An association study of C9orf3, a novel component of the renin-angiotensin system, and hypertension in diabetes

Ichikawa, Mai; Konoshita, Tadashi; Makino, Yasukazu; Suzuki, Jinya; Ishizuka, Tamotsu; Nakamura, Hiroyuki

doi:10.1038/s41598-020-73094-0

Cited by 5 publications

(6 citation statements)

References 37 publications

(36 reference statements)

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“…This may reflect the fact that these genes are more likely to play a critical role for dystonia pathogenesis during brain development and less so in the adult mature brain 30 . Single‐nucleotide polymorphism‐based association studies have shown that more common variations in AOPEP may influence susceptibility to prevalent disease traits, such as arterial hypertension, polycystic ovary syndrome, and atrial fibrillation 31‐33 . We believe, however, that it is currently not possible to bring these observations into a direct pathophysiological context with dystonia because the herein identified loss‐of‐function alterations are likely to have molecular consequences different from those encountered in association to common (non‐neurological) disease risk alleles.…”

Section: Discussionmentioning

confidence: 91%

Biallelic AOPEP Loss‐of‐Function Variants Cause Progressive Dystonia with Prominent Limb Involvement

et al. 2021

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Section: Discussionmentioning

confidence: 91%

Biallelic AOPEP Loss‐of‐Function Variants Cause Progressive Dystonia with Prominent Limb Involvement

et al. 2021

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“…Even though this prediction highlights the potential variability caused by rs2767403, the AOPEP gene encodes a metallo protease linked to the renin-angiotensin system [47]. In particular, it is able to cleave angiotensin III (but not I and II) to generate Angiotensin IV.…”

Section: Analysis Of Single Snpsmentioning

confidence: 97%

Suicide Related Phenotypes in a Bipolar Sample: Genetic Underpinnings

Lybech

Calabrò

Briuglia

et al. 2021

Genes

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Suicide in Bipolar Disorder (BD) is a relevant clinical concern. Genetics may shape the individual risk for suicide behavior in BD, together with known clinical factors. The lack of consistent replication in BD may be associated with its multigenetic component. In the present contribution we analyzed a sample of BD individuals (from STEP-BD database) to identify the genetic variants potentially associated with three different suicide-related phenotypes: 1) a feeling that the life was not worth living; 2) fantasies about committing a violent suicide; 3) previous attempted suicide. The sample under analysis included 1115 BD individuals. None of the SNPs reached genome-wide significance. However, a trend of association was evidenced for rs2767403, an intron variant of AOPEP gene, in association with phenotype #1 (p = 5.977 × 10−6). The molecular pathway analysis showed a significant enrichment in all the investigated phenotypes on pathways related to post synaptic signaling, neurotransmission and neurodevelopment. Further, NOTCH signaling or the γ-aminobutyric acid (GABA) -ergic signaling were found to be associated with specific suicide-related phenotypes. The present investigation contributes to the hypothesis that the genetic architecture of suicide behaviors in BD is related to alteration of entire pathways rather than single genes. In particular, our molecular pathway analysis points on some specific molecular events that could be the focus of further research in this field.

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“…Twenty-one and 24 T2D- associated variants overlapped ER stress- or cytokine-specific opening CREs, respectively (Figure 4A; Supplementary Table 5) . Among these, 11 variants overlapped ER stress-specific opening CREs that are within 500kb of an ER stress response gene (Figure 4B; Supplementary Table 5), including AOPEP - a key gene involved in peptide processing 70 and robustly induced by ER stress in beta cells (Figure 4C; Supplementary Tables 2-3) . We detected an ER stress-specific induced CRE in the AOPEP intron, which harbors the T2D-associated variant rs4744423 (Figure 4D; Supplementary Tables 4-5) .…”

Section: Resultsmentioning

confidence: 99%

Comparative Multi-omic Mapping of Human Pancreatic Islet Endoplasmic Reticulum and Cytokine Stress Responses Provides Insights into Type 2 Diabetes Genetics

Sokolowski,

Kursawe,

Selvam

et al. 2024

Preprint

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Endoplasmic reticulum (ER) and inflammatory stress responses are two pathophysiologic factors contributing to islet dysfunction and failure in Type 2 Diabetes (T2D). However, how human islet cells respond to these stressors and whether T2D-associated genetic variants modulate these responses is unknown. To fill this knowledge gap, we profiled transcriptional (RNA-seq) and epigenetic (ATAC-seq) remodeling in human islets exposed toex vivoER (thapsigargin) or inflammatory (IL-1β+IFN-γ) stress. 5,427 genes (∼32%) were associated with stress responses; most were stressor-specific, including upregulation of genes mediating unfolded protein response (e.g.DDIT3, ATF4) and NFKB signaling (e.g.NFKB1, NFKBIA) in ER stress and cytokine-induced inflammation respectively. Islet single-cell RNA-seq profiling revealed strong but heterogeneous beta cell ER stress responses, including a distinct beta cell subset that highly expressed apoptotic genes. Epigenetic profiling uncovered 14,968 stress-responsivecis-regulatory elements (CREs; ∼14%), the majority of which were stressor-specific, and revealed increased accessibility at binding sites of transcription factors that were induced upon stress (e.g. ATF4 for ER stress, IRF8 for cytokine-induced inflammation). Eighty-six stress-responsive CREs overlapped known T2D-associated variants, including 20 residing within CREs that were more accessible upon ER stress. Among these, we linked the rs6917676 T2D risk allele (T) to increasedin vivoaccessibility of an islet ER stress-responsive CRE and allele-specific beta cell nuclear factor bindingin vitro. We showed thatMAP3K5,the only ER stress-responsive gene in this locus, promotes beta cell apoptosis. Consistent with its pro-apoptotic and putative diabetogenic roles,MAP3K5expression inversely correlated with beta cell abundance in human islets and was induced in beta cells from T2D donors. Together, this study provides new genome-wide insights into human islet stress responses and putative mechanisms of T2D genetic variants.

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An association study of C9orf3, a novel component of the renin-angiotensin system, and hypertension in diabetes

Cited by 5 publications

References 37 publications

Biallelic AOPEP Loss‐of‐Function Variants Cause Progressive Dystonia with Prominent Limb Involvement

Biallelic AOPEP Loss‐of‐Function Variants Cause Progressive Dystonia with Prominent Limb Involvement

Suicide Related Phenotypes in a Bipolar Sample: Genetic Underpinnings

Comparative Multi-omic Mapping of Human Pancreatic Islet Endoplasmic Reticulum and Cytokine Stress Responses Provides Insights into Type 2 Diabetes Genetics

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