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Rett syndrome Flashcards

1
Q

Main characteristics of Rett

A
  1. Normal early development 6-18 months
  2. Loss of acquired fine and gross motor skills and communication
  3. Stereotypic hand movements
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2
Q

Genes associated with Rett

A

MECP2: methyl CpG binding protein (90-95%)

Clinically overlapping phenotype:
CDKL5
Netrin G1

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3
Q

MECP2 gene

A

2 isoforms created by alternative splicing of exon 2 and the use of 2 alternative start codons:

  • e1 (contains exon 1 but alternatively splices out exon 2, predominant in brain)
  • e2 (exon 1 absent, predominant in fibroblasts/lymphocytes)
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4
Q

MECP2 protein

A

Two functional domains:

  1. methyl binding domain (binds specifically to DNA at methylated CpGs)
  2. transcription repression domain (recruits corepressor proteins that repress transcription by deacetylation and condensation of chromatin)

E1 form most abundant

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5
Q

MECP2 mutations

A
  • Almost all de novo
  • Parents can be germline mosaic
  • Majority arise on paternal Chr.
  • 200 known nucleotide changes
  • 8 most common missense and nonsense =70% of mutations
  • ~80% mutations in classic Rett in exons 3-4
  • Exon4 and intron 2 contain highly repetitive regions, recombination between these can lead to del exons 3-4
  • Deletion hotspot in c-terminal 9% of mutations
  • Whole exon deletions described
  • Mutations identfied in 80-95% females with classic Rett
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6
Q

Complication of MECP2 mutations

A

Mutations in MECP2 do not constitute a diagnosis of Rett
Mutations also seen in individuals with Angelman like phenotype, non-syndromic X-linked MR, autism, neonatal encephalopathy

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7
Q

Rett syndrome

A

Severe neurodevelopmental disorder mostly affecting females

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8
Q

Rett in males

A

Classical Rett is infrequently observed

Neonatal onset encephalopathy with breathing abnormalities and early lethality more common

Deleterious mutations in 1 copy of the X result in severe neonatal encephalopathy and early lethality

May be mosaic or have a 47XXY karyotype (more classical symptoms)

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9
Q

Other Rett phenotypes

A

Abnormal breathing patterns
Seizures
Autonomic nervous system dysfunction

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10
Q

Factors influencing severity

A

Skewed X inactivation

Genotype-phenotype correlation (truncation X more severe)

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11
Q

MECP2 duplications

A

Also results in neurodevelopmental impairment

  • early onset infantile hypotonia
  • delayed cognitive development
  • ID
  • epilepsy
  • spasticity
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12
Q

Mutation spectrum

A

Missense mutations predominantly found in methyl biding domain (MBD)

Nonsense mutations found in MBD and transcription repression domain (TRD)

Deletions mostly found in hotspot at c-terminal

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13
Q

Male MECP2 mutations

A

Previously thought to be lethal

Three types of mutations observed in males:

  • Classic Rett mutations
  • Mutations inherited from mother not found in females with Rett
  • Males with deletion of the whole gene and neighbouring genes resulting in a severe phenotype
  • MECP2 duplication syndrome (most common mutation in males)
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14
Q

MECP2 genotype/phenotype correlation

A

Studies have given conflicting results

Milder mutations:

  • missense milder than truncating
  • 3’ to TRD region
  • Females with missense mutations milder than nonsense/fs
  • deletions, if small and towards 3’ end

Skewed X-inactivation may modulate clinical severity

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15
Q

Testing strategy

A

Bidirectional Sanger sequencing detects 85-90% mutations in classic Rett and 30-40% in atypical Rett

MLPA detects deletions/duplications

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16
Q

Possible testing problems

A

reports of false negative results due to primer site polymorphisms

SNPcheck used regularly to look for new SNPs (assess freq info)

PCR primers tagged for use of universal sequencing primers

Analyse sequencing data using Mutation Surveyor

17
Q

Diagnostic referrals (male and female)

A
  • accepted from GPs, paediatrics, clinical genetics
  • parental samples requested if variant identified in child
  • offer testing to other female relatives of proband
  • test male relatives with possible Rett phenotype
18
Q

Referral types

A

Diagnostic
Parental testing following testing in proband
Prenatal

19
Q

Parental referrals

A
  • only accepted from clinical genetics
  • following identification of a variant pathgenic of VUS in proband
  • determine recurrence risk
  • risk of germline mosaicism
20
Q

Prenatal diagnosis

A
  • if mother carries mutation risk is 50%

- test for MCC

21
Q

X inactivation detection

A

Females can show skewed X inactivation

If mother is found to have a mutation, analysis to determine degree of skewing may help in counselling

PCR of polymorphic CAG repeat in exon1 of the Androgen receptor

DNA subject to restriction digest HpaII and CfoI

Can detect ration of 75:25 or unilateral inactivation

may aid in determining the phenotype

22
Q

Alternative testing

A 
CDKL5
Angelman
NTNG1
FOXG1
SLC9A6
23
Q

CDKL5

A

atypical Rett

group characterised by infantile spasms and jerks, early onset seizures

24
Q

Angelman syndrome

A

Present in early childhood and presents with global dev delay, speech and communication problems, stereotypical hand movement, autistic

25
Q

NTNG1

A

NetrinG1- dev of CNS

atypical Rett

26
Q

FOXG1

A

Congenital form presenting within first month

27
Q

SLC9A6

A 
X-linked ID
microcephaly
epilepsy
ataxia
phenotype mimics Angelman
28
Q

Pathophysiology of Rett

A

Regression arises from altered neuronal function rather than neurodegeneration

Maintenance of an appropriate level of MECP2 essential for neuronal function (enhanced as well as reduced function results in impairment)

Brains have smaller and more densely packed neurons

29
Q

Impaired epigenetic transcriptional regulation

A
  • MECP2 binds 2 alternatively methylated forms of DNA (methylated cytosine adjacent non G base and hydroxymethylcytosine)
  • These methylation patterns accumulate postnatally during neuronal maturation
  • This coincides with surge in MECP2 expression
  • Binding of MECP2 may regulate transcription
  • timing coincides with increased synaptogenesis
  • mechanism may contribute to delayed onset of symptoms
30
Q

Altered chromatin architecture

A

MECP2 is able to compact chromatin and influence the higher-order structure of DNA

Impacts the ability of other nuclear proteins to interact with chromatin

e.g. chromatin remodelling protein ATRX, shown to lose normal localisation at heterochromatic foci in null mice (this correlates with disease onset)

31
Q

Neuronal circuit dysfunction

A

Third aspect in timing of Rett onset

Progressive molecular and nuclear changes in neurons impair neuronal function and culminate in altered circuit connectivity (may explain delay)

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