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Overview of Colorectal Cancer and CRC Screening Program
CDC CRC Control Program DHMH—Baltimore City March 29, 2010
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Colorectal Cancer Development and Prevention
Exposures (life style, occupation, and environment) Acquired (not inherited) genetic changes Inherited cancer susceptibility genes Asymptomatic Clinical Disease Disease Advanced Disease Convalescence or Death Birth Age Primary Prevention - Risk Factor reduction Colonoscopy with adenoma removal Secondary Prevention - Screening, early detection and diagnosis Tertiary Prevention Medical care
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CRC Incidence and Mortality
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Annual age-adjusted cancer incidence rates, US, 1975-2004
CA Cancer J Clin Jemal et al. 58 (2): (2008).
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Annual age-adjusted cancer death rates--Males, US, 1930-2004
CA Cancer J Clin Jemal et al. 58 (2): (2008).
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Annual age-adjusted cancer death rates--Females, US, 1930-2004
CA Cancer J Clin Jemal et al. 58 (2): (2008).
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CRC Screening
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Colorectal Cancer Screening Status of People Age 50 Years and Older Maryland Cancer Surveys,
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Provider Recommendation is KEY to Screening
80% of people 50+ in Maryland reported having a provider recommend endoscopy….. of those, 88% got screened Percent Screened with Endoscopy Of the 20% who did NOT report a provider recommendation….only 24% got screened Source: Maryland Cancer Survey, 2008
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Source: Maryland Cancer Survey, 2008
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Source: Maryland Cancer Survey, 2008
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Patient: Family and personal history Past screening Symptoms Primary Doctor: Referral Case Management and Communication Colonoscopist: Risk history Medication changes Prep instructions Post colonoscopy instructions Colonoscopy report Findings Recommendations Pathologist: Pathology report
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Who needs CRC screening?
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Colorectal Cancer Rates by Age and Sex Cancers of the Colon and Rectum: Average Annual Age-Specific SEER Incidence and U.S. Mortality Rates by Gender, Incidence Men Incidence Women Age recommended to start screening Mortality Men Mortality Women Source: SEER Cancer Statistics Review Colon and Rectum Cancer, SEER Incidence and U.S. Death Rates, Age-Adjusted and Age-Specific Rates, By Race and Sex (Rates based on SEER 17 areas)
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Colorectal Cancer Mortality Rates by Race and Sex in Maryland, 1998-2005
Age-adjusted rate per 100,000 population Black men Black women White men White women Source: NCHS Compressed Mortality File in CDC Wonder
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Colorectal Cancer Cases by Risk History
Sporadic (average risk) (65%–85%) (84, ,670 cases/yr.) We are rapidly gaining knowledge about who develops colorectal cancer. The majority of colorectal cancers, 65% to 85%, occur in people with no known cause (i.e., they are considered sporadic). 10% to 30% of cases of colorectal cancer occur in people who have a family member who has had a polyp or colorectal cancer. A small percentage of colorectal cancers occur as part of an inherited syndrome. Approximately 5% are associated with hereditary nonpolyposis colorectal cancers (HNPCC) and 1% are associated with familial adenomatous polyposis (FAP). Less than 0.1% are rare colorectal cancer syndromes. Family history (10%–30%) Rare syndromes (<0.1%) Hereditary nonpolyposis colorectal cancer (HNPCC) (5%) Familial adenomatous polyposis (FAP) (1%)
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Approx. lifetime risk of CRC
Group Approx. lifetime risk of CRC General Population 5-6% One first degree relative (FDR) with CRC 2--3-fold increased over general population Two First Degree Relatives (FDR)s with CRC 3--4-fold increased FDR with CRC diagnosed < 50 One second or third degree relative About 1.5-fold increased Two second degree relatives About 2--3-fold increased One FDR with adenoma About 2-fold increased Inflammatory Bowel Disease (ulcerative colitis and Crohn colitis) [7-10% have CRC after having ulcerative colitis for 20 years; then ~1%/year] Familial Adenomatous Polyposis Hereditary Non-polyposis Colorectal Cancer ~100% ~80+% Burt. Gastroenterology 2000;119:837-53 Winawer et al. Gastroenterology 203;124:
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Maryland Screening Recommendations: Medical Advisory Committee on CRC
Colonoscopy, every 10 years or FOBT annually, plus Flex sig., every 5 years FOBT if refuse endoscopy Colonoscopy (interval for repeat depends on risk, history, and prior results) Average Risk Increased Risk Maryland Screening Recommendations: Medical Advisory Committee on CRC
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Risk Category Age to Begin Screening
Average risk, asymptomatic 50 years Increased risk Family history CRC or adenoma (1 FDR <60 or 2 FDR any age) Colonoscopy at 40 years old or 10 years before the youngest case in the FDRs Family history CRC or adenoma in 1 FDR >= 60 Start screening (any method) at 40 years old Genetic syndrome: FAP HNPCC Puberty 21 years old Inflammatory bowel disease 8 years after start of pancolitis; 12-15 years after start of left sided colitis
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See Program Manual 1A, Attachment 1
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Colonoscopy or other screening test
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CA Cancer J Clin 58: 130-160 (May 2008)
New Guidelines Screening and Surveillance for the Early Detection of Colorectal Cancer and Adenomatous Polyps, 2008: A Joint Guideline from the American Cancer Society, the US Multi-Society Task Force on CRC, and the American College of Radiology CA Cancer J Clin 58: (May 2008)
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for the American Cancer Society Colorectal Cancer Advisory Group,
Bernard Levin, David A. Lieberman, Beth McFarland, Robert A. Smith, Durado Brooks, Kimberly S. Andrews, Chiranjeev Dash, Francis M. Giardiello, Seth Glick, Theodore R. Levin, Perry Pickhardt, Douglas K. Rex, Alan Thorson, Sidney J. Winawer, for the American Cancer Society Colorectal Cancer Advisory Group, the US Multi-Society Task Force, and the American College of Radiology Colon Cancer Committee
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Tests that Find Both Polyps and Cancer
Flexible sigmoidoscopy every 5 years Colonoscopy every 10 years Double contrast barium enema every 5 years CT colonography (virtual colonoscopy) every 5 years New Guidelines American Cancer Society, May 2008
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Tests that Primarily Find Cancer
Guaiac-based fecal occult blood testing (gFOBT) every year Fecal immunochemical test (FIT) every year Stool DNA test (unclear how often this is needed) New Guidelines American Cancer Society, May 2008
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New CRC Screening Guidelines American Cancer Society, May 2008
Beginning at age 50, men and women at average risk for CRC should use one of the screening tests The tests that are designed to find both early cancer and polyps are preferred if these tests are available to you and you are willing to have one of these more invasive tests. Talk to your doctor about which test is best for you.
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CRC Screening Program in Maryland
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Colonoscopy Equipment
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Long Handle Polypectomy Snare
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Polyp Snare
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Reusable Biopsy Forceps
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Hot Biopsy Forceps
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Disposable Retriever
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Prong Retriever
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Brush Biopsy
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Injection
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Colonoscopy Findings: Pathology
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Different types of polyps
Sessile polyp Tubulovillous adenoma Sessile polyp Hyperplastic polyp
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Different types of polyps
Sessile polyp Tubular adenoma Sessile polyp Tubulovillous adenoma Pedunculated polyp
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Different types of polyps
Pedunculated polyp Tubular adenoma Pedunculated polyp Tubular adenoma
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Copyright Mediamed art Milan (Italy)
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Wall of the colon under a low power microscope
Inside of the intestine (feces touch this surface) Atlas of Human Histology. Di Fiore. 1974, Lea& Febiger Mucosa Submucosa Muscularis Serosa
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Robbins Pathologic Basis of Disease, 6th Ed. Cotran, Kumar, and Collins WB Saunders p. 827
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Pedunculated adenoma HEAD OF POLYP SUBMUCOSA STALK RESECTION LINE
INTESTINAL WALL Muscularis
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Pedunculated adenoma HEAD OF POLYP SUBMUCOSA (lymphatics, arteries)
STALK RESECTION LINE INTESTINAL WALL Muscularis
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Polyp with no evidence of invasive carcinoma
2 1 3 Polyp with no evidence of invasive carcinoma SUBMUCOSA Low grade dysplasia Severe dysplasia Carcinoma in-situ, intramucosal carcinoma “High grade dysplasia”
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Polyp with invasive carcinoma
SUBMUCOSA INVASIVE CARCINOMA (invasion in submucosa which contains lymphatics, and arteries = potential for metastases)
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Polyp with invasive carcinoma: Pertinent pathology information
Tumor differentiation Lymphatic/vascular invasion Distance from resection line RESECTION LINE
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Sessile Polyps Usually submitted in several pieces
Difficult to determine the orientation of the specimen (“is the margin free of tumor?”) Other issues—type of polyp?
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Stage 1 Stage 2 Invasive carcinoma: Colon cancer staging
Pathology, Second Edition. Rubin and Farber. 1994:
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Cancer in the regional lymph nodes
Stage 3 Cancer in the regional lymph nodes Stage 4 Invasive carcinoma: Colon cancer staging Pathology, Second Edition. Rubin and Farber. 1994:
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Colonoscopy Findings: Adequacy of the Exam
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Adequacy of Colonoscopy
Cecum
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Adequate Colonoscopy? Reached the cecum? Adequate bowel prep?
Reached and explored? Reached and intubated the terminal ileum? Peeked into the cecum but couldn’t get in Adequate bowel prep? “Adequate to visualize any lesion >5mm” “Adequate enough” “Adequate” “Fair” “Excellent”
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Is the bowel prep “adequate”?
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Adequate prep?
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How can I dictate a picture of what I’m seeing here?
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What to think about if prep was inadequate:
Can you figure out why this patient might have had inadequate prep? Is there anything that could have been done differently? By the provider By your program By the patient Are there lessons learned for future clients and for this client’s next colonoscopy? Different instructions, different prep Discussion with the provider(s) Other
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Case Management
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Roles before Colonoscopy
Administrative Case Manager (nurse or other case manager in program) Obtain information for enrollment Schedule appointment and colonoscopy Instruct about bowel prep and procedures Solve any barriers (transportation, accompaniment home) Medical Case Manager Do an exam and clear the patient for colonoscopy Give instructions about medication changes if needed Instruct on bowel prep and procedures Schedule specifics about the colonoscopy
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Roles after Colonoscopy
Medical Case Manager (doctor who did the endoscopy) Give you a report of the colonoscopy Give you the recall interval Give the client the results Administrative Case Manager Obtain colonoscopy and pathology reports Review recall recommendation—is it correct per program standards? Enter data in computer Notify client of their results (verbal; written) Ask about complications Inform the primary care provider
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“Recall Interval” Recommended screening after initial screening-- rescreening or surveillance colonoscopy
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Keys to the right recall
Colonoscopy Report Pathology Report Recommendation based on guidelines Communication
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After first colonoscopy, then what?
Recall interval between colonoscopies will depend on: findings, risk history, and symptoms
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Interval between colonoscopies
IF Findings on colonoscopy were negative: No CRC; No adenomas; and No or only a few hyperplastic polyps, Average risk, and No CRC symptoms Recall interval will usually be 10 years See guidelines for recommended interval
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Interval between colonoscopies– based on findings
IF Findings showed: Inadequate colonoscopy didn’t reached cecum inadequate bowel preparation Cancer Adenomatous polyp(s)—need to know: Number Size Histology Completeness of removal Many hyperplastic polyps indicating Hyperplastic Polyposis Syndrome Recall interval will usually be LESS THAN 10 years See guidelines for recommended interval
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Interval between colonoscopies– based on risk history
IF first colonoscopy was negative BUT person is at increased risk because of family history: Interval may be LESS THAN 10 years See guidelines for recommended interval
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“several adenomas were found”
Example 53 year old patient had a colonoscopy: “several adenomas were found” What is the recommended recall interval? What else do you need to know to determine the interval? Who will tell the patient? Will anyone remind the patient when the next colonoscopy is needed?
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Answer: You need to know more about the Risk and Colonoscopy Results before you can set the right recall interval: Was the bowel preparation adequate? Was the cecum reached? How many adenomas were found? How big were the adenomas? Were they completely removed? What was the pathology? What is the family and personal risk history of the patient?
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Guidelines for Colonoscopy Surveillance after polypectomy--Winawer et al. CA--A Cancer Journal for Clinicians 56 (3) 143. (2006)
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See Program Manual 1A, Attachment 1
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Recall Interval Based on Finding of First Colonoscopy
“Inadequate” bowel prep (How inadequate was it?) Repeat right away or do other screening (e.g., DCBE) Didn’t reach or view cecum Repeat right away or do other screening to check cecum “Two adenomas” Need to know histology and size Any villous histology (villous, tubulovillous) or high grade dysplasia If completely removed, repeat in 3 years One or more adenomas >1 cm in size Repeat in 3 years Incomplete removal of adenomas Consider short recall interval (2-6 months) 1-2 tubular adenomas, <1 cm size Repeat in 5-10 years
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Recall Interval Based on Finding of First Colonoscopy
“Inadequate” bowel prep (How inadequate was it?) Repeat right away or do other screening (e.g., DCBE) Didn’t reach or view cecum Repeat right away or do other screening to check cecum “Two adenomas” Need to know histology and size Any villous histology (villous, tubulovillous) or high grade dysplasia If completely removed, repeat in 3 years One or more adenomas >1 cm in size Repeat in 3 years Incomplete removal of adenomas Consider short recall interval (2-6 months) 1-2 tubular adenomas, <1 cm size Repeat in 5-10 years
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Standards for Colonoscopy Reports--CoRADS*
Colonoscopy withdrawal time Findings Specimen(s) to path lab Impression Complications Pathology Recommendations, Follow-up Plan/Recall Other Date and Time Procedure Patient description Risk factors- ASA class Indications Consent signed Sedation Colonoscope Bowel Prep Reached cecum * Standardized colonoscopy reporting and data system (CoRADS): report of the Quality Assurance Task Group of the National Colorectal Cancer Roundtable, Lieberman et al., Gastrointestinal Endoscopy 2007; 65:
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Adequacy of First Colonoscopy Among 10,328
Adequacy of First Colonoscopy Among 10,328* Cycle 1 Colonoscopies Maryland 2000-December 2008 *10,328 of the 11,421 first colonoscopies had information on “adequacy” of the col. Source: DHMH, CCSC, Client Database (CDB), Ad-hoc report, 1/12/2009
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Colonoscopy Findings:
Reporting on Colonoscopy Findings: Number of masses, polyps, other lesions (try to give actual or estimated number rather than “several” or “multiple”) Findings: for EACH mass/polyp/lesion-- location size description tattoo biopsy(ies) taken method of each biopsy whether lesion completely removed or not whether there was piecemeal removal whether specimens retrieved whether saline lift used number of specimens sent to pathology
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How will your patients be reminded about their next colonoscopy?
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Communication Patient: Family and personal history Past screening
Symptoms Primary Doctor: Referral Case Management and Communication Colonoscopist: Risk history Medication changes Prep instructions Post colonoscopy instructions Colonoscopy report Findings Recommendations Pathologist: Pathology report
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Acknowledgements -Funding from the Maryland Cigarette Restitution Fund
-Staff and partners of Local Public Health Department Programs in MD and their contracted providers -- DHMH Center for Cancer Surveillance and Control (CCSC) Database and Quality assurance Surveillance and Epidemiology Unit University of Maryland at Baltimore Ciber, Inc. - CCSC Local PH Component - DHMH FHA, Information Technology -- Minority Outreach Technical Assistance Partners
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CDC Benchmarks for CRC Screening Screening Priority Population
Indicator Type, Number and Description CDC Benchmark Screening Priority Population 1 Percent of new clients screened who are at average risk for CRC ≥ 75% 2 Percent of average risk new clients screened who are aged 50 years and older ≥ 95% Completeness of Clinical Follow-up 3 Percent of abnormal test results with diagnostic follow-up completed ≥ 90% 4 Percent of diagnosed cancers with treatment initiated Timeliness of Clinical Follow-up 5 Percent of positive tests (FOBT/FIT, sigmoidoscopy, or DCBE) followed-up with colonoscopy within 90 days ≥ 80% 6 Percent of cancers diagnosed with treatment initiated within 60 days
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