Transcript Document
Susceptibility of Genomic Imprinting to ART
Mellissa Mann
Children’s Health Research Institute
Department of Obstetrics & Gynecology, and Biochemistry
University of Western Ontario
Infertility and Assisted Reproductive Technologies
35-70 million couples involuntarily infertile
1 in 6 people of reproductive age
ART
1-2% children born by ART
Children conceived via ARTs are at increased risk
Intrauterine growth retardation
Premature birth
Low birth weight
Possibly genetic disorders
ART-induced perturbations in the mouse
Reduced viability
Intrauterine growth retardation
Developmental abnormalities
Deviation in behaviour
Developmental abnormalities in in vitro produced
livestock
Large Offspring Syndrome
•Increased prenatal loss
•Large placentas
•Large fetuses
•Polyhydramnios
•Parturition problems
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•
•
•
•
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Higher perinatal mortality
Breathing difficulties
Reluctance to suckle
Skeletal anomalies
Large organs
Cerebellar dysplasia
Epigenetics: Heritable alterations in gene activity
without a change in DNA sequence
Duke University Medical Center
Skinny and Brown
Obese and Yellow
Epigenetics: Mediator of Environment, Development,
and Disease
Nutrition
Vitamins
Drugs
Estrogen
Disruptors
Herbicides
Pesticides
Epigenetics
Reproductive
Disorders
Cardiovascular
Disorders
Neurological
Disorders
Pathology
Growth
Disorders
Pediatric
Disorders
Lupus
Imprinting
Disorders
Cancer
Genomic Imprinting
The unequal expression of the maternal and
paternal alleles of a gene
Maternal allele
Paternal allele
Paternal allele
Maternal allele
Imprinted or marked
with their gametic-origin
Mouse/Human Imprinted Domains
Mouse Distal 7/
Human 11p15.5
Slc22a1l
Kcnq1
Cd81
IC
Nap1l4 Tssc3
Cdkn1c
IC
Ascl2 Th
Kcnq1ot1
Ins2 Igf2
H19
Beckwith-Wiedemann Syndrome
Critical Region 1
Mouse Central 7/
Human 15q11-13
Magel2 Ndn
Snurf Snrpn
Ipw snoRNA Genes
Ube3A
Atp10c
IC
Frat3 Mkrn3
IC Antisense
Prader-Willi Syndrome
IC
Angelman Syndrome
Non-coding RNA
Methylation changes during mouse preimplantation
development
Methylated imprinted allele
Paternal
Genome
Unmethylated imprinted allele
Maternal
Genome
Are genomic imprints maintained in preimplantation
embryos after in vitro culture?
B6(CAST7) mice for use in allelic analyses
B6(CAST7)
Peg3
Chromosome 7
CAST
Snrpn
F1
X
CAST
B6
B6
H19
B6
Kcnq1ot1
In vitro preimplantation culture regimes
Trophectoderm
ICM
Whitten’s
KSOMaa
2-cell
Blastocyst
Loss of H19 imprinted expression occurs in a subset of individual
blastocysts after culture in Whitten’s medium
100
100
100
808080
60
6060
40
4040
20
20200
00
6%
p=0.006
1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17
100
100
100
80
80
80
60
60
60
40
40
40
20
20
20 0
00
14%
p=0.002
1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21
100
80
60
1 00
80
60
63%
40
20
40
20
0
0
1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 27 28 29 30 31 32 33 34 35 36 37 38
Blastocyst
Loss of imprinting occurred during
preimplantation development in culture,
indicating that mechanisms that operate to
maintain imprinting were disrupted.
What are the long-term effects of
preimplantation development in culture?
Cultured Blastocysts
Recipient Mothers
Postimplantation embryos recovered at 9.5 days of pregnancy after
preimplantation culture in Whitten’s medium.
100%
81%
80%
60%
40%
20%
32%
30%
8%
10%
11%
3%
3%
14%
5%
0%
Empt y
Severely
Abnormal
Abnormal
Controls
Whitt en's
Delayed
Normal
Loss of imprinted expression occurs primarily in day 9.5 placentas
after preimplantation culture
100
100
80
60
H19
80
60
40
20
0
40
20
0
100
100
80
60
60
Ascl2
80
40
40
20
20
0
0
100
Snrpn
100
80
80
60
60
40
40
20
20
0
0
100
100
80
Peg3
80
60
60
40
20
40
20
0
0
Vivo
KSOMaa
Whitten’s
Embryo
Vivo
KSOMaa
Whitten’s
Placenta
Loss of imprinted expression occurs primarily in day 9.5 placentas
after preimplantation culture
100
13
H19
80
75
60
100
100
92
100
87
40
20
25
8
0
100
Ascl2
80
75
60
92
100
40
20
25
8
0
100
8
12
Snrpn
80
45
60
100
100
40
92
100
88
55
20
0
100
16
37
Peg3
80
27
60
100
100
40
100
83
63
73
20
0
V
K
Embryo
W
V
K
W
Placenta
Perturbations in imprinting persist long after
embryos have been removed from culture.
Loss of imprinting occurs more frequently in
extraembryonic than embryonic lineages
Preimplantation
Culture
Placenta
Trophectoderm
ICM
Proximity to culture?
ICM vs TE?
Less redundancy?
Blastocyst
Embryo
Day 9.5
ART children diagnosed with imprinting disorders
Angelman Syndrome
OR
X
Loss of
Normal
maternal
methylation
OR
X
Biparental origin
Beckwith-Wiedemann Syndrome
X
OR
X
Biparental origin
OR
Loss of
maternal
methylation
Sporadic imprinting defects may arise during
ART procedures
Assisted Reproductive Technologies
PGC
Oocyte
maturation
Humans
Superovulation
+/- GnRH treatment
Oocyte retrieval
IVF/ICSI
In vitro culture
Mice
Superovulation
In vitro culture
Future Studies
Assisted Reproductive Technologies
PGC
Oocyte
maturation
Mice Superovulation
1
In vitro culture
2,3
4,5
1. Do imprinting defects result from superovulation?
2. When is imprinting lost during preimplantation development in culture?
3. Does loss of imprinting occur in mouse embryos cultured in media used in
human assisted reproduction?
4. Is loss of imprinting tissue-specific?
5. What are the long-term affects of preimplantation culture on genomic imprinting
and development?
1. Determine whether superovulation contributes to
loss of imprinting
Preantral
Early antral
Preovulatory
Extraovarian Sensitivity
Imprint Acquisition
Spontaneous vs Induced Ovulation
2. Determine when imprint maintenance is lost during
preimplantation development in culture.
In vitro culture
Examine imprinting of H19, Snrpn, Kcnq1ot1, Peg3
3. Does loss of imprinting occur in mouse embryos cultured in
media used in human assisted reproduction?
Trophectoderm
ICM
Global
HTF
H19
Snrpn
Peg3
Kncq1ot1
One Step
Two Step
2-cell
G1.2/G2.2
H19
Snrpn
Peg3
Kncq1ot1
P-1/Bl +SSS
Blastocyst
4. Determine how disruptions lead to the selective loss
of imprinting in the placenta
Left horn
Right horn
In Vivo
derived
Whitten’s
Right horn
Day 5.5
Day 6.5
Day 7.5
Day 8.5
Examine imprinting of H19, Snrpn, Kcnq1ot1, Peg3
5. Determine the long-term affects of preimplantation
culture on genomic imprinting and development
Left horn
Whitten’s
Ultrasound biomicroscopy
Day 9.5, Day 13.5, Day 17.5
Right horn
In Vivo
derived
Ultrasound biomicroscopy at Day 9.5-10.5 of gestation
Growth and Viability
U
U
Crown-rump
length
E
D
D
P
Resorption
U
U
D
NT
NT
P
E
D
Variable embryonic growth
Calcium hydroxyapatite deposits
Ultrasound biomicroscopy at Day 13.5 of gestation
Beckwith-Wiedemann Syndrome
Macrosomia
Visceromegaly (liver, heart)
Macroglossia ( tongue)
Liver
Limb
Abdominal wall defects
Polydactyly (limb)
Cardiac defects (heart)
Adrenal defects
Lens defects (eye)
Vertebral defects
Hemihypertrophy
Heart
Polyhydramnios
Placentomegaly/Placental hydrops
Tongue
Eye
Acknowledgements
University of Pennsylvania
Marisa Bartolomei
Richard Schultz
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Michael Golding
Anne Pin
Liyue Zhang
Sarah Lalone
Julia Foster
Brenna Market
Lauren Magri
Michelle Gabriel
Morgan McWilliam
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