Diabetes mellitus: Difference between revisions

	Diabetes mellitus Main page
Patient Information Type 1 Type 2
Overview
Classification Diabetes mellitus type 1 Diabetes mellitus type 2 Gestational diabetes
Differential Diagnosis
Complications
Screening
Diagnosis
Prevention

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Latest revision as of 12:57, 9 September 2020

This page contains general information about Diabetes mellitus. For more information on specific types, please visit the pages:

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Seyedmahdi Pahlavani, M.D. [2]Mehrian Jafarizade, M.D [3]

Synonyms and keywords: Diabetes; DM

Overview

Diabetes mellitus (DM) refers to a spectrum of disorders with different metabolic changes that result in hyperglycemia as a common feature. It is caused by interaction of environmental agents in a genetically susceptible person. The metabolic disarrangement that may result in hyperglycemia will define the pathologic feature of each type of DM. Decreased insulin secretion, insulin resistance, decreased glucose utilization and increased glucose production are the main metabolic dysregulations that are known to cause hyperglycemia.

Hyperglycemia may cause secondary changes in metabolic arrangement in different systems and it can involve every organ systems. DM is the leading cause of end-stage renal disease (ESRD), non-traumatic lower extremity amputations, and adult blindness worldwide.

Accordingly, early diagnosis and treatment can result in significant decrease in mortality and morbidity. The incidence of diabetes has been increased constantly. According to WHO reports, 346 million people worldwide have diabetes and it is projected to double by 2030. It's prevalence is more in developed countries but the death occurring from DM complications is more common in developing countries.

The prevalence of diabetes type 2 is more common than type 1 diabetes. Diabetes can cause many complications. Acute complications (hypoglycemia, ketoacidosis or nonketotic hyperosmolar coma) may occur if the disease is not adequately controlled.^[1] Serious long-term complications include macrovascular (coronary heart disease, peripheral arterial disease and cerebrovascular disease), microvascular (retinopathy, neuropathy and nephropathy) and other organ involvement (gastrointestinal, genitourinary, dermatologic, infectious, cataracts, glaucoma, periodontal disease and hearing loss). The main goals of treatment are:

Elimination of hyperglycemic symptoms
Control of the long term complications
Improvement of the patient's quality of life

Classification

Diabetes mellitus is classified into 3 types based on the pathogenic process that lead to hyperglycemia:

Differential diagnosis

Disease	History and symptoms					Laboratory findings								Additional findings
Disease	Polyuria	Polydipsia	Polyphagia	Weight loss	Weight gain	Serum glucose	Urinary Glucose	Urine PH	Serum Sodium	Urinary Glucose	24 hrs cortisol level	C-peptide level	Serum glucagon	Additional findings
Type 1 Diabetes mellitus	+	+	+	+	-	↑	↑	Normal	Normal	N/↑	Normal	↓	Normal	Auto antibodies present (Anti GAD-65 and anti insulin anti bodies)
Type 2 Diabetes mellitus	+	+	+	+	-	↑	↑	Normal	Normal	↑	Normal	Normal	↑	Acanthosis nigricans
MODY	+	+	+	-	+	↑	↑	Normal	Normal	↑	Normal	Normal	N	-
Psychogenic polydipsia	+	+	-	-	-	Normal	Normal	Normal	↓	Normal	Normal	Normal	Normal	-
Diabetes insipidus	+	+	-	-	-	Normal	Normal	Normal	↑	Normal	Normal	Normal	Normal	-
Transient hyperglycemia	-	-	-	-	-	↑	↑	Normal	Normal	↑	Normal	Normal	N/↑	In hospitalized patients especially in ICU and CCU
Steroid therapy	+	-	-	-	+	↑	↑	Normal	Normal	↑	↑	N/↑	N/↑	Acanthosis nigricans,
RTA 1	-	-	-	+	-	Normal	Normal	↑	Normal	↑	Normal	Normal	Normal	Hypokalemia, nephrolithiasis
Glucagonoma	-	-	-	-	-	↑	Normal	Normal	Normal	-	Normal	Normal	↑	Necrolytic migratory erythema
Cushing syndrome	-	-	-	-	+	↑	-	Normal	↓	N/↑	↑	Normal	Normal	Moon face, obesity, buffalo hump, easy bruisibility

Complications

Complications of diabetes mellitus may be classified as acute or chronic. Acute complications of diabetes mellitus may occur in type 1, type 2, or gestational diabetes. Chronic complications of diabetes mellitus are more likely to occur in long standing type 1 or type 2 diabetes and may be further classified as macrovascular, microvascular, or other (unspecified etiology) as follows:^[2]^[3]^[4]

Acute complications

They include diabetic ketoacidosis (DKA) and Hyperosmolar hyperglycemic state (HHS). DKA could be the presenting feature of type 1 diabetes and it is more common in type 1 diabetes although, it is sometimes seen in type 2 diabetic patients. HHS is mostly seen in the elderly and it is more common in type 2 diabetes.

Chronic complications

Macrovascular

Microvascular

Ophthalmic

Retinopathy (nonproliferative/proliferative)^[6]
Macular edema^[6]

Neuropathy

Sensory and motor (mono- and polyneuropathy)^[6]
Autonomic neuropathy^[6]

Nephropathy

Albuminuria and declining renal function^[6]

Other organs^[6]

Complications of gestational diabetes differs from type 1 and type 2 diabetes primarily due to its pregnancy-specific effects on the mother as well as its effects on the fetus.

For more information on maternal complications of gestational diabetes click here.
For more information on fetal complications of gestational diabetes click here.

Diagnosis

Diabetes mellitus type 1 and type 2

A fasting plasma glucose (FPG) <5.6 mmol/L (100 mg/dL), a plasma glucose <140 mg/dL (11.1 mmol/L) following an oral glucose challenge and an HbA1c <5.7% are considered normal.
Diagnostic criteria for DM are:
- Symptoms of diabetes plus random blood glucose concentration ≥11.1 mmol/L (200 mg/dL)^† OR
- Fasting plasma glucose ≥7.0 mmol/L (126 mg/dL)^‡ OR
- Hemoglobin A1c ≥ 6.5% OR
- 2-hoursplasma glucose ≥11.1 mmol/L (200 mg/dL) during an oral glucose tolerance test^¶

American Diabetes Association Diabetes Diagnostic Criteria 2018 (DO NOT EDIT)

ADA evidence-grading system for “Standards of Medical Care in Diabetes”
Level of evidence	Description
A	Clear evidence from well-conducted, generalizable randomized controlled trials that are adequately powered, including Evidence from a well-conducted multi-center trial Evidence from a meta-analysis that incorporated quality ratings in the analysis Compelling non-experimental evidence, i.e., “all or none” rule developed by the Center for Evidence-Based Medicine at the University of Oxford. Supportive evidence from well-conducted randomized controlled trials that are adequately powered, including Evidence from a well-conducted trial at one or more institutions Evidence from a meta-analysis that incorporated quality ratings in the analysis
B	Supportive evidence from well-conducted cohort studies Evidence from a well-conducted prospective cohort study or registry Evidence from a well-conducted meta-analysis of cohort studies Supportive evidence from a well-conducted case-control study
C	Supportive evidence from poorly controlled or uncontrolled studies Evidence from randomized clinical trials with one or more major or three or more minor flaws that could invalidate the results Evidence from observational studies with high potential for bias (such as case series with comparison with historical controls) Evidence from case series or case reports Conflicting evidence with the weight of evidence supporting the recommendation
D	Supportive evidence from poorly controlled or uncontrolled studies Evidence from randomized clinical trials with one or more major or three or more minor methodological flaws that could invalidate the results Evidence from observational studies with high potential for bias (such as case series with comparison with historical controls) Evidence from case series or case reports Conflicting evidence with the weight of evidence supporting the recommendation
E	Expert consensus or clinical experience

Recommendations for HbA1c:
- To avoid misdiagnosis or missed diagnosis, the A1C test should be performed using a method that is certified by the NGSP and standardized to the Diabetes Control and Complications Trial (DCCT) assay. B
- Marked discordance between measured A1C and plasma glucose levels should raise the possibility of A1C assay interference due to hemoglobin variants (i.e., hemoglobinopathies) and consideration of using an assay without interference or plasma blood glucose criteria to diagnose diabetes. B
- In conditions associated with increased red blood cell turnover, such as sickle cell disease, pregnancy (second and third trimesters), hemodialysis, recent blood loss or transfusion, or erythropoietin therapy, only plasma blood glucose criteria should be used to diagnose diabetes. B

Note:
†:Random is defined as without regard to time since the last meal.

‡:Fasting is defined as no caloric intake for at least 8 hours.

¶:The test should be performed using a glucose load containing the equivalent of 75 g anhydrous glucose dissolved in water, not recommended for routine clinical use.

American Diabetes Association Diabetes Diagnostic Criteria 2018 (DO NOT EDIT)^[6]

Criteria for the diagnosis of diabetes
FPG ≥126 mg/dL (7.0 mmol/L). Fasting is defined as no caloric intake for at least 8 hours.
OR
2-h Plasma Glucose (PG) ≥200 mg/dL (11.1 mmol/L) during an OGTT. The test should be performed as described by the WHO, using a glucose load containing the equivalent of 75 g anhydrous glucose dissolved in water.
OR
A1C ≥6.5% (48 mmol/mol). The test should be performed in a laboratory using a method that is NGSP certified and standardized to the DCCT assay. In the absence of unequivocal hyperglycemia, results should be confirmed by repeat testing.
OR
In a patient with classic symptoms of hyperglycemia or hyperglycemic crisis, a random plasma glucose ≥200 mg/dL (11.1 mmol/L).

Gestational diabetes

There are 2 strategies to confirm the GDM diagnosis.
- One-step 75-g Oral glucose tolerance test (OGTT) OR
- Two-step approach with a 50-g (non-fasting) screen followed by a 100-g OGTT for those who screen positive.^[7]

One Step Strategy

Perform a 75 g glucose tolerance test in 24-28 weeks of pregnancy and read the measures 1 h and 2 hours after glucose ingestion as well as fasting glucose.^[7] The OGTT should be performed in the morning after an overnight fast of at least 8 hours. The diagnosis of GDM is made when any of the following plasma glucose values are met or exceeded:
- Fasting: 92 mg/dL (5.1 mmol/L)
- 1 hour: 180 mg/dL (10.0 mmol/L)
- 2 hours: 153 mg/dL (8.5 mmol/L)

Two Step Strategy

In this approach, screening with a 1 hour 50-g glucose load test (GLT) followed by a 3 hours 100-g OGTT for those who screen positive.^[8]

The diagnosis of GDM is made when at least 2 out of 4 measures of 3 hours 100-g OGTT became abnormal.

The following table summarizes the diagnostic approach for gestational diabetes.

	Cut off (mg/dl)
	Fasting	1 Hour	2 Hours	3 Hours
One step test 2 hour 75 g glucose tolerance test	92	180	153	----
Two step test 1 hour 50 g screening test	----	140	----	----
3 hour 100 g test if screening test became positive Carpenter/Coustan approach^[9]	95	180	155	140
National Diabetes Data Group (NDDG) approach^[10]	105	190	165	145

Screening

Comparing developed and developing countries shows lower rate of progression from glucose intolerance to diabetes, due to better screening in developed and high-income areas.^[11]

Diabetes mellitus type 1

According to the American Diabetic Association, screening for type 1 DM is not recommended.

Diabetes mellitus type 2

Screening is recommended for many people at various stages of life, and for those with risk factors. American Diabetes Association Recommendations for Diabetes screening include:^[12]^[13]^[14]^[15]

Categories of Increased Risk for Diabetes (Prediabetics) Recommendations:

Screening for prediabetes and risk for future diabetes with an informal assessment of risk factors or validated tools should be considered in asymptomatic adults. B

Testing for prediabetes and risk for future diabetes in asymptomatic people should be considered in adults of any age who are overweight or obese (BMI >25 kg/m2 or >23 kg/m2 in Asian Americans) and who have one or more additional risk factors for diabetes. B
For all people, testing should begin at age 45 years. B
If tests are normal, repeat testing carried out at a minimum of 3-year intervals is reasonable. C
To test for prediabetes, fasting plasma glucose, 2-hours plasma glucose during 75-g oral glucose tolerance test, and HbA1C are equally appropriate. B
In prediabetic patients, identify and, if appropriate, treat other risk factors of cardiovascular disease. B
Testing for prediabetes should be considered in children and adolescents who are overweight or obese (BMI = 85th percentile for age and sex, weight for height = 85th percentile, or weight 120% of ideal for height) and who have additional risk factors for diabetes (Table 2.5). E

ADA 2018 [DO NOT EDIT]
Criteria for testing for diabetes or prediabetes in asymptomatic adults
1. Testing should be considered in overweight or obese (BMI 25 kg/m2 or 23 kg/m2 in Asian Americans) adults who have one or more of the following risk factors: First-degree relative with diabetes High-risk race/ethnicity (e.g., African American, Latino, Native American, Asian American, Pacific Islander) History of CVD Hypertension (140/90 mmHg or on therapy for hypertension) HDL cholesterol level <35 mg/dL (0.90 mmol/L) and/or a triglyceride level >250 mg/dL (2.82 mmol/L) Women with polycystic ovary syndrome Physical inactivity Other clinical conditions associated with insulin resistance (e.g., severe obesity, acanthosis nigricans)
2. Patients with prediabetes (A1C > 5.7% [39 mmol/mol], IGT, or IFG) should be tested yearly.
3. Women who were diagnosed with GDM should have lifelong testing at least every 3 years.
4. For all other patients, testing should begin at age 45 years.
5. If results are normal, testing should be repeated at a minimum of 3-year intervals, with consideration of more frequent testing depending on initial results and risk status.

To test for type 2 diabetes, fasting plasma glucose, 2-h plasma glucose after 75-g oral glucose tolerance test, and HbA1C are equally appropriate.


Categories of increased risk for diabetes (prediabetes)
FPG 100 mg/dL (5.6 mmol/L) to 125 mg/dL (6.9 mmol/L) (IFG)
OR
2-h PG during 75-g OGTT 140 mg/dL (7.8 mmol/L) to 199 mg/dL (11.0 mmol/L) (IGT)
OR
A1C 5.7–6.4% (39–47 mmol/mol)

Gestational diabetes

All pregnant women should be screened for gestational diabetes in 24-28 weeks with 50 gram glucose test. Measurements greater than 130 mg/dL are considered positive and should proceed to 100 gram glucose test for diagnosis. High risk mothers should be screened as early as the first prenatal visit. These risk factors include:^[16]^[17]
- A family history of diabetes especially in first degree relatives
- Maternal age >25 yrs
- Certain ethnic groups (such as Native American, Hispanic-American, African-American, South or East Asian, Pacific Islander)
- Body mass index greater than 25 kg/m²
- Gestational diabetes or impaired glucose tolerance test in previous pregnancies
- Previous delivery of a baby >9 pounds
- Personal history of impaired glucose tolerance or impaired fasting glucose (pre-diabetes)
- Glycosuria at the first prenatal visit
- Certain medical conditions (such as metabolic syndrome, polycystic ovary syndrome (PCOS), current use of glucocorticoids, hypertension)
- Previous history of unexplained miscarriage or stillbirth
- Smoking doubles the risk of gestational diabetes
- Multiple gestation
- Genetic predisposition (.e.g. glucokinase mutation)

Prevention

Life style modification is the mainstay of prevention of diabetes mellitus. It includes, changes in diet, weight reduction and exercise.
The strongest evidence for diabetes prevention comes from the Diabetes Prevention Program (DPP). The DPP demonstrated that an intensive lifestyle intervention could reduce the incidence of type 2 diabetes by 58% over 3 years.^[18]
Based on a study, life style modification can improve glucose tolerance and decrease the cardiovascular complications. Even obese diabetic patients in this study showed reduced chance of diabetes mellitus development after 2 years of life style interventions.^[19]
Patients with a modified life style had 58% less chance to develop diabetes, compared to the control group after a 3 years study.^[20] This life style modification includes physical activity, weight loss, limiting the total dietary intake, lowering intake of saturated fat and increasing dietary fiber.^[21]
Traditionally, life style modifications mainly focused on weight loss, which is still one of the main components. Nevertheless other factors, such as better glycemic control, careful food selection, regular physical activity and consistent visits and behavioral interventions to maintain adherence are also considered crucial in new approaches.^[22]
Intensive interdisciplinary intervention (II) on dietary habits and physical activity was related to lower blood pressure, plasma glucose and binge eating disorder (BED) frequency, compared to 9-month traditional (TI) intervention in patients at risk for diabetes. Furthermore, both interventions were effective in lowering the frequency of depression in these people.^[23]
Study on aspirin in diabetic patients with no previous history of cardiovascular disease showed significant reduction in serious vascular events. Nevertheless, the high risk of bleeding with aspirin use overshadows this desirable outcome.^[24]
An intervention done on 682 patients with impaired glucose tolerance test, evaluated the effect of acarbose as a possible agent for preventing the diabetes development. Based on this study, after 3 months, patients who received acarbose showed significant conversion to normal glucose level. On the other hand, patients who received placebo, had increased conversion to diabetic states.^[25]

References

↑ Pasquale LR, Kang JH, Manson JE, Willett WC, Rosner BA, Hankinson SE (2006). "Prospective study of type 2 diabetes mellitus and risk of primary open-angle glaucoma in women". Ophthalmology. 113 (7): 1081–6. doi:10.1016/j.ophtha.2006.01.066. PMID 16757028.
↑ Seshasai SR, Kaptoge S, Thompson A, Di Angelantonio E, Gao P, Sarwar N, Whincup PH, Mukamal KJ, Gillum RF, Holme I, Njølstad I, Fletcher A, Nilsson P, Lewington S, Collins R, Gudnason V, Thompson SG, Sattar N, Selvin E, Hu FB, Danesh J (2011). "Diabetes mellitus, fasting glucose, and risk of cause-specific death". N. Engl. J. Med. 364 (9): 829–41. doi:10.1056/NEJMoa1008862. PMC 4109980. PMID 21366474.
↑ Franco OH, Steyerberg EW, Hu FB, Mackenbach J, Nusselder W (2007). "Associations of diabetes mellitus with total life expectancy and life expectancy with and without cardiovascular disease". Arch. Intern. Med. 167 (11): 1145–51. doi:10.1001/archinte.167.11.1145. PMID 17563022.
↑ Livingstone SJ, Levin D, Looker HC, Lindsay RS, Wild SH, Joss N, Leese G, Leslie P, McCrimmon RJ, Metcalfe W, McKnight JA, Morris AD, Pearson DW, Petrie JR, Philip S, Sattar NA, Traynor JP, Colhoun HM (2015). "Estimated life expectancy in a Scottish cohort with type 1 diabetes, 2008-2010". JAMA. 313 (1): 37–44. doi:10.1001/jama.2014.16425. PMC 4426486. PMID 25562264.
↑ Nicolucci A (2008). "Aspirin for primary prevention of cardiovascular events in diabetes: still an open question". JAMA. 300 (18): 2180–1. doi:10.1001/jama.2008.625. PMID 18997199.
↑ ^6.0 ^6.1 ^6.2 ^6.3 ^6.4 ^6.5 ^6.6 ^6.7 ^6.8 "Standards of Medical Care in Diabetes-2017: Summary of Revisions". Diabetes Care. 40 (Suppl 1): S4–S5. 2017. doi:10.2337/dc17-S003. PMID 27979887.
↑ ^7.0 ^7.1 "Standards of Medical Care in Diabetes-2016 Abridged for Primary Care Providers". Clin Diabetes. 34 (1): 3–21. 2016. doi:10.2337/diaclin.34.1.3. PMID 26807004.
↑ "Professional Practice Committee for the Standards of Medical Care in Diabetes-2016". Diabetes Care. 39 Suppl 1: S107–8. 2016. doi:10.2337/dc16-S018. PMID 26696673.
↑ Carpenter MW, Coustan DR (1982). "Criteria for screening tests for gestational diabetes". Am. J. Obstet. Gynecol. 144 (7): 768–73. PMID 7148898.
↑ "Classification and diagnosis of diabetes mellitus and other categories of glucose intolerance. National Diabetes Data Group". Diabetes. 28 (12): 1039–57. 1979. PMID 510803.
↑ Liu, Xiaoqian; Li, Changping; Gong, Hui; Cui, Zhuang; Fan, Linlin; Yu, Wenhua; Zhang, Cui; Ma, Jun (2013). "An economic evaluation for prevention of diabetes mellitus in a developing country: a modelling study". BMC Public Health. 13 (1). doi:10.1186/1471-2458-13-729. ISSN 1471-2458.
↑ "2. Classification and Diagnosis of Diabetes". Diabetes Care. 40 (Suppl 1): S11–S24. 2017. doi:10.2337/dc17-S005. PMID 27979889.
↑ "International Expert Committee report on the role of the A1C assay in the diagnosis of diabetes". Diabetes Care. 32 (7): 1327–34. 2009. doi:10.2337/dc09-9033. PMC 2699715. PMID 19502545.
↑ Schellenberg ES, Dryden DM, Vandermeer B, Ha C, Korownyk C (2013). "Lifestyle interventions for patients with and at risk for type 2 diabetes: a systematic review and meta-analysis". Ann. Intern. Med. 159 (8): 543–51. doi:10.7326/0003-4819-159-8-201310150-00007. PMID 24126648.
↑ Perreault L, Pan Q, Mather KJ, Watson KE, Hamman RF, Kahn SE (2012). "Effect of regression from prediabetes to normal glucose regulation on long-term reduction in diabetes risk: results from the Diabetes Prevention Program Outcomes Study". Lancet. 379 (9833): 2243–51. doi:10.1016/S0140-6736(12)60525-X. PMC 3555407. PMID 22683134.
↑ "2. Classification and Diagnosis of Diabetes". Diabetes Care. 39 Suppl 1: S13–22. 2016. doi:10.2337/dc16-S005. PMID 26696675.
↑ Moyer VA (2014). "Screening for gestational diabetes mellitus: U.S. Preventive Services Task Force recommendation statement". Ann. Intern. Med. 160 (6): 414–20. doi:10.7326/M13-2905. PMID 24424622.
↑ Lindström J, Ilanne-Parikka P, Peltonen M, Aunola S, Eriksson JG, Hemiö K, Hämäläinen H, Härkönen P, Keinänen-Kiukaanniemi S, Laakso M, Louheranta A, Mannelin M, Paturi M, Sundvall J, Valle TT, Uusitupa M, Tuomilehto J (2006). "Sustained reduction in the incidence of type 2 diabetes by lifestyle intervention: follow-up of the Finnish Diabetes Prevention Study". Lancet. 368 (9548): 1673–9. doi:10.1016/S0140-6736(06)69701-8. PMID 17098085.
↑ Lindstrom, J. (2003). "Prevention of Diabetes Mellitus in Subjects with Impaired Glucose Tolerance in the Finnish Diabetes Prevention Study: Results From a Randomized Clinical Trial". Journal of the American Society of Nephrology. 14 (90002): 108S–113. doi:10.1097/01.ASN.0000070157.96264.13. ISSN 1046-6673.
↑ Tuomilehto, Jaakko; Lindström, Jaana; Eriksson, Johan G.; Valle, Timo T.; Hämäläinen, Helena; Ilanne-Parikka, Pirjo; Keinänen-Kiukaanniemi, Sirkka; Laakso, Mauri; Louheranta, Anne; Rastas, Merja; Salminen, Virpi; Aunola, Sirkka; Cepaitis, Zygimantas; Moltchanov, Vladislav; Hakumäki, Martti; Mannelin, Marjo; Martikkala, Vesa; Sundvall, Jouko; Uusitupa, Matti (2001). "Prevention of Type 2 Diabetes Mellitus by Changes in Lifestyle among Subjects with Impaired Glucose Tolerance". New England Journal of Medicine. 344 (18): 1343–1350. doi:10.1056/NEJM200105033441801. ISSN 0028-4793.
↑ "Primary Prevention of Type 2 Diabetes Mellitus by Lifestyle Intervention: Implications for Health Policy". Annals of Internal Medicine. 140 (11): 951. 2004. doi:10.7326/0003-4819-140-11-200406010-00036. ISSN 0003-4819.
↑ Buse, John B.; Ginsberg, Henry N.; Bakris, George L.; Clark, Nathaniel G.; Costa, Fernando; Eckel, Robert; Fonseca, Vivian; Gerstein, Hertzel C.; Grundy, Scott; Nesto, Richard W.; Pignone, Michael P.; Plutzky, Jorge; Porte, Daniel; Redberg, Rita; Stitzel, Kimberly F.; Stone, Neil J. (2007). "Primary Prevention of Cardiovascular Diseases in People With Diabetes Mellitus". Circulation. 115 (1): 114–126. doi:10.1161/CIRCULATIONAHA.106.179294. ISSN 0009-7322.
↑ Cezaretto, Adriana; Siqueira-Catania, Antonela; de Barros, Camila Risso; Salvador, Emanuel Péricles; Ferreira, Sandra Roberta G. (2011). "Benefits on quality of life concomitant to metabolic improvement in intervention program for prevention of diabetes mellitus". Quality of Life Research. 21 (1): 105–113. doi:10.1007/s11136-011-9919-2. ISSN 0962-9343.
↑ "Effects of Aspirin for Primary Prevention in Persons with Diabetes Mellitus". New England Journal of Medicine. 379 (16): 1529–1539. 2018. doi:10.1056/NEJMoa1804988. ISSN 0028-4793.
↑ Chiasson, Jean-Louis; Josse, Robert G; Gomis, Ramon; Hanefeld, Markolf; Karasik, Avraham; Laakso, Markku (2002). "Acarbose for prevention of type 2 diabetes mellitus: the STOP-NIDDM randomised trial". The Lancet. 359 (9323): 2072–2077. doi:10.1016/S0140-6736(02)08905-5. ISSN 0140-6736.

[pmid16757028-1] Pasquale LR, Kang JH, Manson JE, Willett WC, Rosner BA, Hankinson SE (2006). "Prospective study of type 2 diabetes mellitus and risk of primary open-angle glaucoma in women". Ophthalmology. 113 (7): 1081–6. doi:10.1016/j.ophtha.2006.01.066. PMID 16757028.

[pmid21366474-2] Seshasai SR, Kaptoge S, Thompson A, Di Angelantonio E, Gao P, Sarwar N, Whincup PH, Mukamal KJ, Gillum RF, Holme I, Njølstad I, Fletcher A, Nilsson P, Lewington S, Collins R, Gudnason V, Thompson SG, Sattar N, Selvin E, Hu FB, Danesh J (2011). "Diabetes mellitus, fasting glucose, and risk of cause-specific death". N. Engl. J. Med. 364 (9): 829–41. doi:10.1056/NEJMoa1008862. PMC 4109980. PMID 21366474.

[pmid17563022-3] Franco OH, Steyerberg EW, Hu FB, Mackenbach J, Nusselder W (2007). "Associations of diabetes mellitus with total life expectancy and life expectancy with and without cardiovascular disease". Arch. Intern. Med. 167 (11): 1145–51. doi:10.1001/archinte.167.11.1145. PMID 17563022.

[pmid25562264-4] Livingstone SJ, Levin D, Looker HC, Lindsay RS, Wild SH, Joss N, Leese G, Leslie P, McCrimmon RJ, Metcalfe W, McKnight JA, Morris AD, Pearson DW, Petrie JR, Philip S, Sattar NA, Traynor JP, Colhoun HM (2015). "Estimated life expectancy in a Scottish cohort with type 1 diabetes, 2008-2010". JAMA. 313 (1): 37–44. doi:10.1001/jama.2014.16425. PMC 4426486. PMID 25562264.

[pmid18997199-5] Nicolucci A (2008). "Aspirin for primary prevention of cardiovascular events in diabetes: still an open question". JAMA. 300 (18): 2180–1. doi:10.1001/jama.2008.625. PMID 18997199.

[pmid27979887-6] 6.0 ^6.1 ^6.2 ^6.3 ^6.4 ^6.5 ^6.6 ^6.7 ^6.8 "Standards of Medical Care in Diabetes-2017: Summary of Revisions". Diabetes Care. 40 (Suppl 1): S4–S5. 2017. doi:10.2337/dc17-S003. PMID 27979887.

[pmid26807004-7] 7.0 ^7.1 "Standards of Medical Care in Diabetes-2016 Abridged for Primary Care Providers". Clin Diabetes. 34 (1): 3–21. 2016. doi:10.2337/diaclin.34.1.3. PMID 26807004.

[pmid26696673-8] "Professional Practice Committee for the Standards of Medical Care in Diabetes-2016". Diabetes Care. 39 Suppl 1: S107–8. 2016. doi:10.2337/dc16-S018. PMID 26696673.

[pmid7148898-9] Carpenter MW, Coustan DR (1982). "Criteria for screening tests for gestational diabetes". Am. J. Obstet. Gynecol. 144 (7): 768–73. PMID 7148898.

[pmid510803-10] "Classification and diagnosis of diabetes mellitus and other categories of glucose intolerance. National Diabetes Data Group". Diabetes. 28 (12): 1039–57. 1979. PMID 510803.

[LiuLi2013-11] Liu, Xiaoqian; Li, Changping; Gong, Hui; Cui, Zhuang; Fan, Linlin; Yu, Wenhua; Zhang, Cui; Ma, Jun (2013). "An economic evaluation for prevention of diabetes mellitus in a developing country: a modelling study". BMC Public Health. 13 (1). doi:10.1186/1471-2458-13-729. ISSN 1471-2458.

[pmid27979889-12] "2. Classification and Diagnosis of Diabetes". Diabetes Care. 40 (Suppl 1): S11–S24. 2017. doi:10.2337/dc17-S005. PMID 27979889.

[pmid19502545-13] "International Expert Committee report on the role of the A1C assay in the diagnosis of diabetes". Diabetes Care. 32 (7): 1327–34. 2009. doi:10.2337/dc09-9033. PMC 2699715. PMID 19502545.

[pmid24126648-14] Schellenberg ES, Dryden DM, Vandermeer B, Ha C, Korownyk C (2013). "Lifestyle interventions for patients with and at risk for type 2 diabetes: a systematic review and meta-analysis". Ann. Intern. Med. 159 (8): 543–51. doi:10.7326/0003-4819-159-8-201310150-00007. PMID 24126648.

[pmid22683134-15] Perreault L, Pan Q, Mather KJ, Watson KE, Hamman RF, Kahn SE (2012). "Effect of regression from prediabetes to normal glucose regulation on long-term reduction in diabetes risk: results from the Diabetes Prevention Program Outcomes Study". Lancet. 379 (9833): 2243–51. doi:10.1016/S0140-6736(12)60525-X. PMC 3555407. PMID 22683134.

[pmid26696675-16] "2. Classification and Diagnosis of Diabetes". Diabetes Care. 39 Suppl 1: S13–22. 2016. doi:10.2337/dc16-S005. PMID 26696675.

[pmid24424622-17] Moyer VA (2014). "Screening for gestational diabetes mellitus: U.S. Preventive Services Task Force recommendation statement". Ann. Intern. Med. 160 (6): 414–20. doi:10.7326/M13-2905. PMID 24424622.

[pmid17098085-18] Lindström J, Ilanne-Parikka P, Peltonen M, Aunola S, Eriksson JG, Hemiö K, Hämäläinen H, Härkönen P, Keinänen-Kiukaanniemi S, Laakso M, Louheranta A, Mannelin M, Paturi M, Sundvall J, Valle TT, Uusitupa M, Tuomilehto J (2006). "Sustained reduction in the incidence of type 2 diabetes by lifestyle intervention: follow-up of the Finnish Diabetes Prevention Study". Lancet. 368 (9548): 1673–9. doi:10.1016/S0140-6736(06)69701-8. PMID 17098085.

[Lindstrom2003-19] Lindstrom, J. (2003). "Prevention of Diabetes Mellitus in Subjects with Impaired Glucose Tolerance in the Finnish Diabetes Prevention Study: Results From a Randomized Clinical Trial". Journal of the American Society of Nephrology. 14 (90002): 108S–113. doi:10.1097/01.ASN.0000070157.96264.13. ISSN 1046-6673.

[TuomilehtoLindström2001-20] Tuomilehto, Jaakko; Lindström, Jaana; Eriksson, Johan G.; Valle, Timo T.; Hämäläinen, Helena; Ilanne-Parikka, Pirjo; Keinänen-Kiukaanniemi, Sirkka; Laakso, Mauri; Louheranta, Anne; Rastas, Merja; Salminen, Virpi; Aunola, Sirkka; Cepaitis, Zygimantas; Moltchanov, Vladislav; Hakumäki, Martti; Mannelin, Marjo; Martikkala, Vesa; Sundvall, Jouko; Uusitupa, Matti (2001). "Prevention of Type 2 Diabetes Mellitus by Changes in Lifestyle among Subjects with Impaired Glucose Tolerance". New England Journal of Medicine. 344 (18): 1343–1350. doi:10.1056/NEJM200105033441801. ISSN 0028-4793.

[21] "Primary Prevention of Type 2 Diabetes Mellitus by Lifestyle Intervention: Implications for Health Policy". Annals of Internal Medicine. 140 (11): 951. 2004. doi:10.7326/0003-4819-140-11-200406010-00036. ISSN 0003-4819.

[BuseGinsberg2007-22] Buse, John B.; Ginsberg, Henry N.; Bakris, George L.; Clark, Nathaniel G.; Costa, Fernando; Eckel, Robert; Fonseca, Vivian; Gerstein, Hertzel C.; Grundy, Scott; Nesto, Richard W.; Pignone, Michael P.; Plutzky, Jorge; Porte, Daniel; Redberg, Rita; Stitzel, Kimberly F.; Stone, Neil J. (2007). "Primary Prevention of Cardiovascular Diseases in People With Diabetes Mellitus". Circulation. 115 (1): 114–126. doi:10.1161/CIRCULATIONAHA.106.179294. ISSN 0009-7322.

[CezarettoSiqueira-Catania2011-23] Cezaretto, Adriana; Siqueira-Catania, Antonela; de Barros, Camila Risso; Salvador, Emanuel Péricles; Ferreira, Sandra Roberta G. (2011). "Benefits on quality of life concomitant to metabolic improvement in intervention program for prevention of diabetes mellitus". Quality of Life Research. 21 (1): 105–113. doi:10.1007/s11136-011-9919-2. ISSN 0962-9343.

[24] "Effects of Aspirin for Primary Prevention in Persons with Diabetes Mellitus". New England Journal of Medicine. 379 (16): 1529–1539. 2018. doi:10.1056/NEJMoa1804988. ISSN 0028-4793.

[ChiassonJosse2002-25] Chiasson, Jean-Louis; Josse, Robert G; Gomis, Ramon; Hanefeld, Markolf; Karasik, Avraham; Laakso, Markku (2002). "Acarbose for prevention of type 2 diabetes mellitus: the STOP-NIDDM randomised trial". The Lancet. 359 (9323): 2072–2077. doi:10.1016/S0140-6736(02)08905-5. ISSN 0140-6736.

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@@ Line 5: / Line 5: @@
 <div style="-webkit-user-select: none;">
-{| class="infobox" style="position: fixed; top: 65%; right: 10px; margin: 0 0 0 0; border: 0; float: right;"
-|-
-| {{#ev:youtube|https://https://www.youtube.com/watch?v=QRLZwXL6w1c|350}}
-|-
-|}
 __NOTOC__
 {{Diabetes mellitus}}
@@ Line 18: / Line 13: @@
 ==Overview==
-Diabetes mellitus (DM) refers to a spectrum of disorders with different [[metabolic]] changes that result in [[hyperglycemia]] as a common feature. It is caused by interaction of environmental agents in a genetically susceptible person. The metabolic disarrangement that may result in [[hyperglycemia]] will define the pathologic feature of each type of DM. Decreased [[insulin]] secretion, [[insulin resistance]], decreased [[glucose]] utilization and increased glucose production are the main metabolic dysregulations that are known to cause [[hyperglycemia]].<ref name="pmid21849967">{{cite journal |vauthors=Li C, Balluz LS, Okoro CA, Strine TW, Lin JM, Town M, Garvin W, Murphy W, Bartoli W, Valluru B |title=Surveillance of certain health behaviors and conditions among states and selected local areas --- Behavioral Risk Factor Surveillance System, United States, 2009 |journal=MMWR Surveill Summ |volume=60 |issue=9 |pages=1–250 |year=2011 |pmid=21849967 |doi= |url=}}</ref> [[Hyperglycemia]] may cause secondary changes in [[metabolic]] arrangement in different systems and it can involve every [[Organ (anatomy)|organ]] systems. DM is the leading cause of [[end-stage renal disease]] (ESRD), nontraumatic [[lower extremity]] [[Amputation|amputations]], and adult [[blindness]] worldwide.<ref name="pmid12503980">{{cite journal |vauthors=Mokdad AH, Ford ES, Bowman BA, Dietz WH, Vinicor F, Bales VS, Marks JS |title=Prevalence of obesity, diabetes, and obesity-related health risk factors, 2001 |journal=JAMA |volume=289 |issue=1 |pages=76–9 |year=2003 |pmid=12503980 |doi= |url=}}</ref> Accordingly, early [[diagnosis]] and [[treatment]] can result in significant decrease in [[mortality]] and [[morbidity]]. The [[incidence]] of [[diabetes]] has been increasing constantly.<ref name="pmid1516497">{{cite journal |vauthors=Harris MI, Klein R, Welborn TA, Knuiman MW |title=Onset of NIDDM occurs at least 4-7 yr before clinical diagnosis |journal=Diabetes Care |volume=15 |issue=7 |pages=815–9 |year=1992 |pmid=1516497 |doi= |url=}}</ref> According to [[WHO]] reports, 346 million people worldwide have [[diabetes]] and it is projected to double by 2030. It's [[prevalence]] is more in developed countries but the death occurring from DM [[complications]] is more common in developing countries. The [[prevalence]] of [[diabetes type 2]] is more common than [[type 1 diabetes]]. [[Diabetes]] can cause many [[complications]]. [[Acute]] [[complications]] ([[hypoglycemia]], [[DKA|ketoacidosis]] or [[Diabetic coma Nonketotic hyperosmolar coma|nonketotic hyperosmolar coma]]) may occur if the [[disease]] is not adequately controlled.<ref name="pmid16757028">{{cite journal |vauthors=Pasquale LR, Kang JH, Manson JE, Willett WC, Rosner BA, Hankinson SE |title=Prospective study of type 2 diabetes mellitus and risk of primary open-angle glaucoma in women |journal=Ophthalmology |volume=113 |issue=7 |pages=1081–6 |year=2006 |pmid=16757028 |doi=10.1016/j.ophtha.2006.01.066 |url=}}</ref> Serious long-term complications include [[Macrovascular disease|macrovascular]] ([[coronary heart disease]], [[peripheral arterial disease]] and [[cerebrovascular disease]]), microvascular ([[retinopathy]], [[neuropathy]] and [[nephropathy]]) and other organ involvement (gastrointestinal, genitourinary, dermatologic, infectious, [[Cataract|cataracts]], [[glaucoma]], [[periodontal disease]] and [[hearing loss]]).<ref name="pmid20474067">{{cite journal |vauthors=Obrosova IG, Chung SS, Kador PF |title=Diabetic cataracts: mechanisms and management |journal=Diabetes Metab. Res. Rev. |volume=26 |issue=3 |pages=172–80 |year=2010 |pmid=20474067 |doi=10.1002/dmrr.1075 |url=}}</ref> The main goals of treatment are:
+[[Diabetes mellitus]] ([[Diabetes mellitus|DM]]) refers to a spectrum of disorders with different [[metabolic]] changes that result in [[hyperglycemia]] as a common feature. It is caused by interaction of environmental agents in a genetically susceptible person. The [[Metabolism|metabolic]] disarrangement that may result in [[hyperglycemia]] will define the pathologic feature of each type of [[Diabetes|DM]]. Decreased [[insulin]] secretion, [[insulin resistance]], decreased [[glucose]] utilization and increased [[glucose]] production are the main metabolic dysregulations that are known to cause [[hyperglycemia]].
-#Elimination of hyperglycemic symptoms
-#Control of the long term complications
+[[Hyperglycemia]] may cause secondary changes in [[metabolic]] arrangement in different systems and it can involve every [[Organ (anatomy)|organ]] systems. [[Diabetes|DM]] is the leading cause of [[end-stage renal disease]] ([[Chronic renal failure|ESRD]]), non-traumatic [[lower extremity]] [[Amputation|amputations]], and adult [[blindness]] worldwide.
-#Improvement of the patient's quality of life
+Accordingly, early [[diagnosis]] and [[treatment]] can result in significant decrease in [[mortality]] and [[morbidity]]. The [[incidence]] of [[diabetes]] has been increased constantly. According to [[WHO]] reports, 346 million people worldwide have [[diabetes]] and it is projected to double by 2030. It's [[prevalence]] is more in developed countries but the death occurring from [[Diabetes|DM]] [[complications]] is more common in developing countries.
+The [[prevalence]] of [[diabetes type 2]] is more common than [[type 1 diabetes]]. [[Diabetes]] can cause many [[complications]]. [[Acute]] [[complications]] ([[hypoglycemia]], [[DKA|ketoacidosis]] or [[Diabetic coma Nonketotic hyperosmolar coma|nonketotic hyperosmolar coma]]) may occur if the [[disease]] is not adequately controlled.<ref name="pmid16757028">{{cite journal |vauthors=Pasquale LR, Kang JH, Manson JE, Willett WC, Rosner BA, Hankinson SE |title=Prospective study of type 2 diabetes mellitus and risk of primary open-angle glaucoma in women |journal=Ophthalmology |volume=113 |issue=7 |pages=1081–6 |year=2006 |pmid=16757028 |doi=10.1016/j.ophtha.2006.01.066 |url=}}</ref> Serious long-term [[complications]] include [[Macrovascular disease|macrovascular]] ([[coronary heart disease]], [[peripheral arterial disease]] and [[cerebrovascular disease]]), [[Microvascular disease|microvascular]] ([[retinopathy]], [[neuropathy]] and [[nephropathy]]) and other organ involvement ([[gastrointestinal]], [[genitourinary]], [[Dermatologic disorders|dermatologic]], [[infectious]], [[Cataract|cataracts]], [[glaucoma]], [[periodontal disease]] and [[hearing loss]]). The main goals of [[treatment]] are:
+#Elimination of [[hyperglycemic]] [[symptoms]]
+#[[Control]] of the long term [[complications]]
+#Improvement of the patient's [[quality of life]]
 ==Classification==
-Diabetes mellitus is classified into 3 types based on the pathogenic process that lead to hyperglycemia.
-*[[Diabetes mellitus type 1]]
+* [[Diabetes mellitus]] is classified into 3 types based on the pathogenic process that lead to [[hyperglycemia]]:
-*[[Diabetes mellitus type 2]]
+**[[Diabetes mellitus type 1]]
-*[[Gestational diabetes]]
+**[[Diabetes mellitus type 2]]
+**[[Gestational diabetes]]
 ==Differential diagnosis==
@@ Line 213: / Line 217: @@
 ==Complications==
-Complications of diabetes mellitus may be classified as [[Acute (medicine)|acute]] or [[Chronic (medical)|chronic]]. Acute complications of diabetes mellitus may occur in [[Diabetes mellitus type 1|type 1]], [[Diabetes mellitus type 2|type 2]], or [[gestational diabetes]]. Chronic complications of diabetes mellitus are more likely to occur in long standing [[Diabetes mellitus type 1|type 1]] or [[Diabetes mellitus type 2|type 2]] diabetes and may be further classified as [[Macrovascular disease|macrovascular,]] [[Microvascular disease|microvascular]], or other (unspecified etiology) as follows:<ref name="pmid21366474">{{cite journal |vauthors=Seshasai SR, Kaptoge S, Thompson A, Di Angelantonio E, Gao P, Sarwar N, Whincup PH, Mukamal KJ, Gillum RF, Holme I, Njølstad I, Fletcher A, Nilsson P, Lewington S, Collins R, Gudnason V, Thompson SG, Sattar N, Selvin E, Hu FB, Danesh J |title=Diabetes mellitus, fasting glucose, and risk of cause-specific death |journal=N. Engl. J. Med. |volume=364 |issue=9 |pages=829–41 |year=2011 |pmid=21366474 |pmc=4109980 |doi=10.1056/NEJMoa1008862 |url=}}</ref><ref name="pmid17563022">{{cite journal |vauthors=Franco OH, Steyerberg EW, Hu FB, Mackenbach J, Nusselder W |title=Associations of diabetes mellitus with total life expectancy and life expectancy with and without cardiovascular disease |journal=Arch. Intern. Med. |volume=167 |issue=11 |pages=1145–51 |year=2007 |pmid=17563022 |doi=10.1001/archinte.167.11.1145 |url=}}</ref><ref name="pmid25562264">{{cite journal |vauthors=Livingstone SJ, Levin D, Looker HC, Lindsay RS, Wild SH, Joss N, Leese G, Leslie P, McCrimmon RJ, Metcalfe W, McKnight JA, Morris AD, Pearson DW, Petrie JR, Philip S, Sattar NA, Traynor JP, Colhoun HM |title=Estimated life expectancy in a Scottish cohort with type 1 diabetes, 2008-2010 |journal=JAMA |volume=313 |issue=1 |pages=37–44 |year=2015 |pmid=25562264 |pmc=4426486 |doi=10.1001/jama.2014.16425 |url=}}</ref>
+* [[Complications]] of [[diabetes mellitus]] may be classified as [[Acute (medicine)|acute]] or [[Chronic (medical)|chronic]]. Acute [[Complication (medicine)|complications]] of [[diabetes mellitus]] may occur in [[Diabetes mellitus type 1|type 1]], [[Diabetes mellitus type 2|type 2]], or [[gestational diabetes]]. Chronic [[Complication (medicine)|complications]] of [[diabetes mellitus]] are more likely to occur in long standing [[Diabetes mellitus type 1|type 1]] or [[Diabetes mellitus type 2|type 2]] diabetes and may be further classified as [[Macrovascular disease|macrovascular,]] [[Microvascular disease|microvascular]], or other (unspecified [[etiology]]) as follows:<ref name="pmid21366474">{{cite journal |vauthors=Seshasai SR, Kaptoge S, Thompson A, Di Angelantonio E, Gao P, Sarwar N, Whincup PH, Mukamal KJ, Gillum RF, Holme I, Njølstad I, Fletcher A, Nilsson P, Lewington S, Collins R, Gudnason V, Thompson SG, Sattar N, Selvin E, Hu FB, Danesh J |title=Diabetes mellitus, fasting glucose, and risk of cause-specific death |journal=N. Engl. J. Med. |volume=364 |issue=9 |pages=829–41 |year=2011 |pmid=21366474 |pmc=4109980 |doi=10.1056/NEJMoa1008862 |url=}}</ref><ref name="pmid17563022">{{cite journal |vauthors=Franco OH, Steyerberg EW, Hu FB, Mackenbach J, Nusselder W |title=Associations of diabetes mellitus with total life expectancy and life expectancy with and without cardiovascular disease |journal=Arch. Intern. Med. |volume=167 |issue=11 |pages=1145–51 |year=2007 |pmid=17563022 |doi=10.1001/archinte.167.11.1145 |url=}}</ref><ref name="pmid25562264">{{cite journal |vauthors=Livingstone SJ, Levin D, Looker HC, Lindsay RS, Wild SH, Joss N, Leese G, Leslie P, McCrimmon RJ, Metcalfe W, McKnight JA, Morris AD, Pearson DW, Petrie JR, Philip S, Sattar NA, Traynor JP, Colhoun HM |title=Estimated life expectancy in a Scottish cohort with type 1 diabetes, 2008-2010 |journal=JAMA |volume=313 |issue=1 |pages=37–44 |year=2015 |pmid=25562264 |pmc=4426486 |doi=10.1001/jama.2014.16425 |url=}}</ref>
 ===Acute complications===
-They include [[diabetic ketoacidosis]] (DKA) and [[Hyperosmolar hyperglycemic state]] (HHS). DKA could be the presenting feature of type 1 diabetes and it is more common in type 1 diabetes although, it is sometimes seen in type 2 diabetic patients. [[Hyperosmolar hyperglycemic state|HHS]] is mostly seen in the elderly and it is more common in type 2 diabetes.
+* They include [[diabetic ketoacidosis]] ([[Diabetic ketoacidosis|DKA]]) and [[Hyperosmolar hyperglycemic state]] ([[Hyperosmolar hyperglycemic state|HHS]]). [[Diabetic ketoacidosis|DKA]] could be the presenting feature of [[type 1 diabetes]] and it is more common in [[type 1 diabetes]] although, it is sometimes seen in [[Diabetes mellitus type 2|type 2 diabetic]] patients. [[Hyperosmolar hyperglycemic state|HHS]] is mostly seen in the [[elderly]] and it is more common in [[type 2 diabetes]].
 ===Chronic complications===
@@ Line 232: / Line 237: @@
 =====Neuropathy=====
-*[[Sensory neuropathy|Sensory]] and [[Motor neuron disease|motor]] (mono- and polyneuropathy)<ref name="pmid27979887">{{cite journal |vauthors= |title=Standards of Medical Care in Diabetes-2017: Summary of Revisions |journal=Diabetes Care |volume=40 |issue=Suppl 1 |pages=S4–S5 |year=2017 |pmid=27979887 |doi=10.2337/dc17-S003 |url=}}</ref>
+*[[Sensory neuropathy|Sensory]] and [[Motor neuron disease|motor]] ([[Mononeuropathy|mono]]- and [[polyneuropathy]])<ref name="pmid27979887">{{cite journal |vauthors= |title=Standards of Medical Care in Diabetes-2017: Summary of Revisions |journal=Diabetes Care |volume=40 |issue=Suppl 1 |pages=S4–S5 |year=2017 |pmid=27979887 |doi=10.2337/dc17-S003 |url=}}</ref>
 *[[Autonomic neuropathy]]<ref name="pmid27979887">{{cite journal |vauthors= |title=Standards of Medical Care in Diabetes-2017: Summary of Revisions |journal=Diabetes Care |volume=40 |issue=Suppl 1 |pages=S4–S5 |year=2017 |pmid=27979887 |doi=10.2337/dc17-S003 |url=}}</ref>
 =====Nephropathy=====
@@ Line 238: / Line 243: @@
 ===Other organs<ref name="pmid27979887">{{cite journal |vauthors= |title=Standards of Medical Care in Diabetes-2017: Summary of Revisions |journal=Diabetes Care |volume=40 |issue=Suppl 1 |pages=S4–S5 |year=2017 |pmid=27979887 |doi=10.2337/dc17-S003 |url=}}</ref>===
-*Gastrointestinal ([[gastroparesis]], [[diarrhea]])
+*[[Gastrointestinal tract|Gastrointestinal]] ([[gastroparesis]], [[diarrhea]])
-*Genitourinary ([[uropathy]]/[[sexual dysfunction]])
+*[[Genitourinary system|Genitourinary]] ([[uropathy]]/[[sexual dysfunction]])
 *[[List of skin diseases|Dermatologic]]
-*Infectious
+*[[Infection|Infections]]
 *[[Cataract|Cataracts]]
 *[[Glaucoma]]
@@ Line 247: / Line 252: @@
 *[[Hearing loss]]
-Complications of gestational diabetes differs from type 1 and type 2 diabetes primarily due to its pregnancy-specific effects on the mother as well as its effects on the fetus.
-'''For more information on maternal complications of gestational diabetes [[Gestational diabetes maternal complications|click here]].'''
+* [[Complication (medicine)|Complications]] of [[gestational diabetes]] differs from [[Diabetes mellitus type 1|type 1]] and [[Diabetes mellitus type 2|type 2 diabetes]] primarily due to its [[pregnancy]]-specific effects on the mother as well as its effects on the [[fetus]].
-'''For more information on fetal complications of gestational diabetes [[Gestational diabetes fetal complications|click here]].'''
+* '''For more information on maternal complications of gestational diabetes [[Gestational diabetes maternal complications|click here]].'''
+* '''For more information on fetal complications of gestational diabetes [[Gestational diabetes fetal complications|click here]].'''
-==Screening==
-===Diabetes mellitus type 1===
-According to the American Diabetic Association, screening for type 1 DM is not recommended.
-===Diabetes mellitus type 2===
-Diabetes screening is recommended for many people at various stages of life, and for those with any of several risk factors. '''American Diabetes Association Recommendations''' for Diabetes Screening include:<ref name="pmid27979889">{{cite journal |vauthors= |title=2. Classification and Diagnosis of Diabetes |journal=Diabetes Care |volume=40 |issue=Suppl 1 |pages=S11–S24 |year=2017 |pmid=27979889 |doi=10.2337/dc17-S005 |url=}}</ref><ref name="pmid19502545">{{cite journal |vauthors= |title=International Expert Committee report on the role of the A1C assay in the diagnosis of diabetes |journal=Diabetes Care |volume=32 |issue=7 |pages=1327–34 |year=2009 |pmid=19502545 |pmc=2699715 |doi=10.2337/dc09-9033 |url=}}</ref><ref name="pmid24126648">{{cite journal |vauthors=Schellenberg ES, Dryden DM, Vandermeer B, Ha C, Korownyk C |title=Lifestyle interventions for patients with and at risk for type 2 diabetes: a systematic review and meta-analysis |journal=Ann. Intern. Med. |volume=159 |issue=8 |pages=543–51 |year=2013 |pmid=24126648 |doi=10.7326/0003-4819-159-8-201310150-00007 |url=}}</ref><ref name="pmid22683134">{{cite journal |vauthors=Perreault L, Pan Q, Mather KJ, Watson KE, Hamman RF, Kahn SE |title=Effect of regression from prediabetes to normal glucose regulation on long-term reduction in diabetes risk: results from the Diabetes Prevention Program Outcomes Study |journal=Lancet |volume=379 |issue=9833 |pages=2243–51 |year=2012 |pmid=22683134 |pmc=3555407 |doi=10.1016/S0140-6736(12)60525-X |url=}}</ref>
-'''CATEGORIES OF INCREASED RISK FOR DIABETES (PREDIABETES)'''
-Recommendations:
-* Screening for prediabetes and risk for future diabetes with an informal assessment of risk factors or validated tools should be considered in asymptomatic adults. B
-* Testing for prediabetes and risk for future diabetes in asymptomatic people should be considered in adults of any age who are overweight or obese (BMI $25 kg/m2 or $23 kg/m2 in Asian Americans) and who have one or more additional risk factors for diabetes. B
-* For all people, testing should '''begin at age 45''' years. B
-* If tests are normal, repeat testing carried out at a minimum of '''3-year intervals''' is reasonable. C
-* To test for prediabetes, fasting plasma glucose, 2-h plasma glucose during 75-g oral glucose tolerance test, and A1C are equally appropriate. B
-* In patients with prediabetes, identify and, if appropriate, treat other cardiovascular disease risk factors. B
-* Testing for prediabetes should be considered in children and adolescents who are overweight or obese (BMI .85th percentile for age and sex, weight for height .85th percentile, or weight.120% of ideal for height) and who have additional risk factors for diabetes (Table 2.5). E
-*
-{| class="wikitable"
-|+ADA 2018 [DO NOT EDIT]
-!Criteria for testing for diabetes or prediabetes in asymptomatic adults
-|-
-|1. Testing should be considered in overweight or obese (BMI 25 kg/m2 or 23 kg/m2 in Asian Americans) adults who have one or more of the following risk factors:
-* First-degree relative with diabetes
-* High-risk race/ethnicity (e.g., African American, Latino, Native American, Asian American, Pacific Islander)
-* History of CVD
-* Hypertension (140/90 mmHg or on therapy for hypertension)
-* HDL cholesterol level ,35 mg/dL (0.90 mmol/L) and/or a triglyceride level .250 mg/dL (2.82 mmol/L)
-* Women with polycystic ovary syndrome
-* Physical inactivity
-* Other clinical conditions associated with insulin resistance (e.g., severe obesity, acanthosis nigricans)
-|-
-|2. Patients with prediabetes (A1C 5.7% [39 mmol/mol], IGT, or IFG) should be tested yearly.
-|-
-|3. Women who were diagnosed with GDM should have lifelong testing at least every 3 years.
-|-
-|4. For all other patients, testing should begin at age 45 years.
-|-
-|5. If results are normal, testing should be repeated at a minimum of 3-year intervals, with
-consideration of more frequent testing depending on initial results and risk status.
-|}
-To test for type 2 diabetes, [[fasting plasma glucose]], 2-h plasma glucose after 75-g oral glucose tolerance test, and [[HbA1C]] are equally appropriate.
-{| class="wikitable"
-|+
-!Categories of increased risk for diabetes (prediabetes)
-|-
-|FPG 100 mg/dL (5.6 mmol/L) to 125 mg/dL (6.9 mmol/L) (IFG)
-|-
-| align="center" |OR
-|-
-|2-h PG during 75-g OGTT 140 mg/dL (7.8 mmol/L) to 199 mg/dL (11.0 mmol/L) (IGT)
-|-
-| align="center" |OR
-|-
-|A1C 5.7–6.4% (39–47 mmol/mol)
-|}
-===Gestational diabetes===
-All pregnant women should be screened for gestational diabetes in 24-28 weeks with 50 gram glucose test. Measurements greater than 130 mg/dL are considered positive and should proceed to 100 gram glucose test for diagnosis. High risk mothers should be screened as early as the first prenatal visit. These risk factors include:<ref name="pmid26696675">{{cite journal |vauthors= |title=2. Classification and Diagnosis of Diabetes |journal=Diabetes Care |volume=39 Suppl 1 |issue= |pages=S13–22 |year=2016 |pmid=26696675 |doi=10.2337/dc16-S005 |url=}}</ref><ref name="pmid24424622">{{cite journal |vauthors=Moyer VA |title=Screening for gestational diabetes mellitus: U.S. Preventive Services Task Force recommendation statement |journal=Ann. Intern. Med. |volume=160 |issue=6 |pages=414–20 |year=2014 |pmid=24424622 |doi=10.7326/M13-2905 |url=}}</ref>
-* A [[Family history (medicine)|family history]] of diabetes especially in first degree relatives
-* Maternal age >25 yrs
-* Certain ethnic groups (such as Native American, Hispanic-American, African-American,  South or East Asian, Pacific Islander)
-* [[Body mass index]] greater than 25 kg/m<sup>2</sup>
-* Gestational diabetes or impaired glucose tolerance test in previous pregnancies
-* Previous delivery of a baby >9 pounds
-* Personal history of  [[impaired glucose tolerance]] or [[impared fasting glucose]] (pre-diabetes)
-* [[Glycosuria]] at the first prenatal visit
-* Certain medical conditions (such as [[metabolic syndrome]], [[polycystic ovary syndrome]] (PCOS), current use of [[glucocorticoids]], [[hypertension]])
-* Previous history of unexplained [[miscarriage (patient information)|miscarriage]] or [[stillbirth]]
-* Smoking doubles the risk of gestational diabetes
-* [[Multiple gestation]]
-* Genetic predisposition (.e.g. glucokinase mutation)
 ==Diagnosis==
 ===Diabetes mellitus type 1 and type 2===
-A [[fasting plasma glucose]] (FPG) <5.6 mmol/L (100 mg/dL), a [[plasma glucose]] <140 mg/dL (11.1 mmol/L) following an [[Oral glucose tolerance test|oral glucose challenge]] and an [[HbA1c]] <5.7% are considered normal.<br>
-Diagnostic criteria for DM are:
+* A [[fasting plasma glucose]] ([[Fasting blood sugar|FPG]]) <5.6 mmol/L (100 mg/dL), a [[plasma glucose]] <140 mg/dL (11.1 mmol/L) following an [[Oral glucose tolerance test|oral glucose challenge]] and an [[HbA1c]] <5.7% are considered normal.<br> Diagnostic criteria for [[Diabetes|DM]] are:
-*Symptoms of diabetes plus random blood glucose concentration ≥11.1 mmol/L (200 mg/dL)<sup>†</sup> '''OR'''
+**Symptoms of [[diabetes]] plus random blood glucose concentration ≥11.1 mmol/L (200 mg/dL)<sup>†</sup> '''OR'''
-*[[Fasting plasma glucose]] ≥7.0 mmol/L (126 mg/dL)<sup>‡</sup> '''OR'''
+**[[Fasting plasma glucose]] ≥7.0 mmol/L (126 mg/dL)<sup>‡</sup> '''OR'''
-*[[Hemoglobin A1c]] ≥ 6.5% '''OR'''
+**[[Hemoglobin A1c]] ≥ 6.5% '''OR'''
-*2-h [[plasma glucose]] ≥11.1 mmol/L (200 mg/dL) during an [[oral glucose tolerance test]]<sup>¶</sup>
+**2-hours[[plasma glucose]] ≥11.1 mmol/L (200 mg/dL) during an [[oral glucose tolerance test]]<sup>¶</sup>
 '''American Diabetes Association Diabetes Diagnostic Criteria 2018 (DO NOT EDIT)'''
@@ Line 346: / Line 276: @@
 |A
 |
-* Clear evidence from well-conducted, generalizable randomized controlled trials that are adequately powered, including
+* Clear evidence from well-conducted, generalizable [[Randomized controlled trial|randomized controlled trials]] that are adequately powered, including
-** Evidence from a well-conducted multicenter trial
+** Evidence from a well-conducted multi-center trial
-** Evidence from a meta-analysis that incorporated quality ratings in the analysis
+** Evidence from a [[meta-analysis]] that incorporated quality ratings in the analysis
-* Compelling nonexperimental evidence, i.e., “all or none” rule developed by the Centre for Evidence-Based Medicine at the University of Oxford.
+* Compelling non-experimental evidence, i.e., “all or none” rule developed by the Center for Evidence-Based Medicine at the University of Oxford.
 * Supportive evidence from well-conducted randomized controlled trials that are adequately powered, including
 ** Evidence from a well-conducted trial at one or more institutions
-** Evidence from a meta-analysis that incorporated quality ratings in the analysis
+** Evidence from a [[meta-analysis]] that incorporated quality ratings in the analysis
 |-
 |B
 |
-* Supportive evidence from well-conducted cohort studies
+* Supportive evidence from well-conducted [[Cohort study|cohort studies]]
-** Evidence from a well-conducted prospective cohort study or registry
+** Evidence from a well-conducted [[prospective cohort study]] or registry
-** Evidence from a well-conducted meta-analysis of cohort studies
+** Evidence from a well-conducted [[meta-analysis]] of [[Cohort study|cohort studies]]
-* Supportive evidence from a well-conducted case-control study
+* Supportive evidence from a well-conducted [[Case-control|case-control study]]
 |-
 |C
 |
 * Supportive evidence from poorly controlled or uncontrolled studies
-** Evidence from randomized clinical trials with one or more major or three or more minor methodological flaws that could invalidate the results
+** Evidence from randomized [[Clinical trial|clinical trials]] with one or more major or three or more minor flaws that could invalidate the results
-** Evidence from observational studies with high potential for bias (such as case series with comparison with historical controls)
+** Evidence from [[Observational study|observational studies]] with high potential for [[bias]] (such as [[case series]] with comparison with historical controls)
-** Evidence from case series or case reports
+** Evidence from [[case series]] or [[Case report|case reports]]
 * Conflicting evidence with the weight of evidence supporting the recommendation
 |-
@@ Line 374: / Line 304: @@
 |
 * Supportive evidence from poorly controlled or uncontrolled studies
-** Evidence from randomized clinical trials with one or more major or three or more minor methodological flaws that could invalidate the results
+** Evidence from [[Randomized controlled trial|randomized clinical trials]] with one or more major or three or more minor methodological flaws that could invalidate the results
-** Evidence from observational studies with high potential for bias (such as case series with comparison with historical controls)
+** Evidence from [[Observational study|observational studies]] with high potential for [[bias]] (such as case series with comparison with historical controls)
-** Evidence from case series or case reports
+** Evidence from [[case series]] or [[Case report|case reports]]
 * Conflicting evidence with the weight of evidence supporting the recommendation
 |-
@@ Line 383: / Line 313: @@
 |}
-Recommendations for Hb-A1c:
+* Recommendations for [[Glycosylated hemoglobin|HbA1c]]:
-* To avoid misdiagnosis or missed diagnosis, the A1C test should be performed using a method that is certified by the NGSP and standardized to the Diabetes Control and Complications Trial (DCCT) assay. B
+** To avoid misdiagnosis or missed diagnosis, the [[Glycosylated hemoglobin|A1C]] test should be performed using a method that is certified by the NGSP and standardized to the Diabetes Control and Complications Trial (DCCT) assay. B
+**Marked discordance between measured [[Glycosylated hemoglobin|A1C]] and [[Plasma glucose|plasma glucose levels]] should raise the possibility of [[Glycosylated hemoglobin|A1C]] assay interference due to [[hemoglobin]] variants (i.e., [[Hemoglobinopathy|hemoglobinopathies]]) and consideration of using an assay without interference or [[Blood sugar|plasma blood glucose]] criteria to diagnose [[diabetes]]. B
+**In conditions associated with increased [[red blood cell]] turnover, such as [[Sickle-cell disease|sickle cell disease]], [[pregnancy]] (second and third [[trimesters]]), [[hemodialysis]], recent [[Bleeding|blood loss]] or [[Blood transfusion|transfusion]], or [[erythropoietin]] therapy, only [[Blood glucose|plasma blood glucose]] criteria should be used to diagnose [[diabetes]]. B
-* Marked discordance between measured A1C and plasma glucose levels should raise the possibility of A1C assay interference due to hemoglobin variants (i.e., hemoglobinopathies) and consideration of using an assay without interference or plasma blood glucose criteria to diagnose diabetes. B
-* In conditions associated with increased red blood cell turnover, such as sickle cell disease, pregnancy (second and third trimesters), hemodialysis, recent blood loss or transfusion, or erythropoietin therapy, only plasma blood glucose criteria should be used to diagnose diabetes. B
 <br>Note:<br>
 <small>
 †:Random is defined as without regard to time since the last meal.
-‡:Fasting is defined as no caloric intake for at least 8 h.
+‡:Fasting is defined as no caloric intake for at least 8 hours.
 ¶:The test should be performed using a glucose load containing the equivalent of 75 g anhydrous glucose dissolved in water, not recommended for routine clinical use.
@@ Line 402: / Line 331: @@
 ! align="center" style="background:#DCDCDC;" |'''Criteria for the diagnosis of diabetes'''
 |-
-| align="left" style="background:#F5F5F5;" |[[Fasting plasma glucose|FPG]]  ≥126 mg/dL (7.0 mmol/L). Fasting is defined as no caloric intake for at least 8 h.
+| align="left" style="background:#F5F5F5;" |[[Fasting plasma glucose|FPG]]  ≥126 mg/dL (7.0 mmol/L). Fasting is defined as no caloric intake for at least 8 hours.
 |-
 | align="center" style="background:#F5F5F5;" |'''OR'''
 |-
 | align="left" style="background:#F5F5F5;" |2-h [[Blood glucose|Plasma Glucose]] (PG)  ≥200 mg/dL (11.1 mmol/L) during an [[Glucose tolerance test|OGTT]]. The test should be performed as described
-by the [[WHO]], using a glucose load containing the equivalent of 75 g anhydrous glucose dissolved in water.
+by the [[WHO]], using a glucose load containing the equivalent of 75 g [[anhydrous]] glucose dissolved in water.
 |-
 | align="center" style="background:#F5F5F5;" |'''OR'''
@@ Line 414: / Line 343: @@
 * The test should be performed in a laboratory using a method that is NGSP certified and standardized to the DCCT assay.
-* In the absence of unequivocal hyperglycemia, results should be confirmed by repeat testing.
+* In the absence of unequivocal [[hyperglycemia]], results should be confirmed by repeat testing.
 |-
 | align="center" style="background:#F5F5F5;" |'''OR'''
@@ Line 422: / Line 351: @@
 ===Gestational diabetes===
-There are 2 strategies to confirm the GDM diagnosis.
-*'''One-step''' 75-g Oral glucose tolerance test (OGTT)
+* There are 2 strategies to confirm the [[Gestational diabetes|GDM]] diagnosis.
-::::::'''OR'''
+**'''One-step''' 75-g Oral [[glucose tolerance test]] ([[Glucose tolerance test|OGTT]]) '''OR'''
-*'''Two-step''' approach with a 50-g (nonfasting) ''screen'' followed by a 100-g OGTT for those who screen positive.<ref name="pmid26807004">{{cite journal |vauthors= |title=Standards of Medical Care in Diabetes-2016 Abridged for Primary Care Providers |journal=Clin Diabetes |volume=34 |issue=1 |pages=3–21 |year=2016 |pmid=26807004 |doi=10.2337/diaclin.34.1.3 |url=}}</ref>
+** '''Two-step''' approach with a 50-g (non-fasting) screen followed by a 100-g [[Glucose tolerance test|OGTT]] for those who screen positive.<ref name="pmid26807004">{{cite journal |vauthors= |title=Standards of Medical Care in Diabetes-2016 Abridged for Primary Care Providers |journal=Clin Diabetes |volume=34 |issue=1 |pages=3–21 |year=2016 |pmid=26807004 |doi=10.2337/diaclin.34.1.3 |url=}}</ref>
 ====One Step Strategy====
-Perform a 75 g glucose tolerance test in 24-28 weeks of pregnancy and read the measures 1 h and 2 h after glucose ingestion as well as fasting glucose.<ref name="pmid26807004">{{cite journal |vauthors= |title=Standards of Medical Care in Diabetes-2016 Abridged for Primary Care Providers |journal=Clin Diabetes |volume=34 |issue=1 |pages=3–21 |year=2016 |pmid=26807004 |doi=10.2337/diaclin.34.1.3 |url=}}</ref>
-The OGTT should be performed in the morning after an overnight fast of at least 8 h.
+* Perform a 75 g [[glucose tolerance test]] in 24-28 weeks of [[pregnancy]] and read the measures 1 h and 2 hours after [[glucose]] ingestion as well as fasting glucose.<ref name="pmid26807004">{{cite journal |vauthors= |title=Standards of Medical Care in Diabetes-2016 Abridged for Primary Care Providers |journal=Clin Diabetes |volume=34 |issue=1 |pages=3–21 |year=2016 |pmid=26807004 |doi=10.2337/diaclin.34.1.3 |url=}}</ref> The [[Glucose tolerance test|OGTT]] should be performed in the morning after an overnight fast of at least 8 hours. The diagnosis of [[Gestational diabetes|GDM]] is made when any of the following [[Blood sugar|plasma glucose]] values are met or exceeded:
-The diagnosis of GDM is made when any of the following plasma glucose values are met or exceeded:
+** Fasting: 92 mg/dL (5.1 mmol/L)
-* Fasting: 92 mg/dL (5.1 mmol/L)
+** 1 hour: 180 mg/dL (10.0 mmol/L)
-* 1 h: 180 mg/dL (10.0 mmol/L)
+** 2 hours: 153 mg/dL (8.5 mmol/L)
-* 2 h: 153 mg/dL (8.5 mmol/L)
 ====Two Step Strategy====
-In this approach, screening with a 1 h 50-g glucose load test (GLT) followed by a 3 h 100-g OGTT for those who screen positive.<ref name="pmid26696673">{{cite journal |vauthors= |title=Professional Practice Committee for the Standards of Medical Care in Diabetes-2016 |journal=Diabetes Care |volume=39 Suppl 1 |issue= |pages=S107–8 |year=2016 |pmid=26696673 |doi=10.2337/dc16-S018 |url=}}</ref>
-The diagnosis of GDM is made when at least 2 out of 4 measures of 3 h 100-g OGTT became abnormal.
+* In this approach, screening with a 1 hour 50-g [[glucose]] load test (GLT) followed by a 3 hours 100-g [[Glucose tolerance test|OGTT]] for those who screen positive.<ref name="pmid26696673">{{cite journal |vauthors= |title=Professional Practice Committee for the Standards of Medical Care in Diabetes-2016 |journal=Diabetes Care |volume=39 Suppl 1 |issue= |pages=S107–8 |year=2016 |pmid=26696673 |doi=10.2337/dc16-S018 |url=}}</ref>
-*The following table summarizes the diagnostic approach for gestational diabetes.
+* The diagnosis of [[Gestational diabetes|GDM]] is made when at least 2 out of 4 measures of 3 hours 100-g [[Glucose tolerance test|OGTT]] became abnormal.
+*The following table summarizes the diagnostic approach for [[gestational diabetes]].
 {| class="wikitable"
@@ Line 446: / Line 377: @@
 !Fasting
 !1 Hour
-!2 Hour
+!2 Hours
-!3 Hour
+!3 Hours
 |-
 |
 :One step test
-:::2 hour 75 g glucose tolerance test
+:::2 hour 75 g [[glucose tolerance test]]
 |92
 |180
 |153
-| ----
+|  ----
 |-
 |
 :Two step test
 :::1 hour 50 g screening test
-| ----
+|  ----
 |140
-| ----
+|  ----
-| ----
+|  ----
 |-
 |
@@ Line 480: / Line 411: @@
 |145
 |}
+==Screening==
+* Comparing developed and developing countries shows lower rate of progression from [[glucose intolerance]] to [[diabetes]], due to better [[Screening (medicine)|screening]] in developed and high-income areas.<ref name="LiuLi2013">{{cite journal|last1=Liu|first1=Xiaoqian|last2=Li|first2=Changping|last3=Gong|first3=Hui|last4=Cui|first4=Zhuang|last5=Fan|first5=Linlin|last6=Yu|first6=Wenhua|last7=Zhang|first7=Cui|last8=Ma|first8=Jun|title=An economic evaluation for prevention of diabetes mellitus in a developing country: a modelling study|journal=BMC Public Health|volume=13|issue=1|year=2013|issn=1471-2458|doi=10.1186/1471-2458-13-729}}</ref>
+===Diabetes mellitus type 1===
+* According to the American Diabetic Association, screening for [[Diabetes mellitus type 1|type 1 DM]] is not recommended.
+===Diabetes mellitus type 2===
+* [[Screening (medicine)|Screening]] is recommended for many people at various stages of life, and for those with [[Risk factor|risk factors]]. American Diabetes Association Recommendations for [[Diabetes]] [[Screening (medicine)|screening]] include:<ref name="pmid27979889">{{cite journal |vauthors= |title=2. Classification and Diagnosis of Diabetes |journal=Diabetes Care |volume=40 |issue=Suppl 1 |pages=S11–S24 |year=2017 |pmid=27979889 |doi=10.2337/dc17-S005 |url=}}</ref><ref name="pmid19502545">{{cite journal |vauthors= |title=International Expert Committee report on the role of the A1C assay in the diagnosis of diabetes |journal=Diabetes Care |volume=32 |issue=7 |pages=1327–34 |year=2009 |pmid=19502545 |pmc=2699715 |doi=10.2337/dc09-9033 |url=}}</ref><ref name="pmid24126648">{{cite journal |vauthors=Schellenberg ES, Dryden DM, Vandermeer B, Ha C, Korownyk C |title=Lifestyle interventions for patients with and at risk for type 2 diabetes: a systematic review and meta-analysis |journal=Ann. Intern. Med. |volume=159 |issue=8 |pages=543–51 |year=2013 |pmid=24126648 |doi=10.7326/0003-4819-159-8-201310150-00007 |url=}}</ref><ref name="pmid22683134">{{cite journal |vauthors=Perreault L, Pan Q, Mather KJ, Watson KE, Hamman RF, Kahn SE |title=Effect of regression from prediabetes to normal glucose regulation on long-term reduction in diabetes risk: results from the Diabetes Prevention Program Outcomes Study |journal=Lancet |volume=379 |issue=9833 |pages=2243–51 |year=2012 |pmid=22683134 |pmc=3555407 |doi=10.1016/S0140-6736(12)60525-X |url=}}</ref>
+==== Categories of Increased Risk for [[Diabetes]] ([[Prediabetes|Prediabetics]]) Recommendations: ====
+*[[Screening (medicine)|Screening]] for [[prediabetes]] and risk for future [[diabetes]] with an informal assessment of [[Risk factor|risk factors]] or validated tools should be considered in [[asymptomatic]] adults. B
+* Testing for [[prediabetes]] and risk for future [[diabetes]] in [[asymptomatic]] people should be considered in adults of any age who are [[overweight]] or [[Obesity|obese]] ([[Body mass index|BMI]] >25 kg/m2 or >23 kg/m2 in Asian Americans) and who have one or more additional [[Risk factor|risk factors]] for [[diabetes]]. B
+* For all people, testing should begin at age 45 years. B
+* If tests are normal, repeat testing carried out at a minimum of 3-year intervals is reasonable. C
+* To test for [[prediabetes]], [[Blood sugar|fasting plasma glucose]], 2-hours [[Blood sugar|plasma glucose]] during 75-g oral [[glucose tolerance test]], and [[Glycosylated hemoglobin|HbA1C]] are equally appropriate. B
+* In [[Prediabetes|prediabetic]] patients, identify and, if appropriate, treat other [[Risk factor|risk factors]] of [[cardiovascular disease]]. B
+* Testing for [[prediabetes]] should be considered in children and adolescents who are [[overweight]] or [[Obesity|obese]] ([[Body mass index|BMI]] = 85th [[percentile]] for age and sex, weight for height = 85th [[percentile]], or weight 120% of ideal for height) and who have additional [[Risk factor|risk factors]] for [[diabetes]] (Table 2.5). E
+{| class="wikitable"
+|+ADA 2018 [DO NOT EDIT]
+!Criteria for testing for diabetes or prediabetes in asymptomatic adults
+|-
+|1. Testing should be considered in [[overweight]] or [[Obesity|obese]] (BMI 25 kg/m2 or 23 kg/m2 in Asian Americans) adults who have one or more of the following [[Risk factor|risk factors]]:
+* First-degree relative with [[diabetes]]
+* High-risk [[race]]/[[Ethnicity and health|ethnicity]] (e.g., African American, Latino, Native American, Asian American, Pacific Islander)
+* History of [[Cardiovascular disease|CVD]]
+*[[Hypertension]] (140/90 mmHg or on therapy for hypertension)
+*[[High density lipoprotein|HDL]] [[cholesterol]] level <35 mg/dL (0.90 mmol/L) and/or a [[triglyceride]] level >250 mg/dL (2.82 mmol/L)
+* Women with [[polycystic ovary syndrome]]
+* Physical inactivity
+* Other clinical conditions associated with [[insulin resistance]] (e.g., severe [[obesity]], [[acanthosis nigricans]])
+|-
+|2. Patients with [[prediabetes]] ([[Glycosylated hemoglobin|A1C]] > 5.7% [39 mmol/mol], IGT, or IFG) should be tested yearly.
+|-
+|3. Women who were diagnosed with [[Gestational diabetes|GDM]] should have lifelong testing at least every 3 years.
+|-
+|4. For all other patients, testing should begin at age 45 years.
+|-
+|5. If results are normal, testing should be repeated at a minimum of 3-year intervals, with consideration of more frequent testing depending on initial results and risk status.
+|}
+* To test for [[Diabetes mellitus type 2|type 2 diabetes]], [[fasting plasma glucose]], 2-h plasma glucose after 75-g [[Glucose tolerance test|oral glucose tolerance test]], and [[HbA1C]] are equally appropriate.
+{| class="wikitable"
+|+
+!Categories of increased risk for diabetes (prediabetes)
+|-
+|FPG 100 mg/dL (5.6 mmol/L) to 125 mg/dL (6.9 mmol/L) (IFG)
+|-
+| align="center" |OR
+|-
+|2-h PG during 75-g [[Glucose tolerance test|OGTT]] 140 mg/dL (7.8 mmol/L) to 199 mg/dL (11.0 mmol/L) (IGT)
+|-
+| align="center" |OR
+|-
+|[[Glycosylated hemoglobin|A1C]] 5.7–6.4% (39–47 mmol/mol)
+|}
+===Gestational diabetes===
+* All [[Pregnancy|pregnant]] women should be screened for [[gestational diabetes]] in 24-28 weeks with 50 gram [[glucose]] test. Measurements greater than 130 mg/dL are considered positive and should proceed to 100 gram [[glucose]] test for diagnosis. High risk mothers should be screened as early as the first prenatal visit. These [[Risk factor|risk factors]] include:<ref name="pmid26696675">{{cite journal |vauthors= |title=2. Classification and Diagnosis of Diabetes |journal=Diabetes Care |volume=39 Suppl 1 |issue= |pages=S13–22 |year=2016 |pmid=26696675 |doi=10.2337/dc16-S005 |url=}}</ref><ref name="pmid24424622">{{cite journal |vauthors=Moyer VA |title=Screening for gestational diabetes mellitus: U.S. Preventive Services Task Force recommendation statement |journal=Ann. Intern. Med. |volume=160 |issue=6 |pages=414–20 |year=2014 |pmid=24424622 |doi=10.7326/M13-2905 |url=}}</ref>
+** A [[Family history (medicine)|family history]] of [[diabetes]] especially in first degree relatives
+** Maternal age >25 yrs
+** Certain [[Ethnic group|ethnic]] groups (such as Native American, Hispanic-American, African-American,  South or East Asian, Pacific Islander)
+**[[Body mass index]] greater than 25 kg/m<sup>2</sup>
+**[[Gestational diabetes]] or impaired [[glucose tolerance test]] in previous [[Pregnancy|pregnancies]]
+** Previous [[Childbirth|delivery]] of a baby >9 pounds
+** Personal history of  [[impaired glucose tolerance]] or [[impared fasting glucose|impaired fasting glucose]] ([[Prediabetes|pre-diabetes]])
+**[[Glycosuria]] at the first prenatal visit
+** Certain medical conditions (such as [[metabolic syndrome]], [[polycystic ovary syndrome]] ([[Polycystic ovary syndrome|PCOS]]), current use of [[glucocorticoids]], [[hypertension]])
+** Previous history of unexplained [[miscarriage (patient information)|miscarriage]] or [[stillbirth]]
+**[[Smoking]] doubles the risk of [[gestational diabetes]]
+**[[Multiple gestation]]
+** Genetic predisposition (.e.g. [[glucokinase]] [[mutation]])
 ==Prevention==
-Life style modification is the mainstay of prevention of diabetes mellitus. It includes, changes in diet, weight reduction and exercise. The strongest evidence for diabetes prevention comes from the Diabetes Prevention Program (DPP). The DPP demonstrated that an intensive lifestyle intervention could reduce the incidence of type 2 diabetes by 58% over 3 years.<ref name="pmid17098085">{{cite journal |vauthors=Lindström J, Ilanne-Parikka P, Peltonen M, Aunola S, Eriksson JG, Hemiö K, Hämäläinen H, Härkönen P, Keinänen-Kiukaanniemi S, Laakso M, Louheranta A, Mannelin M, Paturi M, Sundvall J, Valle TT, Uusitupa M, Tuomilehto J |title=Sustained reduction in the incidence of type 2 diabetes by lifestyle intervention: follow-up of the Finnish Diabetes Prevention Study |journal=Lancet |volume=368 |issue=9548 |pages=1673–9 |year=2006 |pmid=17098085 |doi=10.1016/S0140-6736(06)69701-8 |url=}}</ref>
+* Life style modification is the mainstay of prevention of [[diabetes mellitus]]. It includes, changes in diet, weight reduction and [[Physical exercise|exercise]].
+* The strongest evidence for [[diabetes]] prevention comes from the Diabetes Prevention Program (DPP). The DPP demonstrated that an intensive lifestyle intervention could reduce the incidence of [[Diabetes mellitus type 2|type 2 diabetes]] by 58% over 3 years.<ref name="pmid17098085">{{cite journal |vauthors=Lindström J, Ilanne-Parikka P, Peltonen M, Aunola S, Eriksson JG, Hemiö K, Hämäläinen H, Härkönen P, Keinänen-Kiukaanniemi S, Laakso M, Louheranta A, Mannelin M, Paturi M, Sundvall J, Valle TT, Uusitupa M, Tuomilehto J |title=Sustained reduction in the incidence of type 2 diabetes by lifestyle intervention: follow-up of the Finnish Diabetes Prevention Study |journal=Lancet |volume=368 |issue=9548 |pages=1673–9 |year=2006 |pmid=17098085 |doi=10.1016/S0140-6736(06)69701-8 |url=}}</ref>
+*Based on a study, life style modification can improve glucose tolerance and decrease the [[cardiovascular]] [[Complication (medicine)|complications]]. Even [[Obesity|obese]] [[Diabetes|diabetic]] patients in this study showed reduced chance of [[diabetes mellitus]] development after 2 years of life style interventions.<ref name="Lindstrom2003">{{cite journal|last1=Lindstrom|first1=J.|title=Prevention of Diabetes Mellitus in Subjects with Impaired Glucose Tolerance in the Finnish Diabetes Prevention Study: Results From a Randomized Clinical Trial|journal=Journal of the American Society of Nephrology|volume=14|issue=90002|year=2003|pages=108S–113|issn=1046-6673|doi=10.1097/01.ASN.0000070157.96264.13}}</ref>
+*Patients with a modified life style had 58% less chance to develop [[diabetes]], compared to the [[Scientific control|control group]] after a 3 years study.<ref name="TuomilehtoLindström2001">{{cite journal|last1=Tuomilehto|first1=Jaakko|last2=Lindström|first2=Jaana|last3=Eriksson|first3=Johan G.|last4=Valle|first4=Timo T.|last5=Hämäläinen|first5=Helena|last6=Ilanne-Parikka|first6=Pirjo|last7=Keinänen-Kiukaanniemi|first7=Sirkka|last8=Laakso|first8=Mauri|last9=Louheranta|first9=Anne|last10=Rastas|first10=Merja|last11=Salminen|first11=Virpi|last12=Aunola|first12=Sirkka|last13=Cepaitis|first13=Zygimantas|last14=Moltchanov|first14=Vladislav|last15=Hakumäki|first15=Martti|last16=Mannelin|first16=Marjo|last17=Martikkala|first17=Vesa|last18=Sundvall|first18=Jouko|last19=Uusitupa|first19=Matti|title=Prevention of Type 2 Diabetes Mellitus by Changes in Lifestyle among Subjects with Impaired Glucose Tolerance|journal=New England Journal of Medicine|volume=344|issue=18|year=2001|pages=1343–1350|issn=0028-4793|doi=10.1056/NEJM200105033441801}}</ref> This life style modification includes [[Physical exercise|physical activity]], [[weight loss]], limiting the total dietary intake, lowering intake of [[saturated fat]] and increasing [[dietary fiber]].<ref>{{cite journal|title=Primary Prevention of Type 2 Diabetes Mellitus by Lifestyle Intervention: Implications for Health Policy|journal=Annals of Internal Medicine|volume=140|issue=11|year=2004|pages=951|issn=0003-4819|doi=10.7326/0003-4819-140-11-200406010-00036}}</ref>
+*Traditionally, life style modifications mainly focused on [[weight loss]], which is still one of the main components. Nevertheless other factors, such as better [[Diabetes management|glycemic control]], careful food selection, regular [[Physical exercise|physical activity]] and consistent visits and behavioral interventions to maintain adherence are also considered crucial in new approaches.<ref name="BuseGinsberg2007">{{cite journal|last1=Buse|first1=John B.|last2=Ginsberg|first2=Henry N.|last3=Bakris|first3=George L.|last4=Clark|first4=Nathaniel G.|last5=Costa|first5=Fernando|last6=Eckel|first6=Robert|last7=Fonseca|first7=Vivian|last8=Gerstein|first8=Hertzel C.|last9=Grundy|first9=Scott|last10=Nesto|first10=Richard W.|last11=Pignone|first11=Michael P.|last12=Plutzky|first12=Jorge|last13=Porte|first13=Daniel|last14=Redberg|first14=Rita|last15=Stitzel|first15=Kimberly F.|last16=Stone|first16=Neil J.|title=Primary Prevention of Cardiovascular Diseases in People With Diabetes Mellitus|journal=Circulation|volume=115|issue=1|year=2007|pages=114–126|issn=0009-7322|doi=10.1161/CIRCULATIONAHA.106.179294}}</ref>
+*Intensive interdisciplinary intervention (II) on [[Diet (nutrition)|dietary]] habits and [[Physical exercise|physical activity]] was related to lower [[blood pressure]], [[Blood sugar|plasma glucose]] and [[binge eating disorder]] ([[Binge eating disorder|BED]]) frequency, compared to 9-month traditional (TI) intervention in patients at risk for [[diabetes]]. Furthermore, both interventions were effective in lowering the frequency of [[depression]] in these people.<ref name="CezarettoSiqueira-Catania2011">{{cite journal|last1=Cezaretto|first1=Adriana|last2=Siqueira-Catania|first2=Antonela|last3=de Barros|first3=Camila Risso|last4=Salvador|first4=Emanuel Péricles|last5=Ferreira|first5=Sandra Roberta G.|title=Benefits on quality of life concomitant to metabolic improvement in intervention program for prevention of diabetes mellitus|journal=Quality of Life Research|volume=21|issue=1|year=2011|pages=105–113|issn=0962-9343|doi=10.1007/s11136-011-9919-2}}</ref>
+*Study on [[aspirin]] in [[Diabetes|diabetic]] patients with no previous history of [[cardiovascular disease]] showed significant reduction in serious vascular events. Nevertheless, the high risk of [[bleeding]] with [[aspirin]] use overshadows this desirable outcome.<ref>{{cite journal|title=Effects of Aspirin for Primary Prevention in Persons with Diabetes Mellitus|journal=New England Journal of Medicine|volume=379|issue=16|year=2018|pages=1529–1539|issn=0028-4793|doi=10.1056/NEJMoa1804988}}</ref>
+*An intervention done on 682 patients with impaired [[glucose tolerance test]], evaluated the effect of [[acarbose]] as a possible agent for preventing the [[diabetes]] development. Based on this study, after 3 months, patients who received [[acarbose]] showed significant conversion to normal [[glucose]] level. On the other hand, patients who received [[placebo]], had increased conversion to [[Diabetes|diabetic]] states.<ref name="ChiassonJosse2002">{{cite journal|last1=Chiasson|first1=Jean-Louis|last2=Josse|first2=Robert G|last3=Gomis|first3=Ramon|last4=Hanefeld|first4=Markolf|last5=Karasik|first5=Avraham|last6=Laakso|first6=Markku|title=Acarbose for prevention of type 2 diabetes mellitus: the STOP-NIDDM randomised trial|journal=The Lancet|volume=359|issue=9323|year=2002|pages=2072–2077|issn=01406736|doi=10.1016/S0140-6736(02)08905-5}}</ref>
 ==References==
 {{reflist|2}}

Diabetes mellitus: Difference between revisions

Latest revision as of 12:57, 9 September 2020

Overview

Classification

Differential diagnosis

Complications

Acute complications

Chronic complications

Macrovascular

Microvascular

Ophthalmic

Neuropathy

Nephropathy

Other organs[6]

Diagnosis

Diabetes mellitus type 1 and type 2

American Diabetes Association Diabetes Diagnostic Criteria 2018 (DO NOT EDIT)[6]

Gestational diabetes

One Step Strategy

Two Step Strategy

Screening

Diabetes mellitus type 1

Diabetes mellitus type 2

Categories of Increased Risk for Diabetes (Prediabetics) Recommendations:

Gestational diabetes

Prevention

References

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Other organs^[6]

American Diabetes Association Diabetes Diagnostic Criteria 2018 (DO NOT EDIT)^[6]