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Familial Colorectal Cancers

Familial Colorectal Cancers. Francis M. Giardiello, M.D. The Johns Hopkins University. COLORECTAL CANCER. Sporadic. Familial. Familial Syndromes. Hereditary nonpolyposis colorectal cancer Familial adenomatous polyposis Attenuated FAP I 1307K mutation of the APC gene.

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Familial Colorectal Cancers

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  1. Familial Colorectal Cancers Francis M. Giardiello, M.D. The Johns Hopkins University

  2. COLORECTAL CANCER Sporadic Familial

  3. Familial Syndromes • Hereditary nonpolyposis colorectal cancer • Familial adenomatous polyposis • Attenuated FAP • I 1307K mutation of the APC gene

  4. Hereditary Nonpolyposis Colorectal Cancer • Autosomal dominant disease • Due to mismatch repair gene mutation • Proximal location of colorectal cancer • Early age of onset • Multiple primary malignancies • Other family cancer

  5. Hereditary Nonpolyposis Colorectal Cancer • Warthin-Lynch syndrome • Lynch I syndrome • hereditary site specific colorectal cancer • Lynch II syndrome • cancer family syndrome

  6. Amsterdam Criteria 3 or more with CRC 65 2 generations 70 49 1 diagnosed age < 50 yrs

  7. SITE OF COLORECTAL CANCER Sporadic HNPCC right sided left sided

  8. Age of Diagnosis of Colorectal Cancer in HNPCC No. Age in Years

  9. Cancer Risks in HNPCC 100 80 Colorectal 78% % with cancer 60 Endometrial 43% 40 Stomach 19% 20 Biliary tract 18% Urinary tract 10% Ovarian 9% 0 0 20 40 60 80 Age (years) Aarnio M et al. Int J Cancer 64:430, 1995

  10. Screening • At-risk family members • colonoscopy 1-2 yr. starting age 20 to 25, and annually after age 40 • gyn exams in women annually with aspiration of endometrium and/or transvaginal ultrasound • screen for gastric or urologic cancer

  11. Screening: Genetic Testing • Mutation of the mismatch repair genes • hMSH2, hMLH1, hPMS1, hPMS2, hMSH6

  12. T C G A C A G C T G T C A T C A G C T G T T C T A C C A T C A G AT G A G C T G HNPCC Results From Failure of Mismatch Repair (MMR) Genes Normal DNA repair Base pair mismatch Defective DNA repair (MMR+)

  13. HNPCC GENETIC TESTING Germline Somatic MSH2 MLH1 MSH6 Microsatellite Instability/ Immunohistochemistry Cancer Blood

  14. Mismatch Repair Failure Leads to Microsatellite Instability (MSI) Normal Microsatellite instability Addition of nucleotide repeats

  15. Immunohistochemistry • Stain tumor for gene proteins • Pursue absent proteins

  16. Bethesda Criteria • Adenoma < 40 or CRC < 45 yo • right-sided undifferentiated, cribiform; signet cell • Endometrial Cancer < 45 yo • 2 HNPCC cancers including met/syn CRC • CRC and FDR with CRC or HNPCC extra colonic cancer (< 45 , adenoma <40) • ICG criteria

  17. Familial Adenomatous Polyposis • Autosomal dominant disease • Mutation of APC gene • Hundreds of adenomas in colorectum • Presence/absence extracolonic lesions • Colorectal cancer inevitable

  18. Cause of FAP • Mutation of APC gene (Adenomatous Polyposis Coli) • Located chromosome 5q 21 • Discovered 1991

  19. Clinical Course Puberty - polyps appear 15 y.o. - average age onset of polyps 33 y.o. - symptoms appear 36 y.o. - average age of diagnosis 39 y.o. - average age of colorectal cancer dx 42 y.o. - death from colorectal cancer

  20. Treatment • Proctocolectomy with ileostomy • Proctocolectomy with ileoanal pull through • Colectomy with ileorectal anastomosis

  21. Cause of FAP • APC gene mutation • Located chromosome 5q21 • Tumor suppressor gene • 300 different mutations identified • APC protein - cell adhesion, signal transduction, and transcription activation

  22. APC GENE CLASSIC FAP 5’ 3’ codons 0 158 1596 2843 RNA PROTEIN

  23. APC GENE CLASSIC FAP 5’ 3’ codons 0 158 1596 2843 RNA PROTEIN

  24. Attenuated FAP • 5’ and 3’ APC gene mutations • 6% of FAP pedigrees • Oligopolyposis (<100 adenomas), R-sided • Heterogeneous phenotype • Later development of CRC (51 vs 39 y.o.)

  25. Screening • At-risk persons (1st degree relatives) • Sigmoidoscopy q yr. starting age 12, then q 2 yrs after age 25, then q 3 yrs after age 35, then average risk guidelines after age 50

  26. Screening: APC Gene Testing • Gene test for mutation of APC gene by PTT • Start at-risk persons age 10-12 • Pretest genetic counseling/informed consent • Test affected pedigree member first

  27. APC Gene Testing - At Risk APC mutation

  28. APC Gene Test Result • Positive - FAP- sigmoidoscopy yearly • Negative - No FAP- sigmoidoscopy age 25

  29. Multiple Adenomas • Mutation of MYH gene • Base excision gene • Phenotype: multiple adenomas or polyposis • Autosomal recessive

  30. Familial Colorectal Cancer • I1307K APC gene mutation • Mutation in codon 1307 of the APC gene • T to A mutation

  31. APC I1307K Mutation * AGAAA[TAA]AA 5’ 3’ isoleucine mutations * AGAAA[AAA]A * * * * lysine predisposing CRC

  32. APC I1307K Mutation

  33. Lifetime Risk of Colorectal Cancer • Ashkenazi Jew 10-15% • Gene Pos 20-30% • Gene Pos + FH > 50%

  34. I1307K Genetic Testing Allele-Specific Oligonucleotide Analysis Normal Mutant X

  35. Screening • Consideration of genetic counseling and genetic testing in Ashkenazi Jewish person with family history of colorectal cancer • Colonoscopy q 2 yrs starting age 35 in gene positive patients

  36. Summary

  37. Summary • Hereditary Nonpolyposis Colorectal Cancer • colonoscopic screening • MSI testing, MMR gene testing

  38. Summary • Hereditary Nonpolyposis Colorectal Cancer • colonoscopic screening • MSI testing, MMR gene testing • Familial adenomatous polyposis • APC gene testing/ MYH gene testing • sigmoid/colonoscopy screening

  39. Summary • Hereditary Nonpolyposis Colorectal Cancer • colonoscopic screening • MSI testing, MMR gene testing • Familial adenomatous polyposis • APC gene testing/ MYH gene testing • sigmoid/colonoscopy screening • Familial Colorectal Cancer • family history/ I1307K

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