ChIP-seq analysis of histone H3K9 trimethylation in peripheral blood mononuclear cells of membranous nephropathy patients

Sui, Weiguo; He, Hao; Yan, Qiang; Chen, J.J.; Zhang, R.H.; Dai, Yong

doi:10.1590/1414-431x20132809

Cited by 7 publications

(9 citation statements)

References 30 publications

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“…The variants in this gene are associated with developmental delays and mental retardation and may be relevant to autism-related spectrum disorders [ 30 – 32 ]. Disruption of CNTN4 is also thought to cause cognitive defects [ 33 ]. Our study showed strong association of SUA concentrations with CNTN4 SNPs.…”

Section: Discussionmentioning

confidence: 99%

GWAS and transcriptional analysis prioritize ITPR1 and CNTN4 for a serum uric acid 3p26 QTL in Mexican Americans

et al. 2016

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Background: The variation in serum uric acid concentrations is under significant genetic influence. Elevated SUA concentrations have been linked to increased risk for gout, kidney stones, chronic kidney disease, and cardiovascular disease whereas reduced serum uric acid concentrations have been linked to multiple sclerosis, Parkinson's disease and Alzheimer's disease. Previously, we identified a novel locus on chromosome 3p26 affecting serum uric acid concentrations in Mexican Americans from San Antonio Family Heart Study. As a follow up, we examined genome-wide single nucleotide polymorphism data in an extended cohort of 1281 Mexican Americans from multigenerational families of the San Antonio Family Heart Study and the San Antonio Family Diabetes/ Gallbladder Study. We used a linear regression-based joint linkage/association test under an additive model of allelic effect, while accounting for non-independence among family members via a kinship variance component.

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Section: Discussionmentioning

confidence: 99%

GWAS and transcriptional analysis prioritize ITPR1 and CNTN4 for a serum uric acid 3p26 QTL in Mexican Americans

et al. 2016

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“…The combination of computational analyses and experimental validation revealed that a high proportion of unmapped ChIP-Seq reads were mappable after being subjected to a taxonomic classification and subsequent remapping using SHRiMP, a short read aligner capable of mapping reads to highly polymorphic regions of the genome. We discovered that these previously ignored reads, also reported in ChIP-Seq experiments conducted with various modified histones 27 28 29 30 harbor key information that showed novel aspects important for the reconstruction of gene regulatory grids. By focusing on the human TAL1 TF, a set of previously unaligned reads were shown to have mappable properties and have been used for identification and validation of novel TAL1 binding sites, revealing important characteristics on how this TF can regulate cell fate determination, apoptosis, and potential novel role in sensory perception.…”

Section: Discussionmentioning

confidence: 97%

Important biological information uncovered in previously unaligned reads from chromatin immunoprecipitation experiments (ChIP-Seq)

Ouma

Mejía‐Guerra

Yılmaz

et al. 2015

Sci Rep

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Establishing the architecture of gene regulatory networks (GRNs) relies on chromatin immunoprecipitation followed by massively parallel sequencing (ChIP-Seq) methods that provide genome-wide transcription factor binding sites (TFBSs). ChIP-Seq furnishes millions of short reads that, after alignment, describe the genome-wide binding sites of a particular TF. However, in all organisms investigated an average of 40% of reads fail to align to the corresponding genome, with some datasets having as much as 80% of reads failing to align. We describe here the provenance of previously unaligned reads in ChIP-Seq experiments from animals and plants. We show that a substantial portion corresponds to sequences of bacterial and metazoan origin, irrespective of the ChIP-Seq chromatin source. Unforeseen was the finding that 30%–40% of unaligned reads were actually alignable. To validate these observations, we investigated the characteristics of the previously unaligned reads corresponding to TAL1, a human TF involved in lineage specification of hemopoietic cells. We show that, while unmapped ChIP-Seq read datasets contain foreign DNA sequences, additional TFBSs can be identified from the previously unaligned ChIP-Seq reads. Our results indicate that the re-evaluation of previously unaligned reads from ChIP-Seq experiments will significantly contribute to TF target identification and determination of emerging properties of GRNs.

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“…Therefore, studying epigenetic features, such as DNA methylation, may offer new insights by providing a mechanism to understand how each individual’s genome interacts with their environment through the epigenome. However, this review highlights that only a small number of studies have been reported researching differential methylation in rare renal diseases: IgAN [48–50]ADPKD [51–53]Rare diseases causing proteinuria including membranous nephropathy [54, 55] and focal segmental glomerulosclerosis (FSGS) [56–59]Congenital renal agenesis [60]…”

Section: Discussionmentioning

confidence: 99%

“…Rare diseases causing proteinuria including membranous nephropathy [54, 55] and focal segmental glomerulosclerosis (FSGS) [56–59]…”

Section: Discussionmentioning

confidence: 99%

“…Increased H3K4me3 was found to exacerbate proteinuria in membranous nephropathy [55], with murine models showing that targeting shRNA against an H3K4 methyltransferase, MLL3, alleviated proteinuria. H3K9me3 alterations were also found to be a biomarker of membranous nephropathy compared to normal control patients [54]. FSGS, included in the RaDaR elgibility criteria, is a condition describing sclerosis of the kidney, with a variety of causes.…”

Section: Discussionmentioning

confidence: 99%

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Differential methylation as a diagnostic biomarker of rare renal diseases: a systematic review

Kerr¹,

McAneney²,

Flanagan

et al. 2019

BMC Nephrol

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Background The challenges in diagnosis of rare renal conditions can negatively impact patient prognosis, quality of life and result in significant healthcare costs. Differential methylation is emerging as an important biomarker for rare diseases and should be evaluated for rare renal conditions. Methods A comprehensive systematic review of methylation and rare renal disorders was conducted by searching the electronic databases MEDLINE, EMBASE, PubMed, Cochrane Library, alongside grey literature from GreyLit and OpenGrey databases, for publications published before September 2018. Additionally, the reference lists of the included papers were searched. Data was extracted and appraised including the primary focus, measurement and methodological rigour of the source. Eligibility criteria were adapted using the inclusion criteria from ‘The 100,000 Genomes Project’ and The National Registry of Rare Kidney Diseases, with additional focus on methylation. Results Thirteen full text articles were included in the review. Diseases analysed for differential methylation included glomerular disease, IgA nephropathy, ADPKD, rare causes of proteinuria, congenital renal agenesis, and membranous nephropathy. Conclusions Differential methylation has been observed for several rare renal diseases, highlighting its potential for improving molecular characterisation of these disorders. Further investigation of methylation following a standardised reporting structure is necessary to improve research quality. Multi-omic data will provide insights for improved diagnosis, prognosis and support for individuals living and working with rare renal diseases. Electronic supplementary material The online version of this article (10.1186/s12882-019-1517-5) contains supplementary material, which is available to authorized users.

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ChIP-seq analysis of histone H3K9 trimethylation in peripheral blood mononuclear cells of membranous nephropathy patients

Cited by 7 publications

References 30 publications

GWAS and transcriptional analysis prioritize ITPR1 and CNTN4 for a serum uric acid 3p26 QTL in Mexican Americans

GWAS and transcriptional analysis prioritize ITPR1 and CNTN4 for a serum uric acid 3p26 QTL in Mexican Americans

Important biological information uncovered in previously unaligned reads from chromatin immunoprecipitation experiments (ChIP-Seq)

Differential methylation as a diagnostic biomarker of rare renal diseases: a systematic review

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