Risk assessment tools for the symptomatic population Graham Radford-Smith Department of Gastroenterology and Hepatology Royal Brisbane and Women s

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Risk assessment tools for the symptomatic population Graham Radford-Smith Department of Gastroenterology and Hepatology Royal Brisbane and Women s Hospital GI inflammation IBD Group QIMR Berghofer Medical Research Institute

Overview The target population Symptoms Current strategies and endpoints The ideal tool or test Current data Research Institute 2

The Target Population Individuals with lower abdominal symptoms: abdominal pain altered bowel habit rectal bleeding unexplained weight loss Presenting to primary care physician Increasing prevalence Make up majority of patients referred for colonoscopy in Australia 1 over 90% including those on surveillance (as compared to those in a national screening programme) 1 Department of Health AG. Public Release of Linkable 10% Sample of Medicare Benefits Scheme (Medicare) and Pharmaceutical Benefits Scheme (PBS) Data 2016 2 National Bowel Cancer Screening Program: Monitoring Report [press release], 2016 Research Institute 3

Symptoms Poor indicator of underlying significant bowel pathology Lack of either sensitivity and/or specificity where colorectal cancer detection is primary endpoint 1 : Iron deficiency 0.13 (sensitivity) and 0.92 (specificity) rectal bleeding 0.44 (sensitivity) and 0.66 (specificity) Does not add much to demographics age, gender and other items in medical history 2 1 Jellema P, et al. Value of symptoms and additional diagnostic tests for colorectal cancer in primary care: systematic review and meta-analysis. BMJ (Clinical research ed). 2010;340:c1269 2 Adelstein BA, Irwig L, Macaskill P, Turner RM, Chan SF, Katelaris PH. Who needs colonoscopy to identify colorectal cancer? Bowel symptoms do not add substantially to age and other medical history. Aliment Pharmacol Ther. 2010;32(2):270-81 Research Institute 4

PPV of referral symptoms for CRC Symptom or sign at referral Positive predictive value (%) Palpable mass 50.0 Weight loss 14.3 Anaemia 9.0 Rectal bleeding 4.3 Abdominal pain 3.6 Diarrhoea 2.4 Altered bowel habit 2.2 Taken from Mowat, A et al. 755 referred cases who had undergone both FIT test and a colonoscopy. Research Institute 5

Current strategies Refinement and update of guidelines GP education But pick up rate of significant bowel pathology (SBP) (CRC, high risk adenoma, inflammatory bowel disease) in symptomatic patients remains low Simplicity of approach (FIT ± additional data) 1 Mowat C, Digby J, Strachan JA, Wilson R, Carey FA, Fraser CG, et al. Faecal haemoglobin and faecal calprotectin as indicators of bowel disease in patients presenting to primary care with bowel symptoms. Gut. 2016;65(9):1463-9 2 Cubiella J, Vega P, Salve M, Diaz-Ondina M, Alves MT, Quintero E, et al. Development and external validation of a faecal immunochemical test-based prediction model for colorectal cancer detection in symptomatic patients. BMC Med. 2016;14(1):128 Research Institute 6

The ideal diagnostic test Results are different between those with and without condition(s) of interest Patients with specific test results are more likely to have the condition(s) Results distinguish patients between those with and without condition(s) Patients undergoing the diagnostic test fare better than a similar group not undergoing test Sackett D, Haynes RB. BMJ 2002;324:539-41 Research Institute 7

Recent studies Embedded within a primary care setting FIT performance ± Faecal calprotectin (FC) CRC ± significant bowel pathology (SBP) 1043 subjects returned samples 755 of these went on to have a colonoscopy Research Institute 8

CRC in 28 (3.8%), HRA 41 (5.4%), SBP 103 (13.6%) Normal 241 (32%), diverticular disease 190 (25%) For any detectable faecal Hb, NPVs were: CRC 100% High Risk Adenoma 97.8% Inflammatory Bowel Disease 98.4% Adding faecal calprotectin (cut off 200) detected further 3 lesions (2 IBD, 1 HRA, no CRC) Research Institute 9

Simplicity and availability of test More scopes using any detectable FHb Rule out principal for symptomatic patients Requires further user acceptability testing Research Institute 10

Further studies Embedded in a secondary care setting Derivation and validation cohorts Faecal, blood tests and clinical variables Risk stratification of target population Primary endpoint CRC Research Institute 11

1572 subjects in derivation cohort: 214 CRC (13.6%) [3.8%*] 251 HRA (16%) [5.4%] 36 colitis (2.3%) [4.5%] 501 with SBP (31.8%) [13.6%] Study nurses administered questionnaire Stool and blood samples collected per protocol Prediction score identified 11 variables (from 32) *As compared to Mowat A, et al. Research Institute 12

Above table provides two score thresholds Greater number of variables 23% of subjects from primary care Can be used as a rule out test Cut-offs in score cut-offs in FIT Research Institute 13

Summary Active field of investigation A number of issues that require further study: single or multiple variables (simplicity) cut-offs, definitions (HRA, SBP) implementation real-life studies primary care and/or secondary care settings cost-effectiveness dealing with the fear factor Research Institute 14

Thank you www.qimrberghofer.edu.au

Low risk has predict score of < 3.5 High risk predict score of 5.6 Number needed to colonoscope increases Research Institute 16

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