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FRAGILE X 
SYNDROME 
DIVYA NARAYANAN 
OCT 13TH, 2014
HISTORY 
1943 - Discovery 
by Martin & Bell 
1969 - Development 
of Chromosome Tests 
by Herbert Lubs 
1999 – FMR1 gene 
and mutational basis 
discovered
FMR1 5’ LEADER
FMR1 GENE
METHYLATION OF CYTOSINE LEADS TO 
TRANSCRIPTIONAL SILENCING IN FXS
CARRIERS ARE MORE PREMUTATION AFFECTED
CHARACTERIZATION OF 
PREMUTATION CGG EXPANSION
WHEN THE CGG EXPANSION HAPPENS?
TYPES OF FMR1 REPEAT EXPANSION MUTATIONS 
Type No. of CGG 
repeats 
Methylation 
status of FMR1 
Phenotype 
in males 
Phenotype in 
females 
Normal 5-50 Unmethylated Unaffected Unaffected 
Premutation 51-200 Unmethylated Unaffected Unaffected 
Full mutation >200 Hypermethylated Affected 50% affected; 
50% unaffected 
Mosaicism Varies 51 to 
>200 
Partially 
methylated 
Affected Highly variable 
Methylation 
Mosaicism 
>200 Partially 
methylated 
Affected Highly variable 
Unmethylated 
full mutation 
>200 Unmethylated Nearly all 
affected 
Highly variable
FMRP PRESENCE
FMRP ABSENCE
FRAGILE X SYNDROME INDIVIDUALS EXHIBIT 
ALTERED DENDRITIC SPINE MORPHOLOGY 
Weiler et al. Am J Med Genet (1999)
DIAGNOSIS 
Pedigree analysis
DIAGNOSIS 
Karyotyping
DIAGNOSIS 
Direct DNA analysis
DIAGNOSIS 
Southern Blotting
DIAGNOSIS 
Immunocytochemical tests
Sample : Maternal Blood; 
amniotic fluid 
Tests : PCR, Southern Blot; 
Karyotype, FISH 
analysis 
Enzymes : EcoRI; EagI 
Results : a) Deletion in one FMR1 
gene in Linda 
b) one 33 CGG repeat 
allele (normal) and one 
110 CGG repeat allele 
(premutation) in fetus 
CASE STUDY 
35 years old 
10 years old (first child)
CASE STUDY 
1. Molecular size marker 
2. Control (female with premutation) 
3. Control (female with full mutation) 
4. Normal male 
5. Linda’s result 
6. Linda’s fetus result 
7. Female with intermediate result 
8. Female with normal result 
9. Male with full mutation
CASE STUDY 
Electropherogram 
Largest peak : 33 CGG repeats 
Smallest peak : 110 CGG repeats
CASE STUDY 
• After PCR analysis, how many repeat 
length results are expected? 
• What steps can be taken by the 
laboratory to investigate this apparent 
discrepancy? 
• Is Linda a carrier of fragile X syndrome? 
• Is amniotic fluid an appropriate specimen 
type for prenatal fragile X testing? 
• Should these results alleviate Linda’s 
parental anxiety?
REFERENCES 
• Weiler et al, Synaptic Synthesis of the Fragile X Protein: Possible Involvement in Synapse Maturation 
and Elimination; American Journal of Medical Genetics 83:248–252 (1999) 
• Dobson et al, Identifying intrinsic and extrinsic determinants that regulate internal initiation of 
translation mediated by the FMR1 5' leader; BMC Molecular Biology 2008, 9:89 doi:10.1186/1471- 
2199-9-89 
• Tassone et al, Elevated Levels of FMR1 mRNA in Carrier Males: A New Mechanism of Involvement in 
the Fragile-X Syndrome; Am. J. Hum. Genet. 66:6–15, 2000 
• Haas, History Tends to Repeat: FMR-1 Silencing in Fragile X Syndrome; Eukaryon, Vol. 3, February 
2007 
• Berman et al, Mouse Models of the Fragile X-Associated Tremor/Ataxia Syndrome (FXTAS) and the 
Fragile X Premutation; Movement Disorders: Genetics and Models, second edition 
• Jin et al, RNA-Mediated Neurodegeneration Caused by the Fragile X Premutation rCGG Repeats in 
Drosophila; Neuron, Vol. 39, 739–747, August 28, 2003 
• Cheng et al, Astrocytes and Developmental Plasticity in Fragile X; Neural Plasticity Volume 2012, 
Article ID 197491,12 pages doi:10.1155/2012/197491 
• Fragile X syndrome, Atlas of Genetic Diagnosis and Counselling (2006) 
• Eliez et al, Genetics of Childhood Disorders: XI. Fragile X Syndrome; J . Am. Acad. Child Adolesc. 
Psychiatry, 39:2. February 2000 
• Jaquemont et al, Fragile X Premutation Tremor/Ataxia Syndrome : Molecular, clinical and 
Neuroimaginf Correlates; Am J Hum Genet. Apr 2003; 72(4): 869-878 
• Damell et al, FMRP Stalls Ribosomal Translocation on mRNAs Linked to Synaptic Function and 
Autism; Cell 146, 247–261, July 22, 2011 
• Heim, Fragil X syndrome; Diagnostic Molecular Pathology in Practice, 2011
THANKYOU

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Fragile X Syndrome

  • 1. FRAGILE X SYNDROME DIVYA NARAYANAN OCT 13TH, 2014
  • 2. HISTORY 1943 - Discovery by Martin & Bell 1969 - Development of Chromosome Tests by Herbert Lubs 1999 – FMR1 gene and mutational basis discovered
  • 3.
  • 6. METHYLATION OF CYTOSINE LEADS TO TRANSCRIPTIONAL SILENCING IN FXS
  • 7. CARRIERS ARE MORE PREMUTATION AFFECTED
  • 9. WHEN THE CGG EXPANSION HAPPENS?
  • 10. TYPES OF FMR1 REPEAT EXPANSION MUTATIONS Type No. of CGG repeats Methylation status of FMR1 Phenotype in males Phenotype in females Normal 5-50 Unmethylated Unaffected Unaffected Premutation 51-200 Unmethylated Unaffected Unaffected Full mutation >200 Hypermethylated Affected 50% affected; 50% unaffected Mosaicism Varies 51 to >200 Partially methylated Affected Highly variable Methylation Mosaicism >200 Partially methylated Affected Highly variable Unmethylated full mutation >200 Unmethylated Nearly all affected Highly variable
  • 13. FRAGILE X SYNDROME INDIVIDUALS EXHIBIT ALTERED DENDRITIC SPINE MORPHOLOGY Weiler et al. Am J Med Genet (1999)
  • 19. Sample : Maternal Blood; amniotic fluid Tests : PCR, Southern Blot; Karyotype, FISH analysis Enzymes : EcoRI; EagI Results : a) Deletion in one FMR1 gene in Linda b) one 33 CGG repeat allele (normal) and one 110 CGG repeat allele (premutation) in fetus CASE STUDY 35 years old 10 years old (first child)
  • 20. CASE STUDY 1. Molecular size marker 2. Control (female with premutation) 3. Control (female with full mutation) 4. Normal male 5. Linda’s result 6. Linda’s fetus result 7. Female with intermediate result 8. Female with normal result 9. Male with full mutation
  • 21. CASE STUDY Electropherogram Largest peak : 33 CGG repeats Smallest peak : 110 CGG repeats
  • 22. CASE STUDY • After PCR analysis, how many repeat length results are expected? • What steps can be taken by the laboratory to investigate this apparent discrepancy? • Is Linda a carrier of fragile X syndrome? • Is amniotic fluid an appropriate specimen type for prenatal fragile X testing? • Should these results alleviate Linda’s parental anxiety?
  • 23. REFERENCES • Weiler et al, Synaptic Synthesis of the Fragile X Protein: Possible Involvement in Synapse Maturation and Elimination; American Journal of Medical Genetics 83:248–252 (1999) • Dobson et al, Identifying intrinsic and extrinsic determinants that regulate internal initiation of translation mediated by the FMR1 5' leader; BMC Molecular Biology 2008, 9:89 doi:10.1186/1471- 2199-9-89 • Tassone et al, Elevated Levels of FMR1 mRNA in Carrier Males: A New Mechanism of Involvement in the Fragile-X Syndrome; Am. J. Hum. Genet. 66:6–15, 2000 • Haas, History Tends to Repeat: FMR-1 Silencing in Fragile X Syndrome; Eukaryon, Vol. 3, February 2007 • Berman et al, Mouse Models of the Fragile X-Associated Tremor/Ataxia Syndrome (FXTAS) and the Fragile X Premutation; Movement Disorders: Genetics and Models, second edition • Jin et al, RNA-Mediated Neurodegeneration Caused by the Fragile X Premutation rCGG Repeats in Drosophila; Neuron, Vol. 39, 739–747, August 28, 2003 • Cheng et al, Astrocytes and Developmental Plasticity in Fragile X; Neural Plasticity Volume 2012, Article ID 197491,12 pages doi:10.1155/2012/197491 • Fragile X syndrome, Atlas of Genetic Diagnosis and Counselling (2006) • Eliez et al, Genetics of Childhood Disorders: XI. Fragile X Syndrome; J . Am. Acad. Child Adolesc. Psychiatry, 39:2. February 2000 • Jaquemont et al, Fragile X Premutation Tremor/Ataxia Syndrome : Molecular, clinical and Neuroimaginf Correlates; Am J Hum Genet. Apr 2003; 72(4): 869-878 • Damell et al, FMRP Stalls Ribosomal Translocation on mRNAs Linked to Synaptic Function and Autism; Cell 146, 247–261, July 22, 2011 • Heim, Fragil X syndrome; Diagnostic Molecular Pathology in Practice, 2011