Cell and transcriptomic diversity of infrapatellar fat pad during knee osteoarthritis

转录组 髌下脂肪垫 脂肪垫 脂肪组织 医学 骨关节炎 生物 生物信息学 内科学 病理 遗传学 基因表达 基因 替代医学
作者
Hayley Peters,Pratibha Potla,Jason S. Rockel,Teodora Tockovska,Chiara Pastrello,Igor Jurišica,Keemo Delos Santos,Shabana Vohra,Noah Fine,Starlee Lively,K. Perry,Nikita Looby,Sheng Han Li,Vinod Chandran,Katrina Hueniken,Paramvir Kaur,Anthony V. Perruccio,Nizar N. Mahomed,Y. Raja Rampersaud,Khalid Syed
出处
期刊:Annals of the Rheumatic Diseases [BMJ]
卷期号:84 (2): 351-367 被引量:1
标识
DOI:10.1136/ard-2024-225928
摘要

In this study, we employ a multiomic approach to identify major cell types and subsets, and their transcriptomic profiles within the infrapatellar fat pad (IFP), and to determine differences in the IFP based on knee osteoarthritis (KOA), sex and obesity status. Single-nucleus RNA sequencing of 82 924 nuclei from 21 IFPs (n=6 healthy control and n=15 KOA donors), spatial transcriptomics and bioinformatic analyses were used to identify contributions of the IFP to KOA. We mapped cell subclusters from other white adipose tissues using publicly available literature. The diversity of fibroblasts within the IFP was investigated by bioinformatic analyses, comparing by KOA, sex and obesity status. Metabolomics was used to further explore differences in fibroblasts by obesity status. We identified multiple subclusters of fibroblasts, macrophages, adipocytes and endothelial cells with unique transcriptomic profiles. Using spatial transcriptomics, we resolved distributions of cell types and their transcriptomic profiles and computationally identified putative cell-cell communication networks. Furthermore, we identified transcriptomic differences in fibroblasts from KOA versus healthy control donor IFPs, female versus male KOA-IFPs and obese versus normal body mass index (BMI) KOA-IFPs. Finally, using metabolomics, we defined differences in metabolite levels in supernatants of naïve, profibrotic stimuli-treated and proinflammatory stimuli-treated fibroblasts from obese compared to normal BMI KOA-IFPs. Overall, by employing a multiomic approach, this study provides the first comprehensive map of the cellular and transcriptomic diversity of human IFP and identifies IFP fibroblasts as key cells contributing to transcriptomic and metabolic differences related to KOA disease, sex or obesity.
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