Janus Kinase 2 Regulates Transcription Factor EB Expression and Autophagy Completion in Glomerular Podocytes

Alghamdi, Tamadher A.; Majumder, Syamantak; Thieme, Karina; Batchu, Sri Nagarjun; White, Kathryn; Liu, Youan; Brijmohan, Angela S.; Bowskill, Bridgit B.; Advani, Suzanne L.; Woo, Minna; Advani, Andrew

doi:10.1681/asn.2016111208

Cited by 21 publications

(24 citation statements)

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“…Caspase-3 is an important member of Caspase family, which occupies a central position in regulating cell apoptosis process [9]. Cell autophagy plays a momentous role in maintaining the stable structure and function of normal glomerular podocytes and proximal renal tubular epithelial cells [10]. Beclin-1 is a homologous gene of yeast autophagy gene Atg6/Vps30, which is one of the essential molecules of the formation of autophagosome [11].…”

Section: Introductionmentioning

confidence: 99%

Arbutin protects HK-2 cells against high glucose-induced apoptosis and autophagy by up-regulating microRNA-27a

Zhang

Tian³

et al. 2019

Artificial Cells, Nanomedicine, and Biotechnology

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Arbutin (ARB) has been widely used in skin pigmentation disorders. Nevertheless, the involvements of ARB in diabetic nephropathy (DN) are still unknown. We investigated the functions of ARB in high glucose (HG)-induced cell apoptosis and autophagy in HK-2 cells. Cell viability was examined through CCK-8 in HK-2 cells after disposal with 45 mM glucose and ARB (10-50 lM). Flow cytometry and western blot tested cell apoptosis and the related protein levels in HK-2 cells after 45 mM glucose and 50 lM ARB administration. RT-qPCR delved microRNA (miR)-27a expression in HG and ARB co-treated HK-2 cells. Effect of miR-27a on ARB affected cell apoptosis and autophagy was investigated after miR-27a inhibitor transfection. JNK and mTOR pathways were finally assessed by western blot. ARB alleviated HG-induced cell apoptosis, autophagy and regulated the related protein levels in HK-2 cells. MiR-27a expression was reduced in HG-treated cells, but was accelerated in HG and ARB co-treated HK-2 cells with the increased concentration. Inhibition of miR-27a apparently abolished the outcomes of ARB in HG-induced HK-2 cells apoptosis and autophagy. Besides, ARB blocked JNK and mTOR pathways by regulating miR-27a. The findings demonstrated that ARB alleviated apoptosis and autophagy in HGtreated HK-2 cells by regulating miR-27a/JNK/mTOR axis.

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Section: Introductionmentioning

confidence: 99%

Arbutin protects HK-2 cells against high glucose-induced apoptosis and autophagy by up-regulating microRNA-27a

Zhang

Tian³

et al. 2019

Artificial Cells, Nanomedicine, and Biotechnology

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“…In podocytes, Jack/Stat signaling facilitates the binding of STAT1 to the TFEB promoter and increases the expression of TFEB, thus, maintaining autophagosome-lysosome function. JACK2-deficient mice in podocytes exhibited impaired autophagy and increased urinary albumin excretion, while mice with TFEB overexpression in JAK2-deficient podocytes had restored autophagosome-lysosome function and albumin permselectivity [181]. These studies suggest that TFEB is a promising therapeutic target for improving podocyte injury in glomerular diseases.…”

Section: Tfeb-mediated Autophagy Induction and Renal Injurymentioning

confidence: 77%

Autophagy Function and Regulation in Kidney Disease

et al. 2020

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Autophagy is a dynamic process by which intracellular damaged macromolecules and organelles are degraded and recycled for the synthesis of new cellular components. Basal autophagy in the kidney acts as a quality control system and is vital for cellular metabolic and organelle homeostasis. Under pathological conditions, autophagy facilitates cellular adaptation; however, activation of autophagy in response to renal injury may be insufficient to provide protection, especially under dysregulated conditions. Kidney-specific deletion of Atg genes in mice has consistently demonstrated worsened acute kidney injury (AKI) outcomes supporting the notion of a pro-survival role of autophagy. Recent studies have also begun to unfold the role of autophagy in progressive renal disease and subsequent fibrosis. Autophagy also influences tubular cell death in renal injury. In this review, we reported the current understanding of autophagy regulation and its role in the pathogenesis of renal injury. In particular, the classic mammalian target of rapamycin (mTOR)-dependent signaling pathway and other mTOR-independent alternative signaling pathways of autophagy regulation were described. Finally, we summarized the impact of autophagy activation on different forms of cell death, including apoptosis and regulated necrosis, associated with the pathophysiology of renal injury. Understanding the regulatory mechanisms of autophagy would identify important targets for therapeutic approaches.

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“…Under isoflurane anesthesia, the abdominal aorta was cannulated with a 24-gauge angiocath, and the mouse was perfused with 1 × 10 5 Dynabeads in 5 ml HBSS (Thermo Fisher Scientific). Podocytes were isolated using previously reported methods (57,65,66). In brief, glomeruli were seeded on collagen I-coated plates in a 1:1 mixture of F-12 Kaighn's Modification Media (HyClone Laboratories) with media harvested from NIH/3T3 cells (ATCC), and cell cultures were maintained for approximately 4 to 6 days.…”

Section: Primary Culture Of Podocytesmentioning

confidence: 99%