Fragile-X Syndrome
From Iusmgenetics
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**'''Unusual''': some obligate carrier males have a normal phenotype ('''normal transmitting males''', NTM) | **'''Unusual''': some obligate carrier males have a normal phenotype ('''normal transmitting males''', NTM) | ||
**An example is that females heterozygous for full mutation and normal allele may or may not manifest the disease. | **An example is that females heterozygous for full mutation and normal allele may or may not manifest the disease. | ||
| - | *Fathers do not usually pass on large repeats; | + | *Fathers do not usually pass on large repeats; there may be some sort of selection against pass of large alleles through the germ line. |
**This is similar to myotonic dystrophy. | **This is similar to myotonic dystrophy. | ||
*Mothers are usually the source of expansive repeat alleles | *Mothers are usually the source of expansive repeat alleles | ||
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*CGG triplet repeat expansion in the 5' UTR of exon 1 of fmr1 gene. | *CGG triplet repeat expansion in the 5' UTR of exon 1 of fmr1 gene. | ||
**We describe the expansion as small ("premutation)" or large ("full mutation"). | **We describe the expansion as small ("premutation)" or large ("full mutation"). | ||
| + | **Normal: n < 50 repeats promoter unmethylated | ||
| + | **Premutation: n ~ 50-200 promoter unmethylated | ||
| + | ***“Premutation” alleles are slightly expanded; the gene can still be transcribed but is potentially unstable and may expand further (e.g., to full mutation) in next generation. | ||
| + | **Full mutation: n > 200 promoter methylated | ||
| + | ***“Full mutation” alleles have large expansions, '''are not transcribed''', and cause Fragile- X syndrome. | ||
| + | |||
| + | |||
*As the repeat expands '''disease is caused by a loss of FMR1 function'''. | *As the repeat expands '''disease is caused by a loss of FMR1 function'''. | ||
| + | **50-69 repeats: <20% chance of expansion | ||
| + | **70-70 repeats: 39% | ||
| + | **80-89 repeats: 76% | ||
| + | **90-99 repeats: 89% | ||
| + | **99-> repeats: 99% | ||
| + | |||
| + | |||
| + | *Normal transmitting male (NTM): have the premutation but not the syndrome. | ||
| + | *Unaffected female: can be heterozygous for full mutation. | ||
| + | **Females who are heterozygotes for a full mutation and normal allele may or may not develop the syndrome: 50% have mental retardation. | ||
| + | **Therefore, this disorder is not cleanly recessive or dominant. | ||
| + | *Affected male: has the full mutation and the syndrome. | ||
| + | **Affected males (with Fragile X syndrome) generally do not reproduce. | ||
| + | *Expansions from premutation to full mutation are '''usually NOT inherited from fathers'''. | ||
| + | **There may be selection against passage of large alleles through the male germ line. | ||
| + | *Affected female: Heterozygous for full mutation and normal allele | ||
| + | |||
| + | |||
*Fragile X syndrome '''demonstrates germline AND somatic instability''' such that the pt may be mosaic in terms of number of repeats in the UTR of exon 1. | *Fragile X syndrome '''demonstrates germline AND somatic instability''' such that the pt may be mosaic in terms of number of repeats in the UTR of exon 1. | ||
*''As the repeat increases in size, the risk of expansion increases''. | *''As the repeat increases in size, the risk of expansion increases''. | ||
| - | *Sometimes CGG repeats are interrupted by AGG repeats | + | *Sometimes CGG repeats are interrupted by AGG repeats. |
| + | **'''Interrupted repeats are less likely to expand'''. | ||
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===Pathogenesis=== | ===Pathogenesis=== | ||
| + | *The pathogenic mechanism is a “loss of function” of the fmr1 gene or its gene product FMRP. | ||
| + | **Recall that FMRP is expressed in neurons as well as oligodendrocytes (myelin producing cells of CNS). | ||
| + | **Recall that FMRP is involved with the transport of mRNA of other genes. | ||
| + | *A similar syndrome can be caused by rare FMR1 point mutations (mutant protein). | ||
| + | |||
| + | |||
*Fragile-X syndrome manifests according to the number of CGG repeats in the fmr1 gene: | *Fragile-X syndrome manifests according to the number of CGG repeats in the fmr1 gene: | ||
**Normal: < 50 repeats, promotor is unmethylated | **Normal: < 50 repeats, promotor is unmethylated | ||
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**'''Full mutation: > 200 repeats, promotor is methylated''' | **'''Full mutation: > 200 repeats, promotor is methylated''' | ||
***Not transcribed | ***Not transcribed | ||
| + | |||
| + | |||
| + | *Repeats in the fmr1 gene are found in the 5' untranslated region. | ||
| + | **Recall that Muscular Dystrophy occurs by a 3' UTR repeat. | ||
===Phenotypic information=== | ===Phenotypic information=== | ||
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| - | * | + | *'''The premutation state is not completely innocuous!''': |
| - | **Women are at 3-4 fold increase for premature ovarian failure and early menopause. | + | **Women (with the premutation) are at 3-4 fold increase for premature ovarian failure and early menopause. |
| - | **Men over 50 are at risk (1 of 4) for "Fragile X associated tremor / ataxia syndrome (FXTAS)". | + | **Men over 50 (with the premutation) are at risk (1 of 4) for "Fragile X associated tremor / ataxia syndrome (FXTAS)". |
| - | *** | + | ***FXTAS (Fragile X associated tremor / ataxia syndrome) may also be seen in some females |
**Up to 25% of premutation carriers may have mild cognitive and / or behavioral deficits. | **Up to 25% of premutation carriers may have mild cognitive and / or behavioral deficits. | ||
**Perhaps this premutation state of disease is due to an RNA gain of negative function? | **Perhaps this premutation state of disease is due to an RNA gain of negative function? | ||
Current revision as of 17:32, 13 December 2011
Contents |
[edit] Fragile X Syndrome
[edit] General background information
- Called "Fragile X" because in a certain subset the conditions are right for an end of the X chromosome to fall off.
- 1 / 1250 males
- 1 / 2000 females
- All ethnic groups
[edit] Mode of inheritance
- Not clearly dominant or recessive
- Unusual: some obligate carrier males have a normal phenotype (normal transmitting males, NTM)
- An example is that females heterozygous for full mutation and normal allele may or may not manifest the disease.
- Fathers do not usually pass on large repeats; there may be some sort of selection against pass of large alleles through the germ line.
- This is similar to myotonic dystrophy.
- Mothers are usually the source of expansive repeat alleles
[edit] Single important gene
- The fmr1 gene is expressed in neurons and oligodendrocytes.
- Recall that oligodendrocytes are the myelin producing cells of the CNS.
- FMR1 is involved in the transport of mRNA of other genes.
[edit] Etiology
- CGG triplet repeat expansion in the 5' UTR of exon 1 of fmr1 gene.
- We describe the expansion as small ("premutation)" or large ("full mutation").
- Normal: n < 50 repeats promoter unmethylated
- Premutation: n ~ 50-200 promoter unmethylated
- “Premutation” alleles are slightly expanded; the gene can still be transcribed but is potentially unstable and may expand further (e.g., to full mutation) in next generation.
- Full mutation: n > 200 promoter methylated
- “Full mutation” alleles have large expansions, are not transcribed, and cause Fragile- X syndrome.
- As the repeat expands disease is caused by a loss of FMR1 function.
- 50-69 repeats: <20% chance of expansion
- 70-70 repeats: 39%
- 80-89 repeats: 76%
- 90-99 repeats: 89%
- 99-> repeats: 99%
- Normal transmitting male (NTM): have the premutation but not the syndrome.
- Unaffected female: can be heterozygous for full mutation.
- Females who are heterozygotes for a full mutation and normal allele may or may not develop the syndrome: 50% have mental retardation.
- Therefore, this disorder is not cleanly recessive or dominant.
- Affected male: has the full mutation and the syndrome.
- Affected males (with Fragile X syndrome) generally do not reproduce.
- Expansions from premutation to full mutation are usually NOT inherited from fathers.
- There may be selection against passage of large alleles through the male germ line.
- Affected female: Heterozygous for full mutation and normal allele
- Fragile X syndrome demonstrates germline AND somatic instability such that the pt may be mosaic in terms of number of repeats in the UTR of exon 1.
- As the repeat increases in size, the risk of expansion increases.
- Sometimes CGG repeats are interrupted by AGG repeats.
- Interrupted repeats are less likely to expand.
- It should be noted that a syndrome similar to Fragile X can be produced via particular point mutations of fmr1.
[edit] Pathogenesis
- The pathogenic mechanism is a “loss of function” of the fmr1 gene or its gene product FMRP.
- Recall that FMRP is expressed in neurons as well as oligodendrocytes (myelin producing cells of CNS).
- Recall that FMRP is involved with the transport of mRNA of other genes.
- A similar syndrome can be caused by rare FMR1 point mutations (mutant protein).
- Fragile-X syndrome manifests according to the number of CGG repeats in the fmr1 gene:
- Normal: < 50 repeats, promotor is unmethylated
- Premutation: 50-200 repeats, promoter is unmethylated
- Can be transcribed but is unstable and may expand in the next generation.
- Full mutation: > 200 repeats, promotor is methylated
- Not transcribed
- Repeats in the fmr1 gene are found in the 5' untranslated region.
- Recall that Muscular Dystrophy occurs by a 3' UTR repeat.
[edit] Phenotypic information
- Mental retardation:
- Males: moderate; 3-6%
- Females: mild
- Behavioral problems: hyperactivity, tantrums, autistic features
- Physical findings:
- Before pubery: large head
- After pubery: prominent ears / jaw / forehead
- Macroorchidism
- Those will the full mutation usually do not reproduce.
- The premutation state is not completely innocuous!:
- Women (with the premutation) are at 3-4 fold increase for premature ovarian failure and early menopause.
- Men over 50 (with the premutation) are at risk (1 of 4) for "Fragile X associated tremor / ataxia syndrome (FXTAS)".
- FXTAS (Fragile X associated tremor / ataxia syndrome) may also be seen in some females
- Up to 25% of premutation carriers may have mild cognitive and / or behavioral deficits.
- Perhaps this premutation state of disease is due to an RNA gain of negative function?
