Spatial proteomics of human diabetic kidney disease, from health to class III

Kondo, Ayano; McGrady, Monee; Nallapothula, Dhiraj; Ali, Hira; Trevino, Alexandro E.; Lam, A. M.; Preska, Ryan; D'Angio, H Blaize; Wu, Zhenqin; Lopez, Lauren N; Badhesha, Harshanna Kaur; Vargas, Chenoa R.; Ramesh, Achyuta; Wiegley, Nasim; Han, Seung Seok; Dall′Era, Marc; Jen, Kuang-Yu; Mayer, Aaron T.; Afkarian, Maryam

doi:10.1101/2023.04.12.534028

Cited by 2 publications

(1 citation statement)

References 49 publications

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“…To examine the ability of SCGP to recognize known tissue structures, we assessed its performance on a cohort of 17 tissue sections from 12 individuals with diabetes and various stages of diabetic kidney disease (DKD) 39 . Tissue samples were imaged using the mIF platform CO-Detection by indexing (CODEX) 9 and further annotated for four major kidney compartments: glomeruli, blood vessels, distal tubules, and proximal tubules.…”

Section: Scgp Identifies Structures In Kidney Tissuesmentioning

confidence: 99%

Characterizing Tissue Structures from Spatial Omics with Spatial Cellular Graph Partition

Wu,

Kondo,

McGrady

et al. 2023

Preprint

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Spatial transcriptomic and proteomic measurements enable high-dimensional characterization of tissues. However, understanding organizations of cells at different spatial scales and extracting tissue structures of interest remain challenging tasks that require extensive human annotations. To address this need for consistent identification of tissue structures, in this work, we present a novel annotation method Spatial Cellular Graph Partitioning (SCGP) that allows unsupervised identification of tissue structures that reflect the anatomical and functional units of human tissues. We further present a reference-query extension pipeline SCGP-Extension that enables the generalization of existing reference tissue structures to previously unseen samples. Our experiments demonstrate reliable and robust partitionings of both spatial transcriptomics and proteomics datasets encompassing different tissue types and profiling techniques. Downstream analysis on SCGP-identified tissue structures reveals disease-relevant insights regarding diabetic kidney disease and skin disorder, underscoring its potential in facilitating spatial analysis and driving new discoveries.

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Section: Scgp Identifies Structures In Kidney Tissuesmentioning

confidence: 99%

Characterizing Tissue Structures from Spatial Omics with Spatial Cellular Graph Partition

Wu,

Kondo,

McGrady

et al. 2023

Preprint

Self Cite

View full text Add to dashboard Cite

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IL-6 and diabetic kidney disease

Zhang,

Xu,

Hou

2024

Front. Immunol.

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Diabetic kidney disease (DKD) is a severe microvascular complication of diabetes associated with high mortality and disability rates. Inflammation has emerged as a key pathological mechanism in DKD, prompting interest in novel therapeutic approaches targeting inflammatory pathways. Interleukin-6 (IL-6), a well-established inflammatory cytokine known for mediating various inflammatory responses, has attracted great attention in the DKD field. Although multiple in vivo and in vitro studies highlight the potential of targeting IL-6 in DKD treatment, its exact roles in the disease remains unclear. This review presents the roles of IL-6 in the pathogenesis of DKD, including immunoinflammation, metabolism, hemodynamics, and ferroptosis. In addition, we summarize the current status of IL-6 inhibitors in DKD-related clinical trials and discuss the potential of targeting IL-6 for treating DKD in the clinic.

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Spatial proteomics of human diabetic kidney disease, from health to class III

Cited by 2 publications

References 49 publications

Characterizing Tissue Structures from Spatial Omics with Spatial Cellular Graph Partition

Characterizing Tissue Structures from Spatial Omics with Spatial Cellular Graph Partition

IL-6 and diabetic kidney disease

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