Human-Disease Phenotype Map Derived from PheWAS across 38,682 Individuals

Verma, Anurag; Bang, Lisa; Miller, Jason E.; Zhang, Yanfei; Lee, Ming Ta Michael; Zhang, Yu; Byrska-Bishop, Marta; Carey, David J.; Ritchie, Marylyn D.; Pendergrass, Sarah A.; Kim, Dokyoon

doi:10.1016/j.ajhg.2018.11.006

Cited by 54 publications

(54 citation statements)

References 53 publications

(92 reference statements)

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“…Such studies have a limited scope and cannot reveal the “big picture” of disease interconnections. A major breakthrough is the HDN (human disease network) study, under which a large number of diseases are systematically analyzed. The HDN studies have the potential to reveal previously unknown disease interconnections and “globally” describe diseases.…”

Section: Introductionmentioning

confidence: 99%

Human disease cost network analysis

Yang

Shia

et al. 2020

Statistics in Medicine

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Diseases can be interconnected. In the recent years, there has been a surge of multidisease studies. Among them, HDN (human disease network) analysis takes a system perspective, examines the interconnections among diseases along with their individual properties, and has demonstrated great potential. Most of the existing HDN analyses are based on either molecular information (which may be unreliable and have limited clinical relevance) or phenotypic measures (which may have limited implications for disease management and not directly reflect disease severity). In this study, we take advantage of the uniquely valuable Taiwan NHIRD (National Health Insurance Research Database) data and conduct an HDN analysis of disease treatment cost. Complementing the existing literature, treatment cost can serve as a surrogate of disease severity (and hence be clinically highly relevant) and also directly describe the financial burden of illness (and hence be uniquely informative for disease management). With inpatient and outpatient treatment data on close to 1 million randomly selected subjects and collected during the period of 2000 to 2013, the human disease cost network is constructed using a novel copula‐based approach and the weighted correlation‐based network construction technique. Extensive analysis is conducted, and the results are found to be biomedically sensible.

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Section: Introductionmentioning

confidence: 99%

Human disease cost network analysis

Yang

Shia

et al. 2020

Statistics in Medicine

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“…For example, several non‐MHC RA risk alleles have shown pleiotropic effects in several disorders, including type 1 DM, MS, and lupus , and a cross‐phenotype meta‐analysis of 7 common autoimmune diseases (RA, type 1 DM, MS, lupus, psoriasis, Crohn's disease, and celiac disease) showed that ~44% of disease‐associated SNPs were shared by some of these disorders . Similarly, a study that investigated interconnections across multiple diseases in a large EHR system found that the strongest disease network (indicated by the highest number of shared SNPs) was composed of RA, type 1 DM, MS, and psoriasis . The SNPs linking these conditions mapped to 18 loci in the MHC region and 1 in PTPN22 .…”

Section: Discussionmentioning

confidence: 99%

“…Although inflammation is an important component of these cardiometabolic traits, and many inflammatory genes have been associated with susceptibility to some of these traits , we did not find significant genetic pleiotropy between RA and these phenotypes. An alternative explanation is that it is not a genetic predisposition toward RA, but development of the inflammatory milieu that results from disease which causes the associations with these phenotypes .…”

Section: Discussionmentioning

confidence: 99%

Pleiotropy in the Genetic Predisposition to Rheumatoid Arthritis: A Phenome‐Wide Association Study and Inverse Variance–Weighted Meta‐Analysis

Kawai

Shi

Feng

et al. 2020

Arthritis & Rheumatology

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Objective This study was undertaken to investigate the hypothesis that a genetic predisposition toward rheumatoid arthritis (RA) increases the risk of 10 cardiometabolic and autoimmune disorders previously associated with RA in epidemiologic studies, and to define new genetic pleiotropy present in RA. Methods Two approaches were used to test our hypothesis. First, we constructed a weighted genetic risk score (wGRS) and then examined its association with 10 prespecified disorders. Additionally, a phenome‐wide association study (PheWAS) was carried out to identify potential new associations. Second, inverse variance–weighted regression (IVWR) meta‐analysis was used to characterize the association between genetic susceptibility to RA and the prespecified disorders, with the results expressed as odds ratios (ORs) and 95% confidence intervals (95% CIs). Results The wGRS for RA was significantly associated with type 1 diabetes mellitus (DM) (OR 1.10 [95% CI 1.04–1.16]; P = 9.82 × 10−4) and multiple sclerosis (OR 0.82 [95% CI 0.77–0.88]; P = 1.73 × 10−8), but not with other cardiometabolic phenotypes. In the PheWAS, wGRS was also associated with an increased risk of several autoimmune phenotypes including RA, thyroiditis, and systemic sclerosis, and with a decreased risk of demyelinating disorders. In the IVWR meta‐analyses, RA was significantly associated with an increased risk of type 1 DM (P = 1.15 × 10−14), with evidence of horizontal pleiotropy (Mendelian Randomization–Egger intercept estimate P = 0.001) likely driven by rs2476601, a PTPN22 variant. The association between type 1 DM and RA remained significant (P = 9.53 × 10−9) after excluding rs2476601, with no evidence of horizontal pleiotropy (intercept estimate P = 0.939). RA was also significantly associated with type 2 DM and C‐reactive protein levels. These associations were driven by variation in the major histocompatibility complex region. Conclusion This study presents evidence of pleiotropy between the genetic predisposition to RA and associated phenotypes found in other autoimmune and cardiometabolic disorders, including type 1 DM.

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“…Lastly, large data sets containing genetic variants for screening by MPRAs often lack corresponding phenotypic or other relevant 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, 2018; Gusarova et al, 2018;Verma et al, 2019).…”

Section: High-throughput Methods In Splicingmentioning

confidence: 99%

Future directions for high‐throughput splicing assays in precision medicine

et al. 2019

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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.

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Human-Disease Phenotype Map Derived from PheWAS across 38,682 Individuals

Cited by 54 publications

References 53 publications

Human disease cost network analysis

Human disease cost network analysis

Pleiotropy in the Genetic Predisposition to Rheumatoid Arthritis: A Phenome‐Wide Association Study and Inverse Variance–Weighted Meta‐Analysis

Future directions for high‐throughput splicing assays in precision medicine

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