weight loss

SGLT2 inhibitor: [empagliflozin or dapagliflozin [** mg] once daily] for renal and cardiovascular benefit

DPP-4 inhibitor (if GLP-1 not available or tolerated): [sitagliptin]

–Basal insulin (consider if HbA1c remains > 10% or significant symptoms of hyperglycemia)

Sulfonylureas: e.g., glimepiride (cheaper option; monitor for hypoglycemia)

Monitoring for complications

HbA1c: every 3–6 months [**last date]

Fasting lipid panel: annually [**last date]

BMP: annually, or more frequently if CKD is present [**last date]

–Urine ACR: annually [**last date]

–Comprehensive foot exam: annually [**last date]

–Dilated eye exam: annually or every 2 years if low risk [**last date]

–BP, weight, BMI: every visit

ECG [for patients with cardiovascular risk factors]: [**last date]

Cardiovascular risk management

–Target blood pressure: < [**140/90] mm Hg

–[Lisinopril ** mg PO once daily] for patients with albuminuria or hypertension

–High-intensity statin: [atorvastatin ** mg once daily] for all patients with diabetes aged ≥ 40 years

Ezetimibe or PCSK9 inhibitors for LDL ≥ 70 mg/dL despite maximally tolerated statin

–[Aspirin ** mg once daily] for ASCVD prevention

Education and support

–Glucose monitoring: Review frequency and goals for self-monitoring.

–Reinforce signs of hypoglycemia and hyperglycemia and when to seek care.

Immunizations

Influenza: annually

Pneumococcal: for all adults with diabetes

Hepatitis B: series for all adults with diabetes aged ≤ 59 years

Follow-up

–Routine follow-up in [** months] for glycemic control

–Follow-up sooner if symptomatic hyperglycemia or significant therapy adjustments.

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Complicationstoggle arrow icon

Acute complications

Long-term complications [60]

Macrovascular disease (atherosclerosis)

Microvascular disease

Strict glycemic control is crucial in preventing microvascular disease.

Necrobiosis lipoidica [61]

Other complications

Insulin purging [66]

We list the most important complications. The selection is not exhaustive.

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Prognosistoggle arrow icon

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Special patient groupstoggle arrow icon

For management in pregnancy, see “Diabetes in pregnancy.”

Diabetes mellitus in children

The following recommendations are for children and adolescents with T1DM and T2DM. Management of other forms of diabetes in children (e.g., diabetes associated with transplantation or cystic fibrosis) is not addressed here.

Screening indications [11][55][67]

For screening modalities, see “Diagnostics” below.

Diagnostics [11]

Management [35][55]

Diabetes management in children is generally similar to adults, with the following modifications.

Screening and management of associated conditions [55]

Educate all individuals involved in the care of the patient (e.g., family members, school, and childcare personnel) about the treatment plan. [55]

Antidiabetic treatment [55]

Patients with T2DM presenting with diabetic ketoacidosis should be treated with insulin alone. Metformin may be added after acidosis resolves. [55]

T2DM is rare in children under 10 years of age; consider consulting a specialist to determine treatment, as neither metformin nor GLP-1 receptor agonists are FDA-approved for use in this age group.

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