Predicting and elucidating the etiology of fatty liver disease : A machine learning modeling and validation study in the IMI DIRECT cohorts

Adamski, J.; Adamski, J.; Allin, K.; Allin, K.; Atabaki-Pasdar, N.; Atabaki-Pasdar, N.; Bell, J.D.; Bell, J.D.; Beulens, J.; Beulens, J.; Brage, S.; Brage, S.; Brunak, S.; Brunak, S.; Cederberg, H.; Cederberg, H.; Chabanova, E.; Chabanova, E.; Dale, M.; Dale, M.; Dawed, A.; Dawed, A.; Dermitzakis, E.; Dermitzakis, E.; Elders, P.; Elders, P.; Fernandez, J.; Fernandez, J.; Fitipaldi, H.; Fitipaldi, H.; Forgie, I.; Forgie, I.; Franks, P.; Franks, P.; Frau, F.; Frau, F.; Frost, G.; Frost, G.; Giordano, G.; Giordano, G.; Gupta, R.; Gupta, R.; Haid, M.; Haid, M.; Hansen, T.; Hansen, T.; Hansen, T.; Hansen, T.; Hattersley, A.; Hattersley, A.; Heggie, A.; Heggie, A.; Hong, M.; Hong, M.; Häussler, R.; Häussler, R.; Jones, A.; Jones, A.; Kennedy, G.; Kennedy, G.; Koivula, R.; Koivula, R.; Kokkola, T.; Kokkola, T.; Kurbasic, A.; Kurbasic, A.; Laakso, M.; Laakso, M.; Mahajan, A.; Mahajan, A.; Mari, A.; Mari, A.; Masi, F.; Masi, F.; McCarthy, M.; McCarthy, M.; McDonald, T.; McDonald, T.; McEvoy, D.; McEvoy, D.; Musholt, P.; Musholt, P.; Mutie, P.; Mutie, P.; Ohlsson, M.; Ohlsson, M.; Pattou, F.; Pattou, F.; Pavo, I.; Pavo, I.; Pearson, E.; Pearson, E.; Pedersen, H.; Pedersen, H.; Pedersen, O.; Pedersen, O.; Pomares-Millan, H.; Pomares-Millan, H.; Raverdy, V.; Raverdy, V.; Ridderstråle, M.; Ridderstråle, M.; Ruetten, H.; Ruetten, H.; Rutters, F.; Rutters, F.; Schwenk, J.; Schwenk, J.; Sharma, S.; Sharma, S.; Thomas, C.; Thomas, C.; Thomas, E.L.; Thomas, E.L.; Thomsen, H.; Thomsen, H.; Vangipurapu, J.; Vangipurapu, J.; Vestergaard, H.; Vestergaard, H.; Viñuela, A.; Viñuela, A.; Walker, M.; Walker, M.; ‘t Hart, L.; ‘t Hart, L.

Predicting and elucidating the etiology of fatty liver disease : A machine learning modeling and validation study in the IMI DIRECT cohorts

Authors: J. Adamski
J. Adamski
K. Allin
K. Allin
N. Atabaki-Pasdar
N. Atabaki-Pasdar
J.D. Bell
J.D. Bell
J. Beulens
J. Beulens
S. Brage
S. Brage
S. Brunak
S. Brunak
H. Cederberg
H. Cederberg
E. Chabanova
E. Chabanova
M. Dale
M. Dale
A. Dawed
A. Dawed
E. Dermitzakis
E. Dermitzakis
P. Elders
P. Elders
J. Fernandez
J. Fernandez
H. Fitipaldi
H. Fitipaldi
I. Forgie
I. Forgie
P. Franks
P. Franks
F. Frau
F. Frau
G. Frost
G. Frost
G. Giordano
G. Giordano
R. Gupta
R. Gupta
M. Haid
M. Haid
T. Hansen
T. Hansen
T. Hansen
T. Hansen
A. Hattersley
A. Hattersley
A. Heggie
A. Heggie
M. Hong
M. Hong
R. Häussler
R. Häussler
A. Jones
A. Jones
G. Kennedy
G. Kennedy
R. Koivula
R. Koivula
T. Kokkola
T. Kokkola
A. Kurbasic
A. Kurbasic
M. Laakso
M. Laakso
A. Mahajan
A. Mahajan
A. Mari
A. Mari
F. Masi
F. Masi
M. McCarthy
M. McCarthy
T. McDonald
T. McDonald
D. McEvoy
D. McEvoy
P. Musholt
P. Musholt
P. Mutie
P. Mutie
M. Ohlsson
M. Ohlsson
F. Pattou
F. Pattou
I. Pavo
I. Pavo
E. Pearson
E. Pearson
H. Pedersen
H. Pedersen
O. Pedersen
O. Pedersen
H. Pomares-Millan
H. Pomares-Millan
V. Raverdy
V. Raverdy
M. Ridderstråle
M. Ridderstråle
H. Ruetten
H. Ruetten
F. Rutters
F. Rutters
J. Schwenk
J. Schwenk
S. Sharma
S. Sharma
C. Thomas
C. Thomas
E.L. Thomas
E.L. Thomas
H. Thomsen
H. Thomsen
J. Vangipurapu
J. Vangipurapu
H. Vestergaard
H. Vestergaard
A. Viñuela
A. Viñuela
M. Walker
M. Walker
L. ‘t Hart
L. ‘t Hart
Publication date: 1 January 2020
Publisher
Doi

Abstract

Background Non-alcoholic fatty liver disease (NAFLD) is highly prevalent and causes serious health complications in individuals with and without type 2 diabetes (T2D). Early diagnosis of NAFLD is important, as this can help prevent irreversible damage to the liver and, ultimately, hepatocellular carcinomas. We sought to expand etiological understanding and develop a diagnostic tool for NAFLD using machine learning. Methods and findings We utilized the baseline data from IMI DIRECT, a multicenter prospective cohort study of 3,029 European-ancestry adults recently diagnosed with T2D (n= 795) or at high risk of developing the disease (n= 2,234). Multi-omics (genetic, transcriptomic, proteomic, and metabolomic) and clinical (liver enzymes and other serological biomarkers, anthropometry, measures of beta-cell function, insulin sensitivity, and lifestyle) data comprised the key input variables. The models were trained on MRI-image-derived liver fat content (= 5%) available for 1,514 participants. We applied LASSO (least absolute shrinkage and selection operator) to select features from the different layers of omics data and random forest analysis to develop the models. The prediction models included clinical and omics variables separately or in combination. A model including all omics and clinical variables yielded a cross-validated receiver operating characteristic area under the curve (ROCAUC) of 0.84 (95% CI 0.82, 0.86;p = 5%) rather than a continuous one. Conclusions In this study, we developed several models with different combinations of clinical and omics data and identified biological features that appear to be associated with liver fat accumulation. In general, the clinical variables showed better prediction ability than the complex omics variables. However, the combination of omics and clinical variables yielded the highest accuracy. We have incorporated the developed clinical models into a web interface (see:) and made it available to the community.Peer reviewe