Screening strategies

1. Screening strategies Tryggvi Björn Stefánsson Dept of Surgery Landspitali University Hospital

2. WHO criteria for population screening • The condition should be an important health problem. • Treatment must exist. • Latent or early symptomatic stage. • Target population. • Test validated and acceptable • Scientific evidence for program effectiveness (RCT) • Training • Quality control Wilson and Jungner 1968 and Anne Andermann, Ingeborg Blancquaert, Sylvie Beauchamp, Véronique Déry 2008

3. The Condition. Sojourn time Lead time Survival time 5-10 years 5-10 years Adenomatous Polyp CRCancer Symptoms Death 55 – 65 years 65 – 75 years Screening Screening

4. Goals of CRC screening • Detect cancer at an early, curable stage. • Detect and remove adenomatous polyps.

5. The Tests • 1) tests that primarily detect Cancer • gFOBT (guaiac-based fecal occult blood testing) • FIT (immunochemical-based FOBT) • sDNA (testing stool for exfoliated DNA) • 2) tests that can detect cancer and advanced lesions. • Double-contrast barium enema. • CT colonography. • Flexible sigmoidoscopy. • Colonoscopy.

6. gFOBT vs FIT gFOBT FIT • Guiac detects peroxidase activity. • Heme • Plant peroxidases. • Red meat • Vit C • Bleeding from all GI tract • Special diet for 3 days • 3 samples • Globin. • Human blood. • Detects only occult bleeding from the colon. • No dietary interference. • 1 sample

7. gFOBT Finland • Sensitivity for CRC: 55%* • Specificity : 98%* • Compliance: 71%* (23%-78%) • FOBT+ 2,1%* • Cancer in FOBT+ 8,2%* • Highest sensitivity (50%) in the stage of clinical diagnosis** • Very low sensitivity for precancerous lesions *H. Paimela et al. BJS 2010 ** Iris Lansdorp-Vogelaar, Cancer, 2009

8. FIT • FIT is superior to gFOBT in terms of compliance and detection of CRC and advanced adenomas. Rabeneck L et al. Can J Gastroenterol 2012. • FIT+ 5,2% • Cancer in FOBT+ 6% • High positivity rate, High sensitivity, low specificity . J. Faivre, European Journal of Cancer, 2012.

9. sDNA • Stool DNA test: Finds DNA markers for precancerous lesions and cancers. • Multicentered study from the Mayo clinic: • Sensitivity for CRC 85% Sensitivity for adenomas (≥1 cm) 54% • Specificity 90% • Still research • Expensive Ahlquist DA et al, Gastroenterology. 2012 Feb

10. DCBE • 48% sensitivity to detect polyps (> 1cm)compared to colonoscopy. Winawer, Gastroenterology, 2000. • Alternative for those who cannot undergo colonoscopy.

11. DCBE vs CT colonography • CT colonography: Lower radiation dose than DCBE. Neri et al Abd Imaging 2010. Sensitivity Specificity • CT colonogr 83% 86% • DCBE 60% 97% Johnson CD clinical gastroenterol and hepatol 2004 • CTC can be done without cleansing (stool tagging)

12. CT Colonography Polyps > 10mm Sensitivity 93% Specificity 97% Polyps 6-10mm Sensitivity 86% Specificity 86% Cancer Sensitivity 95,9% Halligan S et al Radiology 2005

13. Sigmoideoscopy • Investigates 60 cm. Removal of all polyps within 60 cm. • Followed by colonoscopy in case of advanced lesions. • Sensitivity and specificity for polyps and cancer is high. • Sensitivity for advanced lesions and CRC in the whole colon : 60-70% of the sensitivity of a colonoscopy. Lieberman NEJM 2000

14. Colonoscopy • Investigates all colon and removal of all polyps • The main screening method today • Required for confirmation of positive findings from other tests. • Gold standard for assessment of the efficacy of other screening methods.

15. Effectivity of Screening Programs Incidence Mortality • gFOBT 0 15% * (25%*) • FIT ? ? • sDNA ? ? • DCBE ? ? • CT colonography ? ? • Sigmoidoscopy 21% (33%) 33% (43%) ** • Colonoscopy [over 50%] [53%, 65% ] *Cohrane review, Hewitson P, Am J Gastroenterol. 2008 ** Wendy Atkins 2010

16. Colonoscopy Trials • Many cohort and case control studies on colonoscopy screening showing over 50% decrease in incidence and mortality. Incidence Mortality • Winawer et al NEJM 1993 76%, 88% and 90% • Müller AD et al Ann Int Med 1995 59% • Citarda F et al. Gut 2001 66% • Kahi CJ et alClin Gastroenterol et Hepatol 2009 67% 65% • Brenner H et al. Ann Int Med 2011 77%

17. Two randomized controlled trials • The Spanish trial • 55,000 individuals , 50–69 years • iFOBT or colonoscopy screening. • Started in 2008, results are expected in 2021, after 10 years of follow-up . • TheNordic–European Initiative on Colorectal Cancer (NordICC) • multicentre, multinational randomised trial • 66,000 individuals • colonoscopy or no screening. • started screening in 2009. A 15-year follow-up period after screening is planned,with an interimanalysis after 10 years,due about year 2022 • Landspitalinn has been in the NordICC group from the beginning and there has been an interest to contribute to the trial. • Due to opportunistic screening in Reykjavik we are probably not able to take part.

18. Opportunistic screening • Increasing ! • In 10 years ?? • Are we going to wait for 10 years ? • What if there is no difference ? • Is it ethical to fight pollution in the control groups ? • The control groups are going to be polluted whatever we do.

19. What can we do in Iceland ? • Registry for colonoscopies and polyps (histology) • Improve the quality of the colonoscopies: • Training programmes. • Quality control (Gastronet). • Start screening. • Preferably with colonoscopy. • Within the NordICC study.