Download genetics

Survey
yes no Was this document useful for you?
   Thank you for your participation!

* Your assessment is very important for improving the workof artificial intelligence, which forms the content of this project

Document related concepts
no text concepts found
Transcript
Hereditary Colon Cancer
ACP, October 2013
Steve Lanspa MD, FACP
Magnitude of the Problem
• Annual worldwide incidence of CRC is 1,023,152*:
•
•
• Lynch syndrome (LS) accounts for  2-5%
(20,460-51,160 cases).
•
• < 1% (10,230 cases) constitute FAP.
•
•
•  20% (204,630 cases) are familial (2 or more firstdegree relatives with CRC.
•
• Each family is a cancer prevention target!
• *International Agency for Research on Cancer. Globocan 2002.
Available at: http://www-dep.iarc.fr/.
2
Magnitude
All CRC worldwide –
Approx 1 million per
year
LS associated CRC –
21,000 – 50,000 per
year
JAMA 294:2465-2473, 2005.
4
Two Hit Hypothesis
Molecular Changes-Cell Proliferation
Two Hit Hypothesis
Sporadic
Hereditary
Normal
1stst Hit X
X
Mutant
X
X
X
X
X
nd Hit
2nd
Tumor
XX
Tumor
Maintenance of DNA integrity
Illustration by Jerry Schoendorf, MAMS.
Pages 577-587 (February 2006) GE
Molecular Classification of CRC
• Step-wise accumulations of multiple mutations
• Chromosomal Instability (CIN) 85%
• Microsatellite Instability (MSI) 5%
• CpG island methylator phenotype (CIMP) 10%
Chromosomal Instability Pathway (CIN)
• Chromosomal gains and losses (aneuploidy; copy
number change)
• Allele losses (LOH)
• Is the molecular basis of progression in CRC in
Familial Adenomatous Polyposis
Microsatellite Instability Pathway (MSI)
• Mononucleotide mutations of tumor suppressor
genes
• Arises from defective DNA mismatch repair
• Is the molecular basis of progression in CRC in Lynch
Syndrome
Microsatellite Instability (MSI)
• Microsatellites (short nucleotide repeats) are prone
to replication errors, but corrected by MMR genes
in normal cells
• In tumor DNA, there are altered lengths (instability)
of microsatellites
• MSI is a phenotype that can be used as a surrogate
for MMR mutation/inactivation (now also IHC for
absence of protein expression)
• Inactivation of one copy of MMR = 1st hit
• Subsequent somatic lesion (2nd hit) leads to
mutation rates 1000 times normal
CpG Island Methylation (CIMP)
• Short stretch of DNA with high CG sequences
(phosphodiester bond)
• Located at gene promoter
• Methylation leads to inactivation of many tumor
suppressor genes
• ~200 CpG islands that are methylated have been
identified in tumor DNA
• Epigenetic, biallelic silencing of MLH1
• Tumors highly correlated with a mutation of the
BRAF-kinase encoding gene (Chr 7)
• May be the molecular basis of progression of CRC in
the serrated pathway
Familial Adenomatous Polyposis
FAP
15
Familial Adenomatous Polyposis Syndrome
Oncogenesis - Familial Adenomatous Polyposis Syndrome
212
212
Familial Adenomatous Polyposis Syndrome
Oncogenesis
Oncogenesis -- Familial
Familial Adenomatous
Adenomatous Polyposis
Polyposis Syndrome
Syndrome
213
213
Familial Adenomatous Polyposis Syndrome
Oncogenesis - Familial Adenomatous Polyposis Syndrome
215
215
FAP
• Germline mutation of APC
– Autosomal dominant
• Polyps in teens, cancers in 20’s
– >100 polyps
• Gene testing, colectomy
• Surveillance of UGIT
• nccn.org
Attenuated FAP
aFAP
Attenuated FAP
21

Later onset (CRC ~age 50)

Few colonic adenomas

Not associated with CHRPE

UGI lesions

Associated with mutations at
extreme 5’, 3' ends of APC
gene, & exon 9A
Multiple Adenomatous Polyposis
• MAP
• Biallelic MUTYH mutation
– Autosomal recessive
• 10 polyps
• CRCS > age 50 years
Lynch Syndrome
(HNPCC)
• H.T. Lynch
– Jane Lynch
– Patrick Lynch
• Creighton University
JAMA 2011
Lynch Syndrome associated tumors
•
•
•
•
•
•
•
Colorectal
Endometrial
Ovarian
Genitourinary
Brain
Small bowel
Hepatobiliary
Diagnosing Lynch Syndrome
• Amsterdam criteria
– 3 relatives with cancer
– 2 generations involved
– 1 patient under age 50 Yeats
• Bethesda criteria
– Test familial and synchronous tumors for MSI
– MSI+ tumor in a patient under age 60 years
• Test all tumors for MSI+
Unique Pathology
• Carcinoma of Colon
– mucinous carcinomas
– signet cell carcinomas
– diploid tumors (on flow cytometry)
– TILs (tumor infiltrating lymphocytes)
• Adenoma
– Found in 20% of colons with CRC
– Jass and Stewart (Gut 33:783-786, 1992): adenomas in
LS were larger, more often villous, and had more high
grade dysplasia
– Consistent with our hypothesis that adenomas in LS
have a greater proclivity for malignant degeneration
than sporadic adenomas.
Colon Cancer Surveillance in LS
•
•
•
•
•
Adenoma removal is important
Surveillance must be at an earlier age and
more frequent than that for the general population
Colonoscopy to the cecum is important
Lesions under 1 cm are important
• Would prophylactic subtotal colectomy be better?
Do New Technologies Help?
•
•
•
•
•
•
•
Narrow band imaging colonoscopy
Magnifying colonoscopy
Chromoendoscopy
Autoflorescence
CT colography (computer-assisted)
MRI colography
Chemoprevention
Metachronous CRC in LS
• Overall incidence
22-41%
• Parry al. Metachronous colorectal cancer risk for mismatch repair
gene mutation carriers: the advantage of more extensive colon
surgery. Gut. 2011;60:950–957.
• Cumulative incidence after varying type of resection
– Segmental colectomy: 16%
– Subtotal colectomy:
2%
• de Vos tot Nederveen Cappel et al. Surveillance for hereditary
nonpolyposis colorectal cancer: a long-term study on 114 families.
Dis Colon Rectum. 2002;45:1588–1594.
DisColRec 2010
National Comprehensive Cancer Network
(http://nccn.org)
• Colonoscopy at age 20-25 or 10 years younger than
youngest age of cancer Dx
• Repeat every 1-2 years
• Annual urinalysis with cytology
• Endometrial and ovarian cancer screening age 3035; every 6-12 months; TAH-BSO
Serrated Polyposis Syndrome
•
•
•
•
“Hyperplastic polyposis”
? gene, but there is a familial syndrome
Associated with pancreatic cancer
May have rapid adenoma-carcinoma
sequence, similar to LS
Peutz-Jeghers Syndrome
PJS
42
Peutz-Jeghers Syndrome
• Inactivating mutations of tumor suppressor STK gene on
chromosome 19p13
• Hyperpigmented macules on buccal mucosa and lips,
gastrointestinal (respiratory tract, genitourinary tract)
hamartomatous polyps
• Increased risk of Gastrointestinal, breast, thyroid lung,
pancreatic, uterine cancer, Ovarian sex cord tumors Sertoli cell
testicular tumors
• Lifelong endoscopic, radiologic (SBS), ultrasound incl.
testicular surveillance
– ? Role of capsule endoscopy surveillance
43
Summary
•
•
•
•
•
Complete family history
High index of suspicion
Expert colonoscopy
Hereditary Cancer Institute
nccn.org