Induction of lipogenic differentiation and alveolar regeneration in emphysema via PPARG and SREBP

IF 0.5 4区医学 Q4 RESPIRATORY SYSTEM

Revue des maladies respiratoires Pub Date : 2024-03-01 DOI:10.1016/j.rmr.2024.01.016

G. Justeau , M. Toigo , R. Yilmaz , L. Crepin , J. Boczkowski , B. Ribeiro Baptista , L. Boyer

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Abstract

Introduction

Emphysema is a respiratory disease characterized by chronic alveolar destruction. Lipofibroblasts (LIF) play a key role in the stem cell niche surrounding alveolar type II (AT2) cells and may contribute to alveolar regeneration. We have previously shown that senescent cell elimination induces alveolar regeneration, increased LIF numbers and activation of the sterol regulatory binding protein (SREBP) and peroxisome proliferator-activated receptor gamma (PPARG) pathways [1]. However, it remains unclear whether the activation of these pathways can increase fibroblast stem cell niche properties and promote alveolar regeneration during emphysema.

Methods

Human lung tissue slides were obtained from patients with or without emphysema and immunofluorescent staining was performed to identify LIF (ADRP+Vimentin+). Both human primary fibroblasts and primary AT2 cells were isolated from lobectomies through the explant method and magnetic sorting (HT2-280+) respectively. Fibroblasts were treated with Rosiglitazone and T0901317 for 72 hours. LIF phenotype acquisition was evaluated through IF staining, qPCR and lipidomic analysis. Stem cell niche properties were evaluated by performing alveolar organoid formation assay by co-culturing treated fibroblasts with H-441 cells or primary AT2 cells. Adult C57BL6 mice received intra-tracheal injection of either Elastase or PBS. From D₂₁ mice were treated by intraperitoneal injections of Rosiglitazone (5 μg/g/d), T0901317 (10 μg/g/d) or vehicule, 5/7 days. Lungs were collected at D₉₀. Left lung was fixated for morphological analysis.

Results

Our study showed a decrease in LIF populations among patients with emphysema compared to controls. Furthermore, Rosiglitazone, a PPARG agonist, and T0901317, a SREBP agonist, can induce lipogenic differentiation in human lung fibroblasts. Activation of both pathways increased the expression of ADRP and the activation of the SREBP pathway induced the accumulation of neutral lipids in the fibroblasts. Using an organoid model of alveolar regeneration, we show that activating these pathways increases the stem cell niche properties of fibroblasts and enhances the number of organoids formed with either H441 cells or primary AT2. Lastly, in a murine mode of elastase-induced emphysema, we show that Rosiglitazone partially reverts emphysema.

Conclusion

Activation of PPARG and SREBP pathways promotes lipogenic differentiation of fibroblasts, enhances human alveolar organoid formation and partially reverts emphysema in vivo. These results provide insight into potential therapeutic strategies for promoting alveolar regeneration in patients with emphysema.

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通过 PPARG 和 SREBP 诱导肺气肿中的脂肪分化和肺泡再生

导言肺气肿是一种以慢性肺泡破坏为特征的呼吸系统疾病。成脂纤维细胞（LIF）在肺泡II型（AT2）细胞周围的干细胞龛中发挥着关键作用，可能有助于肺泡再生。我们之前已经证明，衰老细胞的消除可诱导肺泡再生、LIF数量增加以及固醇调控结合蛋白（SREBP）和过氧化物酶体增殖激活受体γ（PPARG）通路的激活[1]。方法从肺气肿患者或无肺气肿患者处获取人体肺组织切片，进行免疫荧光染色以鉴定 LIF（ADRP+Vimentin+）。通过外植法和磁性分选（HT2-280+）分别从肺叶切除术中分离出人原代成纤维细胞和原代 AT2 细胞。成纤维细胞经罗格列酮和 T0901317 处理 72 小时。通过 IF 染色、qPCR 和脂质体分析评估 LIF 表型的获得。通过将处理过的成纤维细胞与 H-441 细胞或原代 AT2 细胞共培养，进行肺泡类器官形成试验，评估干细胞龛特性。成年 C57BL6 小鼠气管内注射弹性蛋白酶或 PBS。从第 21 天起，小鼠腹腔注射罗格列酮（5 μg/g/d）、T0901317（10 μg/g/d）或药物，治疗 5/7 天。D90时收集肺脏。结果我们的研究表明，与对照组相比，肺气肿患者的 LIF 数量减少。此外，PPARG 激动剂罗格列酮和 SREBP 激动剂 T0901317 可诱导人肺成纤维细胞产生脂肪分化。这两种途径的激活都会增加 ADRP 的表达，而 SREBP 途径的激活会诱导成纤维细胞中中性脂质的积累。我们利用肺泡再生的类器官模型表明，激活这些途径可增加成纤维细胞的干细胞龛特性，并提高用H441细胞或原代AT2形成的类器官的数量。最后，在弹性蛋白酶诱导的小鼠肺气肿模式中，我们发现罗格列酮可部分缓解肺气肿。结论激活PPARG和SREBP通路可促进成纤维细胞的脂肪分化，增强人类肺泡类器官的形成，并部分缓解体内肺气肿。这些结果为促进肺气肿患者肺泡再生的潜在治疗策略提供了启示。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Revue des maladies respiratoires 医学-呼吸系统

CiteScore

1.10

自引率

16.70%

发文量

168

审稿时长

4-8 weeks

期刊介绍： La Revue des Maladies Respiratoires est l''organe officiel d''expression scientifique de la Société de Pneumologie de Langue Française (SPLF). Il s''agit d''un média professionnel francophone, à vocation internationale et accessible ici. La Revue des Maladies Respiratoires est un outil de formation professionnelle post-universitaire pour l''ensemble de la communauté pneumologique francophone. Elle publie sur son site différentes variétés d''articles scientifiques concernant la Pneumologie : - Editoriaux, - Articles originaux, - Revues générales, - Articles de synthèses, - Recommandations d''experts et textes de consensus, - Séries thématiques, - Cas cliniques, - Articles « images et diagnostics », - Fiches techniques, - Lettres à la rédaction.