DIFFERENCES FROM MENDELIAN

Question 1

EXPLAIN IMPRINTING

Answer 1

– it is a genetic phenomenon, where the level of gene expression depends on
whether it was inherited from mother or father
-genes transcribed only from 1 allele of 1 parent and the other is inactive and silent (imprinted)

Question 2

WHAT ARE IMPRINTED GENES NEEDED FOR?

Answer 2

are genes which are needed at the beginning of development (embryonic development,
regulation of cell proliferation), however only one active allele must be present, not two, one needs to be inactive
-functionally haploid

Question 3

IS THE MECHANISM OF IMPRINTING LETHAL?

Answer 3

As the mechanism of inactivation is methylation during gamete formation, it is an epigenetic inheritance and an epigenetic mechanism of gene expression regulation (this means errors or mutation in this process are pathological)

Question 4

GIVE AN EXAMPLE OF IMPRINTING IN HUMANS

Answer 4

beginning of embryonic development imprinted gene which prefer paternal genes, help form the placenta (trophoblast). Imprinted genes which prefer maternal genes help in the development of embryo

Question 5

EXPLAIN PRADER WILLI SYNDROME

Answer 5

symptoms include: obesity, small stature, hypogonadism and mental retardation
-caused by the absence of PWS genes, which are inherited from father (mothers are imprinted = inactive)
-genes for PWS and AS are on long arms of chromosome 15, right next to each other
- if there is deletion or faulty inactivation of PWS genes during spermatogenesis à child will suffer with PWS
-if PWS genes were lost or inactivated during spermatogenesis and during oogenesis these genes were not
methylated (not inactivated- remained active) à if these two defects would occur and these defected gametes would from a zygote – child would remain healthy

Question 6

EXPLAIN ANGELMAN SYNDROME

Answer 6

symptoms include: dysmorphic features, problems with sleep, slim figure, mental retardation and uncontrolled
inappropriate laughter
-caused by the absence of AS genes, which are inherited from mother (fathers are imprinted = inactivated)
-genes for PWS and AS are on long arms of chromosome 15, right next to each other
-if there is deletion or faulty inactivation of AS genes during oogenesis à will suffer with AS

Question 7

EXPLAIN BECKWITH WIEDMANN SYNDROME

Answer 7

also, known as EMG syndrome (Exomphalos-Macroglossia-Gigantism)
-symptoms may include abdominal wall defects, macroglossia, gigantism, enlargement of organs, neonatal hypoglycaemia and increased risk of tumours – e.g. Wilms tumour
- Reciprocally imprinted genes are next to teach other on 11p15 IGF2 (expression of paternal allele) and H19 (expression
of maternal allele)
- Same problem as in PWS and AS -> duplication, deletion, uniparental disomy (UDP), translocation or faulty imprinting
can lead to a different state than the normal physiological one (1 active allele IGF2 and 1 active allele H19) and every abnormality of this type causes Beckwith-Wiedmann syndrome

Question 8

EXPLAIN PROTO ONCOGENES

Answer 8

for expression need both alleles active, if one allele is imprinted, the whole gene is disabled
-> if an inactive allele becomes demethylated (loss of imprinting), the proto-oncogene is turned into an oncogene and tumor form

Question 9

EXPLAIN TUMOR SUPPRESSOR GENES

Answer 9

if accidental imprinting of one tumor suppressor gene occurs, the loss of the second healthy allele will cause tumor development
-> imprinting of tumor suppressor genes means high predisposition to tumors

EG: WT1 (11p13)
-> IGF2R (6q26) – gene of receptor for IGF2 (insulin-like growth factor 2), marks IGF2 for degradation, however if there is no receptor, IGF2 is not degraded and cell continues to receive signals to grow
- methylation is however reversible - methylation and demethylation is studied as one of the possible cures in cancers

Question 10

EXPLAIN WILMS TUMOR

Answer 10

malignant tumour of kidneys/kidneys of small children (max. 3 years old)
- locus 11p13 – associated with WAGR
o WAGR = genetic syndrome, predisposition for Wilms tumour, Aniridia (absence of iris), Genital anomalies and
mental Retardation
o WT1 – tumour suppressor gene, if imprinting occurs – predisposition to tumours
- locus 11p15 – associated with BWS -> high no. copies of growth gene IGF2
o gene IGF2 (from father) codes for IGF2 (insulin-like growth factor 2), if there are more genes -> more IGF2 ->
more growth -> BWS
o deletion or translocation of maternal alleles H19 causes activation of maternal allele IGF2 -> more growth -> BWS

Question 11

WHICH MECHAMISM DOES IMPRINTING USUALLY OCCUR THROUGH?

Answer 11

imprinting occurs mainly through methylation, but acetylation of histones also plays a role, as well as any process
which causes the reconstruction of chromatin into inactive state

Question 12

IS IMPRINTING A REVERSIBLE PROCESS?

Answer 12

imprinting is reversible and reprogrammed in gametogenesis

Question 13

HOW CAN IMPRINTING BE A MECHANISM FOR REGULATING GENE EXPRESSION?

Answer 13

play a role in the regulation of growth, cell proliferation and differentiation, code for growth factors, receptors of growth factors, regulatory proteins, transcription factors, proteins involved in splicing

Question 14

EXPLAIN THE POLYMORPHISM OF IMPRINTING

Answer 14

some people have monoallelic expression of genes, but the vast majority has biallelic expression

Question 15

WHAT IS UNIPARENTAL DISOMY?

Answer 15

inheritance of 2 homologous chromosomes from one parent
-results of UPD - abnormality in the case that chromosomes contain imprinted genes

Question 16

EXPLAIN THE EVIDENCE FOR UNIPARENTAL DISOMY

Answer 16

inheritance of haemophilia from father to son (zygote XXY and loss of maternal X chromosome)
- maternal UPD in PWS / paternal UPD in AS (increased age of parents)
- placental mosaic trisomy 15 in CVS (chorionic villus sampling)
- transfer of balanced translocation 22/22 in balanced form onto child and zygotic loss of free 22
- presence of homozygotic inversion on chromosome 4 in daughter of a mother who is a heterozygote for this inversion

Question 17

WHAT ARE THE MECHANISMS OF UPD ORIGIN?

Answer 17

loss of chromosome in trisomic gamete
- gametic complementation – fertilization between nullisomic and disomic gametes
- duplication of single chromosome in monosomic gamete
- postzygotic nondisjunction and duplication or mitotic recombination

Question 18

FRAGILE X

Answer 18

-formed by time, not spontaneously
-triple repeats
-mutation in promotor for gene FMR1 (Fragile X Mental Retardation 1) on X chromosome, most commonly increased
number of CGG trinucleotides in 5’ promoter region FMR1
o cause of mutation – instability of specific microsatellite repeats
- FMR1 gene contains 5-44 CGG trinucleotide repeats in healthy individuals, 45-54 repeats are grey zone, 55-200 is
premutation allele (unstable state individuals with FXS have full mutation of FMR1 gene with more than 200 repeats
- With this number of repeats the promotor becomes methylated and FMR1 gene is not transcribed and there is no
product, which plays a role in the development of brain à mental retardation
- Due to the fact that the inheritance is linked with the X chromosome it is inherited via the maternal line and fathers do
not give this disorder to their sons
- symptoms – mental retardation, prolonged face, large ears, large variety
-the more repeats of CGG, the stronger the symptoms and the more serious the disease
- 30 % of women carriers suffer mental retardation, 20 % of men with FXS are NOT mentally retarded (no one knows why)
- gradual origin of mutation – normal number of copies-> premutation -> full mutation!
- other CGG can be added during oogenesis and/or in early development (can also be a mosaic)

Question 19

WHAT CAN THE AMPLIFICATION IN NON CODING REGIONS RESULT IN?

Answer 19

usually loss of function or abnormal splicing
o Fragile X syndrome (CGG) – in promotor, myotonic dystrophy (CTG) – in introns, Fredrich ataxia (GAA) – in introns

Question 20

WHAT CAN THE AMPLIFICATION IN AN EXON RESULT IN?

Answer 20

usually CAG (glutamine) leads to abnormal protein (Polyglutamine disorders)
-> Huntington disease - abnormal protein huntingtin and inactivation of associated proteins
-progressive neurodegenerative disease, manifestation of disease at around 35 years of age – usually after reproduction and sooner if carried by father (this will be in the statements)
-> Spinocerebral ataxia - neuromuscular disorder, retinal degeneration

Question 21

EXPLAIN THE SPECIFITIES OF DYNAMIC MUTATIONS

Answer 21

homogeneity – there are no more alleles à allelic heterogeneity does not exist
- somatic variability – different number of copies in different tissues
- effect of parental origin on the manifestation of disease – degree of severity of disease, age of manifestation of disease
- does not obey Mendel’s inheritance - expressivity, penetrance
- there is no new mutation – formation is gradual through premutations – familiar diseases
- expressivity is linked with the number of copies - amplification = repeat of triplet; determined in gametogenesis occurs
postzygotically on chromosome of a specific parental origin
- anticipation – worsening clinical symptoms from generation to generation
- postzygotic origin of amplification on maternal chromosome – determined in oogenesis

Question 22

WHAT DO ABNORMALITIES IN IMPRINTING RESULT IN?

Answer 22

partial mole = additional paternal set of chromosomes -> hyperplasia of trophoblast
hypotrophic placenta = additional maternal set of chromosomes
ovarian teratoma = division of ovum without fertilization
complete mole = division of male pronucleus only

Question 23

DYNAMIC MUTATIONS