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Bloom Helicase & Bloom Syndrome

Bloom Helicase & Bloom Syndrome. Aslı Sahin. Bloom Syndrome ( Congenital Telangiectatic Erythema ). Dr. David Bloom in 1954. Autosomal Recessive Disease H igh frequency of breaks and rearrangements in chromosomes Diagnosed i n the first few months of life. Very rare  Total 220 cases

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Bloom Helicase & Bloom Syndrome

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  1. Bloom Helicase &Bloom Syndrome Aslı Sahin

  2. Bloom Syndrome(Congenital TelangiectaticErythema) • Dr. David Bloom in 1954. • Autosomal Recessive Disease • High frequency of breaks and rearrangements in chromosomes • Diagnosed in the first few months of life. • Very rare  Total 220 cases • 1/104 Ashkenazi Jewish person is a carrier of BLMAsh • USA & Japan consanguinity Karyotype of a Normal Individual Karyotype of an individual with Bloom Syndrome Amor-Gueret M. Bloom's syndrome. Orphanet Encyclopedia. February 2004

  3. Main Clinical Features • short stature • photosensitive facial skin lesion & red sun-sensitive skin lesions on the face • Narrow Face&Prominent ears • Immunodeficiency • M/F  infertility/subfertility • Predisposition to malignancy earlier (~25yr) &more frequent(x300) • Death before 30

  4. Nathan E. Allis et al,The Bloom’s Syndrome Gene Product Is Homologous to RecQ Helicases, Cell Vol 83 , November 17, 1995

  5. Gene name:BLM Location: 15q26.1 Protein : The Bloom (BLM) syndrome protein,1417 aa Expression Level:High levels in S phase Localisation: Nuclear Ian D.Hickson et al. RecQ HELICASES: CARETAKERS OFTHE GENOME. Nature Reviews- Cancer. Volume 3/ March 2003

  6. Helicases Unwinds complementary strands at replication fork • Superfamily II: RecQ • Genome Integrity • Tumor Suppressor Gene • Well-conserved

  7. RecQ Helicase Members in Humans • BLM • WRN • RECQ4 • RECQL • RECQ5β • Bloom’s Syndrome • Werner’s Syndrome • Rothmund – Thomson Syndrome

  8. Sequence Generate Mutations Insert Cassettes with viruses Compare sequence with Human BLM mutants Choose most similar one Luo, G. et al. Cancer predisposition caused by elevatedmitotic recombination in Bloom mice. Nature Genet. 26,24–429 (2000).

  9. Luo, G. et al. Cancer predisposition caused by elevatedmitotic recombination in Bloom mice. Nature Genet. 26,24–429 (2000).

  10. Why BLM Cause Cancer? 1- Because of its function......

  11. Maintenance of Genome Integrity Ian D.Hickson et al. RecQ HELICASES: CARETAKERS OFTHE GENOME. Nature Reviews- Cancer. Volume 3/ March 2003

  12. Why BLM Cause Cancer? 1- Because of its function...... 2- Because of its pathways....

  13. BLM’s Interactions with other Tumor-suppresor Proteins Ian D.Hickson et al. RecQ HELICASES: CARETAKERS OFTHE GENOME. Nature Reviews- Cancer. Volume 3/ March 2003

  14. QuestIons ??? References http://www.dnadirect.com/patients/tests/ashkenazi/bloom_syndrome.jsp http://en.wikipedia.org/wiki/Bloom_syndrome http://www.ncbi.nlm.nih.gov/sites/entrez?Db=gene&Cmd=ShowDetailView&TermToSearch=641 http://www.emedicine.com/DERM/topic54.htm http://ghr.nlm.nih.gov/condition=bloomsyndrome http://www.gfmer.ch/genetic_diseases_v2/gendis_detail_list.php?cat3=450 http://www.bio.davidson.edu/Courses/Molbio/MolStudents/spring2003/Baxter/BLMgene.html

  15. THANK YOU FOR YOUR PATIENCE Aslı Sahin

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