IV. Type 1 Diabetes Mellitus

Question 1

German pathologist who, in 1902, noted a small peri-islet cellular infiltrate on microscopic evaluation of the pancreas obtained at autopsy from a 10-year-old child with diabetes

Answer 1

Martin Schimdt

Question 2

Who, in the 1920’s, drew attention to the relationship between the peri-islet infiltrate and the age of diabetes onset

Answer 2

Shields Warren

Question 3

Pathologist who coined the term insulitis

Answer 3

Hanns von Meyenburg

Question 4

Who won the Nobel Prize for purifying insulin from animal pancreata in the 1920’s

Answer 4

Banting and Best

Question 5

4 islet cell autoantibodies / T1DM-associated autoantibodies

Answer 5

Anti-insulin autoantibodies (IAA)
Anti-glutamic acid dexarboxylase (GADA)
Anti-insulinoma-associated antigen 2 (IA2A)
Anti-zinc-transporter 8 (ZnT8A)

Question 6

2 peaks of T1DM presentation in childhood and adolescence

Answer 6

A smaller peak between 5 and 7 years of age and a larger peak at or near puberty

Question 7

Sex that is slightly more affected in T1DM

Answer 7

Males

Question 8

Incidence of T1DM diagnosis is higher during these seasons

Answer 8

Autumn and winter

Question 9

Being born in this season is associated with an increased likelihood for T1DM

Answer 9

Spring

Question 10

TRUE or FALSE: T1DM patients can manifest insulin resistance.

Answer 10

TRUE

T1DM patients may present with diabetes characterized by high serum levels of fasting insulin or C-peptide but loss of stimulated insulin secretion.

Question 11

TRUE or FALSE: Among African-American and Latino children and adolescents in the United States diagnosed with diabetes, almost one half lack any T1DM-associated autoantibody.

Answer 11

TRUE

Question 12

T1D, T2D, both, or neither?

a. Rapid onset with very high to extremely high blood glucose levels, polyphagia, polydipsia, polyuria
b. Family history of autoimmune disease
c. Can be prevented
d. Can be reversed
e. Acute emergencies of hypoglycemia and ketoacidosis leading to hypoglycemic unawareness

Answer 12

a. T1D
b. T1D
c. T2D
d. Neither
e. Both

Question 13

The most intensively studied animal model for T1DM

Answer 13

Nonobese diabetic (NOD) mouse

Question 14

Findings of the Nonobese Diabetic Mouse Model

Answer 14

Same as with humans:

• Housing conditions (i.e., environment) represent an important variable
• Polygenic
• Both destruction and replication/regeneration are present months before the onset of T1DM

Different from humans:

• Strong female bias with respect to disease
• T cells, not autoantibodies, appear to mediate the beta cell destruction
• Insulitis lesion, the hallmark facet of T1DM, appears more intense and quantitatively obvious

Question 15

Drug that is directly toxic to islet beta cells

Answer 15

Streptozotocin

In high doses, it rapidly induces diabetes. In low doses, a more chronic diabetes develops.

Question 16

Histologic features of islet cells in T1D

Answer 16

• Insulitis (mixed mononuclear, adjacent or within islet)
• Loss of beta cells (increase with disease duration)
• Hyper-expression of class I MHC
• Beta cell necrosis/apoptosis (?)
• Diminished insulin in remaining beta cells
• Beta cell expression of interferon alpha

Question 17

TRUE or FALSE: A more vigorous autoimmune response occurs when disease develops in young children.

Answer 17

TRUE

Immunoype as a function of age:
Younger age of onset associated with higher levels of CD20+ B cells, CD45+ cells, and CD8+ T cells, alongside fewer insulin-positive islets.
Older age at onset associated with lower levels of CD45+ cells and CD8+ T cells, as well as more insulin-positive islets.

Question 18

Predominant immune cells in insulitic lesions

Answer 18

CD8+ T lymphocytes and macrophages

Question 19

Definition of “insulitis”

Answer 19

Lesion of 3 islets containing more than 15 CD45+ cells in a pancreas

(defined by nPOD - Network for Pancreatic Organ donors with Diabetes)

Question 20

TRUE or FALSE: The inflammation seen in type 1 diabetes spares the exocrine pancreas.

Answer 20

FALSE

Chronic inflammation, including enhanced CD8+ T-cell infiltration, is present in the exocrine pancreas in T1DM subjects. (appears to be subclinical)

Question 21

What is “pseudoatrophic”?

Answer 21

Term that refers to remaining islets (alpha, delta, pancreatic polypeptide) that lack insulitis and beta cells

Question 22

TRUE or FALSE: There is a notion that T1DM is a relapsing/remitting disease, with waves of immunologic destruction.

Answer 22

TRUE

Question 23

Hypothesis for reduced pancreatic weight in T1D

Answer 23

Resulted from loss of insulinotrophic effects on the exocrine pancreas, as islets constitute only 1-2% of the entire pancreatic volume

Question 24

Gross pathologic characteristics of the pancreas in T1D

Answer 24

• Decreased overall weight
• Atrophy of dorsal region
• Exocrine atrophy
• Hydrophic change (hypertrophy) (?)
• Composed of pseudoatrophic (glucagon staining) islets in type 1D
• Lobular loss of beta cells
• Heterogenous lobular insulitis

Question 25

2 main mechanisms of beta cell death in T1DM

Answer 25

Necrosis and Apoptosis

Question 26

4 mediators of necrotic cell death in T1DM

Answer 26

T cells can induce necrosis following a release of cytolytic granules containing granzymes and perforin, which act on the beta cell membrane

Ischemia which may result from hyperexpression of extracellular matrix materials

Reactive oxygen species

Necrosis of beta cells may release factors, including post-translationally modified antigenic peptides or modifications of “normal” antigens that further stimulate the immune response and thereby perpetuate beta cell death by necrosis

Question 27

Mediators of apoptosis in T1DM

Answer 27

Janus kinases (JAK1, JAK2) and nonreceptor tyrosine-protein kinase (TYK2) pathways

Question 28

In the 25-year old concept of the natural history of T1DM, symptoms of the disease were thought to appear when __ to __% of pancreatic beta cells had met their demise.

Answer 28

85 to 90%

Question 29

Steps in the 25-year old concept of the natural history of T1DM

Answer 29

1. Precipitating events may occur in utero
2. Genetic predisposition likely the key driver or linkage to immune abnormalities
3. Beyond “precipitating”, environment may influence entire natural history
4. While overall loss of beta cells is potentially linear, may be relapsing/remitting
5. Multiple islet autoantibodies (>=2) may represent “Asymptomatic” T1D
6. Increasing glucose excursions as one approaches symptomatic onset
7. Some T1D patients produce low-level C-peptide long after onset
8. Beta cell mass not always zero in long-standing patients

Question 30

Pivotal discovery from combined analysis of data generated in the BABYDIAB, DAISY, and DIPP studies

Answer 30

Once two or more anti-islet autoantibodies are present in a given individual, the individual’s 10-year risk for developing diabetes ranges from 60% in older seroconverters (>3 years) to 75% in those who seroconvert before 3 years of age.

Question 31

Table 36.2 T1DM Clinical Research Consortia and Natural History Trials, page 1409

Answer 31

*

Question 32

TRUE or FALSE: Most persons (>85%) in whom T1DM develops have a first-degree relative with the disease.

Answer 32

FALSE

Most persons (>85%) in whom T1DM develops DO NOT have a first-degree relative with the disease.

Question 33

2 countries with highest incidence of T1DM

Answer 33

Finland and Sardinia

Question 34

Percentage risk of T1DM in families

Answer 34

• Monozygotic twin 50%, but incidence varies with age of index twin
• Dizygotic twin 6%
• Sibling 3.2% (through adolescence); 6% lifetime
• Both parents ~10%
• Father 4.6%
• Mother 2%
• Offspring 1%

Question 35

Progression of disease among discordant monozygotic twins, based on the period of discordance and the age at which the disorder developed in the index twin

Answer 35

The hazard rate for development of diabetes decreased as the period of discordance increased.

If T1DM developed in the index twin after age of 25 years, the concordance rate was <10%. If it developed in the index twin before age 5 years, the concordance rate was 70% after 40 years of follow-up.

Question 36

The most important loci determining the risk of T1DM reside within the ___ on chromosome ___ and, in particular, the ___ molecules.

Answer 36

The most important loci determining the risk of T1DM reside within the MHC on chromosome 6p21 and, in particular, the MHC class II molecules (DR, DQ, and DP).

Question 37

2 molecules which are the major determinants of T1DM susceptibility

Answer 37

DR and DQ

Question 38

Molecules that provide dominant protection from T1DM

Answer 38

1. HLA-DQA101:02-DQB106:02 (termed DQ6)
2. HLA-DRB1*14:01

Question 39

The protective haplotype HLA-DRB115:01-
DQA101:02-DQB1*06:02 is present in __% of the general population and in fewer than __% of patients with T1DM.

Answer 39

20%
3%

Question 40

Simple rule regarding determination of high-risk haplotypes

Answer 40

The presence of aspartic acid at position 57 of the DQbeta chain and arginine at DQalpha 52 is associated with T1DM risk.

Question 41

TRUE or FALSE: The longest group of nucleotide repeat elements located upstream (also known as 5’) of the insulin gene was associated with decreased diabetes risk.

Answer 41

TRUE

Question 42

Third confirmed gene (vs. mere loci) influencing T1DM risk

Answer 42

PTPN22

A gene encoding a lymphoid-specific phosphatase that influences T-cell receptor signaling

Question 43

The most characteristic difference related to age at diabetes onset

Answer 43

Presence of higher levels of IAA in children who develop the disease at an early age (e..g, <5 years).

Question 44

The best single marker for diabetes development in young children

Answer 44

Anti insulin antibodies (IAA)

Question 45

In those children in whom autoantibodies arise during the first 3 years of life, ___ often appear first. In contrast, ___ are more often positive in adults who develop T1DM.

Answer 45

IAA
GADA

Question 46

TRUE or FALSE: Monogenic diabetes can develop spontaneously.

Answer 46

TRUE

In most cases of monogenic diabetes, the gene mutation is inherited; in the remaining cases, the gene mutation develops spontaneously.

Question 47

2 main forms of monogenic diabetes

Answer 47

Neonatal diabetes and maturity-onset diabetes of the young, with ND far less common than MODY.

Question 48

At what age does neonatal diabetes occur.

Answer 48

In newborns through the first 6 months of life

Question 49

TRUE or FALSE: Neonatal diabetes is transient and usually resolves at 6 months of life.

Answer 49

FALSE

For approximately one half of those with ND, the condition is lifelong, yet for the remainder, the condition disappears during infancy but can reappear later in life.

Question 50

Manifestations of neonatal diabetes

Answer 50

Mimic those of T1DM
May be small for gestational age (i.e., IUGR)
Protracted growth and weight gain

Question 51

What is the most common form of neonatal diabetes mellitus?

Answer 51

Transient neonatal diabetes with mutation of ZAC/HYMAI

Question 52

Regarding the most common form of neonatal diabetes mellitus:
a. Gene or syndrome?
b. Typical age at onset?
c. Type of inheritance?
d. Able to cause IUGR?
e. Transient or permanent?
f. Treatment?

Answer 52

a. ZAC/HYMAI
b. Birth to 3 months
c. Autosomal dominant; Spontaneous
d. Yes
e. Transient
f. Initially, treat with insulin; reduce dosage as needed; when diabetes recurs, treat with diet modification and physical activity; may also require insulin

Question 53

Regarding the most common form of PERMANENT neonatal diabetes mellitus:
a. Gene or syndrome?
b. Typical age at onset?
c. Type of inheritance?
d. Able to cause IUGR?
e. Transient or permanent?
f. Treatment?

Answer 53

a. KCNJ11 (affecting the Kir6.2 protein)
b. 3-6 months
c. Autosomal dominant (10%); Spontaneous
d. Yes
e. Permanent
f. Treated with insulin in the past but often can be treated with oral sulfonylureas

Question 54

TRUE or FALSE: MODY patients are generally overweight.

Answer 54

FALSE

MODY patients are generally NOT overweight.

Question 55

Children of a MODY parent have a __% chance of inheriting the disease.

Answer 55

50%

Question 56

Components of the Autoimmune Polyendocrine Syndrome Type 1, and the mutation

Answer 56

T1DM, mucocutaneous candidiasis, hypoparathyroidism, Addison disease, and hepatitis (MATHH)

Mutation (usually autosomal recessive) of the AIRE gene on chromosome 21 (may play an important role in maintaining self tolerance, as well as influence the expression of what immunologists term peripheral antigens (e.g., insulin) in the thymus)

Question 57

Syndrome associated with overwhelming neonatal autoimmunity, in which most children die in the first few days of life or in infancy

Answer 57

X-Linked Polyendocrinopathy, Immune Dysfunction, and Diarrhea (Scurfy Gene)

“XPID” or “IPEX” (Immunodysregulation polyendocrinopathy enteropathy x-linked syndrome)

Question 58

What is the mode of inheritance and mutation of XPID?

Answer 58

X-linked recessive disease affecting only boys, with a frequent clinical history of a lack of male births

Mutation of the gene encoding fork-head box P3 (FOXP3), which functions as transcription factor and master switch for regulatory (suppressor) CD4+CD25+CD127-/low T lymphocytes

Question 59

Proven therapy of XPID/IPEX syndrome

Answer 59

Bone marrow transplantation

Question 60

Table 36.5 Characteristics of Monogenic Diabetes, pages 1414-1415

Answer 60

*

Question 61

Most common form of MODY

Answer 61

MODY 3

Question 62

Second most common form of MODY

Answer 62

MODY 2

Question 63

Only form of MODY which can cause lower than normal birth weight

Answer 63

MODY 2

Question 64

Proteins affected by the different MODY types

Answer 64

MODY 1 - Hepatocyte nuclear factor 4 alpha
MODY 2 - Glucokinase
MODY 3 - Hepatocyte nuclear factor 1 alpha
MODY 4 - Insulin promoter factor 1
MODY 5 - Hepatocyte nuclear factor 1 beta
MODY 6 - Neurogenic differentiation factor 1

Question 65

Mode of inheritance of all types of MODY

Answer 65

Autosomal dominant

Question 66

Only form of MODY wherein mild hyperglycemia may be present at birth; otherwise, early childhood

Answer 66

MODY 2

Question 67

TRUE or FALSE: All types of MODY are permanent.

Answer 67

TRUE

Question 68

Type of MODY in which medications are usually not required

Answer 68

MODY 2

Question 69

Type/s of MODY in which oral sulfonylureas are the primary treatment

Answer 69

MODY 1 and 4

Question 70

Type of MODY in which the initial treatment is diet modification

Answer 70

MODY 3 (2 also)

Question 71

Type/s of MODY in which insulin is the primary treatment

Answer 71

MODY 5 and 6

Question 72

Summary of proteins affected and treatments of MODY

Answer 72

MODY 1 - Hepatocyte nuclear factor 4 alpha (SU)
MODY 2 - Glucokinase (Diet modification and physical activity)
MODY 3 - Hepatocyte nuclear factor 1 alpha (Diet Modification)
MODY 4 - Insulin promoter factor 1 (SU)
MODY 5 - Hepatocyte nuclear factor 1 beta (Insulin)
MODY 6 - Neurogenic differentiation factor 1 (Insulin)

Question 73

TRUE or FALSE: No single enviromental agent has been identified in the pathogenesis of type 1 diabetes.

Answer 73

TRUE

Question 74

The hypothesis that states that childhood obesity increases the insulin demand, overloading the islet cells and accelerating beta-cell autoimmune damage
a. Accelerator and overload hypotheses
b. Copenhagen model
c. Hygiene hypothesis
d. Fertile field hypothesis
e. Old friends hypothesis
f. Threshold hypothesis

Answer 74

A

Question 75

The hypothesis that proposed that beta-cell destruction results from interactions between the environment, immune system, and the beta cells themselves in genetically susceptible individuals
a. Accelerator and overload hypotheses
b. Copenhagen model
c. Hygiene hypothesis
d. Fertile field hypothesis
e. Old friends hypothesis
f. Threshold hypothesis

Answer 75

B

Question 76

The hypothesis that attributes the rising incidence of autoimmune disorders to the decline in infections with reduced stimulation of the immune system
a. Accelerator and overload hypotheses
b. Copenhagen model
c. Hygiene hypothesis
d. Fertile field hypothesis
e. Old friends hypothesis
f. Threshold hypothesis

Answer 76

C

Question 77

The hypothesis that proposes that microbial infection induces a temporary state in which other antigens can more easily react to yield autoreactive T cells.
a. Accelerator and overload hypotheses
b. Copenhagen model
c. Hygiene hypothesis
d. Fertile field hypothesis
e. Old friends hypothesis
f. Threshold hypothesis

Answer 77

D

Question 78

The hypothesis that implicates dietary exposure as a possible direct regulator of the immune system and of self-tolerance by altering gut microbiota and intestinal permeability
a. Accelerator and overload hypotheses
b. Copenhagen model
c. Hygiene hypothesis
d. Fertile field hypothesis
e. Old friends hypothesis
f. Threshold hypothesis

Answer 78

E

Question 79

The hypothesis that suggests that the etiologic influences of genetics and environment, when evaluated as intersecting and reciprocal odds-ratio-based trend lines, result in a method to define the attributable risk for T1DM
a. Accelerator and overload hypotheses
b. Copenhagen model
c. Hygiene hypothesis
d. Fertile field hypothesis
e. Old friends hypothesis
f. Threshold hypothesis

Answer 79

F

Question 80

TRUE or FALSE: Environmental agents can act as both a trigger and modulator of the pathogenesis of T1DM.

Answer 80

TRUE

It is increasingly accepted that enviromental agents may contribute far beyond an initial triggering and rather act throughout the natural history of T1DM development, such as modulating the ongoing autoimmune process.

Question 81

The best evidence, if not the only strong evidence, for a specific environmental agent to contribute to T1DM pathogenesis involves ___.

Answer 81

Congenital rubella infection (mechanism currently unknown)

Question 82

Most often discussed (biologic) agents associated with T1DM

Answer 82

Entroviruses

Question 83

TRUE or FALSE: Childhood vaccine timing has been proven to influence the development of T1DM.

Answer 83

FALSE

Question 84

Dietary factor that has been associated with T1DM
a. Breastfeeding or bovine milk ingestion
b. Late (>6 months) introduction of cereals
c. High vitamin D level
d. High omega-3 fatty acids

Answer 84

A

Factors:
- Breastfeeding or bovine milk ingestion
- Early (<3 months) introduction of cereals
- Low vitamin D level
- Low omega-3 fatty acids

Question 85

TRUE or FALSE: An individual’s timeline to diabetes onset could be determined by the severity of the autoimmune attack rather than the initial beta-cell mass.

Answer 85

FALSE

An individual’s timeline to diabetes onset could be determined NOT by the severity of the autoimmune attack but the starting point for beta-cell mass.

(Beta-cell mass likely mostly determined in the first two decades of life.)

Question 86

TRUE or FALSE: Reduced weight can distinguish the pancreas of patients with long-standing T1DM from pancreas of new-onset T1DM and non-T1DM patients with anti-islet autoantibodies.

Answer 86

FALSE

Reduced pancreatic weight affects not only subjects with long-standing T1DM, but also recent-onset T1DM and nondiabetic persons with anti-islet autoantibodies.

Question 87

TRUE or FALSE: Serum levels of trypsinogen, which are indicative of exocrine pancreas function, are reduced in patients with long-standing T1DM, in those with recent-onset T1DM, and in nondiabetic individuals with anti-islet autoantibodies.

Answer 87

TRUE

Question 88

TRUE or FALSE: Most persons who are within 1 year of developing overt T1DM have no second-phase insulin secretion after intravenous glucose administration (glucose given at 0.5g/kg over 5 mins, and insulin levels measured before and 1 and 3 minutes after glucose infusion).

Answer 88

FALSE

First-phase

Question 89

TRUE or FALSE: HbA1c increases progressively (although in the normal range) 1 or 2 years before overt hyperglycemia develops.

Answer 89

TRUE

Question 90

TRUE or FALSE: Impaired fasting glucose and impaired glucose tolerance are usually present within 6 months before the onset of overt T1DM.

Answer 90

TRUE

Question 91

Why is C-peptide measured to assess remaining beta cell function?

Answer 91

Because it is released in equimolar concentrations with insulin but does not undergo hepatic extraction and has a longer half-life in circulation.

Usually measured in the fasting state, after intravenous glucagon, or with a standard liquid meal.

Associated with impressive metabolic benefit, as shown in the Diabetes Control and Complications Trial (DCCT).

Question 92

2 features that strongly indicate transient hyperglycemia instead of T1DM

Answer 92

Absence of anti-islet autoantibodies
Normal first-phase insulin secretion during an intravenous glucose tolerance test

Question 93

Most reliable predictive biomarker of T1DM identified to date

Answer 93

Seroconversion to anti-islet autoantibody positivity

Question 94

Beta-cell death assays measure ___ from blood or serum which are released from necrotic beta cells.

Answer 94

Cell-free unmethylated insulin DNA

Question 95

___ (Elevated or reduced?) serum proinsulin/C-peptide ratio measured under fasting conditions implies impaired processing of proinsulin and C-peptide within the beta cell, suggesting duress related to metabolic, oxidative, or immunologic stress.

Answer 95

Elevated

Question 96

Index60 has been introduced as a clinical/diagnostic biomarker measuring functional beta-cell mass. The test requires an OGTT with calculations incorporating the log-adjusted fasting C-peptide level, 60-minute C-peptide level, and 60-minute blood glucose level. What is the value considered indicative of T1DM onset?

Answer 96

An Index60 value greater than 2 in an individual with anti-islet autoantibodies is considered indicative of T1DM onset.

Question 97

Microbiome factors that is believed to protect against T1DM
a. High Bacteroides to Firmicutes ratio
b. Presence of butyrate-producing bacteria
c. Low diversity and poor stability of the gut microbial community

Answer 97

B

Microbiome factors that have been suggested as biomarkers of T1DM:
- High Bacteroides to Firmicutes ratio has been associated with anti-islet autoimmunity
- Presence of butyrate-producing bacteria (may protect against T1DM by promoting synthesis of mucin and reducing intestinal leakiness)
- Low diversity and poor stability of the gut microbial community are associated with T1DM

Question 98

Staging of T1DM based on the joint position of ADA, JDRF, and Endocrine Society

Answer 98

Stage 1: Presence of 2 or more anti-islet autoantibodies with normoglycemia (presymptomatic)

Stage 2: Progression to dysglycemia in the setting of 2 or more anti-islet autoantibodies (presymptomatic)

Stage 3: Meets ADA criteria for the diagnosis of diabetes (symptomatic)

Question 99

Immunosuppressive agent that has been shown to prevent further loss of C-peptide secretion and improve metabolic function when it was administered in recent-onset T1DM cases

Answer 99

Cyclosporine

Question 100

A single course of this therapy decreased the loss of C-peptide secretion over a 12- to 24-months period in new-onset T1DM patients, but didn’t go into phase III

Answer 100

Anti-CD3

Question 101

Anti-CD3 monoclonal antibody that delayed progression to clinical T1DM in high-risk patients

Answer 101

Teplizumab

Question 102

Basic concept behind the use of immunologic vaccination in preventing or reversing T1DM

Answer 102

Induction of regulatory T lymphocytes that target a given beta-cell antigen and, on encountering the target antigen (e.g., insulin, GAD) in the context of the vaccine formula or route of administration, produce cytokines and cell-mediated effects that suppress autoimmunity and tissue destruction.

Question 103

___ Route of insulin treatment that, although didn’t document an overall benefit of insulin, showed a statistically significant delay in progression to diabetes in the subgroup with higher levels of IAA at entry.

Answer 103

Oral insulin

Question 104

TRUE or FALSE: Improved results for pancreatic transplantation occur in the setting of pancreas transplantation alone versus concurrent kidney transplantation.

Answer 104

FALSE

Improved results for pancreatic transplantation occur in the setting of simultaneous pancreas and kidney transplantation versus transplantation of pancreas alone.

Question 105

TRUE or FALSE: T1DM patients who underwent pancreas transplantation can experience recurrence of diabetes.

Answer 105

TRUE

Can recur as a result of mechanisms considered attributable to either recurrence autoimmunity or, more often, allograft rejection

Question 106

What is the Edmonton protocol?

Answer 106

Protocol for islet (vs pancreas) transplant which involved meticulous islet isolation techniques, transplantation of islets from multiple pancreata, avoided the use of steroids, and utilized an immunosuppressive regimen involving the drug rapamycin and resulted in improved outcomes for patients with T1DM.

Question 107

Drawbacks and limitations of stem cell or xenogeneic islet cell transplantation

Answer 107

Quantitative paucity of suitable organ donor tissues

Complications associated with immune suppression

Beta cells do not exist in isolation but rather as part of the islets of Langerhans, and hence generating cell therapy in the absence of a full complement of islet cells must be considered in the context of hormonal counterregulation

Question 108

What is the Hirata syndrome?

Answer 108

Insulin Autoimmune Syndrome

Extremely high concentrations of autoantibodies reacting with human insulin in the absence of exogenous insulin therapy –> Hypoglycemia

Most common in Asian descent

Question 109

2 agents associated with the development of Insulin Autoimmune Syndrome

Answer 109

Sulfhydryl-containing medications, particularly methimazole
Alpha-lipoic acid

Question 110

Treatment of Insulin Autoimmune Syndrome

Answer 110

Stopping the sulfhydryl-containing medications, particularly methimazole, as well as alpha-lipoic acid

(For more than 75% of patients, the disease remits)

Question 111

TRUE or FALSE: Essentially all patients treated with recombinant human insulin produce anti-insulin antibodies.

Answer 111

TRUE

Question 112

TRUE or FALSE: Most studies show no relationship between the presence of anti-insulin antibodies and complications associated with T1DM.

Answer 112

TRUE

But there are reports correlating insulin antibodies with macrosomia.

Question 113

Usual mode of therapy for allergic reactions to insulin analogues (though most are due to allergies to lubricants, preservatives, and plastics in bottles, stoppers, syringes, and needles)

Answer 113

Substituting the type of formulation of insulin and administration of oral antihistamines or topical mast cell stabilizers for immunoglobulin E-mediated local reactions, followed by insulin desensitization or addition of small amounts of glucocorticoids to the insulin injected for local delayed hypersensitivity reactions

Question 114

Components and treatment of the syndrome of Anti-Insulin Receptor Autoantibodies

Answer 114

Hypoglycemia, hypercatabolism, severe acanthosis nigricans, and insulin resistance

Various forms of immunosuppression (mixed success)

Question 115

Peak age for presentation of T1DM

Answer 115

At or during puberty (with a smaller peak in children between 5 and 7 years of age)

Question 116

TRUE or FALSE: In children, the onset of symptoms of T1DM is insidious, whereas it can occur over a brief period in older persons.

Answer 116

FALSE

In children, the onset of symptoms can occur over a brief period, and families may be able to date the onset with considerable accuracy. In older persons with T1DM, the onset of symptoms may be insidious over months, and many are mistakenly diagnosed as having T2DM by screening during this asymptomatic period.

Question 117

On diagnosis of T1DM, the plasma glucose concentrations at presentation are usually in the range of ___ to ___ mg/dL.

Answer 117

300 to 500 mg/dL

Question 118

At the time of diagnosis, C-peptide level (a surrogate marker for insulin secretion) is generally in the ___ range and declines over time.

Answer 118

Low-normal

Question 119

In reference laboratories, pancreatic autoantibodies are present in approximately ___% of individuals at diagnosis.
a. 20%
b. 54%
c. 86%
d. 98%

Answer 119

D

Question 120

TRUE or FALSE: The likelihood for residual beta-cell function is greater with an earlier age of onset of disease.

Answer 120

FALSE

The likelihood for residual beta-cell function is greater with an older age of onset of disease.

Question 121

Frequency of initial visits for diabetes care of T1DM patients

Answer 121

Initial visits usually entail 2 to 3 sequential days of multidisciplinary visits, followed by visits in 2 to 3 weeks, then 1 to 2 months later. Thereafter, diabetes follow-up care generally occurs quarterly.

Question 122

Physical parameters to be monitored on clinic visits, and frequency

Answer 122

Weight, height, and vital signs at every quarterly visit

Tanner staging should be performed at least annually for pediatric patients

Timely screening for complications and cardiovascular risk factors

Question 123

TRUE or FALSE: In the DCCT, the conventional therapy group yielded an HbA1c that is 2% lower than the intensive insulin group.

Answer 123

FALSE

Intensive insulin therapy yielded superior control to conventional insulin therapy, with HbA1c levels that were approximately 2% lower in the intensively treated group than in the conventionally treated group (medians of 7% and 9% respectively), and also experienced a 35% to 76% reduction in the occurrence of microvascular complications, and continued to demonstrate a reduced risk of both micro- and macrovascular complications and overall mortality. (DCCT-EDIC)

Question 124

ADA HbA1c targets

Answer 124

Adults <7%
Younger children <7.5% (recently lowered with the advent of insulin analogues and the data that intensive insulin therapy confers no additional risk to neurocognitive function in young children)

Question 125

Frequency of HbA1c monitoring

Answer 125

Quarterly

Question 126

HbA1c targets by:
International Society for Pediatric and Adolescent Diabetes (ISPAD)
National Institute for Health and Clinical Excellence Guidelines (UK)
American Association of Clinical Endocrinologists

Answer 126

ISPAD <7%
NIH and Clinical Excellence Guidelines <=6.5%
AACE <=6.5%

Must be personalized and tailored to individual needs and consideration of risk of severe hypoglycemia

Question 127

Frequency of nutrition education in T1DM

Answer 127

Generally provided by a registered dietitian annually

Question 128

Principles of general nutrition in terms of standard composition of macronutrients, fat intake, and portions of fruit and vegetables

Answer 128

50% of energy intake as carbohydrate, 20% as protein, and 30% as fat

<10% of energy intake as saturated fat, <10% as PUFA, >10% as MUFA

5 portions of fruits and vegetables daily

Question 129

TRUE or FALSE: Low carbohydrate diets are beneficial in T1DM patients.

Answer 129

FALSE

Very low carbohydrates should be avoided, as such diets can lead to elevations in lipid levels and there can be risk for ketosis

Question 130

TRUE or FALSE: Strict and precise carbohydrate counting is essential.

Answer 130

FALSE

Under- or overestimating the carbohydrate content by 5 to 7 g, or by +/- 15%, does not produce significant hypo- or hyperglycemia

It is more important to be consistent rather than exact with carbohydrate counting, because the former is associated with better glycemic control.

Question 131

Recommendations for physical activity and exercise for adults

Answer 131

At least 150 minutes of moderate-intensity aerobic activity or 75 minutes of vigorous-intensity aerobic activity each week plus muscle-strengthening activities on 2 or more days each week

*Should receive medical clearance before embarking on an exercise program

Question 132

Recommendations for physical activity and exercise for youth

Answer 132

60 minutes or more of daily physical activity, which should include muscle- and bone-strengthening activities on 3 or more days each week

*Should receive medical clearance before embarking on an exercise program

Question 133

What is the lag effect of exercise?

Answer 133

Hypoglycemia can occur during and immediately following the activity, and again 7 to 11 hours after the exercise. This likely results from enhanced insulin sensitivity, blunted counterregulatory hormone release, and increased glucose uptake by the liver and skeletal muscles to replenish glycogen stores after exercise.

Question 134

Blood glucose levels that should hinder exercise

Answer 134

<100 mg/dL
>=350 mg/dL (until corrected with insulin)

Also should not exercise when not feeling well or if with significant ketosis

Question 135

Ways to prevent hypoglycemia due to exercise

Answer 135

To prevent hypoglycemia, one should begin exercise with a glucose of 100 mg/dL or higher and plan to ingest carbohydrates during and/or after the exercise according to its duration and intensity.

Alternatively, one can reduce bolus insulin doses, by approximately 50% as a starting point, for any meal or snack within 2 hours of the planned activity.

For those receiving CSII, basal rates can be lowered by approximately 50% or even suspended for periods of 1 to 2 hours for exercise based on the patient’s needs.

Question 136

Amount of carbohydrate that should be ingested during and/or after exercise

Answer 136

One can consider providing 0.25 g to up to 1.00 g of carbohydrate per minute of exercise when the activity lasts 40 minutes or longer, individualized based on the person’s size, his or her needs, and past experience.

Question 137

Ways to manage the lag effect of late hypoglycemia risk after exercise

Answer 137

Basal rates can be reduced by approximately 20% for up to 6 hours at bedtime for those treated with CSII, or long-acting insulin doses can be reduced by approximately 20% at bedtime.

Question 138

Definition of “significant ketosis” which should hinder exercise

Answer 138

More than small urinary ketones or a blood hydroxybutyrate level of 1.5 mmol/L or more

Question 139

Table 36.6 Insulin Types and Action Profiles, page 1427

Answer 139

*

Question 140

Initial management in pediatric patients with newly diagnosed diabetes

Answer 140

Resuscitation with oral or intravenous fluids to rehydrate and correct electrolyte imbalances
Administration of insulin to halt lipolysis and reverse hepatic gluconeogenesis and ketogenesis
Commencement of diabetes education

Question 141

Typical starting insulin dose for young children and postpubertal adults who are not obese and do not present in DKA

Answer 141

0.3 to 0.5 units/kg per day

50% of the TDD delivered as once-daily dose of basal insulin and 50% given as boluses

Question 142

Typical starting insulin dose for young children who are obese, in puberty, or following presentation with DKA

Answer 142

May receive a starting dose of 1 unit/kg per day

50% of the TDD delivered as once-daily dose of basal insulin and 50% given as boluses

Question 143

What is the individualized insulin-to-carbohydrate ratio and how to compute?

Answer 143

The number of grams of carbohydrate covered by 1 unit of insulin (roughly 450 divided by the total daily insulin dose)

Question 144

What is the individualized correction factor (or sensitivity factor or sensitivity index) and how to compute?

Answer 144

The expected decrease in blood glucose resulting from 1 unit of insulin (approximately 1650 divided by the total daily insulin dose)

Question 145

How do we compute for the bolus dose with the meal or snack?

Answer 145

The sum of the calculated carbohydate coverage and the calculated blood glucose correction

Step 1: Count cabrbohydates
- 60 g

Step 2: Determine insulin to-carbohydrate ratio
- If TDD is 20 units - 450 divided by 20 = 22.5 grams of carbohydate is covered by 1 unit of insulin (1:22.5)
- If 60 g meal - 60 divided by 22.5 = 2.7 units needed to cover for 60 g meal

Step 3: Determine the amount of insulin required to correct for the premeal blood glucose level using the individualized correction factor
- If target premeal blood glucose level is 120 mg/dL, and actual level is 220 mg/dL, need to decrease blood sugar by 100 mg/dL
- If TDD is 20 units - 1650 divided by 20 = 82.5 decrease in blood glucose from 1 unit of insulin
- To decrease blood glucose by 100 - 82.5 divided by 100 = 0.825 units needed

Step 4: Add Steps 2 and 3 = 3.525 units or simply 4 units bolus dose

Question 146

Administration of rapid acting insulin should not be more frequent than

Answer 146

Every 3 hours to avoid hypoglycemia from “stacking” of insulin action, since action time is 3 hours

Question 147

Accuracy standard for glucose meters

Answer 147

At least 95% of blood glucose meter results should fall within +/- 15 mg/dL for blood glucose <100 mg/dL and within +/- 15% for blood glucose >=100 mg/dL performed with a reference method

Question 148

Frequency of blood glucose monitoring for persons with T1DM

Answer 148

At least 4 times daily and up to 10-12 times daily

Question 149

Continuous glucose monitoring, continuous subcutaneous insulin infusion, and artificial pancreas, pages 1429-1433

Answer 149

*

Question 150

Adjunctive treatment that has been FDA approved for use in children with T1DM
a. Pramlintide
b. Metformin
c. GLP1-RA
d. DPP4i
e. SGLT1i
f. SGLT2i

Answer 150

None of the above

No adjunctive treatments have been FDA approved for use in children with T1DM.

Question 151

Adjunctive treatment that has been FDA approved for use in adults with T1DM
a. Pramlintide
b. Metformin
c. GLP1-RA
d. DPP4i
e. SGLT1i
f. SGLT2i

Answer 151

A

Question 152

Regarding pramlintide:
a. Drug class
b. HbA1c reduction
c. Weight loss
d. Most frequent side effect

Answer 152

a. Injectable amylin analogue
b. Modest 0.3-0.6%
c. Modest 0.4-1.3kg
d. Nausea

Question 153

TRUE or FALSE: Individuals with T1DM have reduced GLP1 production, leading to ineffective glucagon suppression.

Answer 153

FALSE

Individuals with T1DM have normal GLP1 production but dysregulation between the pancreas and the gut, leading to ineffective glucagon suppression.

Question 154

Mode of reporting for glucose time in range as well as time in hyper- or hypoglycemia

Answer 154

Should be reported per unit time, as in the percentage of the values in the specified range of 24 hours/day

Question 155

Definition of a clinically meaningful episode of hypoglycemia in CGM

Answer 155

15 minutes or more of consecutive CGM readings less than 54 mg/dL

Question 156

TRUE or FALSE: Transition in care from pediatric to adult health care should begin at 18 years old.

Answer 156

Transition is considered as the process that begins during adolescence when the teen accepts more diabetes self-care responsibilities and attends part of the diabetes encounter without parents or guardians.

Question 157

Definition of DKA

Answer 157

Hyperglycemia (blood glucose >200 mg/dL)
Ketonemia (blood beta-hydroxybutyrate >=3 mmol/L or moderate/large urine ketones)
Acidosis (venous pH <7.3 or serum bicarbonate <15 mmol/L)

Question 158

Pathophysiology of DKA

Answer 158

Relative or absolute insulin deficiency –> Increase in glucagon and accompanying increases in epinephrine, norepinephrine, cortisol, and growth hormone levels –> Catabolic state in the periphery, mobilizing substrates to the liver –> Increased production of glucose and ketone bodies

Osmotic diuresis –> dehydration, loss of electrolytes
Vomiting

Cycle of additional stress hormone production

Question 159

Renal threshold for glucose

Answer 159

Approximately 180 mg/dL

Question 160

Patients who are at a greater risk of DKA at diagnosis

Answer 160

Young (<5 years)
Do not have a first-degree relative with T1DM
Lower socioeconomic status

But most cases of DKA, in fact, occur in those with established diabetes

Question 161

TRUE or FALSE: Insulin pump use is associated with higher rates of DKA compared with MDI, due to insulin pump failure.

Answer 161

FALSE

Insulin pump use is actually associated with lower rates of DKA compared with MDI, although insulin pump failure is an important cause of hyperglycemia, ketonemia, and DKA.

Question 162

TRUE or FALSE: Monitoring of ketones using urine ketone strips is preferred over blood ketone meters.

Answer 162

FALSE

Monitoring of ketones using blood ketone meters that measure beta-hydroxybutyrate is preferred over monitoring of urine ketone strips, due to easier sampling, lower rates of hospitalization/emergency department visits, and the potential for earlier and more accurate identification of clinical worsening or improvement.

Question 163

Insulin dosing during sick days

Answer 163

Supplemental rapid-acting insulin boluses:
While ketones persist - every 2 to 3 hours
For ketones with hypoglycemia - consider reducing basal rates for a short period of time for patients on insulin pumps
For ketones, hypoglycemia, and decreased oral intake over a prolonged period - consider reducing the insulin glargine dose for patients on MDI and basal rates for those on insulin pumps

*Also, depending on ketone level and blood sugar level, might even have to increase bolus dose (see Table on page 1436)

Question 164

Target oral fluid intake during sick days to prevent or treat dehydration

Answer 164

A reasonable target oral fluid intake is 0.5 to 1.0 ounce per year of age per hour (maximum 8 ounces/hour).

Question 165

Type of drink for hydration during sick days depending on blood glucose level

Answer 165

If blood glucose is <=250 mg/dL, rehydrate with sugar-containing clear liquids (e.g., sports drinks, soda, popsicles, oral electrolyte solution)

If blood glucose is >250 mg/dL, give sugar-free clear liquids (e.g., water, diet soda, seltzer, diet juices)

Question 166

Frequency of education on sick day management and DKA prevention

Answer 166

ADA: Yearly

Question 167

Glucagon Mini-Dosing for sick days when blood sugars remain low and ketones remain elevated

Answer 167

Age <2 years: 20 ug
Age 2-15 years: 10 ug per year of age (range 20-150)
Age >15 years: 150 ug

Question 168

Patients and families should be aware that they should seek immediate medical attention for:

Answer 168

• Signs of dehydration
• Prolonged vomiting for more than a few hours
• Persistent hyperglycemia (>250-300 mg/dL)
• Ketones that do not improve after 12 hours
• Symptoms of DKA (abdominal pain, nausea, vomiting, fruity-smelling breath, hyperventilation, or altered mental status)

Question 169

Immediate initial treatment of DKA

Answer 169

Fluid replacement, typically with one or two intravenous fluid boluses with normal saline, 10 mL/kg each, followed by continuous cautious rehydration with the goal of replacing the estimated fluid deficit over the first 24 to 48 hours

Question 170

Timing and dosing of insulin drip in the treatment of DKA

Answer 170

Initiation of insulin drip at a rate of 0.05 to 0.1 units/kg per hour, without an insulin bolus, should begin at last 1 hour after fluid replacement is started.

Question 171

Target decrease of blood glucose during treatment for DKA

Answer 171

Blood glucose should fall gradually at a rate of 50 to 75 mg/dL per hour

Question 172

Typical content of fluid replacement in DKA

Answer 172

Fluid should typically contain saline with potassium, phosphate, and acetate

Question 173

TRUE or FALSE: The rate of fluid administration and sodium chloride content of fluids during treatment for DKA have been shown to result in decline in mental status, clinically apparent brain injury, and poor short-term memory and IQ.

Answer 173

FALSE

Question 174

Risk factors for cerebral edema in DKA

Answer 174

Young age (<5 years)
New-onset T1DM
Longer duration of symptoms
Lower initial pH
Higher initial BUN
Treatment with bicarbonate
Serum Na concentrations increasing during initial treatment of DKA

Question 175

Prevalence of autoimmune diseases in T1DM patients are higher in:

Answer 175

Older age
Female sex
Non-Hispanic white race

Question 176

Most common autoimmune disorder associated with T1DM

Answer 176

Thyroid disease (approximately 20%)

Question 177

Recommendation on screening and monitoring for thyroid disease in T1DM patients

Answer 177

ADA and ISPAD recommend measuring thyroid antibodies and TSH levels soon after diagnosis, and every 1 to 2 years, and sooner if the patient develops any new symptoms or signs concerning for thyroid dysfunction

Question 178

What to do if TFTs are slightly abnormal at the time of T1DM diagnosis

Answer 178

This may be due to sick euthyroid syndrome, and TFTs should be reassessed once glycemic control improves

Question 179

TRUE or FALSE: Subclinical hypothyroidism has been associated with decreased linear growth velocity and increased risk of symptomatic hypoglycemia, while celiac disease has been associated with increased glycemic variability and unexplained hypoglycemia.

Answer 179

TRUE

Question 180

Second most common coexistent autoimmune disorder in patients with T1DM

Answer 180

Celiac disease

Question 181

Prevalence of celiac disease is higher in

Answer 181

Younger at T1DM diagnosis
White race

Question 182

Measure that mitigates the risk of celiac disease in those at increased risk for celiac disease and T1DM

Answer 182

Introduction of gluten-containing foods between 4 and 6 months of age (compared with introduction in the first 3 months of life or in the seventh month or later)

Question 183

ADA and ISPAD recommendations for screening for celiac disease in children with T1DM

Answer 183

ADA: Soon after diagnosis, then rescreen within 2 years and again after 5 years

ISPAD: Soon after diagnosis, then rescreen every 1-2 years

Screening includes IgA tissue transglutaminase antibodies. If found to be deficient, send IgG-specific antibody tests

More frequent screening may be necessary if symptoms develop or in children who have a first-degree relative with celiac disease

Typically, a biopsy is done to confirm the diagnosis

Question 184

Interventions if screening for celiac disease is positive and once diagnosis is confirmed

Answer 184

Refer to gastroentereology before prescribing a gluten-free diet

Refer to a dietitian experienced in managing both diabetes and celiac disease

Question 185

Trial that found that IAA is first autoantibody, followed by GADA

Answer 185

BABYDIAB

Question 186

Trial that found that IAA is first autoantibdoy, followed by GADA

Answer 186

BABYDIAB