Your search keyword '"Choi, Chang-Ho Ryan"' showing total 15 results

1. UC Surveillance

Author

Choi, Chang-Ho Ryan, Al-Bakir, Ibrahim, Sheng Ding, Nik, editor, and De Cruz, Peter, editor

Published

2019

2. Systematic Review: The Impact and Importance of Body Composition in Inflammatory Bowel Disease

Author

Ding, Nik Sheng, primary, Tassone, Daniel, additional, Al Bakir, Ibrahim, additional, Wu, Kyle, additional, Thompson, Alexander J, additional, Connell, William R, additional, Malietzis, George, additional, Lung, Phillip, additional, Singh, Siddharth, additional, Choi, Chang-ho Ryan, additional, Gabe, Simon, additional, Jenkins, John T, additional, and Hart, Ailsa, additional

Published

2022

3. Multi-centre derivation and validation of a colitis-associated cancer risk prediction web-tool

Author

Curtius, Kit, Kabir, Misha, Al Bakir, Ibrahim, Choi, Chang-Ho Ryan, Hartono, Juanda, Johnson, Michael, East, James E, Lindsay, James O, Vega, Roser, Thomas-Gibson, Siwan, Wilson, Ana, Graham, Trevor A, and Hart, Ailsa

Abstract

Background and Aims Ulcerative colitis (UC) patients diagnosed with low-grade dysplasia (LGD) have increased risk of developing advanced neoplasia (AN; high-grade dysplasia or colorectal cancer). We aimed to develop and validate a predictor of AN risk in UC patients with LGD and create a visual web-tool to effectively communicate the risk. Methods In our retrospective multi-centre validated cohort study, adult UC patients with an index diagnosis of LGD, identified from four UK centres between 2001-2019, were followed until progression to AN. In the discovery cohort (n=248), a multivariate risk prediction model was derived from clinicopathological features using Cox regression. Validation used data from 3 external centres (n=201). The validated model was embedded in a web-based tool to calculate and illustrate patient-specific risk. Results Four endoscopic variables were significantly associated with future AN progression in the discovery cohort: endoscopically visible LGD > 1 cm (HR = 2.8; 95% CI 1.3-6.0), incomplete endoscopic resection (HR = 2.9; 95% CI 1.3-6.5), moderate/severe histological inflammation within 5 years of LGD diagnosis (HR = 3.0; 95% CI 1.3-6.7), and multifocality (HR = 2.8; 95% CI 1.3-6.1). In the validation cohort, this 4-variable model accurately predicted future AN cases with overall calibration Observed/Expected = 1 (95% CI 0.63-1.5), and achieved perfect specificity for the lowest predicted risk group over 13 years of follow-up. Conclusion Multi-cohort validation confirms that patients with large, unresected, and multifocal LGD and recent moderate/severe inflammation are at the highest risk of developing AN. Personalised risk prediction provided via the Ulcerative Colitis-Cancer Risk Estimator web-tool (www.UC-CaRE.uk) can be used to support treatment decision-making.

Published

2020

4. P115 Low grade dysplasia prognosis in the 21st century – a large multi-centre retrospective cohort study

Author

Kabir, Misha, primary, Curtius, Kit, additional, Al-Bakir, Ibrahim, additional, Choi, Chang-Ho Ryan, additional, Hartono, Juanda, additional, Johnson, Michael, additional, East, James E, additional, Lindsay, James O, additional, Vega, Roser, additional, Thomas-Gibson, Siwan, additional, Hart, Ailsa, additional, Graham, Trevor, additional, and Wilson, Ana, additional

Published

2021

5. O17 Multi-centre validation of UC-CaRE: a cancer risk prediction tool for colitis-associated low grade dysplasia

Author

Curtius, Kit, primary, Kabir, Misha, additional, Bakir, Ibrahim Al, additional, Choi, Chang-Ho Ryan, additional, Hartono, Juanda, additional, Johnson, Michael, additional, East, James E, additional, Lindsay, James O, additional, Vega, Roser, additional, Thomas-Gibson, Siwan, additional, Wilson, Ana, additional, Graham, Trevor A, additional, and Hart, Ailsa, additional

Published

2021

6. Evolutionary history of human colitis-associated colorectal cancer

Author

Baker, Ann-Marie, Cross, William, Curtius, Kit, Al Bakir, Ibrahim, Choi, Chang-Ho Ryan, Davis, Hayley Louise, Temko, Daniel, Biswas, Sujata, Martinez, Pierre, Williams, Marc J, Lindsay, James O, Feakins, Roger, Vega, Roser, Hayes, Stephen J, Tomlinson, Ian P M, McDonald, Stuart A C, Moorghen, Morgan, Silver, Andrew, East, James E, Wright, Nicholas A, Wang, Lai Mun, Rodriguez-Justo, Manuel, Jansen, Marnix, Hart, Ailsa L, Leedham, Simon J, and Graham, Trevor A

Subjects

Male, Colonoscopy/methods, colorectal cancer, Polymorphism, Single Nucleotide, Risk Assessment, Severity of Illness Index, dysplasia, Humans, Colitis, Ulcerative/genetics, Phylogeny, Manchester Cancer Research Centre, ResearchInstitutes_Networks_Beacons/mcrc, Inflammatory Bowel Disease, Cell Transformation, Neoplastic/genetics, Colonoscopy, Middle Aged, Polymorphism, Single Nucleotide/genetics, Colorectal Neoplasms/genetics, digestive system diseases, Gene Expression Regulation, Neoplastic, Cell Transformation, Neoplastic, IBD - genetics, Disease Progression, Colitis, Ulcerative, Female, Colorectal Neoplasms

Abstract

OBJECTIVE: IBD confers an increased lifetime risk of developing colorectal cancer (CRC), and colitis-associated CRC (CA-CRC) is molecularly distinct from sporadic CRC (S-CRC). Here we have dissected the evolutionary history of CA-CRC using multiregion sequencing.DESIGN: Exome sequencing was performed on fresh-frozen multiple regions of carcinoma, adjacent non-cancerous mucosa and blood from 12 patients with CA-CRC (n=55 exomes), and key variants were validated with orthogonal methods. Genome-wide copy number profiling was performed using single nucleotide polymorphism arrays and low-pass whole genome sequencing on archival non-dysplastic mucosa (n=9), low-grade dysplasia (LGD; n=30), high-grade dysplasia (HGD; n=13), mixed LGD/HGD (n=7) and CA-CRC (n=19). Phylogenetic trees were reconstructed, and evolutionary analysis used to reveal the temporal sequence of events leading to CA-CRC.RESULTS: 10/12 tumours were microsatellite stable with a median mutation burden of 3.0 single nucleotide alterations (SNA) per Mb, ~20% higher than S-CRC (2.5 SNAs/Mb), and consistent with elevated ageing-associated mutational processes. Non-dysplastic mucosa had considerable mutation burden (median 47 SNAs), including mutations shared with the neighbouring CA-CRC, indicating a precancer mutational field. CA-CRCs were often near triploid (40%) or near tetraploid (20%) and phylogenetic analysis revealed that copy number alterations (CNAs) began to accrue in non-dysplastic bowel, but the LGD/HGD transition often involved a punctuated 'catastrophic' CNA increase.CONCLUSIONS: Evolutionary genomic analysis revealed precancer clones bearing extensive SNAs and CNAs, with progression to cancer involving a dramatic accrual of CNAs at HGD. Detection of the cancerised field is an encouraging prospect for surveillance, but punctuated evolution may limit the window for early detection.

Published

2018

7. Multicentre derivation and validation of a colitis-associated colorectal cancer risk prediction web tool

Author

Curtius, Kit, Kabir, Misha, Al Bakir, Ibrahim, Choi, Chang Ho Ryan, Hartono, Juanda L, Johnson, Michael, East, James E, Lindsay, James O, Vega, Roser, Thomas-Gibson, Siwan, Warusavitarne, Janindra, Wilson, Ana, Graham, Trevor A, and Hart, Ailsa

Abstract

ObjectivePatients with ulcerative colitis (UC) diagnosed with low-grade dysplasia (LGD) have increased risk of developing advanced neoplasia (AN: high-grade dysplasia or colorectal cancer). We aimed to develop and validate a predictor of AN risk in patients with UC with LGD and create a visual web tool to effectively communicate the risk.DesignIn our retrospective multicentre validated cohort study, adult patients with UC with an index diagnosis of LGD, identified from four UK centres between 2001 and 2019, were followed until progression to AN. In the discovery cohort (n=246), a multivariate risk prediction model was derived from clinicopathological features using Cox regression. Validation used data from three external centres (n=198). The validated model was embedded in a web tool to calculate patient-specific risk.ResultsFour clinicopathological variables were significantly associated with AN progression in the discovery cohort: endoscopically visible LGD >1 cm (HR 2.7; 95% CI 1.2 to 5.9), unresectable or incomplete endoscopic resection (HR 3.4; 95% CI 1.6 to 7.4), moderate/severe histological inflammation within 5 years of LGD diagnosis (HR 3.1; 95% CI 1.5 to 6.7) and multifocality (HR 2.9; 95% CI 1.3 to 6.2). In the validation cohort, this four-variable model accurately predicted future AN cases with overall calibration Observed/Expected=1.01 (95% CI 0.64 to 1.52), and achieved 100% specificity for the lowest risk group over 13 years of available follow-up.ConclusionMulticohort validation confirms that patients with large, unresected, multifocal LGD and recent moderate/severe inflammation are at highest risk of developing AN. Personalised risk prediction provided via the Ulcerative Colitis-Cancer Risk Estimator (www.UC-CaRE.uk) can support treatment decision-making.

Published

2022

8. Evolutionary history of human colitis-associated colorectal cancer

Author

Baker, Ann-Marie, primary, Cross, William, additional, Curtius, Kit, additional, Al Bakir, Ibrahim, additional, Choi, Chang-Ho Ryan, additional, Davis, Hayley Louise, additional, Temko, Daniel, additional, Biswas, Sujata, additional, Martinez, Pierre, additional, Williams, Marc J, additional, Lindsay, James O, additional, Feakins, Roger, additional, Vega, Roser, additional, Hayes, Stephen J, additional, Tomlinson, Ian P M, additional, McDonald, Stuart A C, additional, Moorghen, Morgan, additional, Silver, Andrew, additional, East, James E, additional, Wright, Nicholas A, additional, Wang, Lai Mun, additional, Rodriguez-Justo, Manuel, additional, Jansen, Marnix, additional, Hart, Ailsa L, additional, Leedham, Simon J, additional, and Graham, Trevor A, additional

Published

2018

9. Abstract 5368: The evolutionary history of human colitis-associated colorectal cancer

Author

Baker, Ann-Marie, primary, Cross, William, additional, Curtius, Kathleen, additional, Choi, Chang-ho Ryan, additional, Al-Bakir, Ibrahim, additional, Temko, Daniel, additional, Martinez, Pierre, additional, Williams, Marc, additional, Davis, Hayley, additional, Biswas, Sujata, additional, Wright, Nicholas A., additional, Moorghen, Morgan, additional, Hayes, Stephen J., additional, Rodriguez-Justo, Manuel, additional, Silver, Andrew, additional, Wang, Lai Mun, additional, Jansen, Marnix, additional, Hart, Ailsa L., additional, Leedham, Simon J., additional, and Graham, Trevor A., additional

Published

2018

10. Cumulative burden of inflammation predicts colorectal neoplasia risk in ulcerative colitis: a large single-centre study

Author

Choi, Chang-Ho Ryan, primary, Al Bakir, Ibrahim, additional, Ding, Nik-Sheng (John), additional, Lee, Gui-Han, additional, Askari, Alan, additional, Warusavitarne, Janindra, additional, Moorghen, Morgan, additional, Humphries, Adam, additional, Ignjatovic-Wilson, Ana, additional, Thomas-Gibson, Siwan, additional, Saunders, Brian P, additional, Rutter, Matthew D, additional, Graham, Trevor A, additional, and Hart, Ailsa L, additional

Published

2017

11. Cumulative burden of inflammation predicts colorectal neoplasia risk in ulcerative colitis: a large single-centre study

Author

Choi, Chang-Ho Ryan, Al Bakir, Ibrahim, Ding, Nik-Sheng (John), Lee, Gui-Han, Askari, Alan, Warusavitarne, Janindra, Moorghen, Morgan, Humphries, Adam, Ignjatovic-Wilson, Ana, Thomas-Gibson, Siwan, Saunders, Brian P, Rutter, Matthew D, Graham, Trevor A, and Hart, Ailsa L

Abstract

ObjectiveUlcerative colitis (UC) is a dynamic disease with its severity continuously changing over time. We hypothesised that the risk of colorectal neoplasia (CRN) in UC closely follows an actuarial accumulative inflammatory burden, which is inadequately represented by current risk stratification strategies.DesignThis was a retrospective single-centre study. Patients with extensive UC who were under colonoscopic surveillance between 2003 and 2012 were studied. Each surveillance episode was scored for a severity of microscopic inflammation (0=no activity; 1=mild; 2=moderate; 3=severe activity). The cumulative inflammatory burden (CIB) was defined as sum of: average score between each pair of surveillance episodes multiplied by the surveillance interval in years. Potential predictors were correlated with CRN outcome using time-dependent Cox regression.ResultsA total of 987 patients were followed for a median of 13 years (IQR, 9–18), 97 (9.8%) of whom developed CRN. Multivariate analysis showed that the CIB was significantly associated with CRN development (HR, 2.1 per 10-unit increase in CIB (equivalent of 10, 5 or 3.3 years of continuous mild, moderate or severe active microscopic inflammation); 95% CI 1.4 to 3.0; P<0.001). Reflecting this, while inflammation severity based on the most recent colonoscopy alone was not significant (HR, 0.9 per-1-unit increase in severity; 95% CI 0.7 to 1.2; P=0.5), a mean severity score calculated from all colonoscopies performed in preceding 5 years was significantly associated with CRN risk (HR, 2.2 per-1-unit increase; 95% CI 1.6 to 3.1; P<0.001).ConclusionThe risk of CRN in UC is significantly associated with accumulative inflammatory burden. An accurate CRN risk stratification should involve assessment of multiple surveillance episodes to take this into account.

Published

2019

12. Evolutionary history of human colitis-associated colorectal cancer

Author

Baker, Ann-Marie, Cross, William, Curtius, Kit, Al Bakir, Ibrahim, Choi, Chang-Ho Ryan, Davis, Hayley Louise, Temko, Daniel, Biswas, Sujata, Martinez, Pierre, Williams, Marc J, Lindsay, James O, Feakins, Roger, Vega, Roser, Hayes, Stephen J, Tomlinson, Ian P M, McDonald, Stuart A C, Moorghen, Morgan, Silver, Andrew, East, James E, Wright, Nicholas A, Wang, Lai Mun, Rodriguez-Justo, Manuel, Jansen, Marnix, Hart, Ailsa L, Leedham, Simon J, and Graham, Trevor A

Abstract

ObjectiveIBD confers an increased lifetime risk of developing colorectal cancer (CRC), and colitis-associated CRC (CA-CRC) is molecularly distinct from sporadic CRC (S-CRC). Here we have dissected the evolutionary history of CA-CRC using multiregion sequencing.DesignExome sequencing was performed on fresh-frozen multiple regions of carcinoma, adjacent non-cancerous mucosa and blood from 12 patients with CA-CRC (n=55 exomes), and key variants were validated with orthogonal methods. Genome-wide copy number profiling was performed using single nucleotide polymorphism arrays and low-pass whole genome sequencing on archival non-dysplastic mucosa (n=9), low-grade dysplasia (LGD; n=30), high-grade dysplasia (HGD; n=13), mixed LGD/HGD (n=7) and CA-CRC (n=19). Phylogenetic trees were reconstructed, and evolutionary analysis used to reveal the temporal sequence of events leading to CA-CRC.Results10/12 tumours were microsatellite stable with a median mutation burden of 3.0 single nucleotide alterations (SNA) per Mb, ~20% higher than S-CRC (2.5 SNAs/Mb), and consistent with elevated ageing-associated mutational processes. Non-dysplastic mucosa had considerable mutation burden (median 47 SNAs), including mutations shared with the neighbouring CA-CRC, indicating a precancer mutational field. CA-CRCs were often near triploid (40%) or near tetraploid (20%) and phylogenetic analysis revealed that copy number alterations (CNAs) began to accrue in non-dysplastic bowel, but the LGD/HGD transition often involved a punctuated ‘catastrophic’ CNA increase.ConclusionsEvolutionary genomic analysis revealed precancer clones bearing extensive SNAs and CNAs, with progression to cancer involving a dramatic accrual of CNAs at HGD. Detection of the cancerised field is an encouraging prospect for surveillance, but punctuated evolution may limit the window for early detection.

Published

2019

13. Low-Grade Dysplasia in Ulcerative Colitis: Risk Factors for Developing High-Grade Dysplasia or Colorectal Cancer

Author

Choi, Chang-ho Ryan, primary, Ignjatovic-Wilson, Ana, additional, Askari, Alan, additional, Lee, Gui Han, additional, Warusavitarne, Janindra, additional, Moorghen, Morgan, additional, Thomas-Gibson, Siwan, additional, Saunders, Brian P, additional, Rutter, Matthew D, additional, Graham, Trevor A, additional, and Hart, Ailsa L, additional

Published

2015

14. Forty-Year Analysis of Colonoscopic Surveillance Program for Neoplasia in Ulcerative Colitis: An Updated Overview

Author

Choi, Chang-Ho Ryan, primary, Rutter, Matthew D, additional, Askari, Alan, additional, Lee, Gui Han, additional, Warusavitarne, Janindra, additional, Moorghen, Morgan, additional, Thomas-Gibson, Siwan, additional, Saunders, Brian P, additional, Graham, Trevor A, additional, and Hart, Ailsa L, additional

Published

2015

15. Subclinical miliary Mycobacterium bovis following BCG immunotherapy for transitional cell carcinoma of the bladder.

Author

Choi CH, Lee SO, and Smith G

Subjects

Antitubercular Agents therapeutic use, Diagnosis, Differential, Humans, Male, Middle Aged, Tuberculosis, Miliary diagnosis, Tuberculosis, Miliary drug therapy, Adjuvants, Immunologic adverse effects, BCG Vaccine adverse effects, Carcinoma, Transitional Cell drug therapy, Mycobacterium bovis, Tuberculosis, Miliary etiology, Urinary Bladder Neoplasms drug therapy

Abstract

The authors present an unusual case of a 51-year-old man who developed relatively mild non-specific symptoms following intravesical BCG instillation for superficial transitional cell carcinoma of the bladder, with radiological investigations demonstrating typical features of miliary tuberculosis (TB). Transbronchial biopsy showed small foci of poorly formed granuloma suggestive of Mycobacterium infection. The patient's respiratory symptoms only became apparent 7 days after discharge having had 4 weeks of unremarkable inpatient stay where he remained clinically well. Prompt anti-TB treatment resulted in a remarkable improvement in his symptoms and radiological appearance, supporting the diagnosis of disseminated Mycobacterium bovis infection. This case highlights the importance of recognising miliary M bovis as a potential complication in patients receiving BCG immunotherapy, and that the disease course can be subclinical with delayed onset of symptoms.

Published

2014