UCP2-induced hypoxia promotes lipid accumulation and tubulointerstitial fibrosis during ischemic kidney injury

Ke, Qingqing; Qi, Yuan; Qin, Nan; Shi, Caifeng; Luo, Jing; Fang, Yi; Xu, Lingling; Sun, Qi; Zen, Ke; Jiang, Lei; Zhou, Yang; Yang, Junwei

doi:10.1038/s41419-019-2219-4

Cited by 38 publications

(23 citation statements)

References 46 publications

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“…Ucp1 is highly abundant in brown and beige adipocytes in vivo, while Ucp2 is ubiquitously expressed across various tissues and cell types 27 , 28 . Gene targeting and RNA interference approaches have indicated that UCP2 has a weak uncoupling activity, but UCP2 is physiologically required for different functions such as regulation of mitochondrial oxidative stress and energy metabolism 29 , 30 .…”

Section: Discussionmentioning

confidence: 99%

Transcriptome analysis reveals brown adipogenic reprogramming in chemical compound-induced brown adipocytes converted from human dermal fibroblasts

Takeda

Yoshikawa

Dai

2021

Sci Rep

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Brown adipogenesis contributes to controlling systemic energy balance by enhancing glucose and lipid consumptions. We have previously reported chemical compound-induced brown adipocytes (ciBAs) directly converted from human dermal fibroblasts using a serum-free medium. In this study, genome-wide transcriptional analysis was performed in ciBAs in comparison with the control fibroblasts. A broad range of integrated gene expression was enhanced in functional groups including tricarboxylic acid cycle, electron transfer chain, triglycerides metabolism, fatty acid and glucose metabolism, and adaptive thermogenesis. The results suggested that the chemical conversion underwent metabolic and mitochondrial reprogramming closely associated with functions in brown/beige adipocytes. Moreover, we also compared the transcriptional changes to those of adipocyte browning in adipose tissue-derived mesenchymal stem cells (AdMSCs). Transcriptome analysis indicated that the same sets of metabolic and mitochondria-related genes were similarly changed in the adipocyte browning. Interestingly, ciBAs more expressed Ucp1, while AdMSC-derived adipocytes predominantly expressed Ucp2. UCP1 protein was also more expressed in ciBAs than in AdMSC-derived adipocytes. Based on the evidence that UCP1, but not UCP2, is responsible for adrenergic thermogenesis, ciBAs could be a promising model for human beige adipocytes applicable for basic research, drug development, and clinical uses.

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Section: Discussionmentioning

confidence: 99%

Transcriptome analysis reveals brown adipogenic reprogramming in chemical compound-induced brown adipocytes converted from human dermal fibroblasts

Takeda

Yoshikawa

Dai

2021

Sci Rep

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“…Ke et al reported that UCP2 expression is increased in human biopsy samples and mice kidney tissues with tubulointerstitial fibrosis but UCP2 deficient mice display reduced lipid accumulation and attenuated hypoxia in kidney tissue. Compared with wildtype mice, the expression of PPARα and CPT1α, which are the major regulators of lipid metabolism, is restored in UCP2 deficient mice (Ke et al, 2020). Both CPT1 and ACO2 are the rate-limiting enzymes of FA β-oxidation.…”

Section: Dysregulated Mitochondrial Lipid Utilization In Kidney Diseasesmentioning

confidence: 94%

The Vicious Cycle of Renal Lipotoxicity and Mitochondrial Dysfunction

Fontanesi

Merscher

et al. 2020

Front. Physiol.

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The kidney is one of the most energy-demanding organs that require abundant and healthy mitochondria to maintain proper function. Increasing evidence suggests a strong association between mitochondrial dysfunction and chronic kidney diseases (CKDs). Lipids are not only important sources of energy but also essential components of mitochondrial membrane structures. Dysregulation of mitochondrial oxidative metabolism and increased reactive oxygen species (ROS) production lead to compromised mitochondrial lipid utilization, resulting in lipid accumulation and renal lipotoxicity. However, lipotoxicity can be either the cause or the consequence of mitochondrial dysfunction. Imbalanced lipid metabolism, in turn, can hamper mitochondrial dynamics, contributing to the alteration of mitochondrial lipids and reduction in mitochondrial function. In this review, we summarize the interplay between renal lipotoxicity and mitochondrial dysfunction, with a focus on glomerular diseases.

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“…Primary PTECs were cultured from collagenase-digested cortical fragments of mice (about 21 days) kidneys according to a modified method previously described [ 20 , 21 ]. In brief, after been dissected and collagenase digested, two nylon sieves with the pore sizes of 250 and 80 μm were used to yield proximal tubule fragments, which were then washed, resuspended, and seeded onto collagen-coated permeable PTFE-filter supports and cultured for 48 h in a standard humidified incubator with the medium replaced every 2 days till the organization of a confluent monolayer of cells.…”

Section: Methodsmentioning

confidence: 99%

“…OCT-embedded kidney tissues were sectioned at 12 μm for oil red O (Sigma-Aldrich, US) and 3 μm for bodipy (D3922, Thermo Fisher, US) staining as previously described [ 6 , 21 , 25 ]. Nuclei were viewed by alum haematoxylin staining.…”

Section: Methodsmentioning

confidence: 99%

CPT1α maintains phenotype of tubules via mitochondrial respiration during kidney injury and repair

Ding

et al. 2021

Cell Death Dis

Self Cite

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Impaired energy metabolism in proximal tubular epithelial cells (PTECs) is strongly associated with various kidney diseases. Here, we characterized proximal tubular phenotype alternations during kidney injury and repair in a mouse model of folic acid nephropathy, in parallel, identified carnitine palmitoyltransferase 1α (CPT1α) as an energy stress response accompanied by renal tubular dedifferentiation. Genetic ablation of Cpt1α aggravated the tubular injury and interstitial fibrosis and hampered kidney repair indicate that CPT1α is vital for the preservation and recovery of tubular phenotype. Our data showed that the lipid accumulation and mitochondrial mass reduction induced by folic acid were persistent and became progressively more severe in PTECs without CPT1α. Interference of CPT1α reduced capacities of mitochondrial respiration and ATP production in PTECs, and further sensitized cells to folic acid-induced phenotypic changes. On the contrary, overexpression of CPT1α protected mitochondrial respiration and prevented against folic acid-induced tubular cell damage. These findings link CPT1α to intrinsic mechanisms regulating the mitochondrial respiration and phenotype of kidney tubules that may contribute to renal pathology during injury and repair.

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UCP2-induced hypoxia promotes lipid accumulation and tubulointerstitial fibrosis during ischemic kidney injury

Cited by 38 publications

References 46 publications

Transcriptome analysis reveals brown adipogenic reprogramming in chemical compound-induced brown adipocytes converted from human dermal fibroblasts

Transcriptome analysis reveals brown adipogenic reprogramming in chemical compound-induced brown adipocytes converted from human dermal fibroblasts

The Vicious Cycle of Renal Lipotoxicity and Mitochondrial Dysfunction

CPT1α maintains phenotype of tubules via mitochondrial respiration during kidney injury and repair

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