Novel Therapeutics Identification for Fibrosis in Renal Allograft Using Integrative Informatics Approach

Li, Li; Greene, Ilana; Readhead, Benjamin; Menon, Madhav C.; Kidd, Brian; Uzilov, Andrew; Wei, Chengguo; Philippe, Nimrod; Schröppel, Bernd; He, John Cijiang; Chen, Rong; Dudley, Joel T.; Murphy, Barbara

doi:10.1038/srep39487

Cited by 27 publications

(25 citation statements)

References 109 publications

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“…Differential expression across the entire transcriptome was computed as the difference in rank between case and control (SubDiff), yielding a differential expression value ranging from −1 to +1. Code to generate these signatures was based on a microarray analysis pipeline built in-house 43 . To determine if genes shared by Pb and LPS exposure significantly overlapped, we first identified genes differentially expressed as those with a SubDiff Z-score of > 1.5 or <−1.5 (Pb 1125 genes, LPS 1485 genes).…”

Section: Methodsmentioning

confidence: 99%

Integrative bioinformatics identifies postnatal lead (Pb) exposure disrupts developmental cortical plasticity

Smith

Yevoo

Sadahiro

et al. 2018

Sci Rep

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Given that thousands of chemicals released into the environment have the potential capacity to harm neurodevelopment, there is an urgent need to systematically evaluate their toxicity. Neurodevelopment is marked by critical periods of plasticity wherein neural circuits are refined by the environment to optimize behavior and function. If chemicals perturb these critical periods, neurodevelopment can be permanently altered. Focusing on 214 human neurotoxicants, we applied an integrative bioinformatics approach using publically available data to identify dozens of neurotoxicant signatures that disrupt a transcriptional signature of a critical period for brain plasticity. This identified lead (Pb) as a critical period neurotoxicant and we confirmed in vivo that Pb partially suppresses critical period plasticity at a time point analogous to exposure associated with autism. This work demonstrates the utility of a novel informatics approach to systematically identify neurotoxicants that disrupt childhood neurodevelopment and can be extended to assess other environmental chemicals.

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Section: Methodsmentioning

confidence: 99%

Integrative bioinformatics identifies postnatal lead (Pb) exposure disrupts developmental cortical plasticity

Smith

Yevoo

Sadahiro

et al. 2018

Sci Rep

Self Cite

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“…We restricted our search to gene enrichment analyses in human renal biopsies and to studies describing pathways specific for AMR, TCMR, IFTA, and PVAN. As presented in Table , we identified two studies for AMR, five for TCMR, eight for IFTA, and two for PVAN using statistically validated differentially regulated gene expression and appropriate GO‐, IPA‐, and KEGG‐derived pathway mappings. To perform semantic clustering on these kidney transplantation related disease phenotypes by the software tool ReviGO, we converted IPA and KEGG pathways to GO biological processes using QuickGO, AmiGO, and UniProt.…”

Section: The Molecular View: Mapping Of Molecular Pathwaysmentioning

confidence: 99%

Proteomics in Kidney Allograft Transplantation—Application of Molecular Pathway Analysis for Kidney Allograft Disease Phenotypic Biomarker Selection

Marx

Metzger

Olagne

et al. 2019

Proteomics Clinical Apps

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There is a need for accurate, robust, non-invasive methods to provide early diagnosis of graft lesions after kidney transplantation. A multitude of proteomic biomarkers for the major kidney allograft disease phenotypes defined by the BANFF classification criteria have been described in literature. None of these biomarkers have been established in the clinic. A key reason for this is the lack of clinical validation which is difficult, as even the gold standard of diagnosis, kidney biopsy, is often ambiguous. The semantic clustering by ReviGO on top of transcriptomic pathway analysis is evaluated to connect histological and transcriptomic kidney allograft disease characteristics with proteomic biomarker qualification. By using public data generated in microarray studies of kidney allograft tissue, biological processes and key molecules specifically associated with the different kidney allograft disease phenotypes are identified. Semantic clustering holds the promise to guide adaptation of proteomic marker panels to molecular pathology. This can support the development of noninvasive tests (e.g. in urine, by capillary electrophoresis mass spectrometry) that simultaneously detect diverse kidney allograft phenotypes with high accuracy and sensitivity.

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“…Integration of intrarenal transcriptomic data with patient‐specific non‐invasive molecular profile will allow generation of signatures that reflects individual's kidney progression pathogenesis. Pattern‐matching tools, which have been helpful in understanding disease and advancing the discovery of novel drugs in oncology can be applied to detect similarities among gene expression signatures . The drug‐specific molecular profile with the highest correlation to the patient's molecular profile is hypothesized to be the most appropriate candidate.…”

Section: The Use Of Systems Biology Approach To Predict Patients' Resmentioning

confidence: 99%

“…Pattern-matching tools, which have been helpful in understanding disease and advancing the discovery of novel drugs in oncology can be applied to detect similarities among gene expression signatures. [46][47][48][49] The drug-specific molecular profile with the highest correlation to the patient's molecular profile is hypothesized to be the most appropriate candidate. This type of integrative systems biology approach is "the right drug for the right patients" approach physician will need to advance treatment in DKD.…”

Section: The Identification Of Novel Molecular Markers Associated Wmentioning

confidence: 99%

An integrative systems biology approach for precision medicine in diabetic kidney disease

Mulder

Hamidi

Kretzler

et al. 2018

Diabetes Obesity Metabolism

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Current therapeutic approaches are ineffective in many patients with established Diabetic Kidney Disease (DKD) disease, an epidemic affecting one in three patients with diabetes. Early identification of patients at high risk for progression and individualizing therapies have the potential to mitigate kidney complications due to diabetes. To achieve this, a better understanding of the complex pathophysiology of DKD is needed. A system biology approach integrating large scale omic data is well suited to unravel the molecular mechanisms driving DKD and may offer new perspectives how to personalize therapy. Recent studies indeed demonstrate that integrating genome scale data sets generated from prospectively designed clinical cohort studies with model systems using innovative bioinformatics analysis revealed critical molecular pathways in DKD and led to the development of candidate prognostic molecular biomarkers. This review seeks to provide an overview of the recent progress in the application of the integrative systems biology approaches specifically in the field of molecular biomarkers for DKD. We will mainly focus the discussion on how to use integrative system biology approach to firstly identify patients at high risk of progression, and secondly to identify patients who may or may not respond to treatment. Challenges and opportunities in applying precision medicine in DKD will also be discussed.

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Novel Therapeutics Identification for Fibrosis in Renal Allograft Using Integrative Informatics Approach

Cited by 27 publications

References 109 publications

Integrative bioinformatics identifies postnatal lead (Pb) exposure disrupts developmental cortical plasticity

Integrative bioinformatics identifies postnatal lead (Pb) exposure disrupts developmental cortical plasticity

Proteomics in Kidney Allograft Transplantation—Application of Molecular Pathway Analysis for Kidney Allograft Disease Phenotypic Biomarker Selection

An integrative systems biology approach for precision medicine in diabetic kidney disease

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