Structural Chromosomal Abnormalities Flashcards

Question 1

Q

Visualizing structural abnormalities -

Answer

A

cytogenetics if >5mb

FISH or chromosomal microarray if smaller

Question 2

Q

What kind of DNA damage is required for rearrangements?

Answer

A

Double strand breaks

Question 3

Q

Balance chromosomal aberrations

Answer

A

Normal complement of chromosomal material

e.g. reciprocal translocations
Robertsonian translocations
Inversions

Question 4

Q

Are Robertsonian translcations balanced?

Question 5

Q

Unbalanced chromosomal aberrations
Results in?
Examples?

Answer

A

Results in abnormal chromosomal content
Deletions
duplications
isochromosomes
Marker (Ring) chromosomes
recombinant chromosomes

Question 6

Q

Why are rearrangement common during meiosis?

Answer

A

because DSBs are required

Question 7

Q

Where do most breakpoints occur?

Answer

A

Regions in which repeated sequences are prevalent

Question 8

Q

Individuals with these rearrangements have normal complements of chromosomal material, meaning there is no loss of genetic material

Question 9

Q

Even though there’s no loss of genetic material, what is a consequence of balanced chromosomal rearrangements?

Answer

A

They have varying stability during meiosis and mitosis

Question 10

Q

Inversions

Answer

A

occur when one chromosome undergoes two double stranded breaks of the DNA backbone and the intervening sequence is inverted prior to the rejoining of the broken ends

Question 11

Q

Pericentric inversions

Answer

A

include the centromere

Question 12

Q

paracentric inversions

Answer

A

exclude the centromere

Question 13

Q

Chromosomes with inversions can have normal genetic complement, and therefore carriers may have no phenotype. However, during meiosis, a loop to maximize the association between homologs is created. If a crossover occurs within the inverted region of a paracentric inversion what happens?

Answer

A

If a crossover occurs within the inverted region, both dicentric (2 centromeres) chromosomes and acentric (no centromere) chromosomes can be generated, leading to chromosome breakage or loss

Question 14

Q

Reciprocal translocations - balanced or unbalanced?

Question 15

Q

reciprocal translocations results from?

Answer

A

breakage and rejoining of non homologous chromosomes, with a reciprocal exchange of broken segments.

Question 16

Q

Reciprocal translocations carriers have increased risk of?

Answer

A

unbalanced gametes

Question 17

Q

Because carriers of reciprocal translocations are frequently phenotypically normal, how are they usually uncovered?

Answer

A

when couples have spontaneous abortions

males are infertile

Question 18

Q

What happens when chromosomes of a carrier of a balanced reciprocal translocation pair at meiosis?

Answer

A

a quadrivalent is formed

Question 19

Q

Reciprocal translocation - meiotic quadrivalent

Which segregation pattern will result in normal chromosome complement in gametes?

Answer

A

Alternate segregation

Question 20

Q

Alternate segregation of quadrivalents from reciprocal translocations results in gametes that have….?

Answer

A

Either the normal chromosome complement
or
two reciprocal translocation chromosomes, both of which are balanced with respect to chromosome complement

*See slide 8

Question 21

Q

What happens if adjacent segregation occurs with the quadrivalent in meiosis?

Answer

A

adjacent segregation leads to unbalanced gametes

See slide 8

Question 22

Q

When can a balanced (Apparently) translocation manifest phenotypically in the carrier?

Answer

A

if the breakpoint occurs in a gene, disrupting its function

Question 23

Q

Reciprocal Translocations: Quadrivalent Formation at Meiosis I… how do the homologues arrange themselves?

Answer

A

At zygotene, the partner homologues, both normal and translocated arrange themselves to maximize sequence pairing

Question 24

Q

Reciprocal translocation - quadrivalent segregation is described by?

Answer

A

The relationship of the centromeres to one another

Question 25

Q

In ___________ segregation, centromeres of homologues go to opposite poles

Answer

A

alternate

Question 26

Q

Alternate segregation leads to?

Answer

A

gametes with normal choromosomes

gametes with both derivatives (balanced)

Question 27

Q

In __________ segregation, next door centromeres go to the same pole

Question 28

Q

adjacent segregation –>

Answer

A

abnormal segregation

Question 29

Q

Adjacent segregation is the most common form of malsegregation when…?

Answer

A

the translocated segments are relatively small

Question 30

Q

Adjacent segregation results in?

Answer

A

Trisomy and monosomy for translocated segments

Question 31

Q

What helps to determine the potential viability of zygote(s)

Answer

A

The size of the translocated segment - larger translocated segments offer more opportunity for recombinations

Question 32

Q

Balanced translocation carriers… risk to have unbalanced progeny?

Answer

A

Ranges from 0-30% depending on the type of translocation

Question 33

Q

Balanced translocation carriers

–> The risk for unbalanced progeny depends on

Answer

A

size of exchanged material

sex of carrier: maternal more likely to have unbalanced offspring

Question 34

Q

What are Robertsonian Translocations?

Answer

A

Structural chromosomal rearrangement

centric fusion

joining of two acrocentric chromosomes at the centromere, short arm

Question 35

Q

Robertsonian Translocations occur when there is fusion of two acrocentric chromosomes with their centromeric regions, do we lose any DNA?

Answer

A

We lose the short arm DNA containing satellite DNA and rDNA repeats - but not any significant DNA

Question 36

Q

Roberstonian Translocations - are they considered balanced?

Answer

A

Yes, while Robertsonian Translocations result in reduction in chromosome number, they are considered balanced rearrangements because the loss of some rDNA repeats is not deleterious

Question 37

Q

Carriers of Robertsonian Translocations and offspring risks?

Answer

A

Carriers of Robertsonian Translocations are phentoypically normal, but these rearrangements may lead to unbalanced karyotypes for their offspring, resulting in monosomies and trisomies

Question 38

Q

Human Acrocentric chromosomes

Answer

A

13, 14, 15, 21, and 22

Question 39

Q

Is there a risk of loss of euchromatin with Robertsonian translocations?

Answer

A

No, there is no euchromatin on the p arm of acrocentric chromosomes

Question 40

Q

What is the most common type of chromosomal rearrangement?

Answer

A

Robertsonian translocations

Question 41

Q

Is there a risk to offspring if parent has Robertsonian translocations?

Answer

A

Yes, risk of having unbalanced karyotype

Question 42

Q

Robertsonian translocations and fertility

Answer

A

Increased prevalence of RT in infertile men

Question 43

Q

Most common Robertsonian Translocation, and two other common RT

Answer

A

13;14 = 75% of all RTs (mos common translocation in humans)

14;21
21;21

Question 44

Q

Are Robertsonian Translocations de novo or familial?

Answer

A

They can be de novo or familial

Question 45

Q

De Novo unbalanced Robertsonian Translocations

If we have 46 chromosomes with normal homologue plus RT “homologue” it leads to __________

Question 46

Q

RT invovling chromosomes 13 and 21 can lead to viable trisomies: tri 13 and 21

What would the nomenclature of unbalanced RT 14;21 with normal 21 plus RT look like in a female?

Answer

A

46,XX,+21,der(14;21)(q10;q10)

Question 47

Q

What would be the nomenclature for trisomy 13 derived from RT (13;14) in a male?

Answer

A

46,XY,+13,der(13;14)(q10;q10)

Question 48

Q

What would the nomenclature be for a balanced translocation of 21 to 14 in male?

Answer

A

45,XY,der(14;21)(q10;q10)

Question 49

Q

What would be the nomenclature for an unbalanced translocation of 21 to 14 in male

resulting in trisomy 21?

Answer

A

46,XY,der(14;21)(q10;q10),+21

Question 50

Q

Are familial or de novo inversions more common?

Question 51

Q

Incidence of inversions?

Answer

A

as high as 1% in population

Question 52

Q

Inversion carriers phenotype?

Answer

A

Normally normal

Question 53

Q

Pericentric inversion

Answer

A

Inverted segment includes the centromere

break in both p and q arms

Question 54

Q

Pericentric inversion nomenclature of chromosome 9 involving break at p24 and q21? In female

Answer

A

46,XX,inv(9)(p24q12)

Question 55

Q

Common benign pericentric inversions in the population are called?

Answer

A

Heteromorphic variants

Question 56

Q

What are common heteromorphic variant pericentric inversions containing constitugive heterochromatin in the population?

Answer

A

9qh
16qh
1qh
Yqh
pericentric region of 2 or e

Question 57

Q

Benign pericentric inversion in the population containing G positive bands?

Question 58

Q

Are benign pericentric inversions familial or de novo?

Answer

A

Almost always familial

Question 59

Q

Are benign pericentric inversions associated wtih increased spontaneous abortions / infertility / or recombinant offspring?

Question 60

Q

Which pericentric inversion is so common in the populace (2-3%) that it is no longer even reported?

Answer

A

9qh

report as 46,XX

Question 61

Q

Pericentric inversion behavior during meiosis?

Answer

A

Pericentric inversions form a loop structure during homologue pairing of meiosis

Issue: how to get maximal pairing of like sequences between two homologues

Potential for forming recombinant chromosomes

Question 62

Q

What is the homologue pairing stage of meiosis called?

Question 63

Q

Outcomes of recombination in pericentric inversion carriers?

Answer

A

One recombination even is predicted within the inverted segment of the inversion chromosome and the homologous sequence in the normal chromosome

Crossover between two non-sister chromatids–> Gives rise to:
Two complementary recombinants

Duplication of long arm, deletion of short arm flanking segment

Deletion of long arm, duplication of short arm flanking segment

Question 64

Q

Meiotic Recombination in inversion carriers

Possible gametes? (2)

Answer

A

Normal, unrearranged
Inversion, balanced carrier
- combined about 50%

Two complementary recombinants
- usually one compatible with liveborn and one lethal, but not always

see slide 32

Answer 56

A

inversion 8 carrier

46,XX inv(8)(p23.1q22.1)

Answer 57

A

Trisomy for 8q22.1

Monosomy for 8p23.1

Answer 58

A

Developmental delay
Congenital heart disease
Hypertelorism (large distance between eyes)
Thin upper lip

Answer 59

A

rec(8) offspring

Answer 60

A

not significantly increased

Answer 61

A

founder effect

first described in Hispanic families in West

Kindreds with ancestral lines originating in teh San Luis Valley

Postualte a single common ancestory (founder) with inv(8) 2-300 years ago

Answer 62

A

Inversion segment excludes centromere

two breaks within the same chromosome arm

Answer 63

A

May be more difficult to detect

Under ascertained

Answer 64

A

Familal or sporadic

Answer 65

A

inv(11)(p13p15) aniridia (absence of iris)

Xp/q inversion and Turner syndrome anomalies

Answer 66

A

Either dicentric or acentric

Answer 67

A

Outside the loop

Resulting in dicentric and acentric fragments

Answer 68

A

Evolution of new gene function

Answer 69

A

abnormal phenotypes caused by gain or loss of a set of neighboring genes

Answer 70

A

Cat eye syndrome

Example of contiguous gene Del/DUP syndrome

Answer 71

A

Segmental duplication

Answer 72

A

Chromosome 22 rearrangement mediated by gene duplication

Answer 73

A

Caused by disturbance of migration of neural crest cells into the pharyngeal arches and pouches resulting in cleft lip/palate and heart defects

Thymus defects: T cell
Parathyroid defects: hypocalcemia

Critical protein: TBX-1 - transcription factor that is important for neural crest cell migration!

Answer 74

A

del(4p16.3)
Facial clefting
Prominent ears
microcephaly 
intellectual disabilities

Answer 75

A

del(5p15.2)
microcephaly
characteristic cry
seizures
intellectual disability

Answer 76

A

del(7q11.2)
Congenital heart disease
short stature

Answer 77

A

del(8q24.1)
Tricho-rhino pharangeal syndrome - characterized by thin, sparse scalp hair, unusual facial features, and multiple abnormalities affecting the “growing ends” (epiphyses) of certain bones, especially those in the hands and feet.
Multiple exostoses - (benign outgrowth of cartilagenous tissue)

Answer 78

A

del(11p13)
Wilms tumor
aniridia 
genitourinary anomalies
intellectual disability

Answer 79

A

dup(11p15.5) paternal
overgrowth
omphalocele (gi outside)
Wilms tumor
other tumors

Answer 80

A

del(15q11-q13) maternal
seizures
intellectual disabilties

Answer 81

A

del(15q11-q13) paternal 
hypotonia
hypopigmentation 
hypogenitalism 
obesity

Answer 82

A

del(17p13.3)
lissencephaly (no brain convolutions)
profound intellectual disability

Answer 83

A

del(22q11.2)
absent or hypoplastic thymus and parathyroids
congenital heart disease
Velo-Cardio-Facial Syndrome
- cleft palate, lateral nasal buildup, cardiac septal defects

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Structural Chromosomal Abnormalities Flashcards

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