A Protein-Truncating<i>HSD17B13</i>Variant and Protection from Chronic Liver Disease

Abul‐Husn, Noura S.; Cheng, Xiping; Li, Alexander H.; Xin, Yurong; Schurmann, Claudia; Stevis, Panayiotis E.; Liu, Yashu; Kozlitina, Julia; Stender, Stefan; Wood, G. Craig; Stepanchick, Ann; Still, Matthew D.; McCarthy, Shane; Ó'Dúshláine, Colm; Packer, Jonathan S.; Balasubramanian, Suganthi; Gosalia, Nehal; Esopi, David; Kim, Sun Y.; Mukherjee, Semanti; Lopez, Alexander; Fuller, Erin D.; Penn, John S.; Chu, Xin; Luo, Jonathan Z.; Mirshahi, Uyenlinh L.; Carey, David J.; Still, Christopher D.; Feldman, Michael D.; Small, Aeron; Damrauer, Scott M.; Rader, Daniel J.; Zambrowicz, Brian; Olson, William C.; Murphy, Andrew; Borecki, Ingrid B.; Shuldiner, Alan R.; Reid, Jeffrey G.; Overton, John D.; Yancopouloš, George D.; Hobbs, Helen H.; Cohen, Jonathan C.; Gottesman, Omri; Teslovich, Tanya M.; Baras, Aris; Mirshahi, Tooraj; Gromada, Jesper; Dewey, Frederick E.

doi:10.1056/nejmoa1712191

Cited by 586 publications

(764 citation statements)

References 30 publications

Supporting

Mentioning

695

Contrasting

Unclassified

Order By: Relevance

“…PNPLA3 and TM6SF2 polymorphisms are also associated with increased risk of HCC in ALD . Most recently, Abul‐Husn et al described a polymorphism related to a hepatic lipid droplet protein hydroxysteroid 17‐beta dehydrogenase 13 ( HSD17B13 ), the presence of which confers protection against the progression from steatosis to steatohepatitis in alcohol‐associated and non‐alcohol‐associated chronic liver disease …”

Section: Pathophysiology and Risk Factors For Alcohol‐associated Livementioning

confidence: 99%

Diagnosis and Treatment of Alcohol‐Associated Liver Diseases: 2019 Practice Guidance From the American Association for the Study of Liver Diseases

et al. 2020

View full text Add to dashboard Cite

Section: Pathophysiology and Risk Factors For Alcohol‐associated Livementioning

confidence: 99%

Diagnosis and Treatment of Alcohol‐Associated Liver Diseases: 2019 Practice Guidance From the American Association for the Study of Liver Diseases

et al. 2020

View full text Add to dashboard Cite

“…Among the 502,219 variants initially tested for association with aminotransferase levels, there were 35 variants in 19 target genes that reached exome‐wide significance ( p < 1 × 10 –7 ) in the discovery cohort. Further replication in ~12,527 persons led to refinement of 13 variants in nine genes, which not surprisingly included not only PNPLA3 , TM6SF2 , SERPINA1 , SAMM50 , and ERLIN1 but GPT , GOT1 (the genes encoding ALT and AST), and SLC39A12 . The rs72613567:TA variant of HSD17B13 was found to be reproducibly associated with decreased levels of ALT and AST and with lower odds of both NAFLD and ALD disease severity.…”

Section: The Search Strategymentioning

confidence: 96%

“…Armed with exome‐sequence data coupled to electronic health records of 46,455 participants from a large collaborative study, Abul‐Husn and colleagues explored variants associated with serum alanine aminotransferase (ALT) and aspartate aminotransferase (AST) levels, which were primarily regarded as surrogate indicators of liver damage . The study design consisted of subsequent stages of validation and replication, including functional exploration of the variant at the gene and protein levels that involved RNA sequencing and assessment of HSD17B13 enzymatic activity, respectively . Among the 502,219 variants initially tested for association with aminotransferase levels, there were 35 variants in 19 target genes that reached exome‐wide significance ( p < 1 × 10 –7 ) in the discovery cohort.…”

Section: The Search Strategymentioning

confidence: 99%

“…A new study by Abul‐Husn et al reveals that a loss‐of‐function variation in the 17‐beta‐hydroxysteroid dehydrogenase 13 ( HSD17B13 ) gene confers protection against chronic liver injury and mitigates the progression of NAFLD and ALD in European Americans . These new findings open the possibility that therapeutic inhibition of HSD17B13 could represent a new strategy to treat NAFLD and ALD.…”

mentioning

confidence: 99%

See 1 more Smart Citation

Genetics Meets Therapy? Exome‐wide Association Study Reveals a Loss‐of‐Function Variant in 17‐Beta‐Hydroxysteroid Dehydrogenase 13 That Protects Patients From Liver Damage and Nonalcoholic Fatty Liver Disease Progression

2018

View full text Add to dashboard Cite

Knowledge of the genetic component of nonalcoholic fatty liver disease (NAFLD) has significantly contributed to the understanding of the disease pathogenesis. Genetic studies based either on genome wide association-strategies or candidate-genes approaches showed that variants in loci involved in lipid metabolism and/or lipid-droplets biology have predominant and reproducible effects on the disease phenotype (1). However, it has been a major challenge to translate this information into molecularly-plausible and clinically-safe therapeutic targets. In fact, largest effects are given by missense variants (PNPLA3-I148M and TM6SF2-E167K) that while explaining modest changes in gene / protein expression levels do not represent "druggable" targets. Specifically, variants associated with the progression of NAFLD or alcoholic liver disease (ALD) are located in genes with either pleiotropic metabolic effect/s, for instance PNPLA3-I148M (rs738409) (2), or are associated with dual and opposite effects on critical phenotypes, particularly TM6SF2-E167K variant (3). Consequently, any pharmaceutical drug targeted to modulate PNPLA3 or TM6SF2-enzymatic activity, would be of limited use because of potential undesirable effects. A new study by Abul-Husn et al. reveals that a loss-of-function variation in HSD17B13 (17-beta-hydroxysteroid dehydrogenase 13) gene confers protection against chronic liver injury and mitigates the progression of NAFLD and ALD in European Americans (4). These new findings open the possibility that therapeutic inhibition of HSD17B13 could represent a new strategy to treat NAFLD and ALD. This article is protected by copyright. All rights reserved.

show abstract

“…MyCode participants are also consented for recontact for additional research which allows for additional clinical evaluation with more targeted phenotyping to supplement the rich data set that already exists in the EHR. DiscovEHR has already been proven to be a tremendous resource for genomic discovery (Abul‐Husn et al, ; Gusarova et al, ; Verma et al, ).…”

Section: New Scientific and Healthcare Initiatives: Geisinger Healthmentioning

confidence: 99%

Future directions for high‐throughput splicing assays in precision medicine

et al. 2019

View full text Add to dashboard Cite

Classification of variants of unknown significance is a challenging technical problem in clinical genetics. As up to one‐third of disease‐causing mutations are thought to affect pre‐mRNA splicing, it is important to accurately classify splicing mutations in patient sequencing data. Several consortia and healthcare systems have conducted large‐scale patient sequencing studies, which discover novel variants faster than they can be classified. Here, we compare the advantages and limitations of several high‐throughput splicing assays aimed at mitigating this bottleneck, and describe a data set of ~5,000 variants that we analyzed using our Massively Parallel Splicing Assay (MaPSy). The Critical Assessment of Genome Interpretation group (CAGI) organized a challenge, in which participants submitted machine learning models to predict the splicing effects of variants in this data set. We discuss the winning submission of the challenge (MMSplice) which outperformed existing software. Finally, we highlight methods to overcome the limitations of MaPSy and similar assays, such as tissue‐specific splicing, the effect of surrounding sequence context, classifying intronic variants, synthesizing large exons, and amplifying complex libraries of minigene species. Further development of these assays will greatly benefit the field of clinical genetics, which lack high‐throughput methods for variant interpretation.

show abstract

A Protein-TruncatingHSD17B13Variant and Protection from Chronic Liver Disease

Abstract: A loss-of-function variant in HSD17B13 was associated with a reduced risk of chronic liver disease and of progression from steatosis to steatohepatitis. (Funded by Regeneron Pharmaceuticals and others.).

Cited by 586 publications

References 30 publications

Diagnosis and Treatment of Alcohol‐Associated Liver Diseases: 2019 Practice Guidance From the American Association for the Study of Liver Diseases

Diagnosis and Treatment of Alcohol‐Associated Liver Diseases: 2019 Practice Guidance From the American Association for the Study of Liver Diseases

Genetics Meets Therapy? Exome‐wide Association Study Reveals a Loss‐of‐Function Variant in 17‐Beta‐Hydroxysteroid Dehydrogenase 13 That Protects Patients From Liver Damage and Nonalcoholic Fatty Liver Disease Progression

Future directions for high‐throughput splicing assays in precision medicine

Contact Info

Product

Resources

About