III. Therapeutics of Type 2 Diabetes Mellitus

Question 1

The risk of heart disease and stroke is commonly stated to be ___ times higher for people with diabetes than for those without diabetes.

Answer 1

2-4 times

Question 2

Lower-extremity amputation is approximately ___ times higher for people with diabetes than for those without diabetes.

Answer 2

20 times

Question 3

Life expectancy is reduced by approximately ___ years in people with diabetes.

Answer 3

10 years

Question 4

The hazard ratio for death is most pronounced in those having diabetes under ___ years.

Answer 4

55 years

Question 5

Convert mmol/L to mg/dL by ___

Answer 5

Multiply by 18

Question 6

Fasting plasma glucose in mg/L that is diagnostic for prediabetes and diabetes (no calorie intake at least 8 hours)

Answer 6

100-125
>=126

Question 7

2-hour plasma glucose in mg/L that is diagnostic for prediabetes and diabetes (after 75g oral glucose)

Answer 7

140-199
>=200

Question 8

Random plasma glucose in mg/L that is diagnostic for diabetes (with classic symptoms)

Answer 8

> =200

(not applicable for prediabetes)

Question 9

HbA1c that is diagnostic for prediabetes and diabetes

Answer 9

5.7-6.4%
>=6.5%

Question 10

TRUE or FALSE: Diagnosis of diabetes should be confirmed by repeat testing.

Answer 10

TRUE, in the absence of unequivocal hyperglycemia

A confirmatory test by the same or a different method is usually required to confirm the diagnosis.

Question 11

The primary endpoint used to evaluate the relationship between glucose levels and complications

Answer 11

Retinopathy

Question 12

Not recommended for routine use in diagnosing diabetes
a. Fasting plasma glucose
b. 2-hour plasma glucose (OGTT)
c. Random plasma glucose
d. HbA1c

Answer 12

B

Question 13

People with undiagnosed T2DM have approximately ___fold greater risk for coronary heart disease, stroke, and peripheral vascular disease.

Answer 13

Twofold

Question 14

Who among the following should be tested for diabetes (ADA 2018)? (all that applies)
a. 44/M, Asian, BMI 22, with active lifestyle
b. 32/F, Asian, BMI 24, active lifestyle
c. 24/F, Asian, BMI 22, with PCOS
d. 50/M, Caucasian, BMI 19, with no comorbidity
e. 28/F, Asian, BMI 18, with history of GDM lost to follow-up

Answer 14

A, B, D, and E

Question 15

4 Populations that should be tested for prediabetes

Answer 15

1. Overweight or obese (BMI >=25 or >=23 in Asians) + 1 or more risk factor
2. Patients with prediabetes (yearly)
3. Patients with prior GDM (at least every 3 years)
4. All others - begin at age 45 (begin at age 35 based on ADA 2022)

Question 16

Risk factors that, if present in an overweight/obese person, should prompt testing for prediabetes

Answer 16

General profile:
1. High-risk ethnicity (e.g., African, Latino, Native American, Asian, Pacific Islander)

Past Medical History:
1. History of cardiovascular disease
2. Hypertension (BP >=140/90 or using BP-lowering therapy)
3. PCOS

Personal/Social History:
1. Physical inactivity

Family History:
1. First-degree relatives with diabetes

Objective:
1. Severe obesity
2. Acanthosis nigricans
3. HDL <35 mg/dL and/or triglycerides >250 mg/dL

*Other conditions associated with insulin resistance (e.g., severe obesity, acanthosis nigricans)

Question 17

Level of HDL and triglycerides considered a risk factor for prediabetes in asymptomatic adults

Answer 17

HDL <35 mg/dL and/or triglycerides >250 mg/dL

Question 18

Frequency of testing for asymptomatic adults with prediabetes

Answer 18

Yearly

Question 19

Frequency of testing for asymptomatic adults with history of gestational diabetes

Answer 19

At least every 3 years

Question 20

Age at which to start testing for prediabetes in asymptomatic adults (if without other risk factor)

Answer 20

45 years old (35 based on ADA)

Question 21

If initial results for testing for prediabetes are normal, when to repeat?

Answer 21

At least every 3 years

Question 22

What is the United Kingdom Prospective Diabetes Study (UKPDS)?

Answer 22

Prospective, randomized trial that documented reduced rates of microvascular complications in T2DM patients treated to lower glycemic targets and with pharmacotherapy compared to lifestyle alone

Question 23

Treatment effect of sulfonylurea or insulin in the UKPDS (% relative risk reduction and if significant) at end of randomized treatment
a. Any diabetes-related endpoint
b. Microvascular disease
c. Myocardial infarction
d. All-cause mortality

Answer 23

a. Any diabetes-related endpoint - 12% (significant)
b. Microvascular disease - 25% (significant)
c. Myocardial infarction - 16% (NS)
d. All-cause mortality - 6% (NS)

Question 24

Treatment effect of sulfonylurea or insulin in the UKPDS (% relative risk reduction and if significant) after 10 years of further observation
a. Any diabetes-related endpoint
b. Microvascular disease
c. Myocardial infarction
d. All-cause mortality

Answer 24

a. Any diabetes-related endpoint - 9% (significant)
b. Microvascular disease - 24% (significant)
c. Myocardial infarction - 15% (significant)
d. All-cause mortality - 13% (significant)

Question 25

Treatment effect of metformin in the UKPDS (% relative risk reduction and if significant) at end of randomized treatment
a. Any diabetes-related endpoint
b. Microvascular disease
c. Myocardial infarction
d. All-cause mortality

Answer 25

a. Any diabetes-related endpoint - 32% (significant)
b. Microvascular disease - 29% (NS)
c. Myocardial infarction - 39% (significant)
d. All-cause mortality - 36% (significant)

Question 26

Treatment effect of metformin the UKPDS (% relative risk reduction and if significant) after 10 years of further observation
a. Any diabetes-related endpoint
b. Microvascular disease
c. Myocardial infarction
d. All-cause mortality

Answer 26

a. Any diabetes-related endpoint - 21% (significant)
b. Microvascular disease - 16% (NS)
c. Myocardial infarction - 33% (significant)
d. All-cause mortality - 27% (significant)

Question 27

This “effect” is believed to be responsible for the persistence of the relative benefits of more intensive management of glucose after 10 more years of observation in the UKPDS (even though the difference in glycemic control was not maintained)

Answer 27

“Legacy effect” of initially good glycemic control, likely based on persisting changes of tissue structure in blood vessels and elsewhere

Question 28

Kumamoto study results

Answer 28

Japanese patients with T2DM with normal weight randomized into standard or intensive treatment with insulin –> Lower HbA1c with modestly increased risk of hypoglycemia and weight gain, reduction in microvascular complications, and a (not statistically significant) trend toward reduced rates of cardiovascular events

Question 29

TRUE or FALSE: The Action to Control Cardiovascular Risk in Diabetes (ACCORD), Action in Diabetes and Vascular Disease - Preterax and Diamicron Modified Release Controlled Evaluation (ADVANCE), and the Veterans Affairs Diabetes Trial (VADT) - which randomized middle-aged and older individuals into standard and intensive treatment - all demonstrated significant benefit in combined cardiovascular endpoints.

Answer 29

FALSE

None of the trials demonstrated significant benefit in combined cardiovascular endpoints.

Question 30

The ACCORD study showed that a __% increase in total mortality accompanied intensive therapy.

Answer 30

22%

Question 31

ADA target preprandial plasma glucose

Answer 31

80-130 mg/dL

Question 32

ADA target peak postprandial plasma glucose

Answer 32

<180 mg/dL (1 to 2 hours after any meal)

Question 33

ADA target mean plasma glucose

Answer 33

<154 mg/dL

Question 34

ADA target HbA1c

Answer 34

<7%

Question 35

ADA - may pursue lower target HbA1c in ___

Answer 35

Those with recent-onset disease, long life expectancy, and no significant cardiovascular disease, if they can be achieved without significant hypoglycemia or other adverse effects of treatment

Question 36

ADA - may pursue less stringent HbA1c at 7-8% in ___

Answer 36

Those at high risk, including a history of severe hypoglycemia, limited life expectancy, advanced complications, or extensive comorbid conditions, as well as inability to achieve HbA1c less than 7% despite the usual initial therapeutic efforts

Question 37

ACE target fasting glucose

Answer 37

<110 mg/dL

Question 38

ACE target 2-hour postprandial glucose

Answer 38

<140 mg/dL

Question 39

ACE target HbA1c

Answer 39

<6.5%

Question 40

Frequency of HbA1c monitoring

Answer 40

When treatment is started or intensified, measurement at approximately 3-month intervals will reveal the success of the intervention.

When treatment is established and glycemic control appears stable, testing one or two times a year is usually sufficient.

Question 41

Term used to refer to the mismatch between glucose and HbA1c levels

Answer 41

Glycation cap

Question 42

Increased red cell turnover such as in occult blood loss or iron treatment of iron deficiency anemia could lead to a ___ HbA1c

Answer 42

Lower

Question 43

Low red cell turnover such as in untreated iron deficiency anemia could lead to a ___ HbA1c

Answer 43

Higher

Question 44

Use of self-monitoring of blood glucose is particularly recommended for patients with T2DM who are taking ___

Answer 44

Insulin or sulfonylureas

Question 45

TRUE or FALSE: One basic principle is that patients should test blood glucose at the same time each day.

Answer 45

FALSE

One basic principle is that patients should periodically vary the time of day at which glucose is tested.

Question 46

Finding of the Structured Testing Program (STeP) trial

Answer 46

Use of 7-point daily glucose testing for 3 days each quarter increased the frequency of treatment adjustments and improved HbA1c levels

Question 47

Criteria for ADA Level 1 Hypoglycemia (Alert value)

Answer 47

Blood glucose <70 mg/dL and >=54 mg/dL

Triggers physiologic responses of the so-called counterregulatory hormones

Question 48

Criteria for ADA Level 2 Hypoglycemia (Clinically significant)

Answer 48

Blood glucose <=54 mg/dL

Can cause blunting of compensatory hormone responses and loss of warning symptoms (“hypoglycemia unawareness”)

Question 49

Criteria for ADA Level 3 Hypoglycemia (Severe)

Answer 49

Altered mental and/or physical status requiring assistance

Strongly associated with risk of physical injury, cardiovascular events, and death

Question 50

Diabetes self-management education and support (DSMES) is recommended to be emphasized at these 4 critical settings in the evolution of T2DM

Answer 50

1. At diagnosis
2. Annual assessment
3. When complicating factors arise
4. When critical transitions in medical care occur or life circumstances

Question 51

Recent guidelines recommend ___ MNT sessions in the first 6 months after diagnosis

Answer 51

3-6

Question 52

Medical nutrition therapy has been shown to decrease HbA1c by __ to __%.

Answer 52

0.3% to 2%

Question 53

Achieving a __% weight loss more consistently yields significant metabolic benefits than lower levels of weight loss, and benefits obese and overweight prediabetic and diabetic patients.

Answer 53

5%

Question 54

In general, the critical nutrient for glycemic consistency

Answer 54

Carbohydrate

Question 55

TRUE or FALSE: Whereas the beta cell in T2DM has usually lost its immediate response to glucose, the second phase of insulin secretion is largely spared in T2DM and is in part driven by amino acids and fatty acids.

Answer 55

TRUE

Question 56

TRUE or FALSE: There is no single ideal dietary distribution of calories among macronutrients.

Answer 56

TRUE

Question 57

What is the glycemic index?

Answer 57

The glycemic index refers to the glucose response to equal amounts of carbohydrates in various foods.

Question 58

Nutrient that is most closely associated in epidemiologic studies with the risk of developing T2DM

Answer 58

Fat (but has little effect on glycemia)

Question 59

Critical nutrient for cardiovascular risk management

Answer 59

Fat

Question 60

TRUE or FALSE: Dietary protein has little impact on glucose levels.

Answer 60

TRUE

Question 61

TRUE or FALSE: Metabolism of protein results in the formation of acids and nitrogenous waste, which can lead to bone demineralization and glomerular hyperfiltration.

Answer 61

TRUE

Question 62

At least ___g of high-quality dietary protein per kilogram of body weight is generally recommended.

Answer 62

0.8g

Recent guidelines do not support the notion that dietary protein need to be reduced in those with CKD.
No evidence for a distinction between the effects of vegetable-based versus animal-based protein sources in kidney function.

Question 63

Restriction of protein intake to __ to __% of total calories minimizes potential adverse long-term effects of high protein intake.

Answer 63

10 to 20%

Question 64

Carbohydrate sources high in ___ should be avoided when trying to treat or prevent hypoglycemia.

Answer 64

Proteins

Ingested protein appears to increase insulin response without increasing plasma glucose concentrations.

Question 65

Eating foods rich in ___, such as fatty fish (EPA and DHA) and nuts and seeds (ALA), is recommended to prevent or treat CVD.

Answer 65

Long-chain n-3 fatty acids

(However, evidence does not support a beneficial role for routine use of n-3 dietary supplements.)

Question 66

Eating foods rich in long-chain n-3 fatty acids, such as fatty fish (EPA and DHA) and nuts and seeds (ALA), is recommended to prevent or treat ___.

Answer 66

CVD

Question 67

TRUE or FALSE: Micronutrients and herbal supplements have proven benefit and are generally recommended in T2DM patients.

Answer 67

FALSE

Question 68

There may be some benefit on HbA1c and lipid profiles for those ingesting at least __g of fiber per 1000kcal compared to lower fiber diets.

Answer 68

15g

Question 69

TRUE or FALSE: Alcohol in moderation (up to 1 drink per day for adult women or 2 drinks per day in adult men) is not specifically recommended.

Answer 69

TRUE

..but is considered acceptable.

Question 70

Risk of excessive intake of alcohol by people with T2DM, especially those who use sulfonylureas or insulin

Answer 70

Delayed hypoglycemia, which typically occurs at night when ability to recognize hypoglycemia is impaired

Question 71

TRUE or FALSE: Moderate red wine intake may result in mild improvement in some lipid parameters but seems to have little effect on glucose control.

Answer 71

TRUE

Question 72

TRUE or FALSE: Nonnutritive sweeteners do not appear to impact lipid parameters, insulin secretion, or blood pressure independent of weight loss, and are deemed safe in any amount.

Answer 72

FALSE

Deemed safe for use in T2DM if consumed within the FDA recommended daily intake amounts

Question 73

Recommended sodium restriction in patients with diabetes

Answer 73

Less than 2300 mg per day (as with the general population, but those with hypertension may have additional benefit from lower sodium diets)

Question 74

TRUE or FALSE: Ketogenic diets or low carbohydrate diets have evidence of long-term benefit in patients with diabetes.

Answer 74

FALSE

Limited long-term evidence of benefit or risk at the present time.

Question 75

3 most validated meal plans in T2DM

Answer 75

1. Mediterranean diet
2. Dietary Approaches to Stop Hypertension (DASH)
3. Plant-based diets

Question 76

Meal plan that has the best experiment support for glycemic control, cardiovascular protection, and perhaps other outcomes

Answer 76

Mediterranean diet (emphasizing the use of monounsaturated and polyunsaturated fats)

Question 77

Self-directed structured exercise programs have been associated with mean HbA1c reductions of __ to __%.

Answer 77

0.4 to 0.9%

Question 78

After exercise, improvements in glycemic control are usually apparent immediately, but the improvement in insulin resistance may not last more than __ to __ hours.

Answer 78

48 to 72 hours

Question 79

Recommended duration of physical activity

Answer 79

150 minutes of moderate-intensity physical activity (50-70% of maximum heart rate) or 75 minutes of vigorous exercise (>70% of maximum heart rate) on at least 3 days per week, with no more than 2 consecutive days without exercise

*Max heart rate = 220 - age

Question 80

Recommended type of physical activity

Answer 80

Both aerobic and resistance exercise are effective and recommended.

Question 81

Major role for the physician in terms of physical activity of patients with T2DM

Answer 81

The major role for the physician is to screen for complications (neuropathy, nephropathy, retinopathy, vascular disease) and discover ways for patients to be able to exercise safely.

Question 82

For the average patients with T2DM starting an exercise program it is best to start with ___-level activity such as ___ at a pace of ___.

Answer 82

Low-level
Walking
2 miles per hour

Question 83

TRUE or FALSE: Exercise can increase albuminuria acutely.

Answer 83

TRUE

Exercise does not appear to accelerate kidney disease but will increase albuminuria acutely and could cause false-positive albumin:creatinine ratios temporarily.

Question 84

Recommended frequency of activity break in all individuals

Answer 84

At least every 30 minutes, to include brief walks, resistance exercise, or at least standing

Question 85

Recommended frequency for screening for diabetes distress

Answer 85

At least once yearly, as depression is present in about 25% of screened patients

Question 86

Mechanism of effect on glucose of biguanide

Answer 86

Decrease hepatic glucose production

Question 87

Mechanism of effect on glucose of secretagogue

Answer 87

Increase insulin secretion

Question 88

Mechanism of effect on glucose of thiazolidinedione

Answer 88

Decrease insulin resistance

Question 89

Mechanism of effect on glucose of DPP4 inhibitor

Answer 89

Increase insulin, decrease glucagon

Question 90

Mechanism of effect on glucose of alpha-glucosidase inhibitor

Answer 90

Delay carbohydrate absorption

Question 91

Mechanism of effect on glucose of SGLT inhibitor

Answer 91

Increase renal clearance of glucose, sodium

Question 92

Mechanism of effect on glucose of bile acid sequestrant

Answer 92

Delay carbohydrate absorption?

Question 93

Mechanism of effect on glucose of dopamine agonist

Answer 93

Decrease insulin resistance

Question 94

Mechanism of effect on glucose of insulin

Answer 94

Increase insulin availability

Question 95

Mechanism of effect on glucose of GLP1 receptor agonist

Answer 95

Increase insulin, decrease glucagon, slow gastric emptying

Question 96

Mechanism of effect on glucose of amylin receptor agonist

Answer 96

Decrease glucagon, slow gastric emptying

Question 97

Which classes of agents have +++ basal glucose control?

Answer 97

Insulin
Secretagogue
Biguanide
Thiazolidinedione
GLP1 receptor agonist

Question 98

Which classes of agents have +++ prandial glucose control?

Answer 98

Insulin
GLP1 receptor agonist
Alpha-glucosidase inhibitor
Amylin receptor agonist

Question 99

Which classes of agents have +++ weight control?

Answer 99

SGLT inhibitor
GLP1 receptor agonist
Amylin receptor agonist

Question 100

Which classes of agents cause weight increase?

Answer 100

Insulin
Secretagogue
Thiazolidinedione

Question 101

Which classes of agents have no effect on weight?

Answer 101

DPP4 inhibitor
Bile-acid sequestrant

Question 102

Which classes of agents have ++ BP control?

Answer 102

SGLT inhibitor
GLP1 receptor agonist

Question 103

Which classes of agents have +++ short-term CV reduction?

Answer 103

SGLT inhibitor

Question 104

*Table 35.10 Classes of antihyperglycemic agents for type 2 diabetes. Page 1385

Answer 104

*

Question 105

Most common adverse events of biguanides

Answer 105

Gastrointestinal: nausea, abdominal pain or bloating, and diarrhea

Question 106

Advantage of using sustained-release metformin

Answer 106

Less frequent and less severe upper GI symptoms, but can increase the frequency of diarrhea, which is overall less common

Question 107

TRUE or FALSE: Lactic acidosis from metformin is common.

Answer 107

FALSE

Metformin has been said to cause lactic acidosis, which is quite rate and occurs almost exclusively in patients who are at high risk for development of the condition independent of metformin therapy.

Question 108

Route of metabolism and clearance of metformin

Answer 108

Metformin is not metabolized and is cleared only through the kidney.

Question 109

Recommended eGFR monitoring if metformin is to be given

Answer 109

Obtain an eGFR before starting metformin and at least annually thereafter

Question 110

Treatment decisions regarding metformin if eGFR is below 45 mL/min/1.73m2

Answer 110

Initiation is not recommended;
If treatment is established, consider dose reduction

Question 111

Treatment decisions regarding metformin if eGFR is below 30 mL/min/1.73m2

Answer 111

Initiation is contraindicated;
If treatment is established, metformin should be stopped

Question 112

Contraindications for metformin use

Answer 112

Hepatic insufficiency
Alcohol abuse
eGFR <30 mL/min/1.73m2

Question 113

Vitamin supplementation for patients using metformin

Answer 113

Supplementation with vitamin B 12(e.g., 1000 mcg daily) or intermittent monitoring may sometimes be prudent.

Question 114

Maximal daily dose of metformin

Answer 114

2550 mg

But does not generally provide additional benefit beyond that seen at 2000 mg daily

Question 115

Drug class that arguably has the best record among oral antihyperglycemic agents in medical outcome studies

Answer 115

Metformin

Question 116

Drug that is generally recommended to be started in all patients with T2DM at or near the time of diagnosis of diabetes, provided no contraindications are present

Answer 116

Metformin

Question 117

Currently available secretagogues all bind to the ___ receptor

Answer 117

SUR1, subunit of K ATP potassium channel on the plasma membrane of pancreatic beta cells

Question 118

TRUE or FALSE: The effect of secretagogues on insulin secretion wane on subsequent doses.

Answer 118

TRUE

A direct effect on insulin secretion, independent of ambient glucose levels, is seen with the first dose of any secretagogue. However, this direct effect wanes during continued occupancy of SUR1, while potentiation of the effect of current glucose levels continues.

Question 119

Classes of secretagogues

Answer 119

Sulfonylureas
Non-sulfonylureas: Meglitinides, Nateglinides

Question 120

Differentiate the secretagogues in terms of risk of hypoglycemia, effect on postprandial glucose, and effect on fasting glucose

Answer 120

Long-acting Sulfonylureas (glipizide-ER, glimepiride, gliclazide-MR) - Lower fasting glucose levels with little effect on postprandial glucose levels, and relatively low risk of hypoglycemia compared with other secretagogues

Shorter-acting Sulfonylureas (glipizide, glyburide, gliclazide) - As effective as longer-acting agents in overall glucose control, but have greater effect on postprandial hyperglycemia and can cause daytime hypoglycemia when food intake is reduced

Meglitinides (repaglinide) - Have faster and briefer stimulus to insulin secretion than short-acting sulfonylureas, hence better postprandial control and generally less hypoglycemia, but has long residence time on SUR1 and therefore some effect on fasting glucose

Nateglinide - Quicker onset and shorter duration of action than repaglinide, hence, its effect in lowering postprandial glucose is quite specific, and has little effect on fasting glucose, and less overnight hypoglycemia. Disadvantage is less overall glucose-lowering effectiveness

Question 121

Long-acting sulfonylurea that is cleared only by the kidney and thus can cause severe hypoglycemia when renal function becomes impaired

Answer 121

Chlorpropamide

None of the other agents is strongly dependent on renal excretion

Question 122

Short-acting sulfonylurea that has an active metabolite that can be cleared only by the kidney

Answer 122

Glyburide (hence associated with greater risk of hypoglycemia than other currently used sulfonylureas)

Question 123

Reason for the concern that sulfonylureas might cause increased arrhythmic cardiovascular events in patients with diabetes

Answer 123

They have an effect on SUR2 subunits of the K ATP complex in vascular and cardiac cells. Binding to SUR2 can blunt ischemic preconditioning, a normal cardioprotective mechanism.

Question 124

TRUE or FALSE: The ADVANCE trial did not show any evidence of cardiovascular toxicity with sulfonylureas.

What drug was used as its dominant glucose-lowering strategy?

Answer 124

TRUE

Extended-release gliclazide (Action in Diabetes and Vascular Disease: Preterax and Diamicron Modified Release Controlled Evaluation)

Question 125

TRUE or FALSE: The UKPDS demonstrated long-term safety relative to lifestyle intervention for glyburide, glipizide, and chlorpropamide. (with emphasis on cardiovascular toxicity)

Answer 125

TRUE

Question 126

The adverse effect of increased arrhythmic cardiovascular events has been confirmed with these sulfonylureas

Answer 126

Tolbutamide and glyburide (especially relevant to glyburide)

Question 127

The maximum approved dose for the sulfonylureas is __ to __ times higher than the maximum effective dose.

Answer 127

Two to four times

Question 128

Initiating treatment with no more than a ____ of the maximal approved dose provides significant glucose lowering while limiting costs and adverse events.

Answer 128

Quarter

Small doses of the longer-acting modern sulfonylureas (e.g., 0.5-1 mg of glimepiride or 2.5 mg of extended-release glipizide) are often effective, particularly in patients receiving metformin concomitantly, and are almost always well tolerated.

Question 129

Leading disadvantages of sulfonylureas

Answer 129

Tendency to cause hypoglycemia and usually modest weight gain

Question 130

Maximum dose of repaglinide

Answer 130

4 mg with each meal

Question 131

Rationale of using non-sulfonylureas, and probable reason why they are still only modestly used

Answer 131

They stimulate insulin secretion at mealtime to improve postprandial control without increasing the risk of overnight hypoglycemia. They also demonstrate little binding to the vascular smooth muscle and cardiac SUR2 receptors.

However, there is need for multiple daily doses, higher cost than sulfonylureas, and lack of head-to-head comparative studies that demonstrate superiority over the newer sulfonylureas.

Question 132

Mechanism of thiazolidinediones (pioglitazone and rosiglitazone)

Answer 132

Bind to and modulate the activity of a family of nuclear transcription factors termed peroxisome proliferator-activated receptors (PPARs). They are associated with slow improvement in glycemic control over weeks to months in parallel with an improvement in insulin sensitivity and a reduction in free fatty acid levels.

Question 133

Recommended tests prior to beginning TZD therapy

Answer 133

Liver function tests

Consider assessment of risk factors and measurement of bone density before prescribing a TZD, especially for women

Question 134

Contraindications for TZDs

Answer 134

Active hepatocellular disease
Unexplained serum ALT levels greater than 2.5 times the upper limit of normal

Question 135

TRUE or FALSE: No substantial evidence has linked the newer TZDs to hepatotoxicity.

Answer 135

TRUE

(Nonetheless, recent studies show a favorable effect of pioglitazone on nonalcoholic steatohepatitis, a common an otherwise difficult to treat condition.)

Question 136

Compare the effects of the TZDs to triglyceride, HDL, and LDL levels

Answer 136

Pioglitazone
- Reduced triglycerides by approx 20%
- Modestly greater improvement in HDL particle number and size
- Improvement in LDL particle size and number

Rosiglitazone
- Increased triglycerides on average by 5%
- Increase in LDL particle number and improved LDL particle size

Question 137

What is the PROactive Study

Answer 137

PROactive (PROspective pioglitAzone Clinical Trial In macroVascular Events) Study

Randomized, double-blind, placebo-controlled trial comparing placebo vs 45 mg pioglitazone

Primary endpoint: Time from randomization to macrovascular outcomes –> No significant improvement with pioglitazone

Secondary endpoint: Cardiovascular composite endpoint –> Marginally significant 16% reduction

Question 138

What is the RECORD Trial

Answer 138

Rosiglitazone Evaluated for Cardiovascular Outcomes in Oral Agent Combination Therapy for Type 2 Diabetes (RECORD) Trial

Compared effect of adding rosiglitazone vs either metformin or SU to patients who had T2DM inadequately controlled with SU or metformin –> No difference in cardiovascular hospitalizations or death

Question 139

What is ADOPT

Answer 139

A Diabetes Outcome Progression Trial

Found that patients with early diabetes had a slower rate of secondary glycemic failure when they were treated with rosiglitazone compared with metformin and glyburide

Question 140

Adverse effects and concerns with use of TZDs (5)

Answer 140

Weight gain
Fluid retention
Increased risk of bone fractures
Anemia
Bladder cancer

Question 141

Cause of weight gain during use of TZDs

Answer 141

The weight gain has been shown to result both from extracellular fluid accumulation and an increase in subcutaneous but not visceral fat.

Question 142

Patients most likely to experience edema while using TZDs

Answer 142

Those using insulin and those with preexisting edema

Question 143

Recommendation to patients using TZDs who develop 1) Weight accompanied by increasing edema, 2) Clinically apparent heart failure

Answer 143

1) Restrict sodium intake, start a diuretic, or to increase their diuretic dosage as needed

Many patients with mild edema respond to a thiazide diuretic or spironolactone, and combination therapy with a moderate-dose loop diuretic may be considered.

2) Discontinue TZD

Question 144

Initial and highest approved dose of pioglitazone

Answer 144

Usually prudent to begin therapy with lowest available dose of 15mg daily. May increase to 30mg after 3 months if inadequate glycemic response and no significant edema. Highest approved dose of 45mg is less well tolerated.

Question 145

Regarding bone fractures with TZD use - gender and age mainly affected, and sites primarily affected

Answer 145

Older women
Distal sites

Question 146

Mechanism of increased bone fractures in TZDs

Answer 146

Preclinical studies suggest that activation of PPAR gamma inhibits bone formation by diverting stem cells from the osteogenic to the adipocytic lineage.

Question 147

TRUE or FALSE: Pioglitazone has a confirmed association with bladder cancer.

Answer 147

FALSE

Large, long-term studies have not confirmed this association. However, current recommendations to avoid its use in patients with a history of bladder cancer seem prudent (due to inconsistent preclinical and clinical observations).

Question 148

TRUE or FALSE: Oral glucose has a greater stimulatory effect on insulin secretion than does intravenous glucose at the same circulating glucose concentration.

Answer 148

TRUE

Question 149

Cells that secrete GLP1

Answer 149

Intestinal L cells

Question 150

Duration before secreted GLP is inactivated in plasma by enzyme dipeptidyl peptidase-4

Answer 150

Very rapidly (1-2 minutes)

Question 151

DPP4 inhibitors increase fasting and postprandial levels of GLP1 about __fold.

Answer 151

Twofold

Question 152

TRUE or FALSE: DPP4 inhibitors elevate GLP1 and potentiate glucose-dependent insulin secretion, suppresses basal and postprandial glucagon, improves satiety, and slows gastric emptying.

Answer 152

Elevation of GLP1 potentiates glucose-dependent insulin secretion and suppresses basal and postprandial glucagon. However, NEITHER satiety NOR the rate of gastric emptying is affected.

Question 153

Main clinical effect of DPP4 inhibitors

Answer 153

Lower fasting glucose levels

Question 154

Reduction of HbA1c with use of DPP4i

Answer 154

0.5 to 1%

Relatively weak glucose-lowering power that is partly dependent on retained beta-cell function

Question 155

TRUE or FALSE: DPP4i have no consistent effect on weight and no tendency to cause hypoglycemia when used alone or with metformin.

Answer 155

TRUE

Question 156

Contraindication for DPP4i use

Answer 156

Prior history of pancreatitis

Question 157

DPP4i that has shown increased risk for heart failure hospitalizations in cardiovascular outcome trials.

Answer 157

Saxagliptin

Question 158

DPP4i in current use are partially cleared by the kidney, the usual dose is the maximum marketed dose, and smaller doses are recommended in the setting of stage 3 or greater CKD, except ___.

Answer 158

Linagliptin

Question 159

Mechanism of action of alpha-glucosidase inhibitors (acarbose, miglitol, voglibose)

Answer 159

Slow the terminal step of carbohydrate digestion at the brush border of the intestinal epithelium, hence carbohydrate absorption is shifted more distally in the intestine and is delayed, allowing the sluggish insulin secretory dynamics characteristic of T2DM to catch up with carbohydrate absorption

Question 160

Regarding alpha-glucosidase inhibitors (acarbose, miglitol, voglibose) - timing of administration, common side effect, and intensity of blood glucose reduction

Answer 160

At beginning of each meal
Flatulence (also diarrhea, abdominal discomfort)
Modest reduction in blood glucose level

Question 161

TRUE or FALSE: Some evidence suggest that acarbose improves cardiovascular outcomes better than most antihyperglycemic agents.

Answer 161

TRUE

Question 162

Under normal conditions about ___g of glucose is filtered from plasma at the glomerulus and reabsorbed in the ___ tubule

Answer 162

180g
Proximal tubule

Question 163

Differentiate SGLT2 and SGLT1 with regards to capacity, affinity, and percentage of renal tubular glucose reabsorbed

Answer 163

SGLT2 - high-capacity, low-affinity, responsible for 90%

SGLT1 - low-capacity, high-affinity, responsible for 10% (but critically important for glucose absorption from the gut)

Question 164

TRUE or FALSE: SGLT2 inhibitors reduce both fasting and postprandial glucose levels and promote modest weight loss through loss of calories as glucosuria.

Answer 164

TRUE

Question 165

TRUE or FALSE: SGLT2 inhibitors have no effect on blood pressure.

Answer 165

FALSE

They also reduce blood pressure, at least in part by increasing sodium clearance and reducing extracellular gluid volume.

Question 166

TRUE or FALSE: All SGLT2i are relatively specific for inhibiting SGLT2.

Answer 166

TRUE

But others in development also have some effect on SGLT1

Question 167

In 26-week studies, SGLT2i lead to approximately __ to __kg more weight loss than placebo.

Answer 167

2 to 3 kg

Question 168

What is the EMPA-REG OUTCOME trial?

Answer 168

Empagliflozin Cardiovascular Outcome Event Trial in Type 2 Diabetes Mellitus Patients - Removing Excess Glucose trial

Empagliflozin - 32% relative risk reduction of all-cause mortality, 38% reduction of CV mortality, and 35% reduction of hospitalization for heart failure

Question 169

What is the CANVAS program?

Answer 169

CANagliflozin cardioVascular Assessment Study

Canagliflozin - generally similar effects as EMPA-REG, although quantitatively less prominent, cardiovascular and renal results

Question 170

Most common side effects of SGLT2i

Answer 170

Urinary frequency, genital infections, and relatively rare episodes of lower UTIs as well as dehydration and its consequences

Question 171

Regarding genital infections in SGLT2i use - gender more commonly affected, and type of microbe commonly related

Answer 171

10-15% of women (about a fivefold increase of risk)
Yeast
May recur

In males - genital mycotic infections are much less common and predominantly found in those who have not been circumcised

Question 172

SGLT2i associated with increased lower extremity amputations in a cardiovascular outcome trial

Answer 172

Canagliflozin (CANVAS?)

Question 173

TRUE or FALSE: Good renal function is not essential for full efficacy of SGLT2 inhibitors.

Answer 173

FALSE

Good renal function IS essential for full efficacy of SGLT2 inhibitors.

Question 174

Initiation of SGLT2 is not recommended, or if already in use, should be discontinued when eGFR is below ___.

Answer 174

45 ml/min/1.73m2

Question 175

The only SGLT2 with a warning against use in patients with bladder cancer.

Answer 175

Dapagliflozin

Question 176

Possible mechanisms of euglycemic DKA in T2DM patients on SGLT2i

Answer 176

Tendency toward dehydration, elevation of circulating glucagon levels, and accelerated gluconeogenesis due to glucosuria during fasting

Question 177

Second-generation bile acid sequestrant that has been observed to mediate modest reductions in glucose during the clinical development program

Answer 177

Colesevelam

Question 178

HbA1c reduction with use of colesevelam

Answer 178

0.5% (on table: 0.5 to 1%)

Question 179

Effects of colesevelam on lipid parameters

Answer 179

Approximately 15% improvement in LDL. HDL changes tent to be trivial. Triglycerides can increase by 5-20%. (Correlate with rosiglitazone)

Question 180

Basis for use of bromocriptine in T2DM

Answer 180

It is suggested that creating a circadian peak in central dopaminergic tone improves insulin sensitivity

Question 181

Timing of administration of quick-release formulation of bromocriptine for T2DM

Answer 181

Within 2 hours of rising in the morning

Question 182

HbA1c reduction with use of bromocriptine

Answer 182

As high as 1.2% (on table - 0.5 to 1%)

Question 183

TRUE or FALSE: In a 1-year safety study, bromocriptine has shown that broad cardiovascular outcomes were improved 40% compared with placebo.

Answer 183

TRUE

Question 184

TRUE or FALSE: Based on Table 35.11, T1D and DKA are contraindications to all commonly used OHAs

Answer 184

TRUE

Question 185

HbA1c reduction with use of metformin

Answer 185

1 to 2%

Question 186

HbA1c reduction with use of secretagogues

Answer 186

1 to 2%

Question 187

HbA1c reduction with use of TZDs

Answer 187

0.75 to 1.5%

Question 188

Side effect of DPP4i

Answer 188

Hypersensitivity

Question 189

Side effects of SGLT2i aside from urinary frequency and urogenital infections

Answer 189

Nausea, diarrhea, hypotension

Question 190

HbA1c reduction with use of alpha-glucosidase inhibitors

Answer 190

0.5 to 1%

Question 191

HbA1c reduction with use of SGLT2i

Answer 191

0.5 to 1%

Question 192

OHAs with 1 to 2% HbA1c reduction as first or second therapy (2)

Answer 192

Metformin
Secretagogues

Question 193

OHAs with 0.75 to 1.5% HbA1c reduction as first or second therapy (1)

Answer 193

Thiazolidinediones

Question 194

OHAs with 0.5 to 1% HbA1c reduction as first or second therapy (5)

Answer 194

DPP4i
AGI
SGLT2i
Colesevelam
Bromocriptine

Question 195

Side effects of bromocriptine

Answer 195

Somnolence, dizziness, hypotension

Question 196

Most common adverse effect of bromocriptine, occurring in about 30% of patients and leading to discontinuation in about 10% at highest doses.

Answer 196

Nausea

Question 197

Side effect of colesevelam

Answer 197

Constipation

Question 198

Table 35.13 Clinical Features of Commonly Used Insulins, page 1392

Answer 198

*

Question 199

Molecular basis of longer action of insulin detemir

Answer 199

Fatty acid side chain is covalently bound to the insulin molecule, resulting in slowing of both absorption from subcutaneous tissue and clearance from circulation

Question 200

TRUE or FALSE: Detemir’s time of onset and duration of action are longer than that of NPH.

Answer 200

FALSE

Detemir’s time of onset and duration of action are quite similar to those of NPH, but more consistent from injection to injection.

Question 201

Molecular basis of longer action of insulin glargine

Answer 201

Soluble at acid pH but precipitates when neutralized in tissues after injection

Question 202

Cause for longer action of insulin degludec and insulin glargine 300

Answer 202

Insulin degludec - due both to slower absorption after injection and to delayed clearance

Insulin glargine 300 units/mL - results entirely from an effect on absorption

Question 203

TRUE or FALSE: Regular human insulin administered intravenously is immediately effective, with a half-life on the order of 30 minutes.

Answer 203

FALSE

Regular human insulin administered intravenously is immediately effective, with a half-life on the order of 10 minutes.

Lispro, aspart, and glulisine are approved in the US for intravenous use but offer no advantage over regular insulin for this purpose and cost much more.

Question 204

Peak activity of inhaled human insulin (Afrezza)

Answer 204

In 30 minutes (the tmax is about 10 minutes), much earlier than lispro

Question 205

Required testing prior and during use of inhaled insulin

Answer 205

The current formulation requires spirometry before initiation, at 6 months, and annually thereafter.

Question 206

Side effects of use of inhaled insulin aside from usual hypoglycemic risk

Answer 206

Cough or throat irritation

Question 207

TRUE or FALSE: Allergies to currently available insulins are common, as are chronic skin reactions, which include lipoatrophy and lipohypertrophy.

Answer 207

FALSE

Allergies to currently available insulins are rare, as are chronic skin reactions, which include lipoatrophy and lipohypertrophy.

Question 208

TRUE or FALSE: The onset and time to peak of insulins are similar regardless of dose.

Answer 208

FALSE

Both short-acting and long-acting insulins have profiles of action that vary by the size of the dose injected. With higher doses the onset and time to peak effect become more delayed and the total duration longer.

Question 209

First GLP1-based therapeutic agent to be approved for human use

Answer 209

Exenatide (synthetic exendin-4)

Question 210

Exendin-4 is a naturally occurring component of the saliva of the ___

Answer 210

Gila monster (Heloderma suspectum)

Question 211

TRUE or FALSE: Exendin-4 shares 53% sequences identity with GLP1 but is relatively resistant to degradation by DPP4.

Answer 211

TRUE

Question 212

Exenatide peak of action and total duration of action

Answer 212

Peak of action at about 2 hours
Total duration of action no more than 6 hours

Twice-daily injection before breakfast and dinner

Question 213

HbA1c reduction with use of exenatide

Answer 213

1%

Question 214

Weight loss with use of exenatide

Answer 214

Modest (2-4 kg)

Question 215

Most common adverse effect of exenatide

Answer 215

Nausea (50% of patients)

Question 216

GLP1 agonist that has properties similar to exenatide except for a slightly longer duration of action

Answer 216

Lixisenatide (once daily before breakfast; reduces postprandial increments of glucose during the daytime but has much less effect overnight)

Question 217

Long-acting GLP1 agonist that is administered once daily without any restriction as to timing or relation to meals

Answer 217

Liraglutide (the other long-acting agents are to be given once weekly)

Question 218

TRUE or FALSE: Long-acting GLP1 agonists are associated with greater HbA1c-lowering efficacy than short-acting agonists.

Answer 218

TRUE

Owing to their greater effects on overnight fasting glucose levels. Much less effect on postprandial increments of glucose than short-acting agents.

Question 219

What is the LEADER study?

Answer 219

Liraglutide Effect and Action in Diabetes: Evaluation of Cardiovascular Outcome Results

Randomized to treatment with liraglutide or placebo for a median of more than 3 years –> Significant reductions of risk for primary composite cardiovascular endpoint (CV death, nonfatal MI, or nonfatal stroke) (13%), CV death (22%), all-cause mortality (15%), and progression of albuminuria (26%). No significant effect on hospitalization for heart failure.

Question 220

What is SUSTAIN-6?

Answer 220

Trial to Evaluate Cardiovascular and Other Long-term Outcomes with Semaglutide in Subjects with Type 2 DIabetes

Randomized to semaglutide vs placebo for about 2 years –> Somewhat greater reduction of risk for its primary cardiovascular composite endpoint (26%) compared with LEADER and showed a reduction in renal endpoints. Nonsignificant effect on CV death, all cause death, hospitalization for heart failure, and progression of albuminuria.

Question 221

Endpoint that didn’t show any improvement in both LEADER and SUSTAIN-6

Answer 221

Hospitalizations for heart failure (Up to now, these favorable outcomes have not been found with short-acting GLP1 agonists.)

Question 222

TRUE or FALSE: Hypoglycemia is a direct effect of GLP1 receptor agonists.

Answer 222

FALSE

Hypoglycemia is not a direct effect of GLP1 receptor agonists but can occur when they are added to other agents.

Hence, reduce to minimum dose of secretagogue, and 20% reduction of insulin dosage is advised unless HbA1c is >8%.

Question 223

The only GLP1 agonist that is renally cleared and is contraindicated in the setting of advanced kidney disease (eGFR <30)

Answer 223

Exenatide

Question 224

Contraindications for GLP1 agonists (4)

Answer 224

Type 1 diabetes
Diabetic ketoacidosis
History of pancreatitis
Personal or family history of medullary thyroid cancer (clear increase in preclinical testing with rodents)

Question 225

Side effects of GLP1 agonists

Answer 225

Nausea, diarrhea, abdominal pain
Pancreatitis?

Question 226

TRUE or FALSE: Most of the effect of pramlintide on glycemic pattern is a reduction of basal glucose levels.

Answer 226

FALSE

Most of the effect of pramlintide on glycemic pattern is a reduction of postprandial increments, with little effect on overnight control.

Question 227

HbA1c reduction with use of pramlintide

Answer 227

0.5 to 0.7%

Question 228

Most common adverse effect of pramlintide

Answer 228

Mild or moderate nausea, which wanes with continued therapy

Question 229

Timing of administration of oral medications that require rapid absorption for effectiveness if pramlintide is also being given

Answer 229

Either 1 hour before or 2 hours after injection of pramlintide

Question 230

Contraindication for pramlintide

Answer 230

Confirmed gastroparesis

Question 231

TRUE or FALSE: A deficiency of amylin is evident in patients with T1DM or T2DM.

Answer 231

TRUE

In parallel with insulin deficiency

Question 232

Mechanisms of pramlintide

Answer 232

Amylin and insulin have complementary actions in regulating plasma glucose. Amylin binds to brain nuclei and promotes satiety and reduces appetite. Through efferent neural pathways it mediates a decrease in the rate of gastric emptying and limits inappropriate glucagon secretion in a glucose-dependent fashion. By these means it regulates the rate of plasma glucose appearance from the GI tract and the liver.

Question 233

Largest pathophysiologic subgroup of diabetes

Answer 233

Latent autoimmune diabetes of adulthood

Question 234

Another term for Latent autoimmune diabetes of adulthood

Answer 234

Adult-onset type 1 diabetes

Question 235

Diabetes pathophysiologic subgroup that comprises up to 12% of patients with diabetes after age 20

Answer 235

Latent autoimmune diabetes of adulthood or Adult-onset type 1 diabetes

Question 236

TRUE or FALSE: Regarding Latent autoimmune diabetes of adulthood / Adult-onset type 1 diabetes:
a. Frequently are obese
b. May have other autoimmune disorders or a family history of these
c. Diagnosis requires detection of anti-glutamic acid decarboxylase antibodies or anti-islet cell antibodies
d. Can only be treated with insulin

Answer 236

a. FALSE. Frequently are not obese
b. TRUE
c. FALSE. Lack of antibodies does not exclude an autoimmune process
d. FALSE. Insulin has been considered the main therapy from the outset, but other therapies may be possible in those with slow progression.

Question 237

Leading causes of pancreatic diabetes (Type 3c diabetes)

Answer 237

Acute or chronic pancreatitis, pancreatectomy for cancer or pancreatitis, hemochromatosis, and cystic fibrosis

Question 238

TRUE or FALSE: Patients with pancreatic diabetes share a tendency to have significant deficiency of insulin secretion and prominent fasting hyperglycemia.

Answer 238

FALSE

Patients with pancreatic diabetes share a tendency to have significant deficiency of insulin secretion and prominent postprandial hyperglycemia.

Commonly need insulin at or relatively soon after diagnosis and quite frequently require both basal and prandial

Question 239

TRUE or FALSE: Patients with pancreatic diabetes have significant decreases in glucagon secretion and in the effects of incretin hormones.

Answer 239

TRUE

Question 240

TRUE or FALSE: Regarding maturity-onset diabetes of the young (MODY):
a. Proportion of newly diagnosed adults with one of these conditions is estimated to be between 1 and 2%
b. All have a strong family history consistent with autosomal dominant inheritance with high penetrance

Answer 240

a. TRUE
b. FALSE. A strong family history consistent with autosomal dominant inheritance with high penetrance is typical but not always present.

Question 241

Presentation of GCK-MODY

Answer 241

Presents typically in youth as mild fasting hyperglycemia that is not progressive and causes little or no tissue damage over time (deficiency of glucokinase –> altered glucose sensing in the beta cell)

Question 242

Importance of diagnosis of GCK-MODY

Answer 242

To avoid unnecessary treatment of the patient and other identified members of the family. Current evidence indicates that those with a GCK mutation will not develop chronic complications of diabetes, and treatment is not likely to render significant changes in glucose control.

Question 243

Most common form of monogenic diabetes

Answer 243

Hepatic nucleocyte factor-1A (HNF1A)

Question 244

Presentation of Hepatic nucleocyte factor-1A (HNF1A)

Answer 244

In adulthood with progressive hyperglycemia, more postprandial than fasting, that responds very well to sulfonylureas

Can be suspected when there is a prominent history of adult-onset but quite stable and slowly progressive diabetes on one side of the patient’s family, often in the absence of obesity

Question 245

Default choice for initial drug therapy in type 2 diabetes

Answer 245

Metformin

Used in combination with diet, exercise, and a DSMES program, can usually provide impressive lowering of glucose with essentially no risk of hypoglycemia. Initial use also has evidence for reducing CV risk

Question 246

What is the ORIGIN trial?

Answer 246

Outcome Reduction with an Initial Glargine Intervention trial

Showed effectiveness of combination therapy. Randomized into glargine as basal insulin with continuation of prior oral therapy, and use of oral therapies with insulin added only if necessary. Both regimens maintained HbA1c levels close to 6.5%. No differences in medical outcomes were observed other than more hypoglycemia and less progression from dysglycemia to overt diabetes in the group assigned to initial glargine therapy.

Question 247

Usual initial dose of basal insulin

Answer 247

Treatment can be started either with a fixed daily dose of 10 units or with a dose calculated as 0.1 to 0.2 units per kilogram body weight.

Question 248

Failure to maintain HbA1c close to __% despite use of a regimen that includes properly titrated basal insulin calls for attention to postprandial hyperglycemia.

Answer 248

7%

Question 249

After therapy of basal glucose has been optimized, the postprandial glucose excursion is highest after ___, and the highest postprandial glucose is after ___.

Answer 249

Breakfast
Dinner

Question 250

Recent studies suggest that adding a single injection of short-acting insulin (at the morning meal or at the largest meal) is just as effective as basal-bolus therapy and is less likely to cause weight gain or hypoglycemia. Aim for glucose prior to next meal (or at bedtime if the dose is prior to dinner) approaching __ mg/dL.

Answer 250

120 mg/dL

Question 251

When prandial insulin is added to basal insulin with continuation of one or more oral agents, optimal control often requires total daily insulin doses greater than __ unit per kilogram of body weight daily

Answer 251

1

Question 252

Fig. 35.6. Glucose-lowering medication in type 2 diabetes. Page 1400

Answer 252

*

Question 253

First-line therapy in type 2 diabetes

Answer 253

Metformin and comprehensive lifestyle (including weight management and physical activity)

*To avoid clinical inertia, reassess and modify treatment regularly (3-6 months)

Question 254

Additional treatment if patient has established ASCVD or CKD - ASCVD predominates

Answer 254

EITHER GLP-1 RA with proven CVD benefit OR SGLT2i with proven CVD benefit

liraglutide > semaglutide > exenatide ER
empagliflozin > canagliflozin

Question 255

Additional treatment if patient has established ASCVD or CKD - HF or CKD predominates

Answer 255

PREFERABLY SGLT2i OR GLP-1 RA

Question 256

Medications to avoid if patient has HF

Answer 256

TZD
Saxagliptin

Question 257

Additional treatment if patient has compelling need to minimize hypoglycemia

Answer 257

DPP-4i
GLP-1 RA
SGLT2i
TZD

Question 258

Additional treatment if patient has compelling need to minimize weight gain or promote weight loss

Answer 258

EITHER GLP-1 RA OR SGLT2i
(ADA 2022: PREFERABLY GLP-1 RA OR SGLT2i)

Later on.. preferably DPP4-i if not on GLP-1 RA

Question 259

Additional treatment if cost is a major issue

Answer 259

SU or TZD
(ADA 2022: Certain insulins, SU, TZD)

Question 260

As a general rule, patients diagnosed with HbA1c above 9% should seek a gradual improvement of control with HbA1c below 7% within 6 months, with continuation of at least metformin after that. – What is the rationale for this?

Answer 260

Aside from the risk of hypoglycemia from use of insulin by relatively inexperienced patients, there is potential for worsening of retinopathy or neuropathy accompanying overly rapid reduction of glucose.

Question 261

Risk of reapperance of hyperglycemia consistent with the diagnosis of T2DM in women with history of GDM

Answer 261

50-70% after 15 to 25 years, a risk that is increased 10 to 18-fold

Question 262

Risks of GDM

Answer 262

Complicated delivery
Neonatal complications
Children exposed to hyperglycemia in utero have increased risk of later obesity and/or T2DM

Question 263

Glucose targets during gestation

Answer 263

Fasting <95 mg/dL
1-hr postprandial <140 mg/dL
2-hr postprandial <120 mg/dL

Question 264

OHAs that are sometimes used in GDM instead of insulin, but there are concerns about their safety

Answer 264

Metformin
Glyburide

Question 265

Lifestyle interventions can provide a reduction of ___ to ___ % in progression to diabetes over a period of 3 to 5 years

Answer 265

30 to 60%

Question 266

Intervention with metformin in patients at high risk for T2DM was associated with a somewhat smaller reduction in progression to diabetes. It had LESS effect in the following patients:

Answer 266

Older than 60 years of age
BMI of <30 kg/m2
Fasting plasma glucose <100 mg/dL

Question 267

Metformin therapy brings little risk and offers SUBSTANTIAL benefit for some individuals, notably those:

Answer 267

Under age 60 years
BMI >35 kg/m2
Women with previous gestational diabetes

*Therefore on balance, consideration of metformin in patients who are at particularly high risk is recommended.

Question 268

Best candidates for preventive strategies (preventing type 2 diabetes)

Answer 268

Patients with prediabetes:
- HbA1c >5.7% and particularly >=6%
- FPG >=100 mg/dL and particularly >=110 mg/dL
- Impaired glucose tolerance