1. Management of Hyperglycemia in Type 2 Diabetes: A Patient-Centered Approach Position Statement of the American Diabetes Association (ADA) and the European Association for the Study of Diabetes (EASD)

2. Writing Group American Diabetes Association Richard M. Bergenstal MD
Int’l Diabetes Center, Minneapolis, MN
John B. Buse MD, PhD
University of North Carolina, Chapel Hill, NC
Anne L. Peters MD
Univ. of Southern California, Los Angeles, CA
Richard Wender MD
Thomas Jefferson University, Philadelphia, PA
Silvio E. Inzucchi MD (co-chair)
Yale University, New Haven, CT
European Assoc. for the Study of Diabetes
Michaela Diamant MD, PhD
VU University, Amsterdam, The Netherlands
Ele Ferrannini MD
University of Pisa, Pisa, Italy
Michael Nauck MD
Diabeteszentrum, Bad Lauterberg, Germany
Apostolos Tsapas MD, PhD
Aristotle University, Thessaloniki, Greece
David R. Matthews MD, DPhil (co-chair)
Oxford University, Oxford, UK

3. PATIENT-CENTERED APPROACH 2. BACKGROUND
ADA-EASD Position Statement: Management of
Hyperglycemia in T2DM: A Patient-Centered Approach
PATIENT-CENTERED APPROACH
2. BACKGROUND
Epidemiology and health care impact
Relationship of glycemic control to outcomes
Overview of the pathogenesis of Type 2 diabetes
3. ANTI-HYPERGLYCEMIC THERAPY
Glycemic targets
Therapeutic options
- Lifestyle
- Oral agents & non-insulin injectables
- Insulin
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

4. 3. ANTIHYPERGLYCEMIC THERAPY
ADA-EASD Position Statement: Management of
Hyperglycemia in T2DM: A Patient-Centered Approach
3. ANTIHYPERGLYCEMIC THERAPY
Implementation Strategies
- Initial drug therapy
- Advancing to dual combination therapy
- Advancing to triple combination therapy
- Transitions to and titrations of insulin
4. OTHER CONSIDERATIONS
Age
Weight
Sex/racial/ethnic/genetic differences
Comorbidities (Coronary artery disease, Heart failure, Chronic kidney disease, Liver dysfunction, Hypoglycemia)
5. FUTURE DIRECTIONS / RESEARCH NEEDS
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

5. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
Patient-Centered Approach
“...providing care that is respectful of and responsive to individual patient preferences, needs, and values - ensuring that patient values guide all clinical decisions.”
Gauge patient’s preferred level of involvement.
Explore, where possible, therapeutic choices.
Utilize decision aids.
Shared decision making – final decisions re: lifestyle choices ultimately lies with the patient.
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

6. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
2. BACKGROUND
Epidemiology and health care impact
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

7. Age-adjusted Percentage of U. S
Age-adjusted Percentage of U.S. Adults with Obesity or Diagnosed Diabetes
Obesity (BMI ≥30 kg/m2)
1994
2000
2009
O B E S I T Y
No Data <14.0% % % % >26.0%
Diabetes
D I A B E T E S
1994
2000
2009
Changes in obesity and diabetes rates in the United States over a 15 year period.
No Data <4.5% % % % >9.0%
CDC’s Division of Diabetes Translation. National Diabetes Surveillance System available at

8. The Diabetes Epidemic: Global Projections, 2010–2030
Figures given are: number of people with diabetes in 2011 and predicted number of people that will have diabetes in 2030 according to IDF estimates. Percentage is the increase in diabetes from 2011 to “World” box acts as the legend.
The burden of diabetes is one of the greatest challenges of the 21st century, as seen in the global incidence and projections of diabetes epidemic worldwide.
366 million people have diabetes in 2011 and this is predicted to rise to 552 million by 2030.
Diabetes caused at least $465 billion in healthcare expenditure in 2011 – 11% of the total expenditure, and is expected to exceed $595 billion by 2030.
IDF. Diabetes Atlas 5th Ed. 2011

9. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
2. BACKGROUND
Relationship of glycemic control to outcomes
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

10. Impact of Intensive Therapy for Diabetes: Summary of Major Clinical Trials
Study
Microvasc
CVD
Mortality
UKPDS  
DCCT / EDIC*
ACCORD 
ADVANCE
VADT
Overview of the microvascular, macrovascular and mortality outcomes from large T2DM and T1DM randomized clinical trials that focused on the relationship between glycemic control and complications.
Kendall DM, Bergenstal RM. © International Diabetes Center 2009
UK Prospective Diabetes Study (UKPDS) Group. Lancet 1998;352:854.
Holman RR et al. N Engl J Med. 2008;359: DCCT Research Group. N Engl J Med 1993;329;977.
Nathan DM et al. N Engl J Med. 2005;353: Gerstein HC et al. N Engl J Med. 2008;358:2545.
Patel A et al. N Engl J Med 2008;358: Duckworth W et al. N Engl J Med 2009;360:129. (erratum:
Moritz T. N Engl J Med 2009;361:1024)
Initial Trial
Long Term Follow-up
* in T1DM

11. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
2. BACKGROUND
Overview of the pathogenesis of T2DM
Insulin secretory dysfunction
Insulin resistance (muscle, fat, liver)
Increased endogenous glucose production
Deranged adipocyte biology
Decreased incretin effect
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

12. Main Pathophysiological Defects in T2DM?
gut
carbohydrate
delivery &
absorption
incretin
effect
pancreatic
insulin
secretion + -
pancreatic
glucagon
secretion
HYPERGLYCEMIA
peripheral
glucose
uptake
hepatic
glucose
production
Adapted from: Inzucchi SE, Sherwin RS in: Cecil Medicine 2011

13. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
3. ANTI-HYPERGLYCEMIC THERAPY
Glycemic targets
HbA1c < 7.0% (mean PG  mg/dl [ mmol/l])
Pre-prandial PG <130 mg/dl (7.2 mmol/l)
Post-prandial PG <180 mg/dl (10.0 mmol/l)
Individualization is key:
Tighter targets ( %) - younger, healthier
Looser targets ( %+) - older, comorbidities, hypoglycemia prone, etc.
Avoidance of hypoglycemia
PG = plasma glucose
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

14. Depiction of the elements of decision-making used to determine appropriate efforts to achieve glycaemic targets. Greater concerns about a particular domain are represented by increasing height of the ramp. Thus, characteristics/predicaments towards the left justify more stringent efforts to lower HbA1c, whereas those towards the right are compatible with less stringent efforts. Where possible, such decisions should be made in conjunction with the patient, reflecting his or her preferences, needs and values. This ‘scale’ is not designed to be applied rigidly but to be used as a broad construct to help guide clinical decisions. Adapted with permission from Ismail-Beigi et al [ref 20]
Figure 1
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]
(Adapted with permission from: Ismail-Beigi F, et al. Ann Intern Med 2011;154:554)

15. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
3. ANTI-HYPERGLYCEMIC THERAPY
Therapeutic options: Lifestyle
Weight optimization
Healthy diet
Increased activity level
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

16. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
3. ANTI-HYPERGLYCEMIC THERAPY
Therapeutic options:
Oral agents & non-insulin injectables
Metformin
Sulfonylureas
Thiazolidinediones
DPP-4 inhibitors
GLP-1 receptor agonists
Meglitinides
a-glucosidase inhibitors
Bile acid sequestrants
Dopamine-2 agonists
Amylin mimetics
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

17. Class Mechanism Advantages Disadvantages Cost
Biguanides
Activates AMP-kinase
 Hepatic glucose production
Extensive experience
No hypoglycemia
Weight neutral
?  CVD
Gastrointestinal
Lactic acidosis
B-12 deficiency
Contraindications
Low
SUs / Meglitinides
Closes KATP channels
 Insulin secretion
 Microvasc. risk
Hypoglycemia
Weight gain
Low durability
? Ischemic preconditioning
TZDs
PPAR-g activator
 insulin sensitivity
Durability
 TGs,  HDL-C
?  CVD (pio)
Edema / heart failure
Bone fractures
?  MI (rosi)
? Bladder ca (pio)
High
a-GIs
Inhibits a-glucosidase
Slows carbohydrate absorption
Nonsystemic
 Post-prandial glucose
?  CVD events
Dosing frequency
Modest  A1c
Mod.
Table 1. Properties of anti-hyperglycemic agents
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

18. Class Mechanism Advantages Disadvantages Cost
DPP-4
inhibitors
Inhibits DPP-4
Increases GLP-1, GIP
No hypoglycemia
Well tolerated
Modest  A1c
? Pancreatitis
Urticaria
High
GLP-1 receptor agonists
Activates GLP-1 R
 Insulin,  glucagon
 gastric emptying
 satiety
Weight loss
? Beta cell mass
? CV protection GI
Medullary ca
Injectable
Amylin mimetics
Activates amylin receptor
 glucagon
 PPG
Hypo w/ insulin
Dosing frequency
Bile acid sequestrants
Bind bile acids
 Hepatic glucose production
Nonsystemic
 Post-prandial glucose
 CVD events
Dopamine-2
agonists
Activates DA receptor
Modulates hypothalamic control of metabolism
 insulin sensitivity
No hypoglyemia
?  CVD events
Dizziness/syncope
Nausea
Fatigue
Table 1. Properties of anti-hyperglycemic agents
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

19. Class Mechanism Advantages Disadvantages Cost
Insulin
Activates insulin receptor
 peripheral glucose uptake
Universally effective
Unlimited efficacy
 Microvascular risk
Hypoglycemia
Weight gain
? Mitogenicity
Injectable
Training requirements
“Stigma”
Variable
Table 1. Properties of anti-hyperglycemic agents
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

20. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
3. ANTI-HYPERGLYCEMIC THERAPY
Therapeutic options: Insulin
- Neutral protamine Hagedorn (NPH)
- Regular
- Basal analogues (glargine, detemir)
- Rapid analogues (lispro, aspart, glulisine)
- Pre-mixed varieties
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

21. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
3. ANTI-HYPERGLYCEMIC THERAPY
Therapeutic options: Insulin
Rapid (Lispro, Aspart, Glulisine)
Short (Regular)
Insulin level
Intermediate (NPH)
Diagrammatic representation of the approximate pharmacokinetic properties of various insulin formulations.
Long (Detemir)
Long (Glargine)
Hours
Hours after injection

22. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
3. ANTI-HYPERGLYCEMIC THERAPY
Implementation strategies:
Initial therapy
Advancing to dual combination therapy
Advancing to triple combination therapy
Transitions to & titrations of insulin
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

23. T2DM Antihyperglycemic Therapy: General Recommendations
Moving from the top to the bottom of the figure, potential sequences of anti-hyperglycaemic therapy. In most patients, begin with lifestyle changes; metformin monotherapy is added at, or soon after, diagnosis (unless there are explicit contraindications).
T2DM Antihyperglycemic Therapy: General Recommendations
Diabetes Care, Diabetologia. 19 April 2012
[Epub ahead of print]

24. T2DM Antihyperglycemic Therapy: General Recommendations
If the A1c target is not achieved after ~3 months, consider one of the 5 treatment options combined with metformin (dual combination): a sulfonylurea, TZD, DPP-4 inhibitor, GLP-1 receptor agonist or basal insulin. Note that the order in the chart is determined by historical introduction andr oute of administration and is not meant to denote any specific preference. Choice is based on patient and drug characteristics, with the over-riding goal of improving glycemic control while minimizing side effects. Shared decision-making with the patient may help in the selection of therapeutic options.
Rapid-acting secretagogues (meglitinides) may be used in place of sulfonylureas. Consider in patients with irregular meal schedules or who develop late postprandialhypoglycemia on sulfonylureas. Other drugs not shown (α-glucosidase inhibitors, colesevelam, dopamine agonists, pramlintide) may be used where available in selected patients but have modest efficacy and/or limiting side effects.
In patients intolerant of, or with contraindications for, metformin, select initial drug from other classes depicted, and proceed accordingly.
Consider starting with 2-drug combinations in patients with very high HbA1c (e.g. ≥9%).
T2DM Antihyperglycemic Therapy: General Recommendations
Diabetes Care, Diabetologia. 19 April 2012
[Epub ahead of print]

25. T2DM Antihyperglycemic Therapy: General Recommendations
Further progression to 3-drug combinations are reasonable if 2-drug combinations do not achieve target. If metformin contraindicated or not tolerated, while published trials are generally lacking, it is reasonable to consider 3-drug combinations other than metformin.
Insulin is likely to be more effective than most other agents as a third-line therapy, especially when HbA1c is very high (e.g. ≥9.0%). The therapeutic regimen should include some basal insulin before moving to more complex insulin strategies (see Fig. 3)
T2DM Antihyperglycemic Therapy: General Recommendations
Diabetes Care, Diabetologia. 19 April 2012
[Epub ahead of print]

26. Ultimately, more intensive insulin regimens may be required (see Figure 3.)
Dashed arrow line on the left-hand side of the figure denotes the option of a more rapid progression from a 2-drug combination directly to multiple daily insulin doses, in those patients with severe hyperglycaemia (e.g. HbA1c ≥ %).
Consider beginning with insulin if patient presents with severe hyperglycemia (≥ mg/dl [≥ mmol/l]; HbA1c ≥ %) with or without catabolic features (weight loss, ketosis, etc).
Diabetes Care, Diabetologia.
19 April 2012 [Epub ahead of print]

27. Sequential Insulin Strategies in T2DM
Basal insulin alone is usually the optimal initial regimen, beginning at U/kg body weight, depending on the degree of hyperglycemia. It is usually prescribed in conjunction with 1-2 non-insulin agents. In patients willing to take >1 injection and who have higher A1c levels (≥9.0%), BID pre-mixed insulin or a more advanced basal plus mealtime insulin regimen could also be considered (curved dashed arrow lines).
When basal insulin has been titrated to an acceptable FPG but A1c remains above target, consider proceeding to basal + meal-time insulin, consisting of 1-3 injections of rapid-acting analogues. A less studied alternative—progression from basal insulin to a twice daily pre-mixed insulin—could be also considered (straight dashed arrow line); if this is unsuccessful, move to basal + mealtime insulin.
The figure describes the number of injections required at each stage, together with the relative complexity and flexibility. Once a strategy is initiated, titration of the insulin dose is important, with dose adjustments made based on the prevailing BG levels as reported by the patient.
Non-insulin agents may be continued, although insulin secretagogues (sulfonylureas, meglitinides) are typically stopped once more complex regimens beyond basal insulin are utilized.
Comprehensive education regarding self-monitoring of BG, diet, exercise, and the avoidance of, and response to, hypoglycemia are critical in any patient on insulin therapy.
Sequential Insulin Strategies in T2DM
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

28. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
4. OTHER CONSIDERATIONS
Age
Weight
Sex / racial / ethnic / genetic differences
Comorbidities
Coronary artery disease
Heart Failure
Chronic kidney disease
Liver dysfunction
Hypoglycemia
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

29. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
4. OTHER CONSIDERATIONS
Age: Older adults
Reduced life expectancy
Higher CVD burden
Reduced GFR
At risk for adverse events from polypharmacy
More likely to be compromised from hypoglycemia
Less ambitious targets
HbA1c <7.5–8.0% if tighter targets not easily achieved
Focus on drug safety
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

30. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
4. OTHER CONSIDERATIONS
Weight
Majority of T2DM patients overweight / obese
Intensive lifestyle program
Metformin
GLP-1 receptor agonists
? Bariatric surgery
Consider LADA in lean patients
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

31. T2DM Anti-hyperglycemic Therapy: General Recommendations
Overview of anti-hyperglycemic therapy in T2DM (Figure 2.) What follows are variations of this figure to help guide the clinician in choosing agents which may be most appropriate under certain situations: to avoid weight gain, to avoid hypoglycemia, and to minimize costs.
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]
T2DM Anti-hyperglycemic Therapy: General Recommendations

32. Adapted Recommendations: When Goal is to Avoid Weight Gain
Fig. 2A should be considered when the goal is to avoid hypoglycemia. Note that "hidden" agents may obviously still be used when required, but additional care is needed to avoid adverse events. Here, the risk of hypoglycemia when using the hidden agents will be, in part, dependent on the baseline degree of hyperglycemia, the treatment target, and the adequacy of patient education.
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]
Adapted Recommendations: When Goal is to Avoid Weight Gain

33. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
4. OTHER CONSIDERATIONS
Sex/ethnic/racial/genetic differences
Little is known
MODY & other monogenic forms of diabetes
Latinos: more insulin resistance
East Asians: more beta cell dysfunction
Gender may drive concerns about adverse effects (e.g., bone loss from TZDs)
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

34. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
4. OTHER CONSIDERATIONS
Comorbidities
Coronary Disease
Heart Failure
Renal disease
Liver dysfunction
Hypoglycemia
Metformin: CVD benefit (UKPDS)
Avoid hypoglycemia
? SUs & ischemic preconditioning
? Pioglitazone &  CVD events
? Effects of incretin-based therapies
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

35. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
4. OTHER CONSIDERATIONS
Comorbidities
Coronary Disease
Heart Failure
Renal disease
Liver dysfunction
Hypoglycemia
Metformin: May use unless condition is unstable or severe
Avoid TZDs
? Effects of incretin-based therapies
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

36. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
4. OTHER CONSIDERATIONS
Comorbidities
Coronary Disease
Heart Failure
Renal disease
Liver dysfunction
Hypoglycemia
Increased risk of hypoglycemia
Metformin & lactic acidosis
US: ≥ 1.5 (1.4 women)
UK:  <45 & <30
Caution with SUs (esp. glyburide)
DPP-4-i’s – dose adjust for most
Avoid exenatide if GFR <30
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

37. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
4. OTHER CONSIDERATIONS
Comorbidities
Coronary Disease
Heart Failure
Renal disease
Liver dysfunction
Hypoglycemia
Most drugs not tested in advanced liver disease
Pioglitazone may help steatosis
Insulin best option if disease severe
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

38. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
4. OTHER CONSIDERATIONS
Comorbidities
Coronary Disease
Heart Failure
Renal disease
Liver dysfunction
Hypoglycemia
Emerging concerns regarding association with increased mortality
Proper drug selection in the hypoglycemia prone
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

39. T2DM Anti-hyperglycemic Therapy: General Recommendations
Overview of anti-hyperglycemic therapy in T2DM (Figure 2.) What follows are variations of this figure to help guide the clinician in choosing agents which may be most appropriate under certain situations: to avoid weight gain, to avoid hypoglycemia, and to minimize costs.
T2DM Anti-hyperglycemic Therapy: General Recommendations
Diabetes Care, Diabetologia. 19 April 2012
[Epub ahead of print]

40. Adapted Recommendations: When Goal is to Avoid Hypoglycemia
Fig. 2B should be considered when the goal is to avoid weight gain. Note that "hidden" agents may obviously still be used when required, but additional care is needed to avoid adverse events. Here, the chances of weight gain when using the hidden agents will be mitigated by more rigorous adherence to dietary recommendations and optimal dosing.
Adapted Recommendations: When Goal is to Avoid Hypoglycemia
Diabetes Care, Diabetologia. 19 April 2012
[Epub ahead of print]

41. Adapted Recommendations: When Goal is to Minimize Costs
Fig. 2C should be considered when the goal is to minimize costs. This reflects prevailing costs in the North America and Europe in early 2012; costs of certain drugs may vary considerably from country to country and as generic formulations become available.  
Adapted Recommendations: When Goal is to Minimize Costs
Diabetes Care, Diabetologia. 19 April 2012
[Epub ahead of print]

42. Guidelines for Glycemic, BP, & Lipid Control
American Diabetes Assoc. Goals
HbA1C
< 7.0% (individualization)
Preprandial glucose
mg/dL ( mmol/l)
Postprandial glucose
< 180 mg/dL
Blood pressure
< 130/80 mmHg
Lipids
LDL: < 100 mg/dL (2.59 mmol/l)
< 70 mg/dL (1.81 mmol/l) (with overt CVD)
HDL: > 40 mg/dL (1.04 mmol/l)
> 50 mg/dL (1.30 mmol/l)
TG: < 150 mg/dL (1.69 mmol/l)
Avoiding ‘glucocentricity’ is key in the comprehensive management of the patient with T2DM. Cardiovascular risk factor reduction must incorporate blood pressure and lipid control, in addition to, where indicated, anti-platelet therapy.
HDL = high-density lipoprotein; LDL = low-density lipoprotein; PG = plasma glucose; TG = triglycerides.
ADA. Diabetes Care. 2012;35:S11-63

43. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
4. FUTURE DIRECTIONS / RESEARCH NEEDS
Comparative effectiveness research
Focus on important clinical outcomes
Contributions of genomic research
Perpetual need for clinical judgment!
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

44. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
KEY POINTS
Glycemic targets & BG-lowering therapies must be individualized.
Diet, exercise, & education: foundation of any T2DM therapy program
Unless contraindicated, metformin = optimal 1st-line drug.
After metformin, data are limited. Combination therapy with 1-2 other oral / injectable agents is reasonable; minimize side effects.
Ultimately, many patients will require insulin therapy alone / in combination with other agents to maintain BG control.
All treatment decisions should be made in conjunction with the patient (focus on preferences, needs & values.)
Comprehensive CV risk reduction - a major focus of therapy.
Diabetes Care, Diabetologia. 19 April 2012 [Epub ahead of print]

45. ADA-EASD Position Statement: Management of Hyperglycemia in T2DM
Invited Reviewers
James Best, The University of Melbourne, AU
Henk Bilo, Isala Clinics, Zwolle, NL
John Boltri, Wayne State University, Detroit, MI
Thomas Buchanan, Univ of So California, LA, CA
Paul Callaway, University of Kansas,Wichita, KS
Bernard Charbonnel, University of Nantes, France
Stephen Colagiuri, The University of Sydney, AS
Samuel Dagogo-Jack, Univ of Tenn, Memphis, TN
Margo Farber, Detroit Medical Center, Detroit, MI
Cynthia Fritschi, University of Illinois, Chicago, IL
Rowan Hillson, Hillingdon Hospital, Uxbridge, U.K.
Faramarz Ismail-Beigi, CWR Univ, Cleveland, OH
Devan Kansagara, Oregon H&S Univ, Portland, OR
Ilias Migdalis, NIMTS Hospital, Athens, Greece
Donna Miller, Univ of So California, LA, CA
Robert Ratner, MedStar/Georgetown Univ, DC
Julio Rosenstock, Dallas Diab/Endo Ctr, Dallas, TX
Guntram Schernthaner, Rudolfstiftung Hosp, Vienna, AT
Robert Sherwin, Yale University, New Haven, CT
Jay Skyler, University of Miami, Miami, FL
Geralyn Spollett, Yale University,New Haven, CT
Ellie Strock, Int’l Diabetes Center, Minneapolis, MN
Agathocles Tsatsoulis, University of Ioannina, GR
Andrew Wolf, Univ of Virginia Charlottesville, VA
Bernard Zinman, University of Toronto, CA
Professional Practice Committee, American Diabetes Association
Panel for Overseeing Guidelines and Statements, European Association for the Study of Diabetes
American Association of Diabetes Educators
The Endocrine Society
American College of Physicians