JAK-STAT pathway activation compromises nephrocyte function in a Drosophila high-fat diet model of chronic kidney disease

  1. Yunpo Zhao
  2. Jianli Duan
  3. Joyce van de Leemput
  4. Zhe Han

  • Curated by eLife

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    eLife assessment

    This study presents important new insights linking obesity to kidney disease using a Drosophila model. A series of compelling experiments demonstrated that a high-fat diet induces the excretion of a leptin-like JAK-STAT ligand from the fat body, driving the adipose-nephrocyte axis through activated JAK-STAT signaling and subsequently causing a functional defect in nephrocytes. While the combination of genetic tools and pharmacological intervention provides solid data and confirms the mechanistic link, the phenotypic analysis is restricted to tracer endocytosis and would benefit from immunofluorescence studies and higher animal numbers.

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Abstract

Chronic kidney disease is a major healthy issue and is gaining prevalence. Using a Drosophila model for chronic kidney disease we show that a high-fat diet (HFD) disrupts the slit diaphragm filtration structure in nephrocytes, the fly functional equivalent of mammalian podocytes. The structural disruption resulted in reduced filtration function in the affected nephrocytes. We demonstrate that a HFD activates the JAK-STAT pathway in nephrocytes, which has previously been linked to diabetic kidney disease. JAK-STAT activation was initiated by increased expression and release of the adipokine, Upd2, from the fat body. This leptin-like hormone is a known ligand of JAK-STAT. Both genetic and pharmacological inhibition of JAK-STAT restored nephrocyte HFD-associated dysfunction. Altogether, our study reveals the importance of the JAK-STAT signaling pathway in the adipose tissue−nephrocyte axis and its contribution to HFD-associated nephropathy. These findings open new avenues for intervention in treating diabetic nephropathy and chronic kidney disease.

Article activity feed

  1. Version published to 10.7554/elife.96987.1 on eLife
  2. Version published to 10.7554/elife.96987 on eLife
  3. eLife

    eLife assessment

    This study presents important new insights linking obesity to kidney disease using a Drosophila model. A series of compelling experiments demonstrated that a high-fat diet induces the excretion of a leptin-like JAK-STAT ligand from the fat body, driving the adipose-nephrocyte axis through activated JAK-STAT signaling and subsequently causing a functional defect in nephrocytes. While the combination of genetic tools and pharmacological intervention provides solid data and confirms the mechanistic link, the phenotypic analysis is restricted to tracer endocytosis and would benefit from immunofluorescence studies and higher animal numbers.

  4. eLife

    Reviewer #1 (Public Review):

    Summary:

    Zhao and colleagues employ Drosophila nephrocytes as a model to investigate the effects of a high-fat diet on these podocyte-like cells. Through a highly focused analysis, they initially confirm previous research in their hands demonstrating impaired nephrocyte function and move on to observe the mislocalization of a slit diaphragm-associated protein (pyd). Employing a reporter construct, they identify the activation of the JAK/STAT signaling pathway in nephrocytes. Subsequently, the authors demonstrate the involvement of this pathway in nephrocyte function from multiple angles, using a gain-of-function construct, silencing of an inhibitor, and ectopic overexpression of a ligand. Silencing the effector Stat92E via RNAi or inhibiting JAK/STAT with Methotrexate effectively restored impaired nephrocyte function induced by a high-fat diet, while showing no impact under normal dietary conditions.

    Strengths:

    The findings establish a link between JAK/STAT activity and the impact of a high-fat diet on nephrocytes. This nicely underscores the importance of organ crosstalk for nephrocytes and supports a potential role for JAK/STAT in diabetic nephropathy, as previously suggested by other models.

    Weaknesses:

    The analysis is overly reliant on tracer endocytosis and single lines. Immunofluorescence of slit diaphragm proteins would provide a more specific assessment of the phenotypes.

  5. eLife

    Reviewer #2 (Public Review):

    Summary:

    In their manuscript, Zhao et al. describe a link between JAK-STAT pathway activation in nephrocytes on a high-fat diet. Nephrocytes are the homologs to mammalian podocytes and it has been previously shown, that metabolic syndrome and obesity are associated with worse outcomes for chronic kidney disease. A study from 2021 (Lubojemska et al.) could already confirm a severe nephrocyte phenotype upon feeding Drosophila a high-fat diet and also linking lipid overflow by expressing adipose triglyceride lipase in the fat body to nephrocyte dysfunction. In this study, the authors identified a second pathway and mechanism, how lipid dysregulation impact on nephrocyte function. In detail, they show activation of JAK-STAT signaling in nephrocytes upon feeding them a high-fat diet, which was induced by Upd2 expression (a leptin-like hormone) in the fat body, and the adipose tissue in Drosophila. Further, they could show genetic and pharmacological interventions can reduce JAK-STAT activation and thereby prevent the nephrocyte phenotype in the high-fat diet model.

    Strengths:

    The strength of this study is the combination of genetic tools and pharmacological intervention to confirm a mechanistic link between the fat body/adipose tissue and nephrocytes. Inter-organ communication is crucial in the development of several diseases, but the underlying mechanisms are only poorly understood. Using Drosophila, it is possible to investigate several players of one pathway, here JAK-STAT. This was done, by investigating the functional role of Hop, Socs36E, and Stat92E in nephrocytes and has also been combined with feeding a high-fat diet, to assess restoration of nephrocyte function by inhibiting JAK-STAT signaling. Adding a translational approach was done by inhibiting JAK-STAT signaling with methotrexate, which also resulted in attenuated nephrocyte dysfunction. Expression of the leptin-like hormone upd2 in the fat body is a good approach to studying inter-organ communication and the impact of other organs/tissue on nephrocyte function and expands their findings from nephrocyte function towards whole animal physiology.

    Weaknesses:

    Although the general findings of this study are of great interest, there are some weaknesses in the study, which should be addressed. Overall, the number of flies investigated for the majority of the experiments is very low (6 flies) and it is not clear whether the flies used, are from independent experiments to exclude problems with food/diet. For the analysis, the mean values of flies should be calculated, as one fly can be considered a biological replicate, but not all individual cells. By increasing the number of flies investigated, statistical analysis will become more solid. In addition, the morphological assessment is rather preliminary, by only using a Pyd antibody. Duf or Sns should be visualized as well, also the investigation of the different transgenic fly strains studying the importance of JAK-STAT signaling in nephrocytes needs to include a morphological assessment. Moreover, the expected effect of feeding a high-fat diet on nephrocytes needs to be shown (e.g. by lipid droplet formation) and whether upd2 is actually increased here should also be assessed. The time points of assessment vary between 1, 3, and 7 days and should be consistent throughout the study or the authors should describe why they use different time points.

  6. Version published to 10.1101/2024.03.07.583967v1 on bioRxiv