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2. Individualised variable-interval risk-based screening in diabetic retinopathy: the ISDR research programme including RCT

Author

Harding, Simon, primary, Alshukri, Ayesh, additional, Appelbe, Duncan, additional, Broadbent, Deborah, additional, Burgess, Philip, additional, Byrne, Paula, additional, Cheyne, Christopher, additional, Eleuteri, Antonio, additional, Fisher, Anthony, additional, García-Fiñana, Marta, additional, Gabbay, Mark, additional, James, Marilyn, additional, Lathe, James, additional, Moitt, Tracy, additional, Rahni, Mehrdad Mobayen, additional, Roberts, John, additional, Sampson, Christopher, additional, Seddon, Daniel, additional, Stratton, Irene, additional, Thetford, Clare, additional, Vazquez-Arango, Pilar, additional, Vora, Jiten, additional, Wang, Amu, additional, and Williamson, Paula, additional

Published
2023
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3. Regulation of lymphocyte trafficking to the human gut in physiology and disease

Author

Wang, Amu, Marelli-Berg, Federica, and Orchard, Timothy

Subjects
616.079
Abstract

Memory T cell recruitment to the non-lymphoid tissue of the intestine (the gut lamina propria) requires the interactions between integrin a4B7 and its ligand Mucosal Addressin Cell Adhesion Molecule-1 (MAdCAM-1), which is exclusively expressed in the gut microvasculature. T cell homing to small intestine also requires the expression of chemokine receptor CCR9 on T cells, whose ligand - the gut chemokine CCL25 - is abundantly expressed in the small intestine. The a4B7 integrin and chemokine receptor CCR9 are known as the "homing" molecules whose expression is "imprinted" on T cells by intestinal dendritic cells during antigen presentation. In the first part of this thesis, data from in vitro studies showed that other than retinoic acid, soluble tissue-derived factors such as the gut chemokine CCL25 and T cell growth factor IL-2 also contributed to the induction of gut-homing receptor acquisition. Moreover, the expression of a4B7 integrin and CCR9 appeared to be modulated differently. The present study suggests that under the influence of tissue-derived factors, T cell acquisition of a4B7 integrin is the "default" response at steady state, and that only fully activated T cells are able to express high levels of CCR9. In the second part of this thesis, T cell gut homing was investigated in the context of disease, i.e. inflammatory bowel disease (IBD), including Crohn's disease (CD) and ulcerative colitis (UC). IBD is characterized by excessive lymphocyte infiltration to the intestine. By quantitatively analyzing peripheral blood and intestinal lymphocyte subsets, proportional changes in the circulating gut-homing T cells (a4B7+) was found to be associated with CD. In addition, my data suggest that downregulation of T cell receptor zeta chain (TcRC) correlates to disease severity in both CD and UC. Measuring TcRC expression may thus provide an additional tool for the monitoring and management of IBD.

Published
2012
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4. An electron-donor–acceptor complex between two intermediates enables a N–N bond cleavage cascade process to access 2,3-difunctionalized pyridines.

Author

Liu, Ya-Zhou, Chen, Yu, Wang, Amu, Shen, Zhongke, Zhou, Xueting, Zhang, Jichao, Jian, Yinxiang, and Ma, Xiaofeng

Subjects
ELECTRON donor-acceptor complexes, CHEMICAL amplification, SCISSION (Chemistry), ELECTRON donors, CHARGE exchange, DRUG derivatives, VISIBLE spectra
Abstract

Chemical transformation triggered by an electron donor–acceptor (EDA) complex without the addition of an exogenous stoichiometric electron donor/acceptor is rare. Herein, we report such a process to access 2,3-difunctionalized pyridines from readily available N-aminopyridiniums (1) and activated alkenes (2) promoted by visible light. This procedure offered multi-substituted pyridines in satisfactory yields at room temperature with broad functional group tolerance. The reaction can be easily performed on a gram scale without the loss of yield. The modification of bioactive molecules including derivatives of clinical drugs and natural products was demonstrated. Mechanistic studies and DFT calculations indicated that the formal [3 + 2] cycloaddition and aza-Michael addition between 1 and 2 generated tetrahydropyrazolo[1,5-a]pyridine and a new pyridinium salt, respectively. These two intermediates formed an EDA complex, which under visible-light illumination, triggered the following single electron transfer (SET)/N–N bond cleavage/C–N bond formation cascade process with high atom economy. [ABSTRACT FROM AUTHOR]

Published
2024
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5. Individualised variable-interval risk-based screening in diabetic retinopathy: the ISDR research programme including RCT

Author

Harding, Simon, Alshukri, Ayesh, Appelbe, Duncan, Broadbent, Deborah, Burgess, Philip, Byrne, Paula, Cheyne, Christopher, Eleuteri, Antonio, Fisher, Anthony, García-Fiñana, Marta, Gabbay, Mark, James, Marilyn, Lathe, James, Moitt, Tracy, Rahni, Mehrdad Mobayen, Roberts, John, Sampson, Christopher, Seddon, Daniel, Stratton, Irene, Thetford, Clare, Vazquez-Arango, Pilar, Vora, Jiten, Wang, Amu, Williamson, Paula, Harding, Simon, Alshukri, Ayesh, Appelbe, Duncan, Broadbent, Deborah, Burgess, Philip, Byrne, Paula, Cheyne, Christopher, Eleuteri, Antonio, Fisher, Anthony, García-Fiñana, Marta, Gabbay, Mark, James, Marilyn, Lathe, James, Moitt, Tracy, Rahni, Mehrdad Mobayen, Roberts, John, Sampson, Christopher, Seddon, Daniel, Stratton, Irene, Thetford, Clare, Vazquez-Arango, Pilar, Vora, Jiten, Wang, Amu, and Williamson, Paula

Abstract

Background Systematic annual screening for sight-threatening diabetic retinopathy is established in several countries but is resource intensive. Personalised (individualised) medicine offers the opportunity to extend screening intervals for people at low risk of progression and to target high-risk groups. However, significant concern exists among all stakeholders around the safety of changing programmes. Evidence to guide decisions is limited, with, to the best of our knowledge, no randomised controlled trials to date. Objectives To develop an individualised approach to screening for sight-threatening diabetic retinopathy and test its acceptability, safety, efficacy and cost-effectiveness. To estimate the changing incidence of patient-centred outcomes. Design A risk calculation engine; a randomised controlled trial, including a within-trial cost-effectiveness study; a qualitative acceptability study; and an observational epidemiological cohort study were developed. A patient and public group was involved in design and interpretation. Setting A screening programme in an English health district of around 450,000 people. Participants People with diabetes aged ≥ 12 years registered with primary care practices in Liverpool. Interventions The risk calculation engine estimated each participant’s risk at each visit of progression to screen-positive diabetic retinopathy (individualised intervention group) and allocated their next appointment at 6, 12 or 24 months (high, medium or low risk, respectively). Main outcome measures The randomised controlled trial primary outcome was attendance at first follow-up assessing the safety of individualised compared with usual screening. Secondary outcomes were overall attendance, rates of screen-positive and sight-threatening diabetic retinopathy, and measures of visual impairment. Cost-effectiveness outcomes were cost/quality-adjusted life year and incremental cost savings. Cohort study outcomes were rates of screen-positive diabetic r

Published
2023
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9. Incidence of sight-threatening diabetic retinopathy in an established urban screening programme: An 11-year cohort study

Author

Cheyne, Christopher P, Burgess, Philip I, Broadbent, Deborah M, Garcia-Finana, Marta, Stratton, Irene M, Criddle, Ticiana, Wang, Amu, Alshukri, Ayesh, Rahni, Mehrdad M, Vazquez-Arango, Pilar, Vora, Jiten P, Harding, Simon P, and Grp, ISDR Study

Subjects
Adult, Male, Pediatrics, medicine.medical_specialty, Adolescent, Urban Population, Endocrinology, Diabetes and Metabolism, Eye disease, Population, Type 2 diabetes, Young Adult, Endocrinology, Risk Factors, Internal Medicine, Prevalence, Medicine, Humans, Mass Screening, education, Child, Retrospective Studies, education.field_of_study, Diabetic Retinopathy, business.industry, Incidence (epidemiology), Incidence, Diabetic retinopathy, Middle Aged, medicine.disease, Annual Screening, United Kingdom, Diabetes Mellitus, Type 2, Female, business, Retinopathy, Cohort study, Follow-Up Studies, Forecasting
Abstract

AIMS Systematic annual screening to detect sight-threatening diabetic retinopathy (STDR) is established in the United Kingdom. We designed an observational cohort study to provide up-to-date data for policy makers and clinical researchers on incidence of key screening endpoints in people with diabetes attending one screening programme running for over 30 years. METHODS All people with diabetes aged ≥12 years registered with general practices in the Liverpool health district were offered inclusion. Data sources comprised: primary care (demographics, systemic risk factors), Liverpool Diabetes Eye Screening Programme (retinopathy grading), Hospital Eye Services (slit lamp biomicroscopy assessment of screen positives). RESULTS 133,366 screening episodes occurred in 28,384 people over 11 years. Overall incidences were: screen positive 6.7% (95% CI 6.5-6.8), screen positive for retinopathy 3.1% (3.0-3.1), unassessable images 2.6% (2.5-2.7), other significant eye diseases 1.0% (1.0-1.1). 1.6% (1.6-1.7) had sight-threatening retinopathy confirmed by slit lamp biomicroscopy. The annual incidence of screen positive and screen positive for retinopathy showed consistent declines from 8.8%-10.6% and 4.4%-4.6% in 2007/09 to 4.4%-6.8% and 2.3%-2.9% in 2013/17, respectively. Rates of STDR (true positive) were consistently below 2% after 2008/09. Screen positive rates were higher in first time attenders (9.9% [9.4-10.2] vs. 6.1% [6.0-6.2]) in part due to ungradeable images (4.1% vs. 2.3%) and other eye disease (2.4% vs. 0.8%). 4.5% (3.9-5.2) of previous non-attenders had sight-threatening retinopathy. Compared with people with type 2 diabetes, those with type 1 disease demonstrated higher rates of screen positive (11.9% vs. 6.0%) and STDR (6.4% vs. 1.2%). Overall prevalence of any retinopathy was 27.2% (27.0-27.4). CONCLUSIONS In an established screening programme with a stable population screen, positive rates show a consistent fall over time to a low level. Of those who are screen positive, fewer than 50% are screen positive for diabetic retinopathy. Most are due to sight threatening maculopathy. The annual incidence of STDR is under 2% suggesting future work on redefining screen positive and supporting extended intervals for people at low risk. Higher rates of screen positive and STDR are seen in first time attenders. Those who have never attended for screening should be specifically targeted.

Published
2021

11. Safety and cost-effectiveness of individualised screening for diabetic retinopathy: the ISDR open-label, equivalence RCT

Author

Broadbent, Deborah M., Wang, Amu, Cheyne, Christopher P., James, Marilyn, Lathe, James, Stratton, Irene M., Roberts, John, Moitt, Tracy, Vora, Jiten P., Gabbay, Mark, García-Fiñana, Marta, Harding, Simon P., and Thetford, Clare

Subjects
Adult, Systematic, medicine.medical_specialty, Adolescent, Cost effectiveness, Endocrinology, Diabetes and Metabolism, Cost-Benefit Analysis, A990, 030209 endocrinology & metabolism, Risk-based, Article, Personalised, law.invention, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Randomized controlled trial, law, Risk Factors, Diabetes mellitus, Internal Medicine, medicine, Humans, Mass Screening, Individualised, 030212 general & internal medicine, Aged, Aged, 80 and over, Diabetic Retinopathy, business.industry, Attendance, Diabetic retinopathy, Middle Aged, medicine.disease, Annual Screening, United Kingdom, Physical therapy, Screening, Variable interval, business, Health Utilities Index, Retinopathy
Abstract

Aims/hypothesis Using variable diabetic retinopathy screening intervals, informed by personal risk levels, offers improved engagement of people with diabetes and reallocation of resources to high-risk groups, while addressing the increasing prevalence of diabetes. However, safety data on extending screening intervals are minimal. The aim of this study was to evaluate the safety and cost-effectiveness of individualised, variable-interval, risk-based population screening compared with usual care, with wide-ranging input from individuals with diabetes. Methods This was a two-arm, parallel-assignment, equivalence RCT (minimum 2 year follow-up) in individuals with diabetes aged 12 years or older registered with a single English screening programme. Participants were randomly allocated 1:1 at baseline to individualised screening at 6, 12 or 24 months for those at high, medium and low risk, respectively, as determined at each screening episode by a risk-calculation engine using local demographic, screening and clinical data, or to annual screening (control group). Screening staff and investigators were observer-masked to allocation and interval. Data were collected within the screening programme. The primary outcome was attendance (safety). A secondary safety outcome was the development of sight-threatening diabetic retinopathy. Cost-effectiveness was evaluated within a 2 year time horizon from National Health Service and societal perspectives. Results A total of 4534 participants were randomised. After withdrawals, there were 2097 participants in the individualised screening arm and 2224 in the control arm. Attendance rates at first follow-up were equivalent between the two arms (individualised screening 83.6%; control arm 84.7%; difference −1.0 [95% CI −3.2, 1.2]), while sight-threatening diabetic retinopathy detection rates were non-inferior in the individualised screening arm (individualised screening 1.4%, control arm 1.7%; difference −0.3 [95% CI −1.1, 0.5]). Sensitivity analyses confirmed these findings. No important adverse events were observed. Mean differences in complete case quality-adjusted life-years (EuroQol Five-Dimension Questionnaire, Health Utilities Index Mark 3) did not significantly differ from zero; multiple imputation supported the dominance of individualised screening. Incremental cost savings per person with individualised screening were £17.34 (95% CI 17.02, 17.67) from the National Health Service perspective and £23.11 (95% CI 22.73, 23.53) from the societal perspective, representing a 21% reduction in overall programme costs. Overall, 43.2% fewer screening appointments were required in the individualised arm. Conclusions/interpretation Stakeholders involved in diabetes care can be reassured by this study, which is the largest ophthalmic RCT in diabetic retinopathy screening to date, that extended and individualised, variable-interval, risk-based screening is feasible and can be safely and cost-effectively introduced in established systematic programmes. Because of the 2 year time horizon of the trial and the long time frame of the disease, robust monitoring of attendance and retinopathy rates should be included in any future implementation. Trial registration ISRCTN 87561257 Funding The study was funded by the UK National Institute for Health Research.

Published
2021

13. Individualised screening for diabetic retinopathy: the ISDR study—rationale, design and methodology for a randomised controlled trial comparing annual and individualised risk-based variable-interval screening

Author

Broadbent, Deborah M, Sampson, Christopher J, Wang, Amu, Howard, Lola, Williams, Abigail E, Howlin, Susan U, Appelbe, Duncan, Moitt, Tracy, Cheyne, Christopher P, Rahni, Mehrdad Mobayen, Kelly, John, Collins, John, García-Fiñana, Marta, Stratton, Irene M, James, Marilyn, Harding, Simon P, and Thetford, Clare

Subjects
medicine.medical_specialty, Cost-Benefit Analysis, A990, 030209 endocrinology & metabolism, Workload, Risk Assessment, law.invention, 03 medical and health sciences, 0302 clinical medicine, Randomized controlled trial, Quality of life, law, Protocol, health economics, Humans, Medicine, 030212 general & internal medicine, Referral and Consultation, medical retina, Health policy, Probability, Randomized Controlled Trials as Topic, Research ethics, Diabetic Retinopathy, Health economics, business.industry, general diabetes, Health Policy, Attendance, General Medicine, medical ophthalmology, United Kingdom, Annual Screening, Ophthalmology, Diabetes Mellitus, Type 1, Diabetes Mellitus, Type 2, Family medicine, Disease Progression, Quality of Life, Risk assessment, business
Abstract

IntroductionCurrently, all people with diabetes (PWD) aged 12 years and over in the UK are invited for screening for diabetic retinopathy (DR) annually. Resources are not increasing despite a 5% increase in the numbers of PWD nationwide each year. We describe the rationale, design and methodology for a randomised controlled trial (RCT) evaluating the safety, acceptability and cost-effectiveness of personalised variable-interval risk-based screening for DR. This is the first randomised trial of personalised screening for DR and the largest ophthalmic RCT in the UK.Methods and analysisPWD attending seven screening clinics in the Liverpool Diabetic Eye Screening Programme were recruited into a single site RCT with a 1:1 allocation to individualised risk-based variable-interval or annual screening intervals. A risk calculation engine developed for the trial estimates the probability that an individual will develop referable disease (screen positive DR) within the next 6, 12 or 24 months using demographic, retinopathy and systemic risk factor data from primary care and screening programme records. Dynamic, secure, real-time data connections have been developed. The primary outcome is attendance for follow-up screening. We will test for equivalence in attendance rates between the two arms. Secondary outcomes are rates and severity of DR, visual outcomes, cost-effectiveness and health-related quality of life. The required sample size was 4460 PWD. Recruitment is complete, and the trial is in follow-up.Ethics and disseminationEthical approval was obtained from National Research Ethics Service Committee North West – Preston, reference 14/NW/0034. Results will be presented at international meetings and published in peer-reviewed journals. This pragmatic RCT will inform screening policy in the UK and elsewhere.Trial registration numberISRCTN87561257; Pre-results.

Published
2019

16. Personalized risk‐based screening for diabetic retinopathy: A multivariate approach versus the use of stratification rules

Author

Garcia-Finana, M, Hughes, David, Cheyne, CP, Broadbent, DM, wang, Wang, amu, komarek, Arnost, Stratton, Irene M, Mobayen-Rahni, Mehrdad, Alshukri, AS, Vora, jiten, and Harding, simon

Abstract

Aims To evaluate our proposed multivariate approach to identify patients who will develop sight‐threatening diabetic retinopathy (STDR) within a 1‐year screen interval, and explore the impact of simple stratification rules on prediction. Materials and methods A 7‐year dataset (2009‐2016) from people with diabetes (PWD) was analysed using a novel multivariate longitudinal discriminant approach. Level of diabetic retinopathy, assessed from routine digital screening photographs of both eyes, was jointly modelled using clinical data collected over time. Simple stratification rules based on retinopathy level were also applied and compared with the multivariate discriminant approach. Results Data from 13 103 PWD (49 520 screening episodes) were analysed. The multivariate approach accurately predicted whether patients developed STDR or not within 1 year from the time of prediction in 84.0% of patients (95% confidence interval [CI] 80.4‐89.7), compared with 56.7% (95% CI 55.5‐58.0) and 79.7% (95% CI 78.8‐80.6) achieved by the two stratification rules. While the stratification rules detected up to 95.2% (95% CI 92.2‐97.6) of the STDR cases (sensitivity) only 55.6% (95% CI 54.5‐56.7) of patients who did not develop STDR were correctly identified (specificity), compared with 85.4% (95% CI 80.4‐89.7%) and 84.0% (95% CI 80.7‐87.6%), respectively, achieved by the multivariate risk model. Conclusions Accurate prediction of progression to STDR in PWD can be achieved using a multivariate risk model whilst also maintaining desirable specificity. While simple stratification rules can achieve good levels of sensitivity, the present study indicates that their lower specificity (high false‐positive rate) would therefore necessitate a greater frequency of eye examinations.

Published
2019

17. Incidence of sight‐threatening diabetic retinopathy in an established urban screening programme: An 11‐year cohort study.

Author

Cheyne, Christopher P., Burgess, Philip I., Broadbent, Deborah M., García‐Fiñana, Marta, Stratton, Irene M, Criddle, Ticiana, Wang, Amu, Alshukri, Ayesh, Rahni, Mehrdad M., Vazquez‐Arango, Pilar, Vora, Jiten P., Harding, Simon P., Cheyne, Christopher P, Burgess, Philip, Broadbent, Deborah M, Vora, Jiten P, Harding, Simon P, Byrne, Paula, Fisher, Anthony C, and Gabbay, Mark

Subjects
EVALUATION of human services programs, SCIENTIFIC observation, CONFIDENCE intervals, AUDIOMETRY, RESEARCH funding, DIABETIC retinopathy, METROPOLITAN areas, LONGITUDINAL method
Abstract

Aims: Systematic annual screening to detect sight‐threatening diabetic retinopathy (STDR) is established in the United Kingdom. We designed an observational cohort study to provide up‐to‐date data for policy makers and clinical researchers on incidence of key screening endpoints in people with diabetes attending one screening programme running for over 30 years. Methods: All people with diabetes aged ≥12 years registered with general practices in the Liverpool health district were offered inclusion. Data sources comprised: primary care (demographics, systemic risk factors), Liverpool Diabetes Eye Screening Programme (retinopathy grading), Hospital Eye Services (slit lamp biomicroscopy assessment of screen positives). Results: 133,366 screening episodes occurred in 28,384 people over 11 years. Overall incidences were: screen positive 6.7% (95% CI 6.5–6.8), screen positive for retinopathy 3.1% (3.0–3.1), unassessable images 2.6% (2.5–2.7), other significant eye diseases 1.0% (1.0–1.1). 1.6% (1.6–1.7) had sight‐threatening retinopathy confirmed by slit lamp biomicroscopy. The annual incidence of screen positive and screen positive for retinopathy showed consistent declines from 8.8%–10.6% and 4.4%–4.6% in 2007/09 to 4.4%–6.8% and 2.3%–2.9% in 2013/17, respectively. Rates of STDR (true positive) were consistently below 2% after 2008/09. Screen positive rates were higher in first time attenders (9.9% [9.4–10.2] vs. 6.1% [6.0–6.2]) in part due to ungradeable images (4.1% vs. 2.3%) and other eye disease (2.4% vs. 0.8%). 4.5% (3.9–5.2) of previous non‐attenders had sight‐threatening retinopathy. Compared with people with type 2 diabetes, those with type 1 disease demonstrated higher rates of screen positive (11.9% vs. 6.0%) and STDR (6.4% vs. 1.2%). Overall prevalence of any retinopathy was 27.2% (27.0–27.4). Conclusions: In an established screening programme with a stable population screen, positive rates show a consistent fall over time to a low level. Of those who are screen positive, fewer than 50% are screen positive for diabetic retinopathy. Most are due to sight threatening maculopathy. The annual incidence of STDR is under 2% suggesting future work on redefining screen positive and supporting extended intervals for people at low risk. Higher rates of screen positive and STDR are seen in first time attenders. Those who have never attended for screening should be specifically targeted. [ABSTRACT FROM AUTHOR]

Published
2021
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18. Individualised screening for diabetic retinopathy: the ISDR study—rationale, design and methodology for a randomised controlled trial comparing annual and individualised risk-based variable-interval screening

Author

Broadbent, Deborah M, primary, Sampson, Christopher J, additional, Wang, Amu, additional, Howard, Lola, additional, Williams, Abigail E, additional, Howlin, Susan U, additional, Appelbe, Duncan, additional, Moitt, Tracy, additional, Cheyne, Christopher P, additional, Rahni, Mehrdad Mobayen, additional, Kelly, John, additional, Collins, John, additional, García-Fiñana, Marta, additional, Stratton, Irene M, additional, James, Marilyn, additional, and Harding, Simon P, additional

Published
2019
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19. Safety, Efficacy and Cost Effectiveness of Individualised Screening for Diabetic Retinopathy: The ISDR Randomised Controlled Trial

Author

Broadbent, Deborah, primary, Wang, Amu, additional, Cheyne, Christopher P., additional, James, Marilyn, additional, Lathe, James G., additional, Stratton, Irene M., additional, Roberts, John, additional, Moitt, Tracy, additional, Vora, Jiten P., additional, Gabbay, Mark, additional, García-Fiñana, Marta, additional, and Harding, Simon P., additional

Published
2019
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20. Personalized risk-based screening for diabetic retinopathy: A multivariate approach versus the use of stratification rules

Author

García-Fiñana, Marta, primary, Hughes, David M., additional, Cheyne, Christopher P., additional, Broadbent, Deborah M., additional, Wang, Amu, additional, Komárek, Arnošt, additional, Stratton, Irene M., additional, Mobayen-Rahni, Mehrdad, additional, Alshukri, Ayesh, additional, Vora, Jiten P., additional, and Harding, Simon P., additional

Published
2018
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21. Personalized risk‐based screening for diabetic retinopathy: A multivariate approach versus the use of stratification rules.

Author

García‐Fiñana, Marta, Hughes, David M., Cheyne, Christopher P., Broadbent, Deborah M., Wang, Amu, Komárek, Arnošt, Stratton, Irene M., Mobayen‐Rahni, Mehrdad, Alshukri, Ayesh, Vora, Jiten P., and Harding, Simon P.

Subjects
DIABETIC retinopathy, DIABETES complications, DIABETES, PEOPLE with diabetes, MULTIVARIATE analysis
Abstract

Aims: To evaluate our proposed multivariate approach to identify patients who will develop sight‐threatening diabetic retinopathy (STDR) within a 1‐year screen interval, and explore the impact of simple stratification rules on prediction. Materials and methods: A 7‐year dataset (2009‐2016) from people with diabetes (PWD) was analysed using a novel multivariate longitudinal discriminant approach. Level of diabetic retinopathy, assessed from routine digital screening photographs of both eyes, was jointly modelled using clinical data collected over time. Simple stratification rules based on retinopathy level were also applied and compared with the multivariate discriminant approach. Results: Data from 13 103 PWD (49 520 screening episodes) were analysed. The multivariate approach accurately predicted whether patients developed STDR or not within 1 year from the time of prediction in 84.0% of patients (95% confidence interval [CI] 80.4‐89.7), compared with 56.7% (95% CI 55.5‐58.0) and 79.7% (95% CI 78.8‐80.6) achieved by the two stratification rules. While the stratification rules detected up to 95.2% (95% CI 92.2‐97.6) of the STDR cases (sensitivity) only 55.6% (95% CI 54.5‐56.7) of patients who did not develop STDR were correctly identified (specificity), compared with 85.4% (95% CI 80.4‐89.7%) and 84.0% (95% CI 80.7‐87.6%), respectively, achieved by the multivariate risk model. Conclusions: Accurate prediction of progression to STDR in PWD can be achieved using a multivariate risk model whilst also maintaining desirable specificity. While simple stratification rules can achieve good levels of sensitivity, the present study indicates that their lower specificity (high false‐positive rate) would therefore necessitate a greater frequency of eye examinations. [ABSTRACT FROM AUTHOR]

Published
2019
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22. Regulation of lymphocyte trafficking to the human gut in physiology and disease

Author

Wang, Amu, Marelli-Berg, Federica, and Orchard, Timothy

Abstract

Memory T cell recruitment to the non-lymphoid tissue of the intestine (the gut lamina propria) requires the interactions between integrin a4B7 and its ligand Mucosal Addressin Cell Adhesion Molecule-1 (MAdCAM-1), which is exclusively expressed in the gut microvasculature. T cell homing to small intestine also requires the expression of chemokine receptor CCR9 on T cells, whose ligand - the gut chemokine CCL25 - is abundantly expressed in the small intestine. The a4B7 integrin and chemokine receptor CCR9 are known as the "homing" molecules whose expression is "imprinted" on T cells by intestinal dendritic cells during antigen presentation. In the first part of this thesis, data from in vitro studies showed that other than retinoic acid, soluble tissue-derived factors such as the gut chemokine CCL25 and T cell growth factor IL-2 also contributed to the induction of gut-homing receptor acquisition. Moreover, the expression of a4B7 integrin and CCR9 appeared to be modulated differently. The present study suggests that under the influence of tissue-derived factors, T cell acquisition of a4B7 integrin is the "default" response at steady state, and that only fully activated T cells are able to express high levels of CCR9. In the second part of this thesis, T cell gut homing was investigated in the context of disease, i.e. inflammatory bowel disease (IBD), including Crohn's disease (CD) and ulcerative colitis (UC). IBD is characterized by excessive lymphocyte infiltration to the intestine. By quantitatively analyzing peripheral blood and intestinal lymphocyte subsets, proportional changes in the circulating gut-homing T cells (a4B7+) was found to be associated with CD. In addition, my data suggest that downregulation of T cell receptor zeta chain (TcRC) correlates to disease severity in both CD and UC. Measuring TcRC expression may thus provide an additional tool for the monitoring and management of IBD.

Published
2011
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23. Introducing personalised risk based intervals in screening for diabetic retinopathy: development, implementation and assessment of safety, cost-effectiveness and patient experience (ISDR): a case study in the use of automated systems in trials

Author

Appelbe, Duncan, primary, Broadbent, Deborah, additional, Mobayen-Rahni, Mehrdad, additional, Eleuteri, Antonio, additional, Bennett, Abigail, additional, Moitt, Tracy, additional, Wang, Amu, additional, García-Fiñana, Marta, additional, Fisher, Anthony, additional, and Harding, Simon, additional

Published
2015
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28. 39-LB: Individualised Screening for Diabetic Retinopathy: The ISDR Study—A Randomised Controlled Trial of Safety, Efficacy, and Cost-Effectiveness.

Author

BROADBENT, DEBORAH MARY, WANG, AMU, CHEYNE, CHRISTOPHER P., LATHE, JAMES G., STRATTON, IRENE M., VORA, JITEN, GARCIA-FINANA, MARTA, JAMES, MARILYN, and HARDING, SIMON P.

Abstract

Background: Varying the intervals in retinopathy screening informed by personal risk offers reallocation of resources to better target high risk groups and address the increasing prevalence of diabetes. However, safety data especially on extended intervals is minimal. Aim: To evaluate the safety, efficacy and cost effectiveness (CE) of individualized variable-interval risk-based screening in a population setting compared to usual care. Methods: Masked 2 arm, parallel assignment, equivalence RCT (largest to date in screening) with independent trials unit monitoring in people with diabetes aged ≥12 years attending screening in a single English program. Randomization was 1:1 to individualized screening (active group; 6, 12 or 24 months for high, medium and low risk) determined by a risk calculation engine using real-time local demographic, retinal and clinical data, compared with annual screening (control). CE analysis measuring NHS and societal costs took a 2-year time horizon. Findings: 4534 participants entered the study - after withdrawals/loss to follow-up: active 2097; control 2224. Attendance rates at first follow-up visit (primary outcome, safety) were equivalent (per protocol analysis, 5% margin): active 83.6% control 84.7% (difference 1.0, 90% CI -0.8, 2.9). STDR detection rates were non-inferior (1.5% margin): active 1.43% control 1.71% (difference -0.28, CI -0.93, 0.36). Quality of life (EQ5D5L, HUI3) was not significantly different between the groups. Incremental cost saving per person was £18.75 (NHS cost) rising to £49.96 with societal costs. A 39.3% reduction in number of appointments was seen. Conclusions: All parties involved in diabetes care can be reassured that extended and personalized screening intervals can safely be introduced in established screening program. Scale-up with further validation outside a research setting is recommended. Views expressed are solely those of the authors. Disclosure: D.M. Broadbent: None. A. Wang: None. C.P. Cheyne: None. J.G. Lathe: None. I.M. Stratton: Consultant; Self; Novo Nordisk A/S. Research Support; Self; Bayer AG, Boehringer Ingelheim International GmbH. J. Vora: None. M. Garcia-Finana: None. M. James: None. S.P. Harding: None. Funding: UK National Institute for Health Research [ABSTRACT FROM AUTHOR]

Published
2019
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29. Regioselective Synthesis of Pyrazolo[1,5- a ]pyridine via TEMPO-Mediated [3 + 2] Annulation-Aromatization of N -Aminopyridines and α,β-Unsaturated Compounds.

Author

Wang A, Liu YZ, Shen Z, Qiao Z, and Ma X

Abstract

A TEMPO-mediated [3 + 2] annulation-aromatization protocol for the preparation of pyrazolo[1,5- a ]pyridines from N -aminopyridines and α,β-unsaturated compounds was developed. The procedure offered multisubstituted pyrazolo[1,5- a ]pyridines in good to excellent yield with high and predictable regioselectivity. The modification of marketed drugs including Loratadine, Abiraterone, and Metochalcone, and a one-pot three-step gram scale synthesis of key intermediate for the preparation of Selpercatinib were demonstrated. Mechanism studies show that TEMPO serves both as a Lewis acid and as an oxidant.

Published
2022
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30. Safety and cost-effectiveness of individualised screening for diabetic retinopathy: the ISDR open-label, equivalence RCT.

Author

Broadbent DM, Wang A, Cheyne CP, James M, Lathe J, Stratton IM, Roberts J, Moitt T, Vora JP, Gabbay M, García-Fiñana M, and Harding SP

Subjects
Adolescent, Adult, Aged, Aged, 80 and over, Humans, Middle Aged, Risk Factors, United Kingdom, Young Adult, Cost-Benefit Analysis, Diabetic Retinopathy diagnosis, Mass Screening adverse effects, Mass Screening economics
Abstract

Aims/hypothesis: Using variable diabetic retinopathy screening intervals, informed by personal risk levels, offers improved engagement of people with diabetes and reallocation of resources to high-risk groups, while addressing the increasing prevalence of diabetes. However, safety data on extending screening intervals are minimal. The aim of this study was to evaluate the safety and cost-effectiveness of individualised, variable-interval, risk-based population screening compared with usual care, with wide-ranging input from individuals with diabetes., Methods: This was a two-arm, parallel-assignment, equivalence RCT (minimum 2 year follow-up) in individuals with diabetes aged 12 years or older registered with a single English screening programme. Participants were randomly allocated 1:1 at baseline to individualised screening at 6, 12 or 24 months for those at high, medium and low risk, respectively, as determined at each screening episode by a risk-calculation engine using local demographic, screening and clinical data, or to annual screening (control group). Screening staff and investigators were observer-masked to allocation and interval. Data were collected within the screening programme. The primary outcome was attendance (safety). A secondary safety outcome was the development of sight-threatening diabetic retinopathy. Cost-effectiveness was evaluated within a 2 year time horizon from National Health Service and societal perspectives., Results: A total of 4534 participants were randomised. After withdrawals, there were 2097 participants in the individualised screening arm and 2224 in the control arm. Attendance rates at first follow-up were equivalent between the two arms (individualised screening 83.6%; control arm 84.7%; difference -1.0 [95% CI -3.2, 1.2]), while sight-threatening diabetic retinopathy detection rates were non-inferior in the individualised screening arm (individualised screening 1.4%, control arm 1.7%; difference -0.3 [95% CI -1.1, 0.5]). Sensitivity analyses confirmed these findings. No important adverse events were observed. Mean differences in complete case quality-adjusted life-years (EuroQol Five-Dimension Questionnaire, Health Utilities Index Mark 3) did not significantly differ from zero; multiple imputation supported the dominance of individualised screening. Incremental cost savings per person with individualised screening were £17.34 (95% CI 17.02, 17.67) from the National Health Service perspective and £23.11 (95% CI 22.73, 23.53) from the societal perspective, representing a 21% reduction in overall programme costs. Overall, 43.2% fewer screening appointments were required in the individualised arm., Conclusions/interpretation: Stakeholders involved in diabetes care can be reassured by this study, which is the largest ophthalmic RCT in diabetic retinopathy screening to date, that extended and individualised, variable-interval, risk-based screening is feasible and can be safely and cost-effectively introduced in established systematic programmes. Because of the 2 year time horizon of the trial and the long time frame of the disease, robust monitoring of attendance and retinopathy rates should be included in any future implementation., Trial Registration: ISRCTN 87561257 FUNDING: The study was funded by the UK National Institute for Health Research. Graphical abstract.

Published
2021
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31. T lymphocyte trafficking: molecules and mechanisms.

Author

Fu H, Wang A, Mauro C, and Marelli-Berg F

Subjects
Animals, Humans, Intestinal Mucosa cytology, Liver immunology, Lymphocyte Activation immunology, Lymphoid Tissue immunology, Mice, Phosphatidylinositol 3-Kinases physiology, Receptors, Chemokine immunology, Signal Transduction physiology, T-Lymphocytes, Regulatory physiology, Cell Movement immunology, Receptors, Lymphocyte Homing physiology, T-Lymphocytes physiology
Abstract

Coordinated migratory events are required for the development of effective and regulated immunity. Naïve T lymphocytes are programmed to recirculate predominantly in secondary lymphoid tissue by non-specific stimuli. In contrast, primed T cells must identify specific sites of antigen location in non-lymphoid tissue to exert targeted effector responses. Following priming, T cells acquire the ability to establish molecular interactions mediated by tissue-selective adhesion and chemokine receptors (homing receptors) that facilitate their access to specific organs. Recent studies have shown that an additional level of homing specificity is provided by the induction of T cell migration into the tissue by recognition of antigen displayed by the endothelium. In addition, co-stimulatory signals have been recently shown not only to regulate T cell activation and differentiation, but also to orchestrate the anatomy of the ensuing T cell response. Similarly, the characterization of migratory patterns by regulatory T cells has been the subject of many recent studies. Here, we provide an overview of key concepts, which have contribute to unraveling the complex anatomy of T cell immunity.

Published
2013
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