Human genomics. The Genotype-Tissue Expression (GTEx) pilot analysis: multitissue gene regulation in humans.
- Authors
- GTEx Consortium
- Year
- 2015
- Journal
- Science (New York, N.Y.)
- PMID
- 25954001
- DOI
- 10.1126/science.1262110
- PMCID
- PMC4547484
Understanding the functional consequences of genetic variation, and how it affects complex human disease and quantitative traits, remains a critical challenge for biomedicine. We present an analysis of RNA sequencing data from 1641 samples across 43 tissues from 175 individuals, generated as part of the pilot phase of the Genotype-Tissue Expression (GTEx) project. We describe the landscape of gene expression across tissues, catalog thousands of tissue-specific and shared regulatory expression quantitative trait loci (eQTL) variants, describe complex network relationships, and identify signals from genome-wide association studies explained by eQTLs. These findings provide a systematic understanding of the cellular and biological consequences of human genetic variation and of the heterogeneity of such effects among a diverse set of human tissues.
Sample clustering based on gene expression and exon splicing profiles(A) Clustering performed on the basis of gene expression values for all genes from Gencode v12 annotation. Tissue type is the primary driver of expression differences, with the nonsolid tissues (blood and LCL cell lines) clustering separately from solid tissues. Hierarchical clustering was performed using as distance = 1 β Pearson correlation, and average method. (B) Sample clustering based on the βpercent spliced inβ (PSI) values for exons across samples. Tissue differentiation is less clearly a driver, and brain is now the main outgroup, driven largely by a cluster comprised of cerebellum and cortex samples.
LLM interpretation
This figure consists of two hierarchical clustering dendrograms (A and B) showing sample relationships based on gene expression and exon splicing (PSI) values, respectively. In panel A, samples cluster primarily by tissue type, with a distinct separation between nonsolid tissues (blood and LCL) and solid tissues. In panel B, tissue differentiation is less pronounced, with brain subregions forming the primary outgroup, further divided into Cluster 1 and Cluster 2. Color-coded bars beneath the dendrograms correspond to the provided legends for brain subregions and all tissues.
Number and sharing of significant ciseQTLs per tissue(A) Numbers of significant cis-eQTL genes (eGenes) per tissue according to single-tissue analysis. For each gene, the minimum nominal P value was used as the test statistic and an empirical P value was computed to correct for number of tests per gene, based on either permutation analysis of genotype sample labels applied to the full set of samples per tissue (β) or Bonferroni correction, used for downsampling (line) to reduce computational burden (14). In the range of sample sizes tested, the number of identified eGenes increases linearly with sample size. (B) Dendrogram and heat map of pairwise eQTL sharing using the method of Nica et al. (22). Values are not symmetrical, since each entry in row i and column j is an estimate of Ο1 = Pr(eQTL in tissue i given an eQTL in tissue j). Blood has the lowest levels of eQTL sharing with other tissues while adipose shows higher levels of sharing. (C) Activity probabilities for both multitissue modeling approaches, applied to all nine tissues, indicate that the most likely configurations are for eQTLs that are active in only a few tissues or in many tissues. (D) For eQTLs in each tissue considered separately, analyzing multiple tissues jointly increases the number of discovered eQTL associations (FDR < 0.05), as assessed by the SNP-based multitissue model.
LLM interpretation
This figure consists of four panels analyzing cis-eQTLs across multiple tissues. Panel A is a line plot showing a linear increase in the number of significant eGenes as the sample size increases for various tissues. Panel B features a dendrogram and a heat map illustrating the pairwise sharing of eQTLs between tissues, with adipose showing higher sharing and blood showing lower sharing. Panel C is a line graph showing the activity probabilities for SNP-based and gene-based models across the number of tissues, and Panel D is a line plot demonstrating that joint multi-tissue analysis increases the number of discovered significant SNP-gene pairs compared to single-tissue analysis.
Quantification of regulatory diversity by ASE(A) Proportion of sites with significant ASE (P < 0.005) in each tissue (colored and labeled as in Table 1), with binomial confidence intervals. (B) Proportion of significant ASE sites for the nine tissues with eQTL data as a function of the proportion of eQTLs after regressing out the log of sample size. (C) Partitioning variation in allelic and total gene expression within and between individuals and tissues. We calculated pairwise Spearman rank correlations between all the samples using two metrics [(D) and (E)]. (D) Allelic ratios over sites (sampled to 30 reads each), which captures similarity in allelic effects that are a proxy for cis-regulatory variation. (E) Total read counts over the same sites, which captures similarity in total gene expression levels. The plots show the distributions of pairwise correlations for sample pairs that are from (1) different tissues and different individual, (2) different tissues within an individual, or (3) same tissues in different individuals. Gene expression levels are highly correlated within the same tissue (E3) (see Fig. 1A). However, allelic ratios show highest correlation among different tissues of the same individual that share the same genome (D2).
LLM interpretation
This figure consists of five panels analyzing regulatory diversity through Allelic Specific Expression (ASE). Panel A is a bar chart showing the proportion of sites with significant ASE across various tissues, and Panel B is a scatter plot correlating the proportion of significant ASE sites with the proportion of eQTLs across nine tissues. Panel C is a schematic diagram illustrating three types of sample pairwise correlations: between tissues/individuals (1), between tissues within an individual (2), and within the same tissue between individuals (3). Panels D and E are box plots comparing these three correlation groups for allelic ratios and total read counts, respectively, showing that allelic ratios are most highly correlated within the same individual (group 2), while total counts are most highly correlated within the same tissue (group 3).
Cis-regulatory effects in individuals that are not explained by detected eQTLs(A) An eQTL showing individual homozygous (AA) for the eQTL SNP (left panel) or heterozygous (AG) (right panel). ASE is measured at the TC SNP. (B) An example of replication of an eQTL signal in ASE analysis in the NDRG4 gene, with eQTL heterozygotes showing higher ASE in the eQTL target gene than eQTL homozygotes (only a subset of individuals shown; linear regression P = 5.69 Γ 10β6). The error bars are from a binomial test for the allelic ratio. (C) For each eQTL gene where the eQTL signal was replicated in ASE (linear regression P < 0.05 after Bonferroni correction), the eQTL heterozygotes show higher variance in allelic ratio (Mann-Whitney P = 2.13 Γ 10β7). (D) Permuted P value for the variance between individuals, which is higher than expected in 22/53 genes (9 genes in homozygotes, 20 in heterozygotes).
LLM interpretation
This figure consists of a schematic diagram and three data plots analyzing eQTL signals and allelic imbalance. (A) is a diagram illustrating the difference between eQTL homozygotes and heterozygotes in relation to allelic expression. (B) is a bar chart for the *NDRG4* gene showing that eQTL heterozygotes generally have a higher positive allele ratio than homozygotes, with a linear regression P-value of $5.69 \times 10^{-6}$. (C) is a scatter plot comparing eQTL homozygous versus heterozygous variance, and (D) is a scatter plot of $-\log_{10} p$ values for homozygous versus heterozygous variance, with points color-coded by significance.
Splicing QTLs(A) A splicing QTL that affects the relative usage of alternative splice isoforms for the tRNA methyltransferase 1 homolog gene (TRMT1). TRMT1 has three annotated isoforms, only two of which are abundant in skeletal muscle. The relative abundance of the two isoforms differs by genotype (number of individuals below each genotype), with heterozygotes showing an intermediate behavior. This SNP has not been detected as an eQTL. The right panel shows the exonic structure of the transcripts along with the location of the sQTL SNP (dotted line). (B) The relative proportions of the different types of splicing events detected by the two methods over the nine tested tissues (fig. S23). (C) Functional enrichment of sQTLs from Altrans and sQTLseekeR. For the top-ranked SNPs associated with a given splicing event, we computed the relative frequency with which they map to different biologically determined ENCODE functional domains.
LLM interpretation
This figure analyzes splicing QTLs (sQTLs) across three panels. Panel A features a box plot showing the splicing ratio of *TRMT1* isoforms across three genotypes (CC, CG, GG), with a corresponding gene structure diagram indicating the SNP location. Panel B is a horizontal bar chart comparing the proportion of different splicing event types detected by "sQTLseeker" and "Altrans" methods. Panel C consists of two bar charts showing the functional enrichment of 1st rank variants across various biological domains and transcription factors.
Coexpression networks within tissues and individuals(A) Similarity of coexpression networks discovered in each tissue separately (rows) and replicated across all other tissues (columns), on the basis of the correlation in gene-pair expression levels across all individuals for a given tissue, as quantified by the Ο1 statistic. The tissues in this heat map are ordered as in Fig. 2B. (B) Coexpression modules learned within adipose tissue on the basis of weighted gene coexpression network analysis (WGCNA). The heat map shows the similarity in gene expression patterns (across individuals) for each pair of genes expressed within adipose tissue (red = high correlation, blue = low correlation). Non-gray colors highlight separate modules. (C and D) Genes in the same adipose coexpressed module [(C), rows] show enrichment for similar gene ontology (GO) categories (columns) and are co-bound by the same transcription factors (TF) [(D), columns] in their transcription start site (blue = Benjamini-Hochberg corrected P < 0.01). Dendrogram (top) denotes TF-to-TF similarity in module targeting. (E) Average expression level (red = high, blue = low) in each tissue (rows) across 117 expression modules (columns). Modules highlighted include Mod6, showing highest expression in whole blood and cortex; Mod95, showing highest expression in noncortex brain; and Mod101, showing brainwide expression. (F) Expression pattern of 175 individuals (columns) across 45 tissues (rows) for the ZFP57 gene encoding a KRAB domain transcription factor. Colored entries denote expression levels (heat map). White entries denote missing expression measurements for an individual in a given tissue. (G) Probability of membership of each individual (columns) in each expression module (rows) for the three most significant modules [highlighted in (E)]. (H) Genotype of the three top modQTL SNPs (rows) across individuals (columns) shows correlation with module membership probability.
LLM interpretation
This figure consists of multiple panels analyzing gene coexpression networks across tissues and individuals. Panel A is a heatmap showing network similarity ($\pi_1$ statistic) between tissues, while Panel B displays a WGCNA correlation matrix for adipose tissue with identified modules. Panels C and D use heatmaps to show the enrichment of GO categories and transcription factor binding for these modules (blue indicates $P < 0.01$), and Panel E shows average expression of 117 modules across 45 tissues. Panels F, G, and H utilize heatmaps to illustrate the expression of the *ZFP57* gene across individuals/tissues, membership probabilities for three specific modules, and the corresponding genotypes of three modQTL SNPs.
Integration of transcriptome data improves annotation of putative protein truncating variants (PTVs)(A) The majority of annotated PTV variants are partial PTV, meaning that only a fraction of the RNA-seq transcripts support PTV annotation. (B) For all the predicted PTV variants, we ask what percentage of variants maintain a PTV annotation if we require that a fixed percentage of the dominant isoforms across all sequenced tissues support a PTV prediction; 70% of PTV variants are relevant if the threshold is 10%, whereas only 40% of PTV variants are relevant if the threshold is 100%.
LLM interpretation
Figure A is a pie chart showing that 61.6% of annotated protein truncating variants (PTVs) are "Partial PTV" and 38.4% are "Full PTV." Figure B is an area plot showing the proportion of PTVs in exome sequencing (y-axis) relative to the proportion of tissues with PTV annotation for the major transcript (x-axis). The trend in Figure B shows a decrease in the proportion of relevant PTVs as the tissue annotation threshold increases, dropping from 100% at a 0.0 threshold to approximately 40% at a 1.0 threshold.
Tissue-dependent GWAS eQTL enrichment Q-Q plots(A) eQTLs are enriched for trait associations with an important class of complex diseases. eQTLs discovered in whole blood (plotted in red) show significant enrichment for SNPs associated with autoimmune disorders from the WTCCC study (type 1 diabetes, Crohnβs disease, and rheumatoid arthritis) relative to null expectation (shown in gray) defined by non-eQTLs. (B) Enrichment of eQTLs for disease associations is tissue-dependent. Single-tissue eQTL annotation can be used to increase power to detect associations with hypertension, a disease for which the WTCCC study failed to yield significant associations. Notably, eQTLs discovered in adipose are enriched relative to muscle, lung, thyroid, skin, heart, and tibial artery (P < 0.05, Kolmogorov-Smirnov test) for known SNP associations with the hypertension.
LLM interpretation
This figure consists of several Q-Q plots comparing observed versus expected $-\log_{10}(p)$ values for GWAS trait associations. Panel A shows that eQTLs in whole blood (red) are enriched for associations with autoimmune disorders (Crohnβs disease, Type 1 diabetes, and Rheumatoid arthritis) compared to non-eQTLs (gray). Panel B demonstrates tissue-dependent enrichment for hypertension, with adipose tissue (gray circles) showing the highest enrichment relative to other tissues such as muscle, lung, and heart ($P < 0.05$, Kolmogorov-Smirnov test).
A blood pressure-associated SNP is a significant eQTL in tibial artery, for ARHGAP42 and TMEM133(A) The GWAS SNP, rs633185 in the intron of ARHGAP42, is associated with systolic blood pressure (P = 1.2 Γ 10β17) and diastolic blood pressure (P = 2 Γ 10β15). This GWAS SNP is in tight LD (r2 = 0.93) with the most significant eQTL for ARHGAP42 in tibial artery, rs604723 (P = 1 Γ 10β8), and is the most significant eQTL for TMEM133 in tibial artery (P = 2.7 Γ 10β8). Tibial artery was the only significant tissue at FDR < 0.05 according to the single-tissue eQTL discovery method. (B) Average posterior probability of the most significant cis-eQTL, rs607562 for ARHGAP42 at FDR < 0.05 from the multitissue eQTL methods. (C) Similar plot for TMEM133. The most significant cis-eQTL for TMEM133 from the multitissue methods at FDR < 0.05 is the GWAS SNP, rs633185, in tibial artery.
LLM interpretation
This figure consists of a genomic map and several data plots analyzing the relationship between SNP rs633185 and gene expression. Panel A shows a chromosomal location map and two box plots demonstrating that for both *ARHGAP42* and *TMEM133* in the tibial artery, gene expression decreases from the homozygous reference to the homozygous alternative genotype. Panels B and C are bar charts showing the multi-tissue posterior probability of eQTLs for *ARHGAP42* and *TMEM133*, with the tibial artery (red bar) showing the highest probability for both genes.
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| Elevated NEGR1 in brain induces anxiety or depression-like phenotypes and synaptic dysfunction. | Zhang YQ et al. | β | 2025 | β |
| Eliosin-an alternative product from the HmPKD1 locus is a component of endoplasmic reticulum mitochondria membrane contact sites. | Kurbegovic A et al. | β | 2025 | β |
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| Exploring the protective effect of metformin against sarcopenia: insights from cohort studies and genetics. | Hu Y et al. | β | 2025 | β |
| Exploring therapeutic applications of <i>PTEN, TMPRSS2:ERG</i> fusion, and tumour molecular subtypes in prostate cancer management. | Bugoye FC et al. | β | 2025 | β |
| Exploring the role of EBV in multiple sclerosis pathogenesis through EBV interactome. | Ballerini C et al. | β | 2025 | β |
| Exploring the role of the Rab network in epithelial-to-mesenchymal transition. | Jaygude U et al. | β | 2025 | β |
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| Expression profiling, functional characterization, and potential functional variants of the COL7A1 gene in sheep horn development. | Zhang S et al. | β | 2025 | β |
| Expression quantitative trait loci (eQTL): from population genetics to precision medicine. | Wong ZQ et al. | β | 2025 | β |
| Fast and sensitive detection of targeted gene fusions using frequency minimizers and fuzzy pattern matching with Fuzzion2. | Rice SV et al. | β | 2025 | β |
| From bulk to single-cell and spatial data: An AI framework to characterise breast cancer metabolic dysregulations across modalities. | Doan LMT et al. | β | 2025 | β |
| Functional and evolutionary characteristics of human genes encoding cell surface receptors involved in the regulation of appetite. | Ignatieva E et al. | β | 2025 | β |
| Functional and Practical Insights Into the Genetic Basis of Takayasu Arteritis. | Casares-Marfil D et al. | β | 2025 | β |
| Functional genomics in age-related macular degeneration: From genetic associations to understanding disease mechanisms. | Ratnapriya R et al. | β | 2025 | β |
| GeneCOCOA: Detecting context-specific functions of individual genes using co-expression data. | Zehr S et al. | β | 2025 | β |
| Gene Expression Shifts in Emperor Penguin Adaptation to the Extreme Antarctic Environment. | Paris JR et al. | β | 2025 | β |
| Genetically supported targets and drug repurposing for brain aging: A systematic study in the UK Biobank. | Yi F et al. | β | 2025 | β |
| Genetic and epidemiologic assessment of mandibular cortical indices and bone mineral density in peripubertal children: the Generation R study. | Prijatelj V et al. | β | 2025 | β |
| Genetic architecture of plasma metabolome in 254,825 individuals. | Qiang YX et al. | β | 2025 | β |
| Genetic determinants of monocyte splicing are enriched for disease susceptibility loci. | Nassiri I et al. | β | 2025 | β |
| Genetic determinants of proteomic aging. | MΓΆrseburg A et al. | β | 2025 | β |
| Genetic Evidence Prioritizes Neurocognitive Decline as a Causal Driver of Sleep Disturbances: A Multi-Omics Analysis Identifying Causal Genes and Therapeutic Targets. | Du Y et al. | β | 2025 | β |
| Genetic predisposition to Behcet's disease mediated by a IL10RA enhancer polymorphism. | Tan H et al. | β | 2025 | β |
| Genetic regulation of lncRNA expression in whole human brain and their contribution to CNS disorders. | He Y et al. | β | 2025 | β |
| Genetic Risk Variants for Multiple Sclerosis and Other Loci Linked to Intrathecal Immunoglobulin G Synthesis. | Pukaj A et al. | β | 2025 | β |
| Genetic susceptibility and validation of angiographic patterns in Takayasu arteritis. | Casares-Marfil D et al. | β | 2025 | β |
| Genetic variants of FER and SULF1 in the fibroblast-related genes are associated with non-small-cell lung cancer survival. | Lu G et al. | β | 2025 | β |
| Genetic Variants of <i>UGP2</i> and <i>FBP2</i> in the Glycolysis Pathway Independently Predict Survival of Patients with HBV-Related Hepatocellular Carcinoma. | Gong R et al. | β | 2025 | β |
| Genome-wide and phenome-wide studies provided insights into brain glymphatic system function and its clinical associations. | Ran L et al. | β | 2025 | β |
| Genome-wide association analyses identify distinct genetic architectures for early-onset and late-onset depression. | Shorter JR et al. | β | 2025 | β |
| Genome-wide association study of childhood B-cell acute lymphoblastic leukemia reveals novel African ancestry-specific susceptibility loci. | Im C et al. | β | 2025 | β |
| Genome-wide association study of early-stage non-small cell lung cancer prognosis: a pooled analysis in the International Lung Cancer Consortium. | Dong M et al. | β | 2025 | β |
| Genome-wide association study provides novel insight into the genetic architecture of severe obesity. | Krishnan M et al. | β | 2025 | β |
| Genome-Wide microRNA Expression Profiling in Human Spermatozoa and Its Relation to Sperm Quality. | Cassuto NG et al. | β | 2025 | β |
| Genomic data-driven framework for drug target discovery in atrial fibrillation. | Tao Y et al. | β | 2025 | β |
| Genotype by Environment Interactions in Gene Regulation Underlie the Response to Soil Drying in the Model Grass Brachypodium distachyon. | Yun J et al. | β | 2025 | β |
| Global and tissue-specific transcriptomic dysregulation in human aging: Pathways and predictive biomarkers. | Arif M et al. | β | 2025 | β |
| Heterozygous <i>TBX2</i> frameshift variants cause a novel syndromic hearing loss with incompletely penetrant nystagmus. | Hua W et al. | β | 2025 | β |
| Heterozygous variants in <i>PLCG1</i> affect hearing, vision, cardiac, and immune function. | Ma M et al. | β | 2025 | β |
| HIC2 suppresses glioblastoma progression via transcriptional repression of SEMA3A and inhibition of TGF-Ξ² signaling. | Zhang L et al. | β | 2025 | β |
| Hippo in smooth muscle - a therapeutic target in vascular diseases driven by aging and hypertension. | Albinsson S et al. | β | 2025 | β |
| Histologic and Quality Assessment of Genotype-Tissue Expression (GTEx) Research Samples: A Large Postmortem Tissue Collection. | Sobin L et al. | β | 2025 | β |
| HLA diversity and signatures of selection in the Maniq, a nomadic hunter-gatherer population in Southern Thailand. | Schaschl H et al. | β | 2025 | β |
| HORNET: tools to find genes with causal evidence and their regulatory networks using eQTLs. | Lorincz-Comi N et al. | β | 2025 | β |
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| Human prostacyclin and thromboxane synthases: Molecular interactions, regulation, and pharmacology. | Ershov PV et al. | β | 2025 | β |
| Identification of key biomarkers and potential therapeutic drugs in nasopharyngeal carcinoma based on comprehensive bioinformatics analysis. | Fu C et al. | β | 2025 | β |
| Identification of Npas4 as a biomarker for CICI by transcriptomics combined with bioinformatics and machine learning approaches. | He Z et al. | β | 2025 | β |
| Identification of SAMD9 as an adaptive response gene to environmental changes and its association with overall survival and immunotherapeutic response in glioblastoma. | Li F et al. | β | 2025 | β |
| Identification of Therapeutic Targets for Hyperuricemia: Systematic Genome-Wide Mendelian Randomization and Colocalization Analysis. | Chen N et al. | β | 2025 | β |
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| Identifying causal genes for prostatitis through drug-targeted Mendelian randomization. | Yan K et al. | β | 2025 | β |
| Identifying genes and traits associated with pre-eclampsia using summary statistics. | Zhu W et al. | β | 2025 | β |
| <i>MiR-196a2</i> rs11614913 C Allele is Associated with Increased Wilms Tumor Susceptibility in Chinese Children. | Luo M et al. | β | 2025 | β |
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| Increased burden of rare risk variants across gene expression networks predisposes to sporadic Parkinson's disease. | Eubanks E et al. | β | 2025 | β |
| Insights from a methylome-wide association study of antidepressant exposure. | Davyson E et al. | β | 2025 | β |
| Insights Into Chronic Low Back Pain Etiology: Population-Based Genome-Wide Association Study Identifies 18 Risk Loci. | Martinsen AE et al. | β | 2025 | β |
| Integrated Multi-Omics Analysis and Cross-Model Validation Reveal Mitochondrial Signatures in Alzheimer's Disease. | Xu X et al. | β | 2025 | β |
| Integrated pan-cancer analysis of ADM's role in prognosis, immune modulation and resistance. | Liu Y et al. | β | 2025 | β |
| Integrated pan-cancer and melanoma-specific analysis of angiopoietin-2: prognostic value, immune microenvironment modulation, and ceRNA network regulation. | Ni X et al. | β | 2025 | β |
| Integrating explainable machine learning and transcriptomics data reveals cell-type specific immune signatures underlying macular degeneration. | Ma K et al. | β | 2025 | β |
| Integrating multi-omics data: Methods and applications in human complex diseases. | Sibilio P et al. | β | 2025 | β |
| Integrative Genomics Refines Tissues, Candidate Genes and Putative Regulatory Links Involved in the Humic Adaptation of Keystone Freshwater Fish. | Ozerov MY et al. | β | 2025 | β |
| Isoform-level profiling of m<sup>6</sup>A epitranscriptomic signatures in human brain. | Gleeson J et al. | β | 2025 | β |
| Landscape of chimeric RNAs in COVID-19 patient blood. | Haddox S et al. | β | 2025 | β |
| Large-scale genome-wide analyses of stuttering. | Polikowsky HG et al. | β | 2025 | β |
| Leveraging multiomic approaches to elucidate mechanisms of heterogeneity in Alzheimer's disease: Neuropsychiatric symptoms, co-pathologies, and sex differences. | Shwab EK et al. | β | 2025 | β |
| Li-Fraumeni syndrome: a germline <i>TP53</i> splice variant reveals a novel physiological alternative transcript. | Louis J et al. | β | 2025 | β |
| LILRB4 as a novel immunotherapeutic target for multiple diseases. | Wang X et al. | β | 2025 | β |
| LIPA, a risk locus for coronary artery disease: decoding the variant-to-function relationship. | Li F et al. | β | 2025 | β |
| Long-read RNA-seq demarcates cis- and trans-directed alternative RNA splicing. | Quinones-Valdez G et al. | β | 2025 | β |
| Long term follow-up of multiorgan disease in Kleefstra syndrome 2 in an adult - case report. | Chen Z et al. | β | 2025 | β |
| Machine learning methods for gene regulatory network inference. | Hegde A et al. | β | 2025 | β |
| MADVAR: a lightweight, data-driven tool for automated feature selection in omics data. | Silberberg G | β | 2025 | β |
| Mapping naturally presented T cell antigens in medulloblastoma based on integrative multi-omics. | Velz J et al. | β | 2025 | β |
| Missense variants in FRS3 affect body mass index in populations of diverse ancestries. | Jonsdottir AB et al. | β | 2025 | β |
| Mitigating off-target effects of small RNAs: conventional approaches, network theory and artificial intelligence. | Bereczki Z et al. | β | 2025 | β |
| Mitophagy-mediated S1P facilitates muscle adaptive responses to endurance exercise through SPHK1-S1PR1/S1PR2 in slow-twitch myofibers. | Leng M et al. | β | 2025 | β |
| Molecular and genetic insights into human ovarian aging from single-nuclei multi-omics analyses. | Jin C et al. | β | 2025 | β |
| Molecular hallmarks of hydrocephalus. | Hale AT et al. | β | 2025 | β |
| Multi-ancestry genome-wide association analyses incorporating SNP-by-psychosocial interactions identify novel loci for serum lipids. | Bentley AR et al. | β | 2025 | β |
| Multi-ancestry genome-wide meta-analysis with 472,819 individuals identifies 32 novel risk loci for psoriasis. | Zhang M et al. | β | 2025 | β |
| MultiFusion2HPO: A Multimodal Deep Learning Approach for Enhancing Human Protein-Phenotype Association Prediction. | Zhai W et al. | β | 2025 | β |
| Multimodal analyses reveal genes driving electrophysiological maturation of neurons in the primate prefrontal cortex. | Gao Y et al. | β | 2025 | β |
| Multi-omics analysis indicates an association between TAPBP and prostate cancer. | Wang X et al. | β | 2025 | β |
| Multi-omics approaches for understanding gene-environment interactions in noncommunicable diseases: techniques, translation, and equity issues. | Alemu R et al. | β | 2025 | β |
| Multi-omics dissection of the genetic regulation underlying fatty acid composition in cattle. | Zhang T et al. | β | 2025 | β |
| Multi-omics identification of quantitative trait loci associated with vascular pathogenesis and diagnostic potential in chronic venous disease. | Chuang CH et al. | β | 2025 | β |
| Multiomics in silico analysis identifies TM4SF4 as a cell surface target in hepatocellular carcinoma. | Wong KK et al. | β | 2025 | β |
| Multiomics Investigation of Exhausted T Cells in Glioblastoma Tumor Microenvironment: <i>CCL5</i> as a Prognostic and Therapeutic Target. | Qin R et al. | β | 2025 | β |
| Multivariate Bayesian variable selection for multi-trait genetic fine mapping. | Canida T et al. | β | 2025 | β |
| Muscle Tissue Transcriptome of Idiopathic Inflammatory Myopathy Reflects the Muscle Damage Process by Monocytes and Presence of Skin Lesions. | Izuka S et al. | β | 2025 | β |
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| Notable Histologic Findings in a "Normal" Cohort: The National Institutes of Health Genotype-Tissue Expression (GTEx) Project. | Branton PA et al. | β | 2025 | β |
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| Novel mutations in ZMYND15 are associated with male infertility with oligozoospermia/azoospermia. | Wei C et al. | β | 2025 | β |
| Novel risk loci encompassing genes influencing STAT3, GPCR, and oxidative stress signaling are associated with co-morbid GERD and COPD. | Wilson AC et al. | β | 2025 | β |
| Optimized Method to Generate Well-Characterized Macrophages from Induced Pluripotent Stem Cells. | Hai Q et al. | β | 2025 | β |
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| Overcoming research bias: The untapped potential of biomedically important but understudied proteins. | Grudman S et al. | β | 2025 | β |
| Pan-cancer analysis of DCBLD1 and its association with the diagnosis, immunotherapy, and prognosis of cervical cancer. | Shen Q et al. | β | 2025 | β |
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| Pervasive glycative stress links metabolic imbalance and muscle atrophy in early-onset Parkinson's disease. | de Mello NP et al. | β | 2025 | β |
| Piezo2 in Paraventricular Neurons: Linking Heartbeat Pulsatility to Increased Oxytocin Release and Social Behavior. | Hamill OP | β | 2025 | β |
| Plasma proteomics-based organ-specific aging for all-cause mortality and cause-specific mortality: a prospective cohort study. | Zhao R et al. | β | 2025 | β |
| Plasma Proteomics of Diabetic Kidney Disease Among Asians With Younger-Onset Type 2 Diabetes. | Gurung RL et al. | β | 2025 | β |
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| PM2.5 increases the risk of early-onset COPD mediated by smoking and shared genes: a large-scale genetic analysis. | Wen J et al. | β | 2025 | β |
| Polygenic overlap with granulocyte counts identifies novel loci for clozapine metabolism and clozapine-induced agranulocytosis. | Koch E et al. | β | 2025 | β |
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| PSAT1 regulated by STAT4 enhances the proliferation, invasion and migration of ovarian cancer cells via the PI3K/AKT pathway. | Li X et al. | β | 2025 | β |
| RAB19, SERPINB9P1, and Pancreatitis in Patients Taking Azathioprine in Routine Clinical Practice: Genome and Transcriptome-Wide Association Studies. | Shah SC et al. | β | 2025 | β |
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| RNA interference versus antibody-based PCSK9 inhibition for the prevention of cardiovascular disease: a drug-target Mendelian randomization study. | Gagnon E et al. | β | 2025 | β |
| RNA Sequencing Reveals the Long Non-Coding RNA Signature in Psoriasis Keratinocytes and Identifies CYDAER as a Long Non-Coding RNA Regulating Epidermal Differentiation. | Freisenhausen JC et al. | β | 2025 | β |
| Sex- and APOE Genotype-Dependent Pain Susceptibility and Alzheimer's Risk Mediated by the Lipid Metabolism Enzyme LPCAT2. | Lai RH et al. | β | 2025 | β |
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| Single-cell eQTL Mapping Reveals Cell Subtype-specific Genetic Control and Mechanism in Malignant Transformation of Colorectal Cancer. | Chen C et al. | β | 2025 | β |
| Single-cell RNA sequencing reveals sex differences in the subcellular composition and associated gene-regulatory network activity of human carotid plaques. | Sukhavasi K et al. | β | 2025 | β |
| SMC2 as a potential prognostic biomarker in lung adenocarcinoma and its correlation with immune microenvironment. | Zheng F et al. | β | 2025 | β |
| Spatial and functional profiles distinguish target sets of Parkinson's disease and antipsychotic drugs with different clinical effects. | Karunakaran KB et al. | β | 2025 | β |
| SPP1, LYZ, and MCM5: potential diagnostic biomarkers for rheumatoid arthritis and cervical cancer comorbidity. | Liu X et al. | β | 2025 | β |
| STPath: a generative foundation model for integrating spatial transcriptomics and whole-slide images. | Huang T et al. | β | 2025 | β |
| Strict retroelement regulation is frequently lost following cancer transformation and generates a promising reservoir of cancer biomarkers. | Russ E et al. | β | 2025 | β |
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| Technical and Biological Biases in Bulk Transcriptomic Data Mining for Cancer Research. | Liu H et al. | β | 2025 | β |
| The "double-edged sword" effect of non-steroidal anti-inflammatory drugs (NSAIDs) in the treatment of endometriosis (EMS). | Shi Z et al. | β | 2025 | β |
| The emerging role of multiomics in aging research. | Ruden DM | β | 2025 | β |
| The Importance of Regulatory Network Structure for Complex Trait Heritability and Evolution. | Stone KL et al. | β | 2025 | β |
| The Influence of DNA Repair Genes and Prenatal Tobacco Exposure on Risk of Childhood Acute Lymphoblastic Leukemia: A Gene-Environment Interaction Study. | Wang X et al. | β | 2025 | β |
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| The molecular impact of cigarette smoking resembles aging across tissues. | Ramirez JM et al. | β | 2025 | β |
| The myoblast methylome: multiple types of associations with chromatin and transcription. | Sen S et al. | β | 2025 | β |
| The Overexpression of RTN4 Significantly Associated With an Unfavourable Prognosis in Patients With Lower-Grade Gliomas. | Feng J et al. | β | 2025 | β |
| The prognostic and immune significance of fibronectin type III domain-containing 1 gene in pan-cancer and its relationship with proliferation and migration of stomach adenocarcinoma. | Deng M et al. | β | 2025 | β |
| Therapeutic Potential of Glutaminase Inhibition Targeting Metabolic Adaptations in Resistant Melanomas to Targeted Therapy. | Soumoy L et al. | β | 2025 | β |
| The role of primate-specific genes in the phenotypic evolution of lorises. | Chen C et al. | β | 2025 | β |
| The Role of the Major Histocompatibility Complex Region on Chromosome 6 in Skin Atrophy: A Mendelian Randomization Study. | Zhao C et al. | β | 2025 | β |
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| Tissue-specific expression and functional role of keratin 1 in sheep horn development. | Mei Q et al. | β | 2025 | β |
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| TOPK promotes immune suppression in kidney renal clear cell carcinoma and emerges as a prognostic and therapeutic target. | Zheng Z et al. | β | 2025 | β |
| Trans-ancestry GWAS identifies 59 loci and improves risk prediction and fine-mapping for kidney stone disease. | Cao X et al. | β | 2025 | β |
| Transcriptome Complexity Disentangled: A Regulatory Molecules Approach. | Asiaee A et al. | β | 2025 | β |
| Transcriptome-Wide Association Study Identified Novel Blood Tissue Gene Biomarkers for Prostate Cancer Risk. | Sun Y et al. | β | 2025 | β |
| Transcriptome-wide association study identifies genes associated with bladder cancer risk. | Li S et al. | β | 2025 | β |
| Transcriptome-wide association study of alternative polyadenylation identifies susceptibility genes in non-small cell lung cancer. | Xu X et al. | β | 2025 | β |
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| Analysis of clinical significance and molecular characteristics of methionine metabolism and macrophage-related patterns in hepatocellular carcinoma based on machine learning. | Wen D et al. | β | 2024 | β |
| An Emerging Approach of Age-Related Hearing Loss Research: Application of Integrated Multi-Omics Analysis. | Liu Y et al. | β | 2024 | β |
| An evolutionary timeline of the oxytocin signaling pathway. | Sartorius AM et al. | β | 2024 | β |
| A new test for trait mean and variance detects unreported loci for blood-pressure variation. | Breeyear JH et al. | β | 2024 | β |
| An expression-directed linear mixed model discovering low-effect genetic variants. | Li Q et al. | β | 2024 | β |
| An integrated bioinformatic investigation of kallikrein gene family members in kidney renel cell carcinoma. | Wang B et al. | β | 2024 | β |
| An optimized instrument variable selection approach to improve causality estimation in association studies. | Sharma J et al. | β | 2024 | β |
| Application of Photoactive Compounds in Cancer Theranostics: Review on Recent Trends from Photoactive Chemistry to Artificial Intelligence. | Szymaszek P et al. | β | 2024 | β |
| Applications of Machine Learning (ML) and Mathematical Modeling (MM) in Healthcare with Special Focus on Cancer Prognosis and Anticancer Therapy: Current Status and Challenges. | Hassan J et al. | β | 2024 | β |
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| Cross-Ancestry Genome-Wide Association Study Defines the Extended CYP2D6 Locus as the Principal Genetic Determinant of Endoxifen Plasma Concentrations. | Khor CC et al. | β | 2023 | β |
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| Genetic differences according to onset age and lung function in asthma: A cluster analysis. | Kim HK et al. | β | 2023 | β |
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| Genetic insights into ossification of the posterior longitudinal ligament of the spine. | Koike Y et al. | β | 2023 | β |
| Genetic Modifiers of Age at Onset for Amyotrophic Lateral Sclerosis: A Genome-Wide Association Study. | Li C et al. | β | 2023 | β |
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| Genome-wide analyses identify NEAT1 as genetic modifier of age at onset of amyotrophic lateral sclerosis. | Li C et al. | β | 2023 | β |
| Genome-Wide Association and Inheritance-Based Analyses Implicate Unconventional Myosin Genes in Hypoplastic Left Heart Syndrome. | Theis JL et al. | β | 2023 | β |
| Genome-wide Association Studies Categorized by Class of Antihypertensive Drugs Reveal Complex Pathogenesis of Hypertension with Drug Resistance. | Yamazaki K et al. | β | 2023 | β |
| Genome-wide association study identifies multiple HLA loci for sarcoidosis susceptibility. | Liao SY et al. | β | 2023 | β |
| Genome-Wide Association Study of Age-Related Macular Degeneration Reveals 2 New Loci Implying Shared Genetic Components with Central Serous Chorioretinopathy. | Akiyama M et al. | β | 2023 | β |
| Genome-wide association study of a lipedema phenotype among women in the UK Biobank identifies multiple genetic risk factors. | Klimentidis YC et al. | β | 2023 | β |
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| GWASs Identify Genetic Loci Associated with Human Scalp Hair Whorl Direction. | Luo J et al. | β | 2023 | β |
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| <i>CAV1</i> Impacts the Tumor Immune Microenvironment and Has Potential Value of Predicting Response to Immunotherapy in Esophageal Cancer. | Zhang R et al. | β | 2023 | β |
| <i>De novo</i> identification of complex traits associated with asthma. | Zaied RE et al. | β | 2023 | β |
| Identification and Validation of the Anoikis-Related Gene Signature as a Novel Prognostic Model for Cervical Squamous Cell Carcinoma, Endocervical Adenocarcinoma, and Revelation Immune Infiltration. | Jin QQ et al. | β | 2023 | β |
| Identification of ARMH4 and WIPF3 as human podocyte proteins with potential roles in immunomodulation and cytoskeletal dynamics. | De Luca F et al. | β | 2023 | β |
| Identification of genetic loci jointly influencing COVID-19 and coronary heart diseases. | Wang S et al. | β | 2023 | β |
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| Identification of Rare Genetic Variants in Familial Spontaneous Coronary Artery Dissection and Evidence for Shared Biological Pathways. | Turley TN et al. | β | 2023 | β |
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| Identification of TRPM2 as a prognostic factor correlated with immune infiltration in ovarian cancer. | Huang W et al. | β | 2023 | β |
| Identifying polymorphic cis-regulatory variants as risk markers for lung carcinogenesis and chemotherapy responses in tobacco smokers from eastern India. | Sengupta D et al. | β | 2023 | β |
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| <i>MKX-AS1</i> Gene Expression Associated with Variation in Drug Response to Oxaliplatin and Clinical Outcomes in Colorectal Cancer Patients. | Gonzalez RD et al. | β | 2023 | β |
| Immunosuppression causes dynamic changes in expression QTLs in psoriatic skin. | Xiao Q et al. | β | 2023 | β |
| Improving liver transplant outcomes with transplant-omics and network biology. | Scarpa J | β | 2023 | β |
| Increased G3BP2-Tau interaction in tauopathies is a natural defense against Tau aggregation. | Wang C et al. | β | 2023 | β |
| Inhibition of glutaminase-1 in DLBCL potentiates venetoclax-induced antitumor activity by promoting oxidativeΒ stress. | Gomez Solsona B et al. | β | 2023 | β |
| Insights into Sex and Gender Differences in Brain and Psychopathologies Using Big Data. | Zelco A et al. | β | 2023 | β |
| In Silico Structural and Functional Analyses of NLRP3 Inflammasomes to Provide Insights for Treating Neurodegenerative Diseases. | Ghazi BK et al. | β | 2023 | β |
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| Integrating eQTL and GWAS data characterises established and identifies novel migraine risk loci. | Ghaffar A et al. | β | 2023 | β |
| Integrative analyses for the identification of idiopathic pulmonary fibrosis-associated genes and shared loci with other diseases. | Chen M et al. | β | 2023 | β |
| Integrative genome-wide analyses identify novel loci associated with kidney stones and provide insights into its genetic architecture. | Hao X et al. | β | 2023 | β |
| Integrative Genomic Analyses Identify LncRNA Regulatory Networks across Pediatric Leukemias and Solid Tumors. | Modi A et al. | β | 2023 | β |
| Integrative mapping of the dog epigenome: Reference annotation for comparative intertissue and cross-species studies. | Son KH et al. | β | 2023 | β |
| Integrative Mendelian randomization reveals the soluble receptor for advanced glycation end products as protective in relation to rheumatoid arthritis. | Lee GY et al. | β | 2023 | β |
| Integrative Post-Genome-Wide Association Study Analyses Relevant to Psychiatric Disorders: Imputing Transcriptome and Proteome Signals. | Gedik H et al. | β | 2023 | β |
| Integrin Ξ²3-Mediated Cell Senescence Associates with Gut Inflammation and Intestinal Degeneration in Models of Alzheimer's Disease. | Tun X et al. | β | 2023 | β |
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| Interindividual variation in human cortical cell type abundance and expression. | Johansen N et al. | β | 2023 | β |
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| Involvement in Tumorigenesis and Clinical Significance of CXCL1 in Reproductive Cancers: Breast Cancer, Cervical Cancer, Endometrial Cancer, Ovarian Cancer and Prostate Cancer. | Korbecki J et al. | β | 2023 | β |
| <i>Stranger Twins</i>: A Tale of Resemblance and Contrast Between VAP Proteins. | Subra M et al. | β | 2023 | β |
| ITGA3 acts as a purity-independent biomarker of both immunotherapy and chemotherapy resistance in pancreatic cancer: bioinformatics and experimental analysis. | Zheng X et al. | β | 2023 | β |
| Joint analysis of GWAS and multi-omics QTL summary statistics reveals a large fraction of GWAS signals shared with molecular phenotypes. | Wu Y et al. | β | 2023 | β |
| KISL: knowledge-injected semi-supervised learning for biological co-expression network modules. | Xiao G et al. | β | 2023 | β |
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| Leveraging genetic overlap between irritability and psychiatric disorders to identify genetic variants of major psychiatric disorders. | Jung K et al. | β | 2023 | β |
| Linking Prenatal Environmental Exposures to Lifetime Health with Epigenome-Wide Association Studies: State-of-the-Science Review and Future Recommendations. | Bakulski KM et al. | β | 2023 | β |
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| Loss of RREB1 in pancreatic beta cells reduces cellular insulin content and affects endocrine cell gene expression. | Mattis KK et al. | β | 2023 | β |
| Loss of the Atrial Fibrillation-Related Gene, <i>Zfhx3</i>, Results in Atrial Dilation and Arrhythmias. | Jameson HS et al. | β | 2023 | β |
| Mapping genetic variants for nonsense-mediated mRNA decay regulation across human tissues. | Sun B et al. | β | 2023 | β |
| Mendelian Randomization Analysis Provides Insights into the Pathogenesis of Serum Levels of Branched-Chain Amino Acids in Cardiovascular Disease. | Jiang W et al. | β | 2023 | β |
| Metabolomic Investigation of Major Depressive Disorder Identifies a Potentially Causal Association With Polyunsaturated Fatty Acids. | Davyson E et al. | β | 2023 | β |
| Microbial gene expression analysis of healthy and cancerous esophagus uncovers bacterial biomarkers of clinical outcomes. | SchΓ€ffer DE et al. | β | 2023 | β |
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| Molecular differences in brain regional vulnerability to aging between males and females. | Zhou X et al. | β | 2023 | β |
| Molecular mechanisms of coronary artery disease risk at the PDGFD locus. | Kim HJ et al. | β | 2023 | β |
| MTHFR act as a potential cancer biomarker in immune checkpoints blockades, heterogeneity, tumor microenvironment and immune infiltration. | Peng J et al. | β | 2023 | β |
| Multidimensional conservation analysis decodes the expression of conserved long noncoding RNAs. | Zhou Q et al. | β | 2023 | β |
| multi-GPA-Tree: Statistical approach for pleiotropy informed and functional annotation tree guided prioritization of GWAS results. | Khatiwada A et al. | β | 2023 | β |
| Multi-Omics Studies in Historically Excluded Populations: The Road to Equity. | Yang G et al. | β | 2023 | β |
| Multivariate GWAS analysis reveals loci associated with liver functions in continental African populations. | Soremekun C et al. | β | 2023 | β |
| Myo1e overexpression in lung adenocarcinoma is associated with increased risk of mortality. | Jusue-Torres I et al. | β | 2023 | β |
| Narcolepsy risk loci outline role of T cell autoimmunity and infectious triggers in narcolepsy. | Ollila HM et al. | β | 2023 | β |
| NetBID2 provides comprehensive hidden driver analysis. | Dong X et al. | β | 2023 | β |
| Neural functions in cancer: Data analyses and database construction. | Tan R et al. | β | 2023 | β |
| Neurodevelopmental risk and adaptation as a model for comorbidity among internalizing and externalizing disorders: genomics and cell-specific expression enriched morphometric study. | Kuang N et al. | β | 2023 | β |
| NFIB facilitates replication licensing by acting as a genome organizer. | Zhang W et al. | β | 2023 | β |
| Noncoding RNAs improve the predictive power of network medicine. | Morselli Gysi D et al. | β | 2023 | β |
| Noval ceRNA axis-mediated high expression of <i>TOP2A</i> correlates with poor prognosis and tumor immune infiltration of hepatocellular carcinoma. | Wang XQ et al. | β | 2023 | β |
| Novel rare genetic variants of familial and sporadic pulmonary atresia identified by whole-exome sequencing. | Xing J et al. | β | 2023 | β |
| Omics-driven investigation of the biology underlying intrinsic submaximal working capacity and its trainability. | Hota M et al. | β | 2023 | β |
| OOCDB: A Comprehensive, Systematic, and Real-time Organs-on-a-chip Database. | Li J et al. | β | 2023 | β |
| OrganoidDB: a comprehensive organoid database for the multi-perspective exploration of bulk and single-cell transcriptomic profiles of organoids. | Ma Q et al. | β | 2023 | β |
| Patterns of item nonresponse behaviour to survey questionnaires are systematic and associated with genetic loci. | Mignogna G et al. | β | 2023 | β |
| PFKP is a prospective prognostic, diagnostic, immunological and drug sensitivity predictor across pan-cancer. | Peng J et al. | β | 2023 | β |
| Pharmacogenomics of intravenous immunoglobulin response in Kawasaki disease. | Shrestha S et al. | β | 2023 | β |
| Pleiotropic loci for cannabis use disorder severity in multi-ancestry high-risk populations. | Peng Q et al. | β | 2023 | β |
| Polygenic influences on the behavioral effects of alcohol withdrawal in a mixed-ancestry population from the collaborative study on the genetics of alcoholism (COGA). | Benca-Bachman CE et al. | β | 2023 | β |
| Polygenic overlap with body-mass index improves prediction of treatment-resistant schizophrenia. | O'Connell KS et al. | β | 2023 | β |
| Polymorphisms within Autophagy-Related Genes as Susceptibility Biomarkers for Multiple Myeloma: A Meta-Analysis of Three Large Cohorts and Functional Characterization. | Clavero E et al. | β | 2023 | β |
| Potentially functional genetic variants in RPS6KA4 and MAP2K5 in the MAPK signaling pathway predict HBV-related hepatocellular carcinoma survival. | Qiu M et al. | β | 2023 | β |
| Potentially Functional Genetic Variants in the NRF2 Signaling Pathway Genes are Associated With HBV-related Hepatocellular Carcinoma Survival. | Gong R et al. | β | 2023 | β |
| Prediction Model for Pre-Eclampsia Using Gestational-Age-Specific Serum Creatinine Distribution. | Kang J et al. | β | 2023 | β |
| PrismEXP: gene annotation prediction from stratified gene-gene co-expression matrices. | Lachmann A et al. | β | 2023 | β |
| Programmed cell death 11 modulates but not entirely relies on p53-HDM2 loop to facilitate G2/M transition in colorectal cancer cells. | Ding L et al. | β | 2023 | β |
| Promoter evolution of mammalian gene duplicates. | Fraimovitch E et al. | β | 2023 | β |
| Prospective Blood Transcriptomics Study in a Motor Vehicle Collision Cohort Identified a Protective Function of the SAMD15 Gene Against Chronic Pain. | Parisien M et al. | β | 2023 | β |
| Proteomic sequencing analysis in a rat model of atrial fibrosis caused by chronic intermittent hypoxia. | Zhao B et al. | β | 2023 | β |
| Pulse-SILAC and Interactomics Reveal Distinct DDB1-CUL4-Associated Factors, Cellular Functions, and Protein Substrates. | Raisch J et al. | β | 2023 | β |
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| Refined expression quantitative trait locus analysis on adenocarcinoma at the gastroesophageal junction reveals susceptibility and prognostic markers. | Zhong C et al. | β | 2023 | β |
| Regulator of G-Protein Signalling 9: A New Candidate Gene for Sweet Food Liking? | Graham CA et al. | β | 2023 | β |
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| Repurposing ketamine to treat cocaine use disorder: integration of artificial intelligence-based prediction, expert evaluation, clinical corroboration and mechanism of action analyses. | Gao Z et al. | β | 2023 | β |
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| Screening Plasma Proteins for the Putative Drug Targets for Carpal Tunnel Syndrome. | Han BX et al. | β | 2023 | β |
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| Senescence-associated 13-HODE production promotes age-related liver steatosis by directly inhibiting catalase activity. | Duan J et al. | β | 2023 | β |
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| Targeting IRG1 reverses the immunosuppressive function of tumor-associated macrophages and enhances cancer immunotherapy. | Chen YJ et al. | β | 2023 | β |
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| The Continuing Saga of Tissue Inhibitor of Metalloproteinase 2: Emerging Roles in Tissue Homeostasis and Cancer Progression. | Stetler-Stevenson WG | β | 2023 | β |
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| The evaluation of six genes combined value in glioma diagnosis and prognosis. | Lin P et al. | β | 2023 | β |
| The function of guanylate binding protein 3 (GBP3) in human cancers by pan-cancer bioinformatics. | Jiang T et al. | β | 2023 | β |
| The genetic basis of endometriosis and comorbidity with other pain and inflammatory conditions. | Rahmioglu N et al. | β | 2023 | β |
| The genetic overlap between Alzheimer's disease, amyotrophic lateral sclerosis, Lewy body dementia, and Parkinson's disease. | Wightman DP et al. | β | 2023 | β |
| The Impacts of Slc19a3 Deletion and Intestinal SLC19A3 Insertion on Thiamine Distribution and Brain Metabolism in the Mouse. | Wen A et al. | β | 2023 | β |
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| The Long Non-Coding RNA ANRIL in Cancers. | Sanchez A et al. | β | 2023 | β |
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| The RNA interactome in the Hallmarks of Cancer. | Gabryelska MM et al. | β | 2023 | β |
| The technological landscape and applications of single-cell multi-omics. | Baysoy A et al. | β | 2023 | β |
| The Type 2 Diabetes Knowledge Portal: An open access genetic resource dedicated to type 2 diabetes and related traits. | Costanzo MC et al. | β | 2023 | β |
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| Comprehensive multi-omics analysis of the m7G in pan-cancer from the perspective of predictive, preventive, and personalized medicine. | Huang X et al. | β | 2022 | β |
| Cumulative evidence for associations between genetic variants in interleukin 17 family gene and risk of human diseases. | Liu T et al. | β | 2022 | β |
| DeepPerVar: a multi-modal deep learning framework for functional interpretation of genetic variants in personal genome. | Wang Y et al. | β | 2022 | β |
| Development of Type 1 Diabetes may occur through a Type 2 Diabetes mechanism. | Josefsen K et al. | β | 2022 | β |
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| Discovery of 42 genome-wide significant loci associated with dyslexia. | Doust C et al. | β | 2022 | β |
| Genes Whose Gain or Loss of Function Changes Type 1, 2A, 2X, or 2B Muscle Fibre Proportions in Mice-A Systematic Review. | Kuhnen G et al. | β | 2022 | β |
| Genetic architecture of heart failure with preserved versus reduced ejection fraction. | Joseph J et al. | β | 2022 | β |
| Genome-Transcriptome-Functional Connectivity-Cognition Link Differentiates Schizophrenia From Bipolar Disorder. | Chen J et al. | β | 2022 | β |
| Genome-wide association and multi-trait analyses characterize the common genetic architecture of heart failure. | Levin MG et al. | β | 2022 | β |
| Genome-wide association study identifies novel loci associated with skin autofluorescence in individuals without diabetes. | Vollenbrock CE et al. | β | 2022 | β |
| Genome-wide association study of REM sleep behavior disorder identifies polygenic risk and brain expression effects. | Krohn L et al. | β | 2022 | β |
| Genome-wide imputed differential expression enrichment analysis identifies trait-relevant tissues. | Ghaffar A et al. | β | 2022 | β |
| Germline Genetic and Treatment-Related Risk Factors for Diabetes Mellitus in Survivors of Childhood Cancer: A Report From the Childhood Cancer Survivor Study and St Jude Lifetime Cohorts. | Richard MA et al. | β | 2022 | β |
| Identification and Prioritization of PET Neuroimaging Targets for Microglial Phenotypes Associated with Microglial Activity in Alzheimer's Disease. | Bartolo ND et al. | β | 2022 | β |
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| Identification of transcriptional regulatory variants in pig duodenum, liver, and muscle tissues. | Crespo-Piazuelo D et al. | β | 2022 | β |
| Interleukin-8 in Colorectal Cancer: A Systematic Review and Meta-Analysis of Its Potential Role as a Prognostic Biomarker. | Bazzichetto C et al. | β | 2022 | β |
| Lineage-selective super enhancers mediate core regulatory circuitry during adipogenic and osteogenic differentiation of human mesenchymal stem cells. | Wang C et al. | β | 2022 | β |
| LipGene: Lipschitz Continuity Guided Adaptive Learning Rates for Fast Convergence on Microarray Expression Data Sets. | Prashanth T et al. | β | 2022 | β |
| Mer-tyrosine kinase: a novel susceptibility gene for SLE related end-stage renal disease. | Yavuz S et al. | β | 2022 | β |
| MetGENE: gene-centric metabolomics information retrieval tool. | Srinivasan S et al. | β | 2022 | β |
| Multi-trait genome-wide association study of opioid addiction: OPRM1 and beyond. | Gaddis N et al. | β | 2022 | β |
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| PAIP2 is a potential diagnostic and prognostic biomarker of breast cancer and is associated with immune infiltration. | Wang C et al. | β | 2022 | β |
| Pan-Cancer Analysis Identifies Tumor Cell Surface Targets for CAR-T Cell Therapies and Antibody Drug Conjugates. | Li X et al. | β | 2022 | β |
| Pancan-MNVQTLdb: systematic identification of multi-nucleotide variantΒ quantitative trait loci in 33 cancer types. | Wang D et al. | β | 2022 | β |
| Pan-Tissue and -Cancer Analysis of ROR1 and ROR2 Transcript Variants Identify Novel Functional Significance for an Alternative Splice Variant of ROR1. | John M et al. | β | 2022 | β |
| PCDH9 suppresses melanoma proliferation and cell migration. | Zhang J et al. | β | 2022 | β |
| Positive selection-driven fixation of a hominin-specific amino acid mutation related to dephosphorylation in IRF9. | Chen J et al. | β | 2022 | β |
| Promoter-Adjacent DNA Hypermethylation Can Downmodulate Gene Expression: <i>TBX15</i> in the Muscle Lineage. | Ehrlich KC et al. | β | 2022 | β |
| Robust and rigorous identification of tissue-specific genes by statistically extending tau score. | LΓΌleci HB et al. | β | 2022 | β |
| Systematic analysis of the effects of genetic variants on chromatin accessibility to decipher functional variants in non-coding regions. | Wang D et al. | β | 2022 | β |
| The pathogenesis of coronavirus-19 disease. | Borczuk AC et al. | β | 2022 | β |
| The Role of Long Noncoding RNAs on Male Infertility: A Systematic Review and In Silico Analysis. | Kyrgiafini MA et al. | β | 2022 | β |
| The tamoxifen-regulated, long non-coding RNA LINC00992 affects proliferation, migration, and expression of tamoxifen resistance-associated genes in MCF-7 breast cancer cells. | Graf S et al. | β | 2022 | β |
| The type 1 diabetes gene TYK2 regulates Ξ²-cell development and its responses to interferon-Ξ±. | Chandra V et al. | β | 2022 | β |
| Towards future directions in data-integrative supervised prediction of human aging-related genes. | Li Q et al. | β | 2022 | β |
| Transcriptome-wide and stratified genomic structural equation modeling identify neurobiological pathways shared across diverse cognitive traits. | Grotzinger AD et al. | β | 2022 | β |
| Whole exome sequencing in Brugada and long QT syndromes revealed novel rare and potential pathogenic mutations related to the dysfunction of the cardiac sodium channel. | Chen J et al. | β | 2022 | β |
| XCVATR: detection and characterization of variant impact on the Embeddings of single -cell and bulk RNA-sequencing samples. | Harmanci A et al. | β | 2022 | β |