Back

Variants in MARC1 and HSD17B13 reduce severity of NAFLD in children, perturb phospholipid metabolism, and suppress fibrotic pathways

Hudert, C. A.; Alisi, A.; Anstee, Q. M.; Crudele, A.; Draijer, L. G.; EU-PNAFLD investigators, ; Furse, S.; Hengstler, J. G.; Jenkins, B.; Karnebeek, K.; Kelly, D. A.; Koot, B. G.; Koulman, A.; Meierhofer, D.; Snowden, S. G.; van Mourik, I.; Vreugdenhil, A.; Wiegand, S.; Mann, J. P.

2020-06-07 gastroenterology
10.1101/2020.06.05.20120956 medRxiv
Show abstract

Background & aimsGenome-wide association studies in adults have identified variants in HSD17B13 and MARC1 as protective against NAFLD. It is not known if they are similarly protective in children and, more generally, whether the peri-portal inflammation of pediatric NAFLD and lobular inflammation seen in adults share common genetic influences. Therefore, we aimed to: establish if these variants are associated with NAFLD in children, and to investigate the function of these variants in hepatic metabolism using metabolomics. Methods960 children (590 with NAFLD, 394 with liver histology) were genotyped for rs72613567T>TA in HSD17B13, rs2642438G>A in MARC1. Genotype-histology associations were tested using ordinal regression. Untargeted hepatic proteomics and plasma lipidomics were performed in a subset of samples. In silico tools were used to model the effect of rs2642438G>A (p.Ala165Thr) on MARC1. Resultsrs72613567T>TA in HSD17B13 was associated with lower odds of NAFLD diagnosis (OR 0.7 (95%CI 0.6-0.9) and lower grade of portal inflammation (P<0.001) whilst rs2642438G>A in MARC1 was associated with lower grade of hepatic steatosis (P=0.02). Proteomics found reduced expression of HSD17B13 in carriers of the protective allele, whereas MARC1 levels were not affected by genotype. Both variants showed downregulation of hepatic fibrotic pathways, upregulation of retinol metabolism and perturbation of phospholipid species. Modelling suggests that p.Ala165Thr would disrupt the stability and metal-binding of MARC1. ConclusionsThere are shared genetic mechanisms between pediatric and adult NAFLD, despite their differences in histology. MARC1 and HSD17B13 are involved in phospholipid metabolism and suppress fibrosis in NAFLD.

Matching journals

The top 8 journals account for 50% of the predicted probability mass.

1
JHEP Reports
11 papers in training set
Top 0.1%
15.3%
2
Journal of Hepatology
21 papers in training set
Top 0.1%
6.8%
3
The Journal of Clinical Endocrinology & Metabolism
36 papers in training set
Top 0.1%
6.8%
4
Hepatology Communications
22 papers in training set
Top 0.1%
6.3%
5
Metabolomics
14 papers in training set
Top 0.1%
5.5%
6
Metabolites
53 papers in training set
Top 0.2%
4.9%
7
PLOS ONE
5266 papers in training set
Top 34%
4.1%
8
Hepatology
22 papers in training set
Top 0.1%
3.3%
50% of probability mass above
9
BMC Medicine
176 papers in training set
Top 2%
2.5%
10
Scientific Reports
3612 papers in training set
Top 43%
2.4%
11
Diabetes
56 papers in training set
Top 0.4%
2.4%
12
Communications Medicine
113 papers in training set
Top 1%
2.4%
13
BMC Cancer
67 papers in training set
Top 1%
1.4%
14
Gut
40 papers in training set
Top 0.6%
1.4%
15
Nature Communications
5641 papers in training set
Top 50%
1.1%
16
Frontiers in Cell and Developmental Biology
233 papers in training set
Top 3%
1.1%
17
Epigenomics
11 papers in training set
Top 0.1%
1.1%
18
Obesity
21 papers in training set
Top 0.3%
1.1%
19
Molecular Metabolism
112 papers in training set
Top 1%
1.1%
20
The FASEB Journal
194 papers in training set
Top 4%
1.1%
21
Journal of Lipid Research
39 papers in training set
Top 0.5%
1.0%
22
Biochimica et Biophysica Acta (BBA) - Molecular and Cell Biology of Lipids
15 papers in training set
Top 0.2%
1.0%
23
Gastro Hep Advances
11 papers in training set
Top 0.3%
1.0%
24
Free Radical Biology and Medicine
36 papers in training set
Top 0.6%
1.0%
25
PLOS Genetics
862 papers in training set
Top 10%
1.0%
26
Medicine & Science in Sports & Exercise
16 papers in training set
Top 0.4%
0.9%
27
eBioMedicine
183 papers in training set
Top 6%
0.9%
28
Journal of Clinical Medicine
97 papers in training set
Top 4%
0.9%
29
American Journal of Gastroenterology
17 papers in training set
Top 0.3%
0.9%
30
Diabetes, Obesity and Metabolism
22 papers in training set
Top 0.8%
0.9%