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Dr. Tejas M. Tamhane.
JRI
Introduction
 In 1866 Langdon Down noted that common characteristics
of patients with trisomy 21 are skin deficient in elasticity,
giving the appearance of being too large for the body and
flat face with a small nose.
 In the 1990s, it was realized that the excess skin of
individuals with Down’s syndrome can be visualized by
ultrasonography as increased nuchal translucency in the
third month of intrauterine life.
 Fetal nuchal translucency thickness at the 11–13+6 weeks
scan has been combined with maternal age to provide an
effective method of screening for Trisomy 21.
Benefits Of The 11–13+6 Weeks Scan
 Assessment of risk for trisomy 21 & other.
chromosomal defects.
 Major abnormalities of the heart and great arteries.
 Confirmation-fetus is alive.
 Accurate dating of the pregnancy.
 Early diagnosis of major fetal abnormalities.
 Detection of multiple pregnancies with reliable
identification of chorionicity.
Diagnosis Of Chromosomal Defects.
 Non invasive diagnosis- Examination of fetal cells
from maternal peripheral blood
 Invasive diagnosis-
1. Amniocentesis- between 14-20weeks.
2. CVS- performed only after 11 weeks.
 The risk of miscarriage from chorionic villus sampling
in the first trimester is the same as for amniocentesis
in the second trimester.
Screening For Chromosomal Defects
Maternal age
Gestational age
Fetal Nuchal Translucency
Nasal Bone And Other First-trimester Sonographic
Markers
 At 11–13+6 weeks the nasal bone is not visible by
ultrasonography in about 60–70% of fetuses with
Trisomy 21 and in about 2% of chromosomally normal
fetuses.
 Abnormalities in the flow velocity waveform from the
ductus venosus are observed in about 80% of fetuses
with trisomy 21.
Maternal Serum Biochemistry In The
First-trimester
 In trisomy 21 pregnancies
-free b-hCG is increased.
-level of PAPP-A in maternal blood is decreased.
 The higher the level of b-hCG and the lower the level
of PAPP-A the higher the risk for trisomy 21
Cystic Hygromas,Nuchal Edema & Nuchal
Translucency
 During the second and third trimesters of pregnancy,
abnormal accumulation of fluid behind the fetal neck
can be classified as nuchal cystic hygroma or nuchal
edema.
 In about 75% of fetuses with cystic hygromas, there is a
chromosomal abnormality and in about 95% of cases,
the abnormality is Turner syndrome.
 Edema is also associated with fetal cardiovascular and
pulmonary defects, skeletal dysplasias, congenital
infections and metabolic and hematological disorders.
 In the first trimester, the term translucency is used.
Nuchal Translucency
 Nuchal translucency is the sonographic appearance of
subcutaneous accumulation of fluid behind the fetal
neck in the first trimester of pregnancy.
 The term translucency is used, irrespective of whether
it is septated or not and whether it is confined to the
neck or envelopes the whole fetus.
 The incidence of chromosomal and other abnormalities
is related to the size, rather than the appearance of NT.
 During the second trimester, the translucency usually
resolves and in a few cases, it evolves into either nuchal
edema or cystic hygromas with or without generalized
hydrops.
Pathophysiology Of Increased Fetal NT
 Cardiac dysfunction.
 Venous congestion in the
head and neck.
 Altered composition of the
extracellular matrix.
 Failure of lymphatic drainage.
 Fetal anemia.
 Fetal hypoproteinemia.
 Fetal infection.
Measurement Of Nuchal Translucency
 The optimal gestational age for measurement of fetal NT is 11 weeks
to 13 weeks and 6 days.
 The minimum fetal crown–rump length should be 45 mm and the
maximum 84 mm.
 Only the fetal head and upper thorax should be included in the
image for measurement of NT.
 A good sagittal section of the fetus, as for measurement of fetal
crown–rump length.
 fetus in the neutral position. i.e.
 Hyperextended the measurement can be increased by 0.6 mm and
when the neck is flexed, the measurement can be decreased by 0.4
mm.
 The calipers should be placed on the lines that define the NT
thickness.
 Care must be taken to distinguish between fetal skin and amnion.
 More than one measurement must be taken and the maximum one
should be recorded
 Fetal NT increases with crown–rump length and
therefore it is essential to take gestation into
account when determining whether a given NT
thickness is increased.
 In a study involving 96,127 pregnancies, the
median and 95th centile at a crown-rump-length
of 45 mm were 1.2 and 2.1 mm and the respective
values at crown rump length of 84 mm were 1.9
and 2.7 mm (Snijders et al 1998).
Fetal NT And Maternal Serum Testing In
The First-trimester
b- HCG PAPP-A
Trisomy 21 Increased Decreased
Trisomy 18 Decreased Decreased
Trisomy 13 Normal Decreased
Absence Of Fetal Nasal Bone
 The fetal nasal bone can be visualized by sonography
at 11–13+6 weeks of gestation (Cicero et al 2001).
 Several studies have demonstrated a high association
between absent nasal bone at 11–13+6 weeks and
trisomy 21, as well as other chromosomal
abnormalities.
 In the image of the nose there should be three
distinct lines.
 The top line represents the skin and the bottom one,
which is thicker and more echogenic than the
overlying skin, represents the nasal bone. A third
line, almost in continuity with the skin, but at a
higher level, represents the tip of the nose.
Nasal Bone absent in –
60-70% Trisomy 21,
50% Trisomy 18,
30% Trisomy 13.
Crown–Rump Length
 Crown-rump length and chromosomal defects -
 Trisomy 18 and triploidy are associated with
moderately severe growth restriction.
 Trisomy 13 and Turner syndrome are associated with
mild growth restriction.
 In trisomy 21 growth is essentially normal.
Femur And Humerus Length
 Trisomy 21 is characterized by short stature and during
the second trimester the condition is associated with
relative shortening of the femur and more so the
humerus.
 At 11–13+6 weeks in trisomy 21 fetuses the median
femur and humerus lengths are significantly below
the appropriate normal median for crown-rump
length.
Single Umbilical Artery
 At 11–13+6 weeks single umbilical artery is found in
about 3% of chromosomally normal fetuses and in
80% of fetuses with Trisomy 18.
Megacystis
 Defined by a longitudinal bladder diameter of 7 mm or
more, is found in about 1 in 1,500 pregnancies.
 When the long bladder dia. is 7–15 mm the incidence of
chromosomal defects,mainly trisomies 13 and 18, is about
20%.
 In the chromosomally normal group there is
spontaneous resolution of the megacystis in about 90%
of cases
 Megacystis is associated with increased NT, which is
observed in about 75% of those with chromosomal
defects.
Exomphalos
 At 11–13+6 weeks the prevalence of exomphalos is about
1 in 1000.
 The incidence of chromosomal defects, mainly trisomy
18, is about 60%, compared to about 30% at mid-
gestation and 15% in neonates.
Ultrasound picture of a
12-weeks Trisomy 18
fetus with exomphalos
and increased nuchal
translucency thickness.
Choroid Plexus Cysts, Pyelectasis And Cardiac
Echogenic Foci
At 11–14 weeks the prevalences of
 Choroid plexus cysts - 2.2 %
 Pyelectasis - 0.9 %
 Cardiac echogenic foci - 0.6%
 The placental volume, determined at 11–13+6 by 3D
ultrasound, increases with fetal crown-rump length.
 In Trisomy 21 fetuses, placental volume is not significantly
different from normal but in Trisomy 18 placental volume is
substantially decreased.
Placental Volume
Fetal Heart Rate
 In normal pregnancy, the fetal heart rate (FHR)
increases from about 100 bpm at 5 weeks of
gestation to 170 bpm at 10 weeks and then
decreases to 155 bpm by 14 weeks.
Trisomy 21 Mild Tachycardia
Trisomy 13 Tachycardia
Trisomy 18 Bradycardia
Turner’s Syndrome Tachycardia
Doppler In The Ductus Venosus
 At 11–13+6 weeks abnormal
ductal flow is observed in
5% of chromosomally
normal fetuses and in about
80% of fetuses with trisomy
21.
 Assessment of the ductus
venosus can be combined
with measurement of fetal
NT to improve the
effectiveness of early
sonographic screening for
trisomy 21.
Flow velocity waveforms from
the fetal ductus venosus at 12
weeks’ gestation
demonstrating normal pattern
(top) and abnormal a-wave
(bottom).
Doppler In Other Vessels
 Uterine arteries- Uterine artery Doppler studies at 11–
13+6 weeks found no significant differences in pulsatility
index between chromosomally normal and abnormal
fetuses.
 Umbilical artery- not useful in screening for trisomy 21
but in trisomy 18, impedance to flow is increased.
 Umbilical vein- In second and third-trimester fetuses,
pulsatile umbilical venous flow is a late and ominous
sign of fetal compromise. At 11–13+6 weeks there is
pulsatile flow in about 25% of chromosomally normal
fetuses and in 90% of fetuses with trisomy 18 or 13 but
normal flow in trisomy 21.
Management Of Pregnancies With Increased NT
Fetal NT Below The 99th Centile (3.5 Mm)
 The parents can be reassured that the chances of
delivering a baby with no major abnormalities is about
97% for NT below the 95th centile and 93% for NT
between the 95th and 99th centiles.
 Best to carry out a detailed fetal scan at 20 weeks to
determine fetal growth and diagnose or exclude major
abnormalities.
Fetal NT Above The 99th Centile
 A fetal NT above 3.5 mm is found in about 1% of
pregnancies.
 The risk of major chromosomal defects is very high and
increases from about 20% for NT of 4.0 mm to 33% for
NT of 5.0 mm, 50% for NT of 6.0 mm and 65% for NT
of 6.5 mm or more.
 Consequently, the first line of management of such
pregnancies should be the offer of fetal karyotyping by
CVS.
Resolution of Increased NT
 In the chromosomally normal group, a detailed scan,
including fetal echocardiography, should be carried
out at 14–16 weeks to determine the evolution of the
NT and to diagnose or exclude many fetal defects.
Evolution To Nuchal Edema
 Persistence of unexplained increased NT at the 14–16
weeks scan or evolution to nuchal edema or hydrops
fetalis at 20–22 weeks, raise the possibility of congenital
infection or a genetic syndrome.
 Maternal blood should be tested for toxoplasmosis,
cytomegalovirus, and parvovirus B19.
 Follow-up scans to define the evolution of the edema
should be carried out every four weeks.
Multiple Pregnancy
 Multiple pregnancy results from the ovulation and
subsequent fertilisation of more than one oocyte -
genetically different (polyzygotic or non-identical)
 Also result from splitting of one embryonic mass to
form two or more genetically identical fetuses
(monozygotic).
 Twins account for about 1% of all pregnancies with
two-thirds being dizygotic and one-third
monozygotic.
Determination Of Zygosity And Chorionicity
 Zygosity can only be determined by DNA fingerprinting,
which requires amniocentesis, chorion villus sampling
or cordocentesis.
 Determination of chorionicity can be performed by
ultrasonography and relies on the assessment of fetal
gender, number of placentas, and characteristics of the
membrane between the two amniotic sacs.
 Different-sex twins are dizygotic and therefore
dichorionic.
 In about two-thirds of twin pregnancies the fetuses are
of the same sex and these may be either monozygotic or
dizygotic.
 If there are two separate placentas the pregnancy is
dichorionic.
 The best way to determine chorionicity is by an
ultrasound examination at 6–9 weeks of gestation.
Ultrasound appearance of monochorionic (left) and dichorionic (right)
twin pregnancies at 12 weeks of gestation. Note that in both types there
appears to be a single placental mass but in the dichorionic type there is
an extention of placental tissue into the base of the intertwin membrane
forming the lambda sign.
 Monochorionic Diamniotic (MCDA)
 One placenta
 Thin membrane
 ‘T’ shaped insertion
 Same sex
 One chorion, 2 amnions (visible early)
 Dichorionic Diamniotic (DCDA)
 One or two placentae
 ‘Twin peak’ or ‘Lambda’ sign
Chorionicity And Pregnancy Complications
 Miscarriage - In singleton pregnancies- rate of
subsequent miscarriage or fetal death before 24 weeks
is about 1%
 Rate of fetal loss in dichorionic twins is about 2% and
in monochorionic twins it is about 10%
 Perinatal mortality - In twins it is about 5-times
higher than in singletons.
 This increased mortality, which is mainly due to
prematurity-related complications, is higher in
monochorionic (5%) than dichorionic (2%) twin
pregnancies
 Early preterm delivery - The chance of spontaneous
delivery between 24 and 32 weeks is about 1% in
singletons, 5% in dichorionic and 10% in
monochorionic twin pregnancies.
 Growth restriction - In singleton pregnancies the
prevalence of babies with birth weight below the 5th
centile is 5%, in dichorionic twins it is about 20% and
in monochorionic twins it is 30%
 Pre-eclampsia - The prevalence of pre-eclampsia is
about 4-times greater in twin than in singleton
pregnancies.
Twin-to-twin transfusion syndrome –TTTS
 Anastomoses which allow communication of the two
fetoplacental circulations;
 May be A-A, A-V or V-V.
 The prevalence of increased NT thickness is about 30%
Twin Reversed Arterial Perfusion Sequence –
 The most extreme manifestation of twin-to-twin
transfusion syndrome, found in approximately 1% of
monozygotic twin pregnancies, is acardiac twinning.
 This twin disorder has been named Twin Reversed Arterial
Perfusion (TRAP) sequence.
 At least 50% of donor twins die due to congestive heart
failure or severe preterm delivery, due to polyhydramnios.
To Conclude…
 The 11-13+6 weeks scan along with consideration of
maternal age & serum biochemical markers can help
in early detection of various chromosomal
abnormalities in the fetus.
 It helps in timely evaluation of various fetal anomalies
& thus helps in appropriate counseling of the parents
for further management.
THANK YOU..!!

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11-13+6 weeks scan

  • 1. Dr. Tejas M. Tamhane. JRI
  • 2. Introduction  In 1866 Langdon Down noted that common characteristics of patients with trisomy 21 are skin deficient in elasticity, giving the appearance of being too large for the body and flat face with a small nose.  In the 1990s, it was realized that the excess skin of individuals with Down’s syndrome can be visualized by ultrasonography as increased nuchal translucency in the third month of intrauterine life.  Fetal nuchal translucency thickness at the 11–13+6 weeks scan has been combined with maternal age to provide an effective method of screening for Trisomy 21.
  • 3. Benefits Of The 11–13+6 Weeks Scan  Assessment of risk for trisomy 21 & other. chromosomal defects.  Major abnormalities of the heart and great arteries.  Confirmation-fetus is alive.  Accurate dating of the pregnancy.  Early diagnosis of major fetal abnormalities.  Detection of multiple pregnancies with reliable identification of chorionicity.
  • 4. Diagnosis Of Chromosomal Defects.  Non invasive diagnosis- Examination of fetal cells from maternal peripheral blood  Invasive diagnosis- 1. Amniocentesis- between 14-20weeks. 2. CVS- performed only after 11 weeks.  The risk of miscarriage from chorionic villus sampling in the first trimester is the same as for amniocentesis in the second trimester.
  • 6.
  • 10. Nasal Bone And Other First-trimester Sonographic Markers  At 11–13+6 weeks the nasal bone is not visible by ultrasonography in about 60–70% of fetuses with Trisomy 21 and in about 2% of chromosomally normal fetuses.  Abnormalities in the flow velocity waveform from the ductus venosus are observed in about 80% of fetuses with trisomy 21.
  • 11. Maternal Serum Biochemistry In The First-trimester  In trisomy 21 pregnancies -free b-hCG is increased. -level of PAPP-A in maternal blood is decreased.  The higher the level of b-hCG and the lower the level of PAPP-A the higher the risk for trisomy 21
  • 12. Cystic Hygromas,Nuchal Edema & Nuchal Translucency  During the second and third trimesters of pregnancy, abnormal accumulation of fluid behind the fetal neck can be classified as nuchal cystic hygroma or nuchal edema.  In about 75% of fetuses with cystic hygromas, there is a chromosomal abnormality and in about 95% of cases, the abnormality is Turner syndrome.  Edema is also associated with fetal cardiovascular and pulmonary defects, skeletal dysplasias, congenital infections and metabolic and hematological disorders.  In the first trimester, the term translucency is used.
  • 13. Nuchal Translucency  Nuchal translucency is the sonographic appearance of subcutaneous accumulation of fluid behind the fetal neck in the first trimester of pregnancy.  The term translucency is used, irrespective of whether it is septated or not and whether it is confined to the neck or envelopes the whole fetus.  The incidence of chromosomal and other abnormalities is related to the size, rather than the appearance of NT.  During the second trimester, the translucency usually resolves and in a few cases, it evolves into either nuchal edema or cystic hygromas with or without generalized hydrops.
  • 14. Pathophysiology Of Increased Fetal NT  Cardiac dysfunction.  Venous congestion in the head and neck.  Altered composition of the extracellular matrix.  Failure of lymphatic drainage.  Fetal anemia.  Fetal hypoproteinemia.  Fetal infection.
  • 15. Measurement Of Nuchal Translucency  The optimal gestational age for measurement of fetal NT is 11 weeks to 13 weeks and 6 days.  The minimum fetal crown–rump length should be 45 mm and the maximum 84 mm.  Only the fetal head and upper thorax should be included in the image for measurement of NT.  A good sagittal section of the fetus, as for measurement of fetal crown–rump length.  fetus in the neutral position. i.e.  Hyperextended the measurement can be increased by 0.6 mm and when the neck is flexed, the measurement can be decreased by 0.4 mm.  The calipers should be placed on the lines that define the NT thickness.  Care must be taken to distinguish between fetal skin and amnion.  More than one measurement must be taken and the maximum one should be recorded
  • 16.
  • 17.  Fetal NT increases with crown–rump length and therefore it is essential to take gestation into account when determining whether a given NT thickness is increased.  In a study involving 96,127 pregnancies, the median and 95th centile at a crown-rump-length of 45 mm were 1.2 and 2.1 mm and the respective values at crown rump length of 84 mm were 1.9 and 2.7 mm (Snijders et al 1998).
  • 18. Fetal NT And Maternal Serum Testing In The First-trimester b- HCG PAPP-A Trisomy 21 Increased Decreased Trisomy 18 Decreased Decreased Trisomy 13 Normal Decreased
  • 19. Absence Of Fetal Nasal Bone  The fetal nasal bone can be visualized by sonography at 11–13+6 weeks of gestation (Cicero et al 2001).  Several studies have demonstrated a high association between absent nasal bone at 11–13+6 weeks and trisomy 21, as well as other chromosomal abnormalities.
  • 20.  In the image of the nose there should be three distinct lines.  The top line represents the skin and the bottom one, which is thicker and more echogenic than the overlying skin, represents the nasal bone. A third line, almost in continuity with the skin, but at a higher level, represents the tip of the nose. Nasal Bone absent in – 60-70% Trisomy 21, 50% Trisomy 18, 30% Trisomy 13.
  • 21. Crown–Rump Length  Crown-rump length and chromosomal defects -  Trisomy 18 and triploidy are associated with moderately severe growth restriction.  Trisomy 13 and Turner syndrome are associated with mild growth restriction.  In trisomy 21 growth is essentially normal.
  • 22. Femur And Humerus Length  Trisomy 21 is characterized by short stature and during the second trimester the condition is associated with relative shortening of the femur and more so the humerus.  At 11–13+6 weeks in trisomy 21 fetuses the median femur and humerus lengths are significantly below the appropriate normal median for crown-rump length.
  • 23. Single Umbilical Artery  At 11–13+6 weeks single umbilical artery is found in about 3% of chromosomally normal fetuses and in 80% of fetuses with Trisomy 18.
  • 24. Megacystis  Defined by a longitudinal bladder diameter of 7 mm or more, is found in about 1 in 1,500 pregnancies.  When the long bladder dia. is 7–15 mm the incidence of chromosomal defects,mainly trisomies 13 and 18, is about 20%.  In the chromosomally normal group there is spontaneous resolution of the megacystis in about 90% of cases  Megacystis is associated with increased NT, which is observed in about 75% of those with chromosomal defects.
  • 25. Exomphalos  At 11–13+6 weeks the prevalence of exomphalos is about 1 in 1000.  The incidence of chromosomal defects, mainly trisomy 18, is about 60%, compared to about 30% at mid- gestation and 15% in neonates. Ultrasound picture of a 12-weeks Trisomy 18 fetus with exomphalos and increased nuchal translucency thickness.
  • 26. Choroid Plexus Cysts, Pyelectasis And Cardiac Echogenic Foci At 11–14 weeks the prevalences of  Choroid plexus cysts - 2.2 %  Pyelectasis - 0.9 %  Cardiac echogenic foci - 0.6%  The placental volume, determined at 11–13+6 by 3D ultrasound, increases with fetal crown-rump length.  In Trisomy 21 fetuses, placental volume is not significantly different from normal but in Trisomy 18 placental volume is substantially decreased. Placental Volume
  • 27. Fetal Heart Rate  In normal pregnancy, the fetal heart rate (FHR) increases from about 100 bpm at 5 weeks of gestation to 170 bpm at 10 weeks and then decreases to 155 bpm by 14 weeks. Trisomy 21 Mild Tachycardia Trisomy 13 Tachycardia Trisomy 18 Bradycardia Turner’s Syndrome Tachycardia
  • 28. Doppler In The Ductus Venosus  At 11–13+6 weeks abnormal ductal flow is observed in 5% of chromosomally normal fetuses and in about 80% of fetuses with trisomy 21.  Assessment of the ductus venosus can be combined with measurement of fetal NT to improve the effectiveness of early sonographic screening for trisomy 21. Flow velocity waveforms from the fetal ductus venosus at 12 weeks’ gestation demonstrating normal pattern (top) and abnormal a-wave (bottom).
  • 29. Doppler In Other Vessels  Uterine arteries- Uterine artery Doppler studies at 11– 13+6 weeks found no significant differences in pulsatility index between chromosomally normal and abnormal fetuses.  Umbilical artery- not useful in screening for trisomy 21 but in trisomy 18, impedance to flow is increased.  Umbilical vein- In second and third-trimester fetuses, pulsatile umbilical venous flow is a late and ominous sign of fetal compromise. At 11–13+6 weeks there is pulsatile flow in about 25% of chromosomally normal fetuses and in 90% of fetuses with trisomy 18 or 13 but normal flow in trisomy 21.
  • 30. Management Of Pregnancies With Increased NT
  • 31. Fetal NT Below The 99th Centile (3.5 Mm)  The parents can be reassured that the chances of delivering a baby with no major abnormalities is about 97% for NT below the 95th centile and 93% for NT between the 95th and 99th centiles.  Best to carry out a detailed fetal scan at 20 weeks to determine fetal growth and diagnose or exclude major abnormalities.
  • 32. Fetal NT Above The 99th Centile  A fetal NT above 3.5 mm is found in about 1% of pregnancies.  The risk of major chromosomal defects is very high and increases from about 20% for NT of 4.0 mm to 33% for NT of 5.0 mm, 50% for NT of 6.0 mm and 65% for NT of 6.5 mm or more.  Consequently, the first line of management of such pregnancies should be the offer of fetal karyotyping by CVS.
  • 33. Resolution of Increased NT  In the chromosomally normal group, a detailed scan, including fetal echocardiography, should be carried out at 14–16 weeks to determine the evolution of the NT and to diagnose or exclude many fetal defects.
  • 34. Evolution To Nuchal Edema  Persistence of unexplained increased NT at the 14–16 weeks scan or evolution to nuchal edema or hydrops fetalis at 20–22 weeks, raise the possibility of congenital infection or a genetic syndrome.  Maternal blood should be tested for toxoplasmosis, cytomegalovirus, and parvovirus B19.  Follow-up scans to define the evolution of the edema should be carried out every four weeks.
  • 35. Multiple Pregnancy  Multiple pregnancy results from the ovulation and subsequent fertilisation of more than one oocyte - genetically different (polyzygotic or non-identical)  Also result from splitting of one embryonic mass to form two or more genetically identical fetuses (monozygotic).  Twins account for about 1% of all pregnancies with two-thirds being dizygotic and one-third monozygotic.
  • 36.
  • 37.
  • 38. Determination Of Zygosity And Chorionicity  Zygosity can only be determined by DNA fingerprinting, which requires amniocentesis, chorion villus sampling or cordocentesis.  Determination of chorionicity can be performed by ultrasonography and relies on the assessment of fetal gender, number of placentas, and characteristics of the membrane between the two amniotic sacs.  Different-sex twins are dizygotic and therefore dichorionic.  In about two-thirds of twin pregnancies the fetuses are of the same sex and these may be either monozygotic or dizygotic.
  • 39.  If there are two separate placentas the pregnancy is dichorionic.  The best way to determine chorionicity is by an ultrasound examination at 6–9 weeks of gestation. Ultrasound appearance of monochorionic (left) and dichorionic (right) twin pregnancies at 12 weeks of gestation. Note that in both types there appears to be a single placental mass but in the dichorionic type there is an extention of placental tissue into the base of the intertwin membrane forming the lambda sign.
  • 40.  Monochorionic Diamniotic (MCDA)  One placenta  Thin membrane  ‘T’ shaped insertion  Same sex  One chorion, 2 amnions (visible early)  Dichorionic Diamniotic (DCDA)  One or two placentae  ‘Twin peak’ or ‘Lambda’ sign
  • 41.
  • 42.
  • 43.
  • 44.
  • 45. Chorionicity And Pregnancy Complications  Miscarriage - In singleton pregnancies- rate of subsequent miscarriage or fetal death before 24 weeks is about 1%  Rate of fetal loss in dichorionic twins is about 2% and in monochorionic twins it is about 10%  Perinatal mortality - In twins it is about 5-times higher than in singletons.  This increased mortality, which is mainly due to prematurity-related complications, is higher in monochorionic (5%) than dichorionic (2%) twin pregnancies
  • 46.  Early preterm delivery - The chance of spontaneous delivery between 24 and 32 weeks is about 1% in singletons, 5% in dichorionic and 10% in monochorionic twin pregnancies.  Growth restriction - In singleton pregnancies the prevalence of babies with birth weight below the 5th centile is 5%, in dichorionic twins it is about 20% and in monochorionic twins it is 30%  Pre-eclampsia - The prevalence of pre-eclampsia is about 4-times greater in twin than in singleton pregnancies.
  • 47. Twin-to-twin transfusion syndrome –TTTS  Anastomoses which allow communication of the two fetoplacental circulations;  May be A-A, A-V or V-V.  The prevalence of increased NT thickness is about 30%
  • 48. Twin Reversed Arterial Perfusion Sequence –  The most extreme manifestation of twin-to-twin transfusion syndrome, found in approximately 1% of monozygotic twin pregnancies, is acardiac twinning.  This twin disorder has been named Twin Reversed Arterial Perfusion (TRAP) sequence.  At least 50% of donor twins die due to congestive heart failure or severe preterm delivery, due to polyhydramnios.
  • 49. To Conclude…  The 11-13+6 weeks scan along with consideration of maternal age & serum biochemical markers can help in early detection of various chromosomal abnormalities in the fetus.  It helps in timely evaluation of various fetal anomalies & thus helps in appropriate counseling of the parents for further management.