Gestational diabetes mellitus

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Gestational diabetes mellitus

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Dr. Kanakamani Madhivanan, M.D., D.M. (Endocrinology), Assistant Professor Department of Endocrinology, Diabetes, Metabolism Christian Medical College, Vellore – PowerPoint PPT presentation

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Title: Gestational diabetes mellitus

1
Gestational diabetes mellitus
Dr. Kanakamani Madhivanan, M.D., D.M.
(Endocrinology), Assistant Professor Department
of Endocrinology, Diabetes, Metabolism Christian
Medical College, Vellore
2
Plan of presentation

Introduction
Physiology of fuel metabolism in normal pregnancy
Pathophysiology of GDM
Epidemiology of GDM
Screening and diagnosis
Maternal and fetal risks
Management of GDM
Obstetric management

3
Introduction
4
Introduction

Global increase in prevalence of DM
Individual importance - Hyperglycemia in
pregnancy has adverse effects on both mother and
fetus
Public health importance rising epidemic of DM
in part attributed to the diabetic pregnancies
Prevention of type 2 DM should start intrauterine
and continue throughout life

5
Introduction

Gestational diabetes (GDM) is defined as any
degree of impaired glucose tolerance of with
onset or first recognition during pregnancy .
Many are denovo pregnancy induced
Some are type 2 ( 35-40)
10 have antibodies

6
Introduction

Difficult to distinguish pregestational Type 2 DM
and denovo GDM
Fasting hyperglycemia
blood glucose greater than 180 mg/dL on OGT
acanthosis nicgrans
HbA1C gt 5.3
a systolic BP gt 110 mm Hg
BMI gt 30 kg/m2
Fetal anomalies
Clues for Type 1
Lean
DKA during pregnancy
Severe hyperglycemia with large doses of insulin

7
Fuel metabolism in pregnancy
8
Fuel metabolism in pregnancy

Goal is uninterrupted nutrient supply to fetus
The metabolic goals of pregnancy are
1) in early pregnancy to develop anabolic stores
to meet metabolic demands in late pregnancy
2) in late pregnancy to provide fuels for fetal
growth and energy needs.

9
Glucose metabolism in pregnancy

Early pregnancy
E2/PRL stimulates b cells Insulin sensitivity
same and peripheral glucose utilisation 10
fall in BG levels
Late pregnancy
Fetoplacental unit extracts glucose and
aminoacids, fat is used mainly for fuel
metabolism
Insulin sensitivity decreases progressively upto
50-80 during the third trimester
variety of hormones secreted by the placenta,
especially hPL and placental growth hormone
variant, cortisol, PRL,E2 and Prog

10
Glucose metabolism in pregnancy
FASTING accelerated starvation and esxaggerated
ketosis (maternal hypoglycemia, hypoinsulinemia,
hyperlipidemia, and hyperketonemia)
FED hyperglycemia, hyperinsulinemia,
hyperlipidemia, and reduced tissue sensitivity to
insulin
Fat
Hyperinsulinemia
Insulin resistance
Glucose
Aminoacids
Fetus
11

24-hour insulin requirement before conception is
approximately 0.8 units / kg.
In the first trimester, the insulin requirement
rises to 0.7units / kg of the pregnant weight
more unstable glycemia with a tendency to low
fasting plasma glucose and high postprandial
excursions and the occurrence of nocturnal
hypoglycemia
By the second trimester, the insulin requirement
is 0.8 units per kilogram. From 24th month
onwards steady increase in insulin requirement
and glycemia stabilises
By third trimester the insulin requirement is 0.9
- 1.0 unit /kg pregnant weight per day
Last month may be a decrease in insulin and
hypoglycemias esp. nocturnal

12
EPIdemiology AND Risk factors
13
Magnitude of problem Global

Prevalence of GDM varies worldwide and among
different racial and ethnic groups within a
country
America white women (3.9) and Asian (8.7)
Europe 0.6 to 3.6
Australia 3.6 to 4.7 (Indian women 17.7)
China 2.3 Japan 2.9
Variability is partly because of the different
criteria and screening regimens

14
Magnitude of the problem - India

Chennai, hospital based, universal screening
18.9 had FPG 126 and PPPG 140.
Trivandrum 15
Bangalore 12
Erode 18.8
Chennai, community based, universal screning,
17.8 in urban, 13.8 in semi urban and 9.9 in
rural areas.
Chennai 0.56
Mysore Parthenon Study 6
Maharashtra, hospital based, selective screening
7.7 had GDM 13.9 had IGGT.

15
Risk factors

A family history of diabetes, especially in first
degree relatives
Prepregnancy weight 110 of ideal body weight or
body mass index over 30 kg/m2 or significant
weight gain in early adulthood, between
pregnancies, or in early pregnancy
Age greater than 25 years
Previous delivery of a baby greater than 4.1 kg
Personal history of abnormal glucose tolerance
Member of an ethnic group with higher than the
background rate of type 2 diabetes (in most
populations, the background rate is approximately
2 percent)
Previous unexplained perinatal loss or birth of a
malformed child
Maternal birthweight greater than 4.1 kg or less
than 6 pounds 2.7 kg
Glycosuria at the first prenatal visit
Polycystic ovary syndrome
Current use of glucocorticoids
Essential hypertension or pregnancy-related
hypertension

16
Maternal and Fetal risks
17
Maternal complications

Worsening retinopathy 10 new DR, 20 mild NPDR
and 55 mod-severe NPDR progresses
Worsening proteinuria. GFR decline depends on
preconception creatinine and proteinuria
Hypertension and Cardiovascular disease
Neuropathy No worsening (gastroparesis, nausea,
orthostatic dizziness can be worsened)
Infection

18
Maternofetal complications

Macrosomia 63 percent
Cesarean delivery 56 percent
Preterm delivery 42 percent
Preeclampsia 18 percent
Respiratory distress syndrome 17 percent
Congenital malformations 5 percent
Perinatal mortality 3 percent
Spontaneous abortion, third trimester fetal
deaths, Polyhydramnios, preterm birth, ?adverse
neurodevelopmental outcome
Risk for type 2 DM

19
Neonatal complications

Morbidity associated with preterm birth
Macrosomia birth injury (shouldeer dystocia,
brachial plexus injury)
Polycythemia and hyperviscosity
Hyperbilirubinemia
Cardiomyopathy
Hypoglycemia and other metabolic abnormalities
(hypocalcemia, hypomagnesemia)
Respiratory problems
Congenital anomalies

20
Congenital anomalies

2/3rd CVS or CNS, 13-20 times common
Cardiac( including great vessel anomalies) most
common
Central nervous system (spina bifida/anencephaly)
7.2
Skeletal cleft lip/palate, caudal regression
syndrome
Genitourinary tract ureteric duplication
Gastrointestinal anorectal atresia

Skeletal and central nervous system
Caudal regression syndrome
Neural tube defects excluding anencephaly
Anencephaly with or without herniation of neural
elements
Microcephaly
Cardiac
Transposition of the great vessels with or
without ventricular
Ventricular septal defects
Coarctation of the aorta with or without
ventricular septal defects or patent ductus
arteriosus
Atrial septal defects
Cardiomegaly
Renal anomalies
Hydronephrosis
Renal agenesis
Ureteral duplication
Gastrointestinal
Duodenal atresia
Anorectal atresia
Small left colon syndrome

22
Caudal regression syndrome
23
Caudal regression syndrome
24
SCREENING AND DIAGNOSIS
25
Whom to screen ?

No consensus
recommended screening ranges from selective
screening of average- and high-risk individuals
to universal diagnostic testing of the entire
population dependent on the risk of diabetes in
the population.
Risk stratification based on certain variables
Low risk no screening
Average risk at 24-28 weeks
High risk as soon as possible

26
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27
Low risk for GDM

To satisfy all these criteria
Age lt25 years
Not a member of an ethnic group with high
prevalence of GDM (not Hispanic, Native
American/Alaskan, Asian/Pacific Islander, African
American)
Normal prepregnancy body weight (not 20 or more
over desired body weight or BMI 27 kg/m2 or more)
No family history of diabetes in first-degree
relatives.
No history of abnormal glucose tolerance
No history of poor obstetric outcome

28
High risk

Marked obesity
Prior GDM (30-50 risk for recurrence)
Glycosuria
Strong family history

29
When and how to screen?

24-28 weeks
High risk
First prenatal visit
50 g glucose loading test
High risk women 3 hr GTT with 100 g glucose

30
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31
50 g GTT

A 50-g oral glucose load is given without regard
to the time elapsed since the last meal and
plasma or serum glucose is measured one hour
later
A value 130 mg/dL is considered abnormal we
use 130 mg/dL as the threshold for our patients.
Capillary blood should not be used for screening
unless the precision of the glucose meter is
known, it has been correlated with simultaneously
drawn venous plasma samples, and has met federal
standards for laboratory testing.

32
100 g GTT

Oral glucose tolerance test ( OGTT) with 100 gm
glucose
Overnight fast of at least 8 hours
At least 3 days of unrestricted diet and
unlimited physical activity
gt 2 values must be abnormal

Fasting gt 95 mg/dl
1-h gt 180 mg/dl
2-h gt 155 mg/dl
3-h gt 140 mg/dl
33
75 g GTT
ADA
WHO
Fasting gt 95 mg/dl
1-h gt 180 mg/dl
2-h gt 155 mg/dl
Fasting gt 95 mg/dl
OR OR
2-h gt 140 mg/dl
34
Whom and when to screen? Indian Scenario -The
DIPSI Guidelines

75 gm GCT with single PG at 2 hrs
140 mg/dL is GDM
120 mg/dL is DGGT
Universal screening
First trimester, if negative at 24 28 weeks and
then at 32 34 weeks

35
Management of gdm

36
MANAGEMENT ISSUES

Patient education
Medical Nutrition therapy
Pharmacological therapy
Glycemic monitoring SMBG and targets
Fetal monitoring ultrasound
Planning on delivery

37
Medical nutrition therapy

Goals
Achieve normoglycemia
Prevent ketosis
Provide adequate weight gain
Contribute to fetal well-being
Nutritional plan
Calorie allotment
Calorie distribution
CH2O intake

38
Calorie allotment

30 kcal per kg current weight per day in pregnant
women who are BMI 22 to 25.
24 kcal per kg current weight per day in
overweight pregnant women (BMI 26 to 29).
12 to 15 kcal per kg current weight per day for
morbidly obese pregnant women (BMI gt30).
40 kcal per kg current weight per day in pregnant
women who are less than BMI 22.

39
Carb intake

Postprandial blood glucose concentrations can be
blunted if the diet is carbohydrate restricted.
Complex carbohydrates, such as those in starches
and vegetables, are more nutrient dense and raise
postprandial blood glucose concentrations less
than simple sugars.
Carbohydrate intake is restricted to 33-40 of
calories, with the remainder divided between
protein (about 20) and fat (about 40).
With this calorie distribution, 75 to 80 percent
of women with GDM will achieve normoglycemia.

40
Calorie distribution

Variable opinion
Most programs suggest three meals and three
snacks however, in overweight and obese women
the snacks are often eliminated
Breakfast The breakfast meal should be small
(approximately 10of total calories) to help
maintain postprandial euglycemia. Carbohydrate
intake at breakfast is also limited since insulin
resistance is greatest in the morning.
Lunch 30 of total calories
Dinner 30 of total calories
Snacks Leftover calories (approximately 30 of
total calories) are distributed, as needed, as
snacks.

41
Monitoring BG

Atleast 4 times
Fasting and 3 one hr postprandial
Pre vs postprandial monitoring
Better glycemic control (HbA1c value 6.5 versus
8.1 percent)
A lower incidence of large-for-gestational age
infants (12 versus 42 percent)
A lower rate of cesarean delivery for
cephalopelvic disproportion (12 versus 36
percent)

42
Monitoring BG

Home monitoring
Maintain log book
Use a memory meter
Calibrate the glucometer frequently
HbA1C
Ancillary test for feedback to the patient
Lower values when compared to nonpregnant state
lower BG and increase in red cell mass and slight
decrease in life span measured every 2-4 weeks
Target lt 5.1

Studies report no to moderate correlations
between HbA1 and different components of the
glucose profile when an HbA1 result of 4 to 5
includes a capillary blood glucose range of 50 to
160 mg/dL.
Levels of HbA1c are related to the rate of
congenital anomalies and spontaneous early
abortions in pre-existing diabetes, but the use
of this measure, which retrospectively reflects
glycemic profile in the last 10 weeks, for
treatment evaluation in GDM is questionable. In
addition, the association between glycosylated
hemoglobin and pregnancy outcome in GDM or
prediction of macrosomia is poor
Glycosylated protein and fructosamine widely
variable and not yet established

44
Glycemic targets (ACOG)

ACOG
Fasting venous plasma 95 mg/dl
1 hour postprandial 140 mg/dl
2 hour postprandial 120 mg/dl
Pre-meal 100 mg/dl
A1C 6
ADA
premeal 80-110
2 hr postmeal not more than 155

These are venous plasma targets, not glucometer
targets
45
PHARMACOLOGICAL INTERVENTION

If the FPG at diagnosis is 120, can consider
immediate therapy.
Otherwise, MNT for 2 weeks
If majority FPG (4/7) gt 95 or PP gt 120 then to
start on insulin.

46
Insulin

15 need insulin
Total dose varies. 0.7 to 2 units per kilogram
(present pregnant weight)
FBG high Night NPH 0.2 units/kg
PPBG high bolus 1.5 units/10 gm CH2O for
breakfast and 1 unit /10 gm CH2O for lunch and
dinner
If both pre and postprandial BG high or if the
woman's postprandial glucose levels can only be
blunted if starvation ketosis occurs - four
injection/day regimen.
Total 0.7 unit/kg up to week 18
0.8 unit/kg for weeks 18 to 26
0.9 unit/kg for weeks 26 to 36
1. unit/kg for weeks 36 to term.
In a morbidly obese woman, the initial doses of
insulin may need to be increased to 1.5 to 2.
units/kg to overcome the combined insulin
resistance of pregnancy and obesity.

47
OHA in pregnancy

Systematic review by John Hopkins University
maternal glucose levels did not differ
substantially between gravidae treated with
insulin versus those treated with oral
glucose-lowering agents
there was no consistent evidence of an increase
in any adverse maternal or neonatal outcome with
use of glyburide, acarbose, or metformin compared
with use of insulin
Inconsistent data. ADA, ACOG, USFDA do not
endorse.

48
OHA in pregnancy

Tolbutamide and chlorpropamide
Cross placenta. Fetal hperinsulinemia. Prolonged
fetal hypoglycemia
Glibenclamide
Minimal transplacental transport
Observational studies no excess anomalies or
hypoglycemia
Only RCT 404 women. Glib vs insulin. No
difference

second-generation sulfonylureas especially
glyburide, do not significantly cross the
diabetic or nondiabetic placenta. Fetal
concentrations reached no more than 1 to 2 of
maternal concentrations.
tolbutamide diffused across the placenta most
freely, followed by chlorpropamide, then
glipizide, with glyburide crossing the least.
Metformin crosses placenta not teratogenic in
rat models

50
OHA in pregnancy

Metformin
Category B
No adverse outcome after first trimester
Second, third trimester safe and effective
Vs. insulin no serious adverse effects
No studies vs. glibenclamide
Acarbose
Two prelim studies
Thiazolidinediones and GLP-1
Not studied

51
Obstetric management
52
Fetal monitoring

Baseline ultrasound fetal size
At 18-22 weeks major malformations
fetal
echocardiogram
26 weeks onwards growth and liquor volume
III trimester frequent USG for accelerated
growth
( abdominal head circumference)

53
Timing of delivery

Small risk of late IUD even with good control
Delivery at 38 weeks to avoid late still birth
and fetal growth leading to shoulder dystocia
Vaginal delivery preferred
Caesarian section only for routine obstetric
indication
just GDM is not an indication !
Unfavorable condition of the cervix is a problem
4500 grams, cesarean delivery may reduce the
likelihood of brachial plexus injury in the
infant (ACOG). Assessing fetal weight accurately
is a problem

54
Management of labor and delivery

Maternal hyperglycemia in labor fetal
hyperinsulinemia,
worsen fetal acidosis and neonatal
hypoglycemia
Insulin requirements come down
Maintain sugars 70-90 mg/dl
Routine GDM diet
Maintain basal glucose requirements
Monitor sugars 1-4 hrly intervals during labour
Give insulin as infusion only if sugars more than
120 mg/dl

55
Glycemic management during labour

Later stages of labour start dextrose to
maintain basal nutritional requirements 150-200
ml/hr of 5 dextrose
Elective LSCS check FBS, if in target no
insulin, start dextrose drip
Continue hourly SMBG
Post delivery keep patients on dextrose-normal
saline till fed
No insulin unless sugars more than normal
nonpregnant levels

56
Post partum follow up

Check BG before discharge
Breast feeding helps in weight loss. Insulin,
tolbutamide compatible. Chlropropamide secreted
small amounts watch for hypoglycemia in infant.
Glyburide and glipizide not secreted Metformin
secreted - no adverse effects
Lifestyle modification exercise, weight
reduction
OGTT at 6-12 weeks postpartum classify patients
into normal/impaired glucose tolerance and
diabetes
Contraception low dose EP can be used.
Progestin only pills shown to increase risk of
T2DM in GDM
Preconception counseling for next pregnancy

57
Immediate management of neonate

Hypoglycemia 50 of macrosomic infants
515 optimally
controlled GDM
Starts when the cord is clamped
Exaggerated insulin release secondary to
pancreatic ß-cell hyperplasia
Increased risk blood glucose during labor and
delivery exceeds 90 mg/dl

Anticipate and treat hypoglycemia in the infant
58
Management of neonate

Hypoglycemia lt40 mg/dl
Encourage early breast feeding
If symptomatic give a bolus of 2- 4 ml/kg, IV 10
dextrose
Check after 30 minutes, start feeds
IV dextrose 6-8 mg/kg/min infusion
Check for calcium, if seizure/irritability/RDS
Examine infant for other congenital abnormalities

59
Future risks in mother and child
60
Future risks - Mother

Atleast 6 weeks post delivery, 75 g OGTT for all
GDM
90 normoglycemic
Recurrence of GDM 30-60
Older
Multipara
Weight gain interpregnancy
Higher infant BW in index pregnancy
IGT and T2DM
20 IGT postpartum
3.7 _at_ 6m , 4.9 _at_ 15m and 18.9 _at_ 9 y

61
Who will progress to DM?

WC and BMI stronset predictors
Autoantibodies
DM at earlier gestational age
Gestational requirement of insulin
Higher FBG
Higher BG on OGTT
Neonatal hypoglycemia
Recurrent GDM

62
Preconception counselling

Diabetic mother glycemic control with
insulin/SMBG
Target HbA1c lt 7
Folic acid supplementation 5 mg/day
Ensure no transmissible diseases HBsAg, HIV,
rubella
Try and achieve normal body weight diet/exercise
Stop drugs oral hypoglycemic drugs, ACE
inhibitors, beta blockers

63
Risk of developing DM in offspring

Type 1 -
Father - 1 in 17 risk
Mother - 1 in 25 risk if, at the time of
pregnancy, the mother is lt 25 years of age but a
1 in 100 risk if the mother is 25 years of age or
older.
These risks are doubled if the affected parent
developed diabetes before age 11.
Both parents have type 1 diabetes - 1 in 10 - 1
in 4.
Type 2 polyglandular autoimmune syndrome 50
Type 2
Single parent - 1 in 7 if the parent was
diagnosed before age 50 and 1 in 13 if the parent
was diagnosed after age 50.
There is some evidence that the offspring's risk
is greater when the parent with type 2 diabetes
is the mother. I
Both parents - 1 in 2.