Parp3 promotes astrocytic differentiation through a tight regulation of Nox4-induced ROS and mTorc2 activation

Rodríguez-Vargas, José Manuel; Martin-Hernandez, Kathline; Wang, Wei; Kunath, Nicolas; Suganthan, Rajikala; Amé, Jean‐Christophe; Oliver, F. Javier; Ye, Jing; Bjørås, Magnar; Dantzer, Françoise

doi:10.1038/s41419-020-03167-5

Cited by 20 publications

(12 citation statements)

References 72 publications

(85 reference statements)

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“…PARP1 and PARP3 were implicated in regulating mitochondrial morphology [20,85,86]; hence, we assessed the possible involvement of PARP1 and PARP3. Silencing PARP1 in scPARP2 and shPARP2 C2C12 cells (Figure 11A) led to the loss of PARP1 auto-PARylation (Figure 11A).…”

Section: Parp1 and Parp3 Are Not Involved In Mitochondrial Fragmentation Elicited By The Silencing Of Parp2mentioning

confidence: 99%

Silencing of Poly(ADP-Ribose) Polymerase-2 Induces Mitochondrial Reactive Species Production and Mitochondrial Fragmentation

Jankó

Kovàcs

Laczik

et al. 2021

Cells

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PARP2 is a DNA repair protein. The deletion of PARP2 induces mitochondrial biogenesis and mitochondrial activity by increasing NAD+ levels and inducing SIRT1 activity. We show that the silencing of PARP2 causes mitochondrial fragmentation in myoblasts. We assessed multiple pathways that can lead to mitochondrial fragmentation and ruled out the involvement of mitophagy, the fusion–fission machinery, SIRT1, and mitochondrial unfolded protein response. Nevertheless, mitochondrial fragmentation was reversed by treatment with strong reductants, such as reduced glutathione (GSH), N-acetyl-cysteine (NAC), and a mitochondria-specific antioxidant MitoTEMPO. The effect of MitoTEMPO on mitochondrial morphology indicates the production of reactive oxygen species of mitochondrial origin. Elimination of reactive oxygen species reversed mitochondrial fragmentation in PARP2-silenced cells.

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Section: Parp1 and Parp3 Are Not Involved In Mitochondrial Fragmentation Elicited By The Silencing Of Parp2mentioning

confidence: 99%

Silencing of Poly(ADP-Ribose) Polymerase-2 Induces Mitochondrial Reactive Species Production and Mitochondrial Fragmentation

Jankó

Kovàcs

Laczik

et al. 2021

Cells

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“…Poly (ADP-ribose) polymerase 3 (Parp3) is a member of ARTD (Parp) family which can synthesize poly (ADP-ribose) at the expense of NAD + [30]. Previous studies showed that Parp3 was involved in the cellular response to DNA damage [31], mitotic progression [32], chromosomal rearrangements [33], the regulation of redox homeostasis [34] and tumor aggressiveness [35]. Moreover, Parp3 inhibitor ME0328 was found to cause cell cycle arrest in breast cancer cells [36].…”

Section: Discussionmentioning

confidence: 99%

Fall of Parp3 restrains Lgr5+ stem cells proliferation and mucosal renovation in intestinal aging

Peng

Liu

Wang

et al. 2022

Preprint

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Background The aging small intestine has a great impact on body health. One of the obvious characteristics is the degeneration of epithelium turnover. The acknowledged Lgr5+ intestinal stem cell is the key factor. Methods We used Lgr5-EGFP transgenic mice in three different ages (young group:3-6 months, middle group:12-14 months and old group:22-24 months) to mark the Lgr5+ISCs. We collected the jejunum for histology, immunofluorescence, western-blotting and PCR, we isolated the crypts for organoid culture and sorted out the Lgr5hi cells for bulk RNA sequence. Results In tissue, the crypts depth, proliferating cells and Lgr5+ISCs number increased in middle group (12-14 months) and then decreased in old group (22-24 months). The number of proliferating Lgr5+ISCs gradually decreased from young to old. In organoids, the buddings number and projected area, Lgr5+ISCs ratio also decreased from young to old. Both gene expression of Parp3 and protein level of Parp3 increased in middle and old group. Parp3 inhibitors slowed down organoids’ growth of the middle age. Conclusion Parp3 might participate in regulating the proliferation capacity of Lgr5+ISCs during aging.

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“…Thus, identifying the PARP12-interacting mitochondrial proteins would help us to understand the underlying mechanisms. Some pathways that are independent of PARylation may also participate in maintaining mitochondria homomasis, in light of not all PARPs family members exert its role by PARylation [ 38 , 39 ]. Besides, given that some RNA binding proteins (RBPs) have been identified as essential for adipogenesis and thermoregulation [ 40–42 ], as an RBP, PARP12 may also exert its function by affecting RNA processes and post transcription.…”

Section: Discussionmentioning

confidence: 99%

PARP12 is required for mitochondrial function maintenance in thermogenic adipocytes

et al. 2022

Adipocyte

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PARP12 is a member of poly-ADP-ribosyl polymerase (PARPs), which has been characterized for its antiviral function. Yet its physiological implication in adipocytes remains unknown. Here, we report a central function of PARP12 in thermogenic adipocytes. We show that PARP12 is highly expressed in brown adipose tissue and is mainly localized to the mitochondria. Knockdown of PARP12 in vitro reduced UCP1 expression. In parallel, the deficiency of PARP12 reduced mitochondrial respiration in adipocytes, while overexpression of PARP12 reversed these effects.

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Parp3 promotes astrocytic differentiation through a tight regulation of Nox4-induced ROS and mTorc2 activation

Cited by 20 publications

References 72 publications

Silencing of Poly(ADP-Ribose) Polymerase-2 Induces Mitochondrial Reactive Species Production and Mitochondrial Fragmentation

Silencing of Poly(ADP-Ribose) Polymerase-2 Induces Mitochondrial Reactive Species Production and Mitochondrial Fragmentation

Fall of Parp3 restrains Lgr5+ stem cells proliferation and mucosal renovation in intestinal aging

PARP12 is required for mitochondrial function maintenance in thermogenic adipocytes

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