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Publications
in Top 10% Journal Percentiles
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56.3%
Corporate
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8.8%
Annual research
funding
£5m+
Data for 2020-2025 from SciVal
Selected Publications
2022
2.
Cianci, Nicole; Subhani, Mohsan; Hill, Trevor; Khanna, Amardeep; Zheng, Dong; Sheth, Abhishek; Crooks, Colin; Aithal, Guruprasad P
Prognostic non-invasive biomarkers for all-cause mortality in non-alcoholic fatty liver disease: A systematic review and meta-analysis Journal Article
In: World J. Hepatol., vol. 14, no. 5, pp. 1025–1037, 2022.
Abstract | Tags: biomarkers, mortality, Non-invasive, Nonalcoholic fatty liver disease, Nonalcoholic steatohepatitis, Prognosis
@article{Cianci2022-xi,
title = {Prognostic non-invasive biomarkers for all-cause mortality in
non-alcoholic fatty liver disease: A systematic review and
meta-analysis},
author = {Nicole Cianci and Mohsan Subhani and Trevor Hill and Amardeep Khanna and Dong Zheng and Abhishek Sheth and Colin Crooks and Guruprasad P Aithal},
year = {2022},
date = {2022-05-01},
journal = {World J. Hepatol.},
volume = {14},
number = {5},
pages = {1025\textendash1037},
publisher = {Baishideng Publishing Group Inc.},
abstract = {BACKGROUND: Non-alcoholic fatty liver disease (NAFLD) represents
a growing public health concern, with patients having higher
risk of morbidity and mortality. It has a considerably high
prevalence in the general population, estimated 20%-40% in
Europe, and is asymptomatic until late in the disease course. It
is therefore important to identify and validate tools that
predict hard outcomes such as mortality for use in clinical
practice in risk-stratifying NAFLD patients. AIM: To evaluate
available evidence on the use of non-invasive test(s) as
prognostic factors for mortality in NAFLD. METHODS: We performed
electronic searches of Medline and EMBASE (Ovid) until 7th
January 2021 of studies in NAFLD populations. Prognostic markers
included serum biomarkers, non-invasive scoring systems, and
non-invasive imaging. The population included all spectrums of
disease severity, including NAFLD and non-alcoholic
steatohepatitis (NASH). Outcomes included all-cause, and
cardiovascular mortality. All non-invasive tests were
synthesised in a narrative systematic review. Finally, we
conducted a meta-analysis of non-invasive scoring systems for
predicting all-cause and cardiovascular mortality, calculating
pooled hazard ratios and 95% confidence (STATA 16.1). RESULTS:
Database searches identified 2850 studies - 24 were included. 16
studies reported non-invasive scoring systems, 10 studies
reported individual biomarkers, and 1 study reported imaging
modalities. 4 studies on non-invasive scoring systems (6324
participants) had data available for inclusion in the
meta-analysis. The non-invasive scoring system that performed
best at predicting all-cause mortality was NAFLD fibrosis score
(NFS) [pHR 3.07 (1.62-5.83)], followed by fibrosis-4 index [pHR
3.06 (1.54-6.07)], BARD [pHR 2.87 (1.27-6.46)], and AST to
platelet ratio index [pHR 1.90 (1.32-2.73)]. NFS was also
prognostic of cardiovascular-related mortality [pHR 3.09
(1.78-5.34)]. CONCLUSION: This study reaffirms that non-invasive
scoring systems, especially NFS, are reliable prognostic markers
of all-cause mortality and cardiovascular mortality in NAFLD
patients. These findings can inform clinical practice in risk
stratifying NAFLD patients.},
keywords = {biomarkers, mortality, Non-invasive, Nonalcoholic fatty liver disease, Nonalcoholic steatohepatitis, Prognosis},
pubstate = {published},
tppubtype = {article}
}
BACKGROUND: Non-alcoholic fatty liver disease (NAFLD) represents
a growing public health concern, with patients having higher
risk of morbidity and mortality. It has a considerably high
prevalence in the general population, estimated 20%-40% in
Europe, and is asymptomatic until late in the disease course. It
is therefore important to identify and validate tools that
predict hard outcomes such as mortality for use in clinical
practice in risk-stratifying NAFLD patients. AIM: To evaluate
available evidence on the use of non-invasive test(s) as
prognostic factors for mortality in NAFLD. METHODS: We performed
electronic searches of Medline and EMBASE (Ovid) until 7th
January 2021 of studies in NAFLD populations. Prognostic markers
included serum biomarkers, non-invasive scoring systems, and
non-invasive imaging. The population included all spectrums of
disease severity, including NAFLD and non-alcoholic
steatohepatitis (NASH). Outcomes included all-cause, and
cardiovascular mortality. All non-invasive tests were
synthesised in a narrative systematic review. Finally, we
conducted a meta-analysis of non-invasive scoring systems for
predicting all-cause and cardiovascular mortality, calculating
pooled hazard ratios and 95% confidence (STATA 16.1). RESULTS:
Database searches identified 2850 studies - 24 were included. 16
studies reported non-invasive scoring systems, 10 studies
reported individual biomarkers, and 1 study reported imaging
modalities. 4 studies on non-invasive scoring systems (6324
participants) had data available for inclusion in the
meta-analysis. The non-invasive scoring system that performed
best at predicting all-cause mortality was NAFLD fibrosis score
(NFS) [pHR 3.07 (1.62-5.83)], followed by fibrosis-4 index [pHR
3.06 (1.54-6.07)], BARD [pHR 2.87 (1.27-6.46)], and AST to
platelet ratio index [pHR 1.90 (1.32-2.73)]. NFS was also
prognostic of cardiovascular-related mortality [pHR 3.09
(1.78-5.34)]. CONCLUSION: This study reaffirms that non-invasive
scoring systems, especially NFS, are reliable prognostic markers
of all-cause mortality and cardiovascular mortality in NAFLD
patients. These findings can inform clinical practice in risk
stratifying NAFLD patients.
a growing public health concern, with patients having higher
risk of morbidity and mortality. It has a considerably high
prevalence in the general population, estimated 20%-40% in
Europe, and is asymptomatic until late in the disease course. It
is therefore important to identify and validate tools that
predict hard outcomes such as mortality for use in clinical
practice in risk-stratifying NAFLD patients. AIM: To evaluate
available evidence on the use of non-invasive test(s) as
prognostic factors for mortality in NAFLD. METHODS: We performed
electronic searches of Medline and EMBASE (Ovid) until 7th
January 2021 of studies in NAFLD populations. Prognostic markers
included serum biomarkers, non-invasive scoring systems, and
non-invasive imaging. The population included all spectrums of
disease severity, including NAFLD and non-alcoholic
steatohepatitis (NASH). Outcomes included all-cause, and
cardiovascular mortality. All non-invasive tests were
synthesised in a narrative systematic review. Finally, we
conducted a meta-analysis of non-invasive scoring systems for
predicting all-cause and cardiovascular mortality, calculating
pooled hazard ratios and 95% confidence (STATA 16.1). RESULTS:
Database searches identified 2850 studies - 24 were included. 16
studies reported non-invasive scoring systems, 10 studies
reported individual biomarkers, and 1 study reported imaging
modalities. 4 studies on non-invasive scoring systems (6324
participants) had data available for inclusion in the
meta-analysis. The non-invasive scoring system that performed
best at predicting all-cause mortality was NAFLD fibrosis score
(NFS) [pHR 3.07 (1.62-5.83)], followed by fibrosis-4 index [pHR
3.06 (1.54-6.07)], BARD [pHR 2.87 (1.27-6.46)], and AST to
platelet ratio index [pHR 1.90 (1.32-2.73)]. NFS was also
prognostic of cardiovascular-related mortality [pHR 3.09
(1.78-5.34)]. CONCLUSION: This study reaffirms that non-invasive
scoring systems, especially NFS, are reliable prognostic markers
of all-cause mortality and cardiovascular mortality in NAFLD
patients. These findings can inform clinical practice in risk
stratifying NAFLD patients.
2020
1.
Wilde, Craig; Awad, Mary; Giannouladis, Konstantinos; Lakshmanan, Arun; Yeung, Aaron Ming-Hon; Dua, Harminder; Amoaku, Winfried M K
Natural course of adult-onset vitelliform lesions in eyes with and without comorbid subretinal drusenoid deposits Journal Article
In: Int. Ophthalmol., vol. 40, no. 6, pp. 1501–1508, 2020.
Abstract | Tags: Adult-onset vitelliform lesions, Adult-onset foveomacular vitelliform dystrophy, Prognosis, Pseudodrusen, Reticular drusen, Subretinal drusenoid deposits
@article{Wilde2020-td,
title = {Natural course of adult-onset vitelliform lesions in eyes with
and without comorbid subretinal drusenoid deposits},
author = {Craig Wilde and Mary Awad and Konstantinos Giannouladis and Arun Lakshmanan and Aaron Ming-Hon Yeung and Harminder Dua and Winfried M K Amoaku},
year = {2020},
date = {2020-06-01},
journal = {Int. Ophthalmol.},
volume = {40},
number = {6},
pages = {1501\textendash1508},
publisher = {Springer Science and Business Media LLC},
abstract = {PURPOSE: Adult vitelliform lesions (AVL) are associated with age
related macular degeneration (AMD) and subretinal drusenoid
deposits (SRDD). We evaluated the natural course of AVL,
assessing the influence of SRDD on disease progression, visual
function and incidence of macular atrophy (MA) and choroidal
neovascular membranes (CNVM). METHODS: A retrospective cohort
study was conducted between January 2011 and March 2016.
Demographic, clinical and imaging data from 26 consecutive AVL
patients were analysed following case note review. Optical
coherence tomography images were graded for SRDD and patients
divided into those with/without SRDD. Outcomes included
presenting/changes in best corrected visual acuity (BCVA) and
incidence of MA/CNVM. RESULTS: Mean age was 78.6 $±$ 7.6
years. Mean follow-up was 51.5 $±$ 25.6 months. Twelve
patients (46.2%) had SRDD at presentation with 3 more (11.5%)
developing them. Subjects with SRDD were older (mean 81.7 $±$ 6.1 years vs 74.3 $±$ 7.6 year},
keywords = {Adult-onset vitelliform lesions, Adult-onset foveomacular vitelliform dystrophy, Prognosis, Pseudodrusen, Reticular drusen, Subretinal drusenoid deposits},
pubstate = {published},
tppubtype = {article}
}
PURPOSE: Adult vitelliform lesions (AVL) are associated with age
related macular degeneration (AMD) and subretinal drusenoid
deposits (SRDD). We evaluated the natural course of AVL,
assessing the influence of SRDD on disease progression, visual
function and incidence of macular atrophy (MA) and choroidal
neovascular membranes (CNVM). METHODS: A retrospective cohort
study was conducted between January 2011 and March 2016.
Demographic, clinical and imaging data from 26 consecutive AVL
patients were analysed following case note review. Optical
coherence tomography images were graded for SRDD and patients
divided into those with/without SRDD. Outcomes included
presenting/changes in best corrected visual acuity (BCVA) and
incidence of MA/CNVM. RESULTS: Mean age was 78.6 $±$ 7.6
years. Mean follow-up was 51.5 $±$ 25.6 months. Twelve
patients (46.2%) had SRDD at presentation with 3 more (11.5%)
developing them. Subjects with SRDD were older (mean 81.7 $±$ 6.1 years vs 74.3 $±$ 7.6 year
related macular degeneration (AMD) and subretinal drusenoid
deposits (SRDD). We evaluated the natural course of AVL,
assessing the influence of SRDD on disease progression, visual
function and incidence of macular atrophy (MA) and choroidal
neovascular membranes (CNVM). METHODS: A retrospective cohort
study was conducted between January 2011 and March 2016.
Demographic, clinical and imaging data from 26 consecutive AVL
patients were analysed following case note review. Optical
coherence tomography images were graded for SRDD and patients
divided into those with/without SRDD. Outcomes included
presenting/changes in best corrected visual acuity (BCVA) and
incidence of MA/CNVM. RESULTS: Mean age was 78.6 $±$ 7.6
years. Mean follow-up was 51.5 $±$ 25.6 months. Twelve
patients (46.2%) had SRDD at presentation with 3 more (11.5%)
developing them. Subjects with SRDD were older (mean 81.7 $±$ 6.1 years vs 74.3 $±$ 7.6 year
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