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  1. Article ; Online: Variant to gene mapping for carpal tunnel syndrome risk loci implicates skeletal muscle regulatory elements.

    Pahl, Matthew C / Liu, Lin / Pippin, James A / Wagley, Yadav / Boehm, Keith / Hankenson, Kurt D / Wells, Andrew D / Yang, Wenli / Grant, Struan F A

    EBioMedicine

    2024  Volume 101, Page(s) 105038

    Abstract: Background: Carpal tunnel syndrome (CTS) is a common disorder caused by compression of the median nerve in the wrist, resulting in pain and numbness throughout the hand and forearm. While multiple behavioural and physiological factors influence CTS risk, ...

    Abstract Background: Carpal tunnel syndrome (CTS) is a common disorder caused by compression of the median nerve in the wrist, resulting in pain and numbness throughout the hand and forearm. While multiple behavioural and physiological factors influence CTS risk, a growing body of evidence supports a strong genetic contribution. Recent genome-wide association study (GWAS) efforts have reported 53 independent signals associated with CTS. While GWAS can identify genetic loci conferring risk, it does not determine which cell types drive the genetic aetiology of the trait, which variants are "causal" at a given signal, and which effector genes correspond to these non-coding variants. These obstacles limit interpretation of potential disease mechanisms.
    Methods: We analysed CTS GWAS findings in the context of chromatin conformation between gene promoters and accessible chromatin regions across cellular models of bone, skeletal muscle, adipocytes and neurons. We identified proxy variants in high LD with the lead CTS sentinel SNPs residing in promoter connected open chromatin in the skeletal muscle and bone contexts.
    Findings: We detected significant enrichment for heritability in skeletal muscle myotubes, as well as a weaker correlation in human mesenchymal stem cell-derived osteoblasts. In myotubes, our approach implicated 117 genes contacting 60 proxy variants corresponding to 20 of the 53 GWAS signals. In the osteoblast context we implicated 30 genes contacting 24 proxy variants coinciding with 12 signals, of which 19 genes shared. We subsequently prioritized BZW2 as a candidate effector gene in CTS and implicated it as novel gene that perturbs myocyte differentiation in vitro.
    Interpretation: Taken together our results suggest that the CTS genetic component influences the size, integrity, and organization of multiple tissues surrounding the carpal tunnel, in particular muscle and bone, to predispose the nerve to being compressed in this disease setting.
    Funding: This work was supported by NIH Grant UM1 DK126194 (SFAG and WY), R01AG072705 (SFAG & KDH) and the Center for Spatial and Functional Genomics at CHOP (SFAG & ADW). SFAG is supported by the Daniel B. Burke Endowed Chair for Diabetes Research. WY is supported by the Perelman School of Medicine of the University of Pennsylvania.
    MeSH term(s) Humans ; Carpal Tunnel Syndrome/genetics ; Genome-Wide Association Study ; Muscle, Skeletal ; Chromosome Mapping ; Chromatin/genetics ; DNA-Binding Proteins/genetics
    Chemical Substances Chromatin ; BZW2 protein, human ; DNA-Binding Proteins
    Language English
    Publishing date 2024-02-27
    Publishing country Netherlands
    Document type Journal Article
    ZDB-ID 2851331-9
    ISSN 2352-3964
    ISSN (online) 2352-3964
    DOI 10.1016/j.ebiom.2024.105038
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  2. Article ; Online: Osteoporosis GWAS-implicated

    Kaur, Gurcharan / Pippin, James A / Chang, Solomon / Redmond, Justin / Chesi, Alessandra / Wells, Andrew D / Maerz, Tristan / Grant, Struan F A / Coleman, Rhima M / Hankenson, Kurt D / Wagley, Yadav

    JBMR plus

    2024  Volume 8, Issue 5, Page(s) ziae051

    Abstract: Genome wide association study (GWAS)-implicated bone mineral density (BMD) signals have been shown to localize in cis-regulatory regions of distal effector genes using 3D genomic methods. Detailed characterization of such genes can reveal novel causal ... ...

    Abstract Genome wide association study (GWAS)-implicated bone mineral density (BMD) signals have been shown to localize in cis-regulatory regions of distal effector genes using 3D genomic methods. Detailed characterization of such genes can reveal novel causal genes for BMD determination. Here, we elected to characterize the "
    Language English
    Publishing date 2024-04-10
    Publishing country England
    Document type Journal Article
    ISSN 2473-4039
    ISSN (online) 2473-4039
    DOI 10.1093/jbmrpl/ziae051
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  3. Article ; Online: Perturbation of the insomnia WDR90 GWAS locus pinpoints rs3752495 as a causal variant influencing distal expression of neighboring gene, PIG-Q.

    Sonti, Shilpa / Littleton, Sheridan H / Pahl, Matthew C / Zimmerman, Amber J / Chesi, Alessandra / Palermo, Justin / Lasconi, Chiara / Brown, Elizabeth B / Pippin, James A / Wells, Andrew D / Doldur-Balli, Fusun / Pack, Allan I / Gehrman, Phillip R / Keene, Alex C / Grant, Struan F A

    Sleep

    2024  

    Abstract: Although genome wide association studies (GWAS) have identified loci for sleep-related traits, they do not directly uncover the underlying causal variants and corresponding effector genes. The majority of such variants reside in non-coding regions and ... ...

    Abstract Although genome wide association studies (GWAS) have identified loci for sleep-related traits, they do not directly uncover the underlying causal variants and corresponding effector genes. The majority of such variants reside in non-coding regions and are therefore presumed to impact cis-regulatory elements. Our previously reported 'variant-to-gene mapping' effort in human induced pluripotent stem cell (iPSC)-derived neural progenitor cells (NPCs), combined with validation in both Drosophila and zebrafish, implicated PIG-Q as a functionally relevant gene at the insomnia 'WDR90' GWAS locus. However, importantly that effort did not characterize the corresponding underlying causal variant. Specifically, our previous 3D genomic datasets nominated a shortlist of three neighboring single nucleotide polymorphisms (SNPs) in strong linkage disequilibrium within an intronic enhancer region of WDR90 that contacted the open PIG-Q promoter. We sought to investigate the influence of these SNPs collectively and then individually on PIG-Q modulation to pinpoint the causal "regulatory" variant. Starting with gross level perturbation, deletion of the entire region in NPCs via CRISPR-Cas9 editing and subsequent RNA sequencing revealed expression changes in specific PIG-Q transcripts. Results from individual luciferase reporter assays for each SNP in iPSCs revealed that the region with the rs3752495 risk allele induced a ~2.5-fold increase in luciferase expression. Importantly, rs3752495 also exhibited an allele specific effect, with the risk allele increasing the luciferase expression by ~2-fold versus the non-risk allele. In conclusion, our variant-to-function approach and in vitro validation implicates rs3752495 as a causal insomnia variant embedded within WDR90 while modulating the expression of the distally located PIG-Q.
    Language English
    Publishing date 2024-04-04
    Publishing country United States
    Document type Journal Article
    ZDB-ID 424441-2
    ISSN 1550-9109 ; 0161-8105
    ISSN (online) 1550-9109
    ISSN 0161-8105
    DOI 10.1093/sleep/zsae085
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  4. Article: GWAS-informed data integration and non-coding CRISPRi screen illuminate genetic etiology of bone mineral density.

    Conery, Mitchell / Pippin, James A / Wagley, Yadav / Trang, Khanh / Pahl, Matthew C / Villani, David A / Favazzo, Lacey J / Ackert-Bicknell, Cheryl L / Zuscik, Michael J / Katsevich, Eugene / Wells, Andrew D / Zemel, Babette S / Voight, Benjamin F / Hankenson, Kurt D / Chesi, Alessandra / Grant, Struan F A

    bioRxiv : the preprint server for biology

    2024  

    Abstract: Over 1,100 independent signals have been identified with genome-wide association studies (GWAS) for bone mineral density (BMD), a key risk factor for mortality-increasing fragility fractures; however, the effector gene(s) for most remain unknown. ... ...

    Abstract Over 1,100 independent signals have been identified with genome-wide association studies (GWAS) for bone mineral density (BMD), a key risk factor for mortality-increasing fragility fractures; however, the effector gene(s) for most remain unknown. Informed by a variant-to-gene mapping strategy implicating 89 non-coding elements predicted to regulate osteoblast gene expression at BMD GWAS loci, we executed a single-cell CRISPRi screen in human fetal osteoblast 1.19 cells (hFOBs). The BMD relevance of hFOBs was supported by heritability enrichment from cross-cell type stratified LD-score regression involving 98 cell types grouped into 15 tissues. 24 genes showed perturbation in the screen, with four (
    Language English
    Publishing date 2024-03-20
    Publishing country United States
    Document type Preprint
    DOI 10.1101/2024.03.19.585778
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  5. Article ; Online: Colorectal Cancer-Associated Smad4 R361 Hotspot Mutations Boost Wnt/β-Catenin Signaling through Enhanced Smad4-LEF1 Binding.

    Lanauze, Claudia B / Sehgal, Priyanka / Hayer, Katharina / Torres-Diz, Manuel / Pippin, James A / Grant, Struan F A / Thomas-Tikhonenko, Andrei

    Molecular cancer research : MCR

    2021  Volume 19, Issue 5, Page(s) 823–833

    Abstract: About 10% to 30% of patients with colorectal cancer harbor either loss of or missense mutations in SMAD4, a critical component of the TGFβ signaling pathway. The pathophysiologic function of missense mutations in Smad4 is not fully understood. They ... ...

    Abstract About 10% to 30% of patients with colorectal cancer harbor either loss of or missense mutations in SMAD4, a critical component of the TGFβ signaling pathway. The pathophysiologic function of missense mutations in Smad4 is not fully understood. They usually map to the MH2 domain, specifically to residues that are involved in heterodimeric complex formation with regulatory Smads (such as Smad2/3) and ensuing transcriptional activation. These detrimental effects suggest that SMAD4 missense mutations can be categorized as loss-of-function. However, they tend to cluster in a few hotspots, which is more consistent with them acting by a gain-of-function mechanism. In this study, we investigated the functional role of Smad4 R361 mutants by re-expressing two R361 Smad4 variants in several Smad4-null colorectal cancer cell lines. As predicted, R361 mutations disrupted Smad2/3-Smad4 heteromeric complex formation and abolished canonical TGFβ signaling. In that, they were similar to SMAD4 loss. However, RNA sequencing and subsequent RT-PCR assays revealed that Smad4mut cells acquired a gene signature associated with enhanced Lef1 protein function and increased Wnt signaling. Mechanistically, Smad4 mutant proteins retained binding to Lef1 protein and drove a commensurate increase in downstream Wnt signaling as measured by TOP/FOP luciferase assay and Wnt-dependent cell motility. Consistent with these findings, human colorectal cancers with SMAD4 missense mutations were less likely to acquire activating mutations in the key Wnt pathway gene CTNNB1 (encoding β-catenin) than colorectal cancers with truncating SMAD4 nonsense mutations. IMPLICATIONS: Our studies suggest that in colorectal cancer hotspot mutations in Smad4 confer enhanced Wnt signaling and possibly heightened sensitivity to Wnt pathway inhibitors. VISUAL OVERVIEW: http://mcr.aacrjournals.org/content/molcanres/19/5/823/F1.large.jpg.
    MeSH term(s) Colorectal Neoplasms/genetics ; Colorectal Neoplasms/pathology ; Humans ; Lymphoid Enhancer-Binding Factor 1/metabolism ; Mutation ; Smad4 Protein/metabolism ; Transfection ; Wnt Signaling Pathway/genetics
    Chemical Substances LEF1 protein, human ; Lymphoid Enhancer-Binding Factor 1 ; SMAD4 protein, human ; Smad4 Protein
    Language English
    Publishing date 2021-02-19
    Publishing country United States
    Document type Journal Article ; Research Support, N.I.H., Extramural ; Research Support, Non-U.S. Gov't
    ZDB-ID 2098788-2
    ISSN 1557-3125 ; 1541-7786
    ISSN (online) 1557-3125
    ISSN 1541-7786
    DOI 10.1158/1541-7786.MCR-20-0721
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  6. Article: Variant-to-function analysis of the childhood obesity chr12q13 locus implicates rs7132908 as a causal variant within the 3' UTR of

    Littleton, Sheridan H / Trang, Khanh B / Volpe, Christina M / Cook, Kieona / DeBruyne, Nicole / Ann Maguire, Jean / Ann Weidekamp, Mary / Boehm, Keith / Chesi, Alessandra / Pippin, James A / Anderson, Stewart A / Wells, Andrew D / Pahl, Matthew C / Grant, Struan F A

    bioRxiv : the preprint server for biology

    2023  

    Abstract: The ch12q13 obesity locus is among the most significant childhood obesity loci identified in genome-wide association studies. This locus resides in a non-coding region ... ...

    Abstract The ch12q13 obesity locus is among the most significant childhood obesity loci identified in genome-wide association studies. This locus resides in a non-coding region within
    Language English
    Publishing date 2023-08-22
    Publishing country United States
    Document type Preprint
    DOI 10.1101/2023.08.21.553157
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  7. Article ; Online: Variant-to-gene mapping followed by cross-species genetic screening identifies GPI-anchor biosynthesis as a regulator of sleep.

    Palermo, Justin / Chesi, Alessandra / Zimmerman, Amber / Sonti, Shilpa / Pahl, Matthew C / Lasconi, Chiara / Brown, Elizabeth B / Pippin, James A / Wells, Andrew D / Doldur-Balli, Fusun / Mazzotti, Diego R / Pack, Allan I / Gehrman, Phillip R / Grant, Struan F A / Keene, Alex C

    Science advances

    2023  Volume 9, Issue 1, Page(s) eabq0844

    Abstract: Genome-wide association studies (GWAS) in humans have identified loci robustly associated with several heritable diseases or traits, yet little is known about the functional roles of the underlying causal variants in regulating sleep duration or quality. ...

    Abstract Genome-wide association studies (GWAS) in humans have identified loci robustly associated with several heritable diseases or traits, yet little is known about the functional roles of the underlying causal variants in regulating sleep duration or quality. We applied an ATAC-seq/promoter focused Capture C strategy in human iPSC-derived neural progenitors to carry out a "variant-to-gene" mapping campaign that identified 88 candidate sleep effector genes connected to relevant GWAS signals. To functionally validate the role of the implicated effector genes in sleep regulation, we performed a neuron-specific RNA interference screen in the fruit fly,
    MeSH term(s) Animals ; Humans ; Glycosylphosphatidylinositols/genetics ; Drosophila melanogaster/genetics ; Genome-Wide Association Study/methods ; Zebrafish/genetics ; Chromosome Mapping ; Genetic Testing ; Sleep/genetics
    Chemical Substances Glycosylphosphatidylinositols
    Language English
    Publishing date 2023-01-06
    Publishing country United States
    Document type Journal Article
    ZDB-ID 2810933-8
    ISSN 2375-2548 ; 2375-2548
    ISSN (online) 2375-2548
    ISSN 2375-2548
    DOI 10.1126/sciadv.abq0844
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  8. Article: Perturbation of the insomnia

    Sonti, Shilpa / Littleton, Sheridan H / Pahl, Matthew C / Zimmerman, Amber J / Chesi, Alessandra / Palermo, Justin / Lasconi, Chiara / Brown, Elizabeth B / Pippin, James A / Wells, Andrew D / Doldur-Balli, Fusun / Pack, Allan I / Gehrman, Phillip R / Keene, Alex C / Grant, S F A

    bioRxiv : the preprint server for biology

    2023  

    Abstract: Although genome wide association studies (GWAS) have been crucial for the identification of loci associated with sleep traits and disorders, the method itself does not directly uncover the underlying causal variants and corresponding effector genes. The ... ...

    Abstract Although genome wide association studies (GWAS) have been crucial for the identification of loci associated with sleep traits and disorders, the method itself does not directly uncover the underlying causal variants and corresponding effector genes. The overwhelming majority of such variants reside in non-coding regions and are therefore presumed to impact the activity of
    Language English
    Publishing date 2023-08-18
    Publishing country United States
    Document type Preprint
    DOI 10.1101/2023.08.17.553739
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  9. Article ; Online: 3D chromatin maps of the human pancreas reveal lineage-specific regulatory architecture of T2D risk.

    Su, Chun / Gao, Long / May, Catherine L / Pippin, James A / Boehm, Keith / Lee, Michelle / Liu, Chengyang / Pahl, Matthew C / Golson, Maria L / Naji, Ali / Grant, Struan F A / Wells, Andrew D / Kaestner, Klaus H

    Cell metabolism

    2022  Volume 34, Issue 9, Page(s) 1394–1409.e4

    Abstract: Three-dimensional (3D) chromatin organization maps help dissect cell-type-specific gene regulatory programs. Furthermore, 3D chromatin maps contribute to elucidating the pathogenesis of complex genetic diseases by connecting distal regulatory regions and ...

    Abstract Three-dimensional (3D) chromatin organization maps help dissect cell-type-specific gene regulatory programs. Furthermore, 3D chromatin maps contribute to elucidating the pathogenesis of complex genetic diseases by connecting distal regulatory regions and genetic risk variants to their respective target genes. To understand the cell-type-specific regulatory architecture of diabetes risk, we generated transcriptomic and 3D epigenomic profiles of human pancreatic acinar, alpha, and beta cells using single-cell RNA-seq, single-cell ATAC-seq, and high-resolution Hi-C of sorted cells. Comparisons of these profiles revealed differential A/B (open/closed) chromatin compartmentalization, chromatin looping, and transcriptional factor-mediated control of cell-type-specific gene regulatory programs. We identified a total of 4,750 putative causal-variant-to-target-gene pairs at 194 type 2 diabetes GWAS signals using pancreatic 3D chromatin maps. We found that the connections between candidate causal variants and their putative target effector genes are cell-type stratified and emphasize previously underappreciated roles for alpha and acinar cells in diabetes pathogenesis.
    MeSH term(s) Chromatin ; Diabetes Mellitus, Type 2/genetics ; Diabetes Mellitus, Type 2/pathology ; Gene Expression Regulation ; Humans ; Insulin-Secreting Cells/pathology ; Islets of Langerhans/pathology
    Chemical Substances Chromatin
    Language English
    Publishing date 2022-10-12
    Publishing country United States
    Document type Journal Article ; Research Support, N.I.H., Extramural ; Research Support, Non-U.S. Gov't
    ZDB-ID 2176834-1
    ISSN 1932-7420 ; 1550-4131
    ISSN (online) 1932-7420
    ISSN 1550-4131
    DOI 10.1016/j.cmet.2022.08.014
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  10. Article ; Online: Variant-to-gene-mapping analyses reveal a role for pancreatic islet cells in conferring genetic susceptibility to sleep-related traits.

    Lasconi, Chiara / Pahl, Matthew C / Pippin, James A / Su, Chun / Johnson, Matthew E / Chesi, Alessandra / Boehm, Keith / Manduchi, Elisabetta / Ou, Kristy / Golson, Maria L / Wells, Andrew D / Kaestner, Klaus H / Grant, Struan F A

    Sleep

    2022  Volume 45, Issue 8

    Abstract: We investigated the potential role of sleep-trait associated genetic loci in conferring a degree of their effect via pancreatic α- and β-cells, given that both sleep disturbances and metabolic disorders, including type 2 diabetes and obesity, involve ... ...

    Abstract We investigated the potential role of sleep-trait associated genetic loci in conferring a degree of their effect via pancreatic α- and β-cells, given that both sleep disturbances and metabolic disorders, including type 2 diabetes and obesity, involve polygenic contributions and complex interactions. We determined genetic commonalities between sleep and metabolic disorders, conducting linkage disequilibrium genetic correlation analyses with publicly available GWAS summary statistics. Then we investigated possible enrichment of sleep-trait associated SNPs in promoter-interacting open chromatin regions within α- and β-cells, intersecting public GWAS reports with our own ATAC-seq and high-resolution promoter-focused Capture C data generated from both sorted human α-cells and an established human beta-cell line (EndoC-βH1). Finally, we identified putative effector genes physically interacting with sleep-trait associated variants in α- and EndoC-βH1cells running variant-to-gene mapping and establish pathways in which these genes are significantly involved. We observed that insomnia, short and long sleep-but not morningness-were significantly correlated with type 2 diabetes, obesity and other metabolic traits. Both the EndoC-βH1 and α-cells were enriched for insomnia loci (p = .01; p = .0076), short sleep loci (p = .017; p = .022) and morningness loci (p = 2.2 × 10-7; p = .0016), while the α-cells were also enriched for long sleep loci (p = .034). Utilizing our promoter contact data, we identified 63 putative effector genes in EndoC-βH1 and 76 putative effector genes in α-cells, with these genes showing significant enrichment for organonitrogen and organophosphate biosynthesis, phosphatidylinositol and phosphorylation, intracellular transport and signaling, stress responses and cell differentiation. Our data suggest that a subset of sleep-related loci confer their effects via cells in pancreatic islets.
    MeSH term(s) Chromosome Mapping ; Diabetes Mellitus, Type 2/genetics ; Diabetes Mellitus, Type 2/metabolism ; Genetic Predisposition to Disease/genetics ; Genome-Wide Association Study ; Humans ; Islets of Langerhans/metabolism ; Obesity/metabolism ; Sleep ; Sleep Initiation and Maintenance Disorders/metabolism
    Language English
    Publishing date 2022-05-02
    Publishing country United States
    Document type Journal Article ; Research Support, N.I.H., Extramural
    ZDB-ID 424441-2
    ISSN 1550-9109 ; 0161-8105
    ISSN (online) 1550-9109
    ISSN 0161-8105
    DOI 10.1093/sleep/zsac109
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