What we are going to review today: Imprinting Beckwith-Weidman
Syndrome Angelman Syndrome Prader-Willi Syndrome 3 DNA Methylation
Beckwith-Wiedemann syndrome 4 DNA Methylation Beckwith-Wiedemann
syndrome Above average birth weight Increase growth after birth
(>95% growth curve) Enlarged organs Hypoglycemic following birth
Increase risk of cancers Imprinting defect located at 11p15.5 5
Beckwith-Wiedemann syndrome Genetic causes of BWS: Maternal DMR
hypermethylation UPD Remainder unknown 6 The Journal of Pathology
Volume 211, Issue 3, pages , 18 DEC 2006 DOI: /path Volume 211,
Issue 3, The Journal of Pathology Volume 211, Issue 3, pages , 18
DEC 2006 DOI: /path Volume 211, Issue 3, 9 Genes Dev. Vol. 11, No.
23, pp , December 1, 1997 Mouse mutant embryos overexpressing
IGF-II exhibit phenotypic features of the Beckwith-Wiedemann and
Simpson-Golabi- Behmel syndromes Jonathan Eggenschwiler,1 Thomas
Ludwig,2 Peter Fisher,3 Philip A. Leighton,4,5 Shirley M.
Tilghman,4 and Argiris Efstratiadis1,656 14 Prader-Willi and
Angelman Syndrome Prader-WilliAngelman Mild mental
retardationSevere impairment and loss of speech endocrine
abnormalitiesseizures and ataxia temper tantrumsunprovoked laughter
Obesityhyperactivity 1 in 15,000 15 Prader-Willi and Angelman
Syndrome Angelman syndrome UBE3A Paternally imprinted Prader-Willi
syndrome Maternally imprinted genes 15q11-13 16 Prader-Willi and
Angelman Syndrome UBE3A is paternally silenced This primarily
occurs in brain, other tissues show biallelic expression 17
Prader-Willi and Angelman Syndrome What happens in each
pathologies? If the maternal copy of chromosome 15 is missing, then
genes normally expressed from this parental origin are not
expressed Consequences 21 Prader-Willi and Angelman Syndrome If
paternal chromosome 15 is missing, then only the maternally
expressed proteins are made Consequence: UBE3A is ok, but other
genes in the region are not expressedPrader-Willi syndrome 22
Prader-Willi and Angelman Syndrome Thus, two different diseases
based on the cells memory of methylation alter the memory, alter
the phenotype 23 Prader-Willi and Angelman Syndrome How do you lose
chromosome 15? Microdeletion of 15q11-13 on one chromsome 70%
Single gene mutation 15% of AS Defect in imprinting centre (IC) 5%
Uniparental Disomy 30% of PWS, 5% AS 24 Prader-Willi and Angelman
Syndrome 25 Uniparental Disomy Receive two chromosomes from one
parent Eg. Paternal disomy both of chromosome 15 are from father,
thus both have silenced UBE3A 26 Uniparental Disomy How does it
happen? Trisomic Rescue - majority Monosomic Duplication 27 Meiosis
I 28 Meiosis II 29 Meiosis I Non-disjunction 30 Meiosis I
Non-disjunction Fertilization Trisomy Meiosis I non-disjunction
always creates a problem 31 Meiosis II Non-disjunction
Fertilization Trisomy Normal 2/3 gametes following Meiosis II
non-disjunction are normal 32 Trisomy Trisomy for most autosomal
chromosomes is lethal BIG exception: Trisomy 21, smallest autosomal
chromosome, fewest genes, not lethal Under rare conditions, some
autosomal trisomies can escape Trisomic Rescue 33 Trisomic Rescue
following Meiosis I Non-disjunction Two copies of homologous, but
not identical, chromosomes + Maternal Paternal M,M 1/3 M,P 1/3 M,P
1/3 Anaphase lag 34 Trisomic Rescue following Meiosis II
Non-disjunction + M,M 1/3 M,P 2/3 Two copies of identical
chromosomes Anaphase lag 35 Uniparental Disomy How does it happen?
Trisomic Rescue - majority Monosomic Duplication 36 Monosomic
Duplication + P,P Two identical copies of paternal chromosome -
isodisomy 37 Parental Origin Determines Phenotype Prader-Willi
Syndrome M,M { 15 M,M Prader-Willi Syndrome P,P Angelman Syndrome
38 Prader-Willi and Angelman syndrome Non-disjunction is more
common in Meiosis I in females In human females, Meiosis I starts
before birth but is arrested at diplotene stage (late prophase I)
Oocytes sit like this for decades Complete meiosis II once each
month While arrested at the diplotene stage, the tetrad chromosomes
are held together by chiasmata (formed during recombination) If a
pair of chromosomes dont undergo recombination, the lack of
chiasmata can contribute to non-disjunction Uniparental Disomy 30%
of PWS, 5% AS Maternal non-disjunction and trisomic rescue leading
to the pair of maternal chromosomes 39 Uniparental Disomy and Human
Disease Eric Engel. Some lessons from uniparental disomy (UPD) in
the framework of contemporary cytogenetics and molecular biology.
Atlas Genet Cytogenet Oncol Haematol. December 2003. 40 Trisomic
rescue of Meiosis II non- disjunction can have other problems
Anaphase lag { Pair of identical chromosomes (isochromosomes) 41
Uniparental disomy as a mechanism for human genetic disease. Spence
JE, Perciaccante RG, Greig GM, Willard HF, Ledbetter DH, Hejtmancik
JF, Pollack MS, O'Brien WE, Beaudet AL. Am J Hum Genet Feb;42(2):
CFTR -/+ CFTR +/+ CFTR -/- { Pair of identical Chromosome 7
Harboring CFTR mutation Uniparental isodisomy and reduction to
homozygosity
