Title: Preconception and early post conception counseling
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2Preconception and early post conception
counseling in D.M
Fakhrolmolouk Yassaee. MD. Assistant professor
OBS GYN. Obstetric gynecologic department,
perinatology center Taleghani Hospital Shaheed
Beheshti medical science university Evin, Tehran,
IRAN
3- The question raised most frequently by diabetic
women are - What is know about the heritability of diabetes?
- What health measure can be implemented before
conception? - What type of obstetric care is recommended?
- Will retinal and renal complications worsen
during pregnancy and shorten life expectancy? - What sort of malformations do infants of diabetic
mothers have and what causes them?
4- The obstetrician, internist, genetic counselor
all have important roles in providing advice to
diabetic women both before and throughout
pregnancy. Genetic transmission of diabetes is
complex and depends upon the type of carbohydrate
intolerance. - It is a chronic autoimmune disorder that occurs
in genetically susceptible individuals. Major
histocompatibility haplotype (HLA) strongly - influence susceptibility. No genetic marker has
been identified for IDDM but a major component of
genetic susceptibility has been identified as a
gene or genes located near within the HLA complex
on the short arm of chromosome 6.
5- Genetic couseling and a careful medical
assessment before conception are recommended for
all diabetic women and those with a history of
gestational diabetes during a previous pregnancy.
In infants of diabetic mother (IDM), congenital
malformation occur about 2-3 times as often as in
those of nondiabetic women. (Mill 1982)
6- Ylinen and associates (1984) have also reported a
higher risk of minor and major malformation is
infants of diabetic mothers with elevated HbA1c
concentrations.
7- The majority of lesions involve the central
nervous system and the cardiovascular system,
genitourinary and limb defects (cousins 1991). - There is no increase in birth defects among
offspring of diabetic fathers, prediabetic
women, and women who develop gestational diabetes
after the first trimester, suggesting that
glycemic control during embryogenesis is the main
factor in the genesis of diabetes- associated
birth defects.
8- Miller and coauthors( 1981) compared the
frequency of congenital anomalies in patients
with normal or high first- trimester maternal
glycohemoglobin and found only 3.4 rate of
anomalies with HbA1c less than 8.5 whereas the
rate of malformations in patient with poorer
glycemic control in the periconceptional period
(HbA1c gt 8.5) was 22.4
9- Because the critical time for teratogenesis is
during the period 3-6 weeks after conception,
nutritional and metabolic intervention must be
institutes preconseptionally to be effective.
10- Fetal overgrowth is a major problem in
pregnancies complicated by diabetes. Defined
typically as birth weight above the 90th
percentile for gestational age or greater than
4000 g, macrosomia occurs in 15- 45 of diabetic
pregnancies. - Neonatal morbidity hypoglycemia, macrosomia,
neonatal jaundice, one fifth of IDMS had
disproportionate macrosomia (Hunter ,1993) - (abdominal circumference greater than head
circumference) compared with 1 control infants
(Ballard, 1993) - Birth injury, including shoulder dystocia and
brachial plexus trauma is more common among IDM,
and macrosomic fetuses are at the highest risk.(
Keller 1991)
11- Acceleration of growth, stimulated by excessive
glucose delivery during diabetic pregnancy, may
extend into childhood and adult life. Silverman
(1995) reported on the follow up of macrosomic
IDMS through 8 years of age in which half of the
IDMS weighed more than the heaviest 10 of the
nondiabetic children. These investigator also
found that the diabetic offspring have permanent
derangement in glucose- insulin kinetics,
resulting in increased incidence of impaired
glucose tolerance in later childhood.
12- The macrosomic IDM dose not follow the growth
pattern observed in euglycemic pregnancies.
During the first and second trimesters,
differentiation of diabetic from nondiabetic
fetuses is extremely difficult using ultrasound
measurements, suggesting that the period of fetal
fat deposition (28 weeks and onward) is when
abnormal fetal growth primarily occurs.
13- Morphologic studies of the IDM neonate indicate
that the increased growth of the abdominal
circumference (AC) is due to deposition of fat in
the abdominal and interscapular area. This
central deposition of fat is a key characteristic
of diabetic macrosomic and underlies the dangers
associated with vaginal delivery in these
pregnancies. Acker (1980) reported that although
the incidence of shoulder dystocia is 3 among
infants weighing greater than 4000g, 16 of
infant from diabetic pregnancies weighing greater
than 4000g, sustained shoulder dysticia.
14- Key features of a preconceptional diabetes
management program should include the following - A through assessment of cardiovascular, renal,
ophthalmologic, status. Blood pressures, 24- hour
protein and creatinine, and retinal examination
should be performed. Thyroid function ( TSH and
FT4) should be evaluated. Antihypertensive agents
should be initiated and regulated - A regimen of frequent and regular monitoring of
both pre-prandial and postprandial glucose
capillary glucose levels. - Target levels are fasting glucose 80- 95 mg/dl
and 1- hour postprandial glucose less than
130mg/dl or 2 hour postprandial glucose less than
120 mg/dl -
15- The insulin regimen should result in a smooth
glucose profile throughout the day with no
hypoglycemic reaction between meals or at night.
The regimen should be initiated early enough
before pregnancy so that the glycohemoglobin
level is lowered into the normal range for at
least 3 months prior to conception. - Taking a daily prenatal vitamin ( including 400
µg of folic acid ) at least 3 months prior to
conception to minimize risk of neural tube
defects in fetus. - Particular attention should be paid to support
systems that permit extended bed rest in the
third trimester if necessary.
16- The goals of management of diabetic pregnancy are
to prevent stillbirth and asphyxia while
minimizing maternal morbidity associated with
delivery. This involves monitoring fetal growth
in order to select the proper timing and route of
delivery. The first is testing fetal well- being
at frequent intervals and fetal size.
17 Fetal surveillance in type I and type II
diabetic pregnancies
- Time
Test - Preconception Maternal glycemic control
- 8-10 w sonographic crown rump
measurement - 16 w Maternal serum alpha-
fetoprotein level - 20-22 w high resolution
sonography, fetal cardiac
echography in women in in
suboptimal diabetic control (HbA1c ) at
first prenatal visit - 24w Baseline sonographic
growth assessment of the fetus - 28 w Daily fetal movement
counting by the mother - 32 w Repeat sonography for
fetal growth - 34 w Biophysical seting
- 2X weekly NST or
- weekly CST or
- weekly biophysical
profile - 36w Estimation of fetal
weight by sonography - 37-38.5 w Amniocentesis and delivery
for patients in poor control
(persistent
daily hyperglycemia) - 38.5 40 w Delivery without
amniocentesis for patients in good control who
have excellent dating criteria
18TESTS OF FETAL WELL - BEING
comment Reassuring result frequency test
Performed in all patients Ten movement in lt60 min Every night from 28 w Fetal movement counting
Being at 28-34 w with insulin dependent diabetes Two heart rate acceleration in 20 minutes Twice weekly Non- stress test
Same as for non stress test No heart rate decelerations in response to 3 contrations in 10 minutes weekly Contraction stress test
3 movement 2 1 flexion 2 30 sec breathing 2 2 cm amniotic fluid 2 Score of 8 in 30 minutes weekly Ultrasound biophysical profile
19CHOOSING TIMING AND ROUTE OF DELIVERY
- Timing of delivery should be selected to minimize
maternal and neonatal morbidity and mortality and
mortality. Delivery delaying as near as possible
to the EDC helps maximize cervical ripeness and
improves the chances of spontaneous labor and
vaginal delivery. Yet at the risks of fetal
macrosomia, birth injury, and fetal death
increase. - ( Rasmussen, 1992). Although earlier delivery at
37 wks. gestation might reduce the risk of
shoulder dystocia, an increase in failed labor
induction and poor neonatal pulmonary status must
be considered. Thus, an optimal time for
delivery of most diabetic pregnancies is between
38.5 and 40 wks.
20Indication for delivery diabetic pregnancy
- Fetal Non reactive NST
- Positive CST
- Reactive NST,
positive CST, mature fetus - Sonographic
evidence of fetal growth arrest - Decline in
fetal growth rate with decreased amnionic - fluid 40
41 w gestation -
- Maternal Severe preeclampsia
- Mild
preeclampsia, mature fetus - Markedly
falling renal function - Obstetric preterm labor with failure of
tocolysis - Mature fetus
, inducible cervix -
-
21CONFIRMATION OF FETAL MATURTY BEFORE INDUCTION OF
LABOR OR PLANNING CESAREAN DELIVERY W DIABETIC
PREGNANCY
- Phosphatidyl glycerol gt 3 in amniotic fluid
collected from vaginal pool or by amniocentesis - Completion of 38.5 weeks gestation
- Normal LMP
- First pelvic examination before 12 weeks confirm
dates. - Sonogram before 24 weeks confirm dates
- Documentation of more than 18 weeks by fetoscope
of FHT
22- After 38.5 weeks gestation, the obstetrician can
await spontaneous labor if the fetus is not
macrosomic and biophysical testing is reassuring.
In patients with GDM and super glycemic control,
continued fetal testing and expectant management
can be considered until 41 weeks ( Lurie 1992)
23- In the fetus with on AC measurably greater than
head circumference, induction should be
considered. After 40 weeks, the benefits of
continued conservative management are likely to
be less than the danger of fetal compromise.
Induction of labor 42 weeks in diabetic
pregnancy- regardless of the readiness of the
cervix- is prudent.
24- Given these data, the decision to attempt vaginal
delivery or perform a cesarean is inevitably
based on very limited data. The patients past
obstetric history, the best EFW, a fetal adipose
profile (abdomen larger than head), and clinical
pelvimetry should all be considered. Most large
series of diabetic pregnancies report a cesarean
section rate of 30- 50. The best means by which
this rate can be lowered is by early and strict
glycemic control in pregnancy. Conducting long
labor inductions in patients with a large fetus
and marginal pelvis may increase morbidity and
costs.
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