Genetic Testing- TNR Expansion Flashcards

Question 1

Q

What is trinucleotide repeat expansion (TNR)?

Answer

A

a unique mutations mechanisms where mutant alleles are unstable and actually change in size from one generation to the next

Question 2

Q

What is trinucleotide repeat expansion (TNR)?

Answer

A

a unique mutations mechanisms where mutant alleles are unstable and actually change in size from one generation to the next

Question 3

Q

T or F. allele size shows a direct correlation with disease severity

Question 4

Q

Name four important TNR disorders

Answer

A

Fragile X syndrome
Huntington disease
Friedrich ataxia
Myotonic dystrophy

Question 5

Q

What is the disease gene for Fragile X syndrome?

Answer

A

CGG repeat on the 5’ untranslated end of FMR1 gene on the X chromosome

Question 6

Q

What are the symptoms of Fragile X syndrome?

Answer

A

developmental delay and cognitive impairment

Question 7

Q

What is the number of CGG repeats for a normal FMR1 gene?

Answer

A

5-54 alleles

Question 8

Q

What is the number of CGG repeats for an intermediate FMR1 gene? What are the results of having this number of repeats?

Answer

A

In fragile X syndrome, there are intermediate alleles (gray, 55-200 repeats) that are not large enough to cause disease in a person who carries such an allele, but are large enough to be unstable during meiosis (aka the ‘premutation’ range). Thus, a full mutation and disease may arise in the next generation.

Question 9

Q

What is the number of CGG repeats for a fully mutated FMR1 gene?

Answer

A

> 200 alleles. symptomatic

Question 10

Q

What is the disease gene for Huntington disease?

Answer

A

CAG repeat within an exon of the HTT gene on chromosome 4

Question 11

Q

What are the symptoms of Huntington disease?

Answer

A

progressive neuropsychiatric disorder

Question 12

Q

What is the number of CAG repeats for a normal HTT gene?

Question 13

Q

What is the number of CAG repeats for a fully mutated HTT gene?

Answer

A

>

Note that there is a small intermediate range, ranging from 36-40

Question 14

Q

What is the disease gene for Friedrich ataxia?

Answer

A

GAA repeat within an intron of the FXN gene on chromosome 9

Question 15

Q

What are the symptoms of Friedrich ataxia?

Answer

A

progressive ataxia

Question 16

Q

What is the number of CAG repeats for a normal FXN gene?

Question 17

Q

What is the number of CAG repeats for a fully mutated FXN gene?

Answer

A

> ~70-200

Question 18

Q

What is the disease gene for Myotonic dystrophy?

Answer

A

CTG repeat in the 3’ untranslated region of the DMPK gene on chromosome 19

Question 19

Q

What are the symptoms of Myotonic dystrophy?

Answer

A

progressive muscle wasting

Question 20

Q

What is the number of CAG repeats for a normal DMPK gene?

Question 21

Q

What is the number of CAG repeats for an intermediate DMPK gene?

Answer

A

35-49 (premutation)

Question 22

Q

What is the number of CAG repeats for a fully mutated DMPK gene?

Answer

A

mild phenotype: ~50-150
classic phenotype: ~100-1000
congenital: >1000

Question 23

Q

TNR expansion disorders are typically associated with what kinds of symptoms?

Answer

A

neurologic and muscular

Question 24

Q

T or F. Within the normal size range, the repeats are perfectly stable, and there is no risk of disease

Answer

A

T. In general, if we examined multiple generations from a normal family, we would expect allele sizes to be perfectly maintained. However, at the same time, there is variation in allele sizes across the normal population. Using the HD gene in normal families as an example, if we looked at one family, we could track an allele with 6 repeats through multiple generations, and there would be no change in its size. A different normal family can have allele sizes anywhere within the normal range (up to ~35 repeats for HD), and these will segregate through that family in a stable manner. 

Question 25

Q

What is the molecular mechanism for allele expansion?

Answer

A

In spite of much research, unanswered questions remain about the molecular mechanism for allele expansion. There is evidence of “looping” out of one strand of the repeat segment during DNA repair or replication that is thought to account for increased copy number.

 In alleles that are large enough to be unstable, expansion occurs in germ cells, and an expanded mutant allele may be passed to the next generation. 

Question 26

Q

Diseases caused by TNR expansion can be put in what two categories?

Answer

A

Those where the triplet repeat is in coding sequence, and those where the triplet repeat is in a noncoding portion of the gene. 

Question 27

Q

In TNR related diseases where the triplet repeat is in coding sequence (exon), the trinucleotide repeating sequence is always?

Answer

A

CAG, coding for glutamine

Question 28

Q

What happens when runs of glutamine get too high?

Answer

A

When runs of glutamine get too big, the protein has a toxic effect on neurons. In affected individuals, fragments of the abnormal protein are visible as aggregates within neurons

Question 29

Q

The associated toxicity of too much glutamine on neuron is called?

Answer

A

a gain of function abnormality, since presence of the abnormal protein exerts a dominant deleterious effect. Although loss of function (absence) of huntington protein (for example) may have serious developmental consequences, it does NOT cause huntington disease. It’s the TNR expansion that accounts for the observed pathogenicity. 

Question 30

Q

In TNR related diseases where the triplet repeat is in non-coding sequence (be it at either end of the gene transcript or in an intron), the trinucleotide repeating sequence is always?

Answer

A

variable, could be CGG, GAA, CTG, and locations vary within the genes

Question 31

Q

In TNR related diseases where the triplet repeat is in non-coding sequence (be it at either end of the gene transcript or in an intron), what is the result of TNR expansion?

Answer

A

no protein produced and RNA toxicity

Question 32

Q

In fragile X, an expanded CGG repeat in the 5’ UTR (in exon 1, upstream of the initiating AUG) leads to what?

Answer

A

methylation of the promoter region and silencing of the gene

Question 33

Q

In myotonic dystrophy, an expanded repeat in in the 3’ UTR causes what?

Answer

A

since it is downstream of the normal stop codon, it’s deleterious effects of repeat expansion are exerted at the RNA level

Question 34

Q

In Huntington disease, the CAG repeat is within the encoded protein. What results from expansion?

Answer

A

expanded polyglutamine causes toxic aggregates to form

Question 35

Q

What is genetic anticipation?

Answer

A

a condition where disease severity worsens in successive generations. Anticipation is explained by the fact that repeat copy number tends to expand each time it passes through meiosis (gametogenesis), and disease severity does correlate with repeat copy number.

leads to earlier progressive onset (not always) and increased severity in subsequent generations

Question 36

Q

What is the general approach to testing for TNR expansion?

Answer

A

Considered a targeted approach to testing since assays look directly at the TNR and provide an estimate of repeat number. Tests use patient DNA, and the result is reported as the number of repeats in each allele that the patient has.  Main approach is PCR

Question 37

Q

T or F. Although the repeat copy number may vary, the flanking sequences are highly conserved

Answer

A

T. The goal of TNR testing is to generate a PCR product that spans the repeat segment and has defined end points in conserved flanking sequences. Thus, the size of the PCR product reflects the number of repeats present. The forward and reverse PCR primers would be specific for the relevant gene sequences on either side of the TNR repeat. Thus, for example, a PCR product from a mutant allele with 40 repeats would be 90bp larger than the product from a normal allele that had 10 repeats. Since a person has two copies of the HTT gene, both alleles would be sized. T

Question 38

Q

Notes on the accuracy of genetic allele testing

Answer

A

For all indications, testing has the capacity to provide an accurate estimate of allele size. While testing can determine allele size in a parent and, also in a fetus or child, it is not possible to make precise predictions about how much a parent’s unstable allele will expand in the next generation

Question 39

Q

Is Huntington disease the only TNR expansion disease related to coding segments?

Answer

A

NO, others include:

Spinocerebellar ataxia
Kennedy disease
Machado-Joseph disease

Note that all these disorders are autosomal dominant, except for Kennedy disease, which is caused by expansion within a gene on the X chromosome

Question 40

Q

What is the inheritance mode of HD?

Answer

A

autosomal dominant

Question 41

Q

What is the average age of onset of HD and average life expectancy?

Answer

A

40 y/o; 15 years; progressive disease

Question 42

Q

What is the prevalence of HD?

Answer

A

~5;100,000

Question 43

Q

What causes HD?

Answer

A

TNR expansion leading to toxic aggregates of neurons involved in protein-protein interactions. The polyglutamine tract resulting from the expansion is near the N-terminus

Question 44

Q

Notes on the ranges of TNR repeats of normal, unstable, and mutated genes for HD.

Answer

A

normal- 10-35 (most common is 18)
unstable- 36-40 (reduced penetrance and may expand during meiosis)
mutated- >40 (symptomatic and will continue to expand in further generations)

Question 45

Q

T or F. People who are heterozygous for a repeat number in the low 40s will have the typical onset of symptoms in middle age.

Answer

A

T. However, while we think of HD as an adult onset disorder, those with very large expansions (100+) can express symptoms in the first or second decade of life. 

Question 46

Q

What is the mode of inheritance of Friedrich ataxia?

Answer

A

autosomal recessive

Question 47

Q

What is the mode of inheritance of myotonic dystrophy type 1 (MDT1)?

Answer

A

autosomal dominant

Question 48

Q

What are some common symptoms of MDT1?

Answer

A

progressive muscle weakness and wasting, cardiac conduction defects, cataracts, prolonged muscle contraction, variable expressivity correlated to allele size

A common description of people with this disorder is that when they engage in a handshake or grab a doorknob, they often have difficulty letting go. 

Question 49

Q

Doe MDT1 show anticipation?

Answer

A

Yes, there is earlier onset and increased severity with successive generations

In comparison, in HD, the primary evidence of anticipation is age of onset. Anticipation may vary in the specifics, but it is a general feature of TNR disorders. 

Question 50

Q

How does TNR expansion cause disease in MDT1?

Answer

A

The pathogenic mechanism in DM1 is not well understood. The expanded TNR in the 3’ UTR of the mRNA causes the mRNA to accumulate in cells and to sequester certain RNA-binding proteins. This sequestration seems to exert a negative trans effect on the ability of other mRNAs to undergo normal translation (i.e. mutant alleles are transcribed but not translated). Thus, the mutation is thought to exert a dominant toxic effect on the DMPK gene and other genes

Question 51

Q

What is a normal DMPK gene typically used for?

Answer

A

the normal protein is a protein kinase involved in intercellular conduction and impulse transmission in heart and skeletal muscle

Question 52

Q

What is the prevalence of MDT1?

Answer

A

~1:20,000

Question 53

Q

What is friedrich ataxia? when is the typical onset?

Answer

A

slow progressive ataxia with onset at puberty. Cardiomyopathy is common

Question 54

Q

What does the normal FXN gene (that when mutated causes Friedrich ataxia) code for?

Answer

A

FXN encoded Frataxin, a nuclear-encoded gene involved in mitochondrial function

Question 55

Q

T or F. Friedreich ataxia is the only TNR disorder with autosomal recessive inheritance

Question 56

Q

What does Friedrich ataxia result from?

Answer

A

TNR is located in an intron of the FXN gene, where its expansion disrupts normal transcription (loss of function mutation)

Question 57

Q

What is the most common form of inherited intellectual disability?

Answer

A

Fragile X syndrome

Question 58

Q

What is the inheritance mode of Fragile X syndrome and its prevalence?

Answer

A

mode: X linked
prevalence: 1:5000 men

Females heterozygous for a mutation may be affected, but phenotypes are more variable than in males (1/2-2/3 of full mutation females are affected). This variability presumably stems from effects of X inactivation.. All full mutation males are affected

Question 59

Q

What are some of the symptoms of Fragile X syndrome?

Answer

A

characteristic appearance of long face, large ears, a prominent jaw, and macro-orchidist (enlarged testes)

typical IQ in the 30-50 range, delayed developmental milestones, abnormal temperament with tantrums, hyperactivity, autism (Autistic features are common, and for this reason, testing for fragile X syndrome is fairly routine in the work up of children with suspected autism)

Question 60

Q

How dis Fragile X syndrome get its name?

Answer

A

The syndrome’s name comes from early observations that during chromosome analysis of affected individuals, a physical break could be elicited at the end of the X chromosome long arm. This is the site of the FMR1 gene, and long trinucleotide expansions cause the chromosome fragility.

Question 61

Q

What is the role of the normal FMR1 gene?

Answer

A

abundant in neurons and plays a role in binding mRNA and shuttling it from the nucleus to the cytoplasm

Question 62

Q

What does TNR expansion of the FMR1 gene cause?

Answer

A

excessive DNA methylation in the 5’ UTR of the gene which turns off the gene (loss of function)

Question 63

Q

Normal FMR1 gene have how many alleles?

Answer

A

6-54. These alleles are stable from one generation to the next, with no risk of fragile X syndrome. 

Question 64

Q

What is the most common allele number of normal FMR1 genes?

Answer

A

~30 repeats, although it is variable like other TNRs

Answer 60

A

females. The larger the premutation, the more likely it is to expand in the next generation.

NOTE: Premutation carriers (male and female) do not have fragile X syndrome; their intellect is normal. 

Answer 61

A

Male premutation carriers are called transmitting males because they will transmit their premutation to all their daughters, but it will not expand in size.

Thus, In fragile X, expansion from premutation to full mutation occurs only in female meiosis and never in male meiosis.

Answer 62

A

Similarly, in myotonic dystrophy, expansion risk is concentrated in females. In particular, children affected with the severe, congenital form almost always have inherited a greatly expanded maternal allele. 

Answer 63

A

In contrast, although Huntington alleles can expand in both males and females, the most dramatic expansions are transmitted from fathers.  Juvenile onset also more likely to come from expansion of paternal allele

Answer 64

A

There are interesting phenotypic abnormalities associated with premutations, which I’ll take a minute to discuss. First, whereas full mutations are heavily methylated and not expressed (loss of function), premutations are overexpressed, and once again, we see evidence of ill-defined “RNA toxicity”.  This is associated with minor phenotypic abnormalities. In both male and female premutation carriers, intellect is normal, but there is increased risk for adult onset cerebellar ataxia and intention tremor (FXTAS-fragile X-associated tremor/ataxia syndrome). As expected for X-linked inheritance, this problem is milder in females. However, female premutation carriers have an additional risk; they are at risk for premature ovarian failure (menopause prior to age 40). The broader significance of these observations is that they add another example to a growing list of examples where carriers, once thought to be phenotypically normal, are now known to have mild phenotypic risks. 

Answer 65

A

Fragile X syndrome
Huntington disease
Friedrich ataxia
Myotonic dystrophy

Answer 66

A

CGG repeat on the 5’ untranslated end of FMR1 gene on the X chromosome

Answer 67

A

developmental delay and cognitive impairment

Answer 68

A

5-54 alleles

Answer 69

A

In fragile X syndrome, there are intermediate alleles (gray, 55-200 repeats) that are not large enough to cause disease in a person who carries such an allele, but are large enough to be unstable during meiosis (aka the ‘premutation’ range). Thus, a full mutation and disease may arise in the next generation.

Answer 70

A

> 200 alleles. symptomatic

Answer 71

A

CAG repeat within an exon of the HTT gene on chromosome 4

Answer 72

A

progressive neuropsychiatric disorder

Answer 73

A

>

Note that there is a small intermediate range, ranging from 36-40

Answer 74

A

GAA repeat within an intron of the FXN gene on chromosome 9

Answer 75

A

progressive ataxia

Answer 76

A

less than 30

Answer 77

A

> ~70-200

Answer 78

A

CTG repeat in the 3’ untranslated region of the DMPK gene on chromosome 19

Answer 79

A

progressive muscle wasting

Answer 80

A

less than 35

Answer 81

A

35-49 (premutation)

Answer 82

A

mild phenotype: ~50-150
classic phenotype: ~100-1000
congenital: >1000

Answer 83

A

neurologic and muscular

Answer 84

A

T. In general, if we examined multiple generations from a normal family, we would expect allele sizes to be perfectly maintained. However, at the same time, there is variation in allele sizes across the normal population. Using the HD gene in normal families as an example, if we looked at one family, we could track an allele with 6 repeats through multiple generations, and there would be no change in its size. A different normal family can have allele sizes anywhere within the normal range (up to ~35 repeats for HD), and these will segregate through that family in a stable manner. 

Answer 85

A

In spite of much research, unanswered questions remain about the molecular mechanism for allele expansion. There is evidence of “looping” out of one strand of the repeat segment during DNA repair or replication that is thought to account for increased copy number.

 In alleles that are large enough to be unstable, expansion occurs in germ cells, and an expanded mutant allele may be passed to the next generation. 

Answer 86

A

Those where the triplet repeat is in coding sequence, and those where the triplet repeat is in a noncoding portion of the gene. 

Answer 87

A

CAG, coding for glutamine

Answer 88

A

When runs of glutamine get too big, the protein has a toxic effect on neurons. In affected individuals, fragments of the abnormal protein are visible as aggregates within neurons

Answer 89

A

a gain of function abnormality, since presence of the abnormal protein exerts a dominant deleterious effect. Although loss of function (absence) of huntington protein (for example) may have serious developmental consequences, it does NOT cause huntington disease. It’s the TNR expansion that accounts for the observed pathogenicity. 

Answer 90

A

variable, could be CGG, GAA, CTG, and locations vary within the genes

Answer 91

A

no protein produced and RNA toxicity

Answer 92

A

methylation of the promoter region and silencing of the gene

Answer 93

A

since it is downstream of the normal stop codon, it’s deleterious effects of repeat expansion are exerted at the RNA level

Answer 94

A

expanded polyglutamine causes toxic aggregates to form

Answer 95

A

a condition where disease severity worsens in successive generations. Anticipation is explained by the fact that repeat copy number tends to expand each time it passes through meiosis (gametogenesis), and disease severity does correlate with repeat copy number.

leads to earlier progressive onset (not always) and increased severity in subsequent generations

Answer 96

A

Considered a targeted approach to testing since assays look directly at the TNR and provide an estimate of repeat number. Tests use patient DNA, and the result is reported as the number of repeats in each allele that the patient has.  Main approach is PCR

Answer 97

A

T. The goal of TNR testing is to generate a PCR product that spans the repeat segment and has defined end points in conserved flanking sequences. Thus, the size of the PCR product reflects the number of repeats present. The forward and reverse PCR primers would be specific for the relevant gene sequences on either side of the TNR repeat. Thus, for example, a PCR product from a mutant allele with 40 repeats would be 90bp larger than the product from a normal allele that had 10 repeats. Since a person has two copies of the HTT gene, both alleles would be sized. T

Answer 98

A

For all indications, testing has the capacity to provide an accurate estimate of allele size. While testing can determine allele size in a parent and, also in a fetus or child, it is not possible to make precise predictions about how much a parent’s unstable allele will expand in the next generation

Answer 99

A

NO, others include:

Spinocerebellar ataxia
Kennedy disease
Machado-Joseph disease

Note that all these disorders are autosomal dominant, except for Kennedy disease, which is caused by expansion within a gene on the X chromosome

Answer 100

A

autosomal dominant

Answer 101

A

40 y/o; 15 years; progressive disease

Answer 102

A

~5;100,000

Answer 103

A

TNR expansion leading to toxic aggregates of neurons involved in protein-protein interactions. The polyglutamine tract resulting from the expansion is near the N-terminus

Answer 104

A

normal- 10-35 (most common is 18)
unstable- 36-40 (reduced penetrance and may expand during meiosis)
mutated- >40 (symptomatic and will continue to expand in further generations)

Answer 105

A

T. However, while we think of HD as an adult onset disorder, those with very large expansions (100+) can express symptoms in the first or second decade of life. 

Answer 106

A

autosomal recessive

Answer 107

A

autosomal dominant

Answer 108

A

progressive muscle weakness and wasting, cardiac conduction defects, cataracts, prolonged muscle contraction, variable expressivity correlated to allele size

A common description of people with this disorder is that when they engage in a handshake or grab a doorknob, they often have difficulty letting go. 

Answer 109

A

Yes, there is earlier onset and increased severity with successive generations

In comparison, in HD, the primary evidence of anticipation is age of onset. Anticipation may vary in the specifics, but it is a general feature of TNR disorders. 

Answer 110

A

The pathogenic mechanism in DM1 is not well understood. The expanded TNR in the 3’ UTR of the mRNA causes the mRNA to accumulate in cells and to sequester certain RNA-binding proteins. This sequestration seems to exert a negative trans effect on the ability of other mRNAs to undergo normal translation (i.e. mutant alleles are transcribed but not translated). Thus, the mutation is thought to exert a dominant toxic effect on the DMPK gene and other genes

Answer 111

A

the normal protein is a protein kinase involved in intercellular conduction and impulse transmission in heart and skeletal muscle

Answer 112

A

~1:20,000

Answer 113

A

slow progressive ataxia with onset at puberty. Cardiomyopathy is common

Answer 114

A

FXN encoded Frataxin, a nuclear-encoded gene involved in mitochondrial function

Answer 115

A

TNR is located in an intron of the FXN gene, where its expansion disrupts normal transcription (loss of function mutation)

Answer 116

A

Fragile X syndrome

Answer 117

A

mode: X linked
prevalence: 1:5000 men

Females heterozygous for a mutation may be affected, but phenotypes are more variable than in males (1/2-2/3 of full mutation females are affected). This variability presumably stems from effects of X inactivation.. All full mutation males are affected

Answer 118

A

characteristic appearance of long face, large ears, a prominent jaw, and macro-orchidist (enlarged testes)

typical IQ in the 30-50 range, delayed developmental milestones, abnormal temperament with tantrums, hyperactivity, autism (Autistic features are common, and for this reason, testing for fragile X syndrome is fairly routine in the work up of children with suspected autism)

Answer 119

A

The syndrome’s name comes from early observations that during chromosome analysis of affected individuals, a physical break could be elicited at the end of the X chromosome long arm. This is the site of the FMR1 gene, and long trinucleotide expansions cause the chromosome fragility.

Answer 120

A

abundant in neurons and plays a role in binding mRNA and shuttling it from the nucleus to the cytoplasm

Answer 121

A

excessive DNA methylation in the 5’ UTR of the gene which turns off the gene (loss of function)

Answer 122

A

6-54. These alleles are stable from one generation to the next, with no risk of fragile X syndrome. 

Answer 123

A

~30 repeats, although it is variable like other TNRs

Answer 124

A

females. The larger the premutation, the more likely it is to expand in the next generation.

NOTE: Premutation carriers (male and female) do not have fragile X syndrome; their intellect is normal. 

Answer 125

A

Male premutation carriers are called transmitting males because they will transmit their premutation to all their daughters, but it will not expand in size.

Thus, In fragile X, expansion from premutation to full mutation occurs only in female meiosis and never in male meiosis.

Answer 126

A

Similarly, in myotonic dystrophy, expansion risk is concentrated in females. In particular, children affected with the severe, congenital form almost always have inherited a greatly expanded maternal allele. 

Answer 127

A

In contrast, although Huntington alleles can expand in both males and females, the most dramatic expansions are transmitted from fathers.  Juvenile onset also more likely to come from expansion of paternal allele

Answer 128

A

There are interesting phenotypic abnormalities associated with premutations, which I’ll take a minute to discuss. First, whereas full mutations are heavily methylated and not expressed (loss of function), premutations are overexpressed, and once again, we see evidence of ill-defined “RNA toxicity”.  This is associated with minor phenotypic abnormalities. In both male and female premutation carriers, intellect is normal, but there is increased risk for adult onset cerebellar ataxia and intention tremor (FXTAS-fragile X-associated tremor/ataxia syndrome). As expected for X-linked inheritance, this problem is milder in females. However, female premutation carriers have an additional risk; they are at risk for premature ovarian failure (menopause prior to age 40). The broader significance of these observations is that they add another example to a growing list of examples where carriers, once thought to be phenotypically normal, are now known to have mild phenotypic risks. 

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Genetic Testing- TNR Expansion Flashcards

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