A Repertoire of MicroRNAs Regulates Cancer Cell Starvation by Targeting Phospholipase D in a Feedback Loop That Operates Maximally in Cancer Cells

Fite, Kristen; Elkhadragy, Lobna; Gómez‐Cambronero, Julian

doi:10.1128/mcb.00711-15

Cited by 19 publications

(15 citation statements)

References 45 publications

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“…We have studied previously post-translational modification of PLD2 transcripts and reported how that is under regulation of certain miRs. 18,22 For macrophages, we selected miR-138 and miR-887 that bind to the 3'UTR of PLD2 ( Figure 5B). The demonstration that transfected miR-138 and miR-887 decrease PLD2 expression in M0 macrophages is shown in Figure 5C,D.…”

Section: Mechanism For Pld-mediated Effect Of Rvd5 In Macrophages: mentioning

confidence: 99%

“…[15][16][17] PLD is upregulated in response to various cell stressors, such as hypoxia and nutrient starvation. 18,19 Moreover, it has been shown that PLD2 -/mice produce less pro-inflammatory cytokines in a sepsis model. 20 PA is a mitogen and a critical secondary messenger that activates many downstream pathways leading to cell growth and proliferation, vesicle trafficking and cell migration.…”

Section: Introductionmentioning

confidence: 99%

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D‐series Resolvins activate Phospholipase D in phagocytes during inflammation and resolution

et al. 2020

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A successful acute inflammatory response results in the elimination of infectious agents by neutrophils and monocytes, followed by resolution and repair through tissue-resident and recruited macrophages. Resolvins (D-series and E-series) are proresolving lipid mediators involved in resolution and tissue repair, whose intracellular signaling remains of interest. Here, we report that D-series resolvins (RvD1-RvD5) activate phospholipase D (PLD), a ubiquitously expressed membrane lipase enzyme activity in modulating phagocyte functions. The mechanism for PLD-mediated actions of Resolvin-D5 (RvD5) in polarizing macrophages (M1-like toward M2-like) was found to be two-pronged: (a) RvD5 inhibits post-transcriptional modifications, by miRs and 3'exonucleases that process PLD2 mRNA, thus increasing PLD2 expression and activity; and (b) RvD5 enhances PLD2-S6Kinase signaling required for membrane expansion and efferocytosis. In an in vivo model of second organ reflow injury, we found that RvD5 did not reduce lung neutrophil myeloperoxidase levels in PLD2-/mice compared to WT and PLD1-/mice, confirming a novel role of PLD2 2 | GANESAN Et Al.

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Section: Mechanism For Pld-mediated Effect Of Rvd5 In Macrophages: mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

D‐series Resolvins activate Phospholipase D in phagocytes during inflammation and resolution

et al. 2020

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“…Increased levels of miR-887 were previously reported in endometrial and rectal cancer (77,78). In contrast, other authors have demonstrated that miR-887 may act as a tumor suppressor in prostate cancer, breast cancer and small cell lung cancer (SCLC) (79)(80)(81). We have shown that mutations in miRNA genes and known cancer driver genes are not mutually exclusive, but a substantial number of miRNA gene mutations were identified in samples without mutations in known protein-coding drivers.…”

Section: Discussionmentioning

confidence: 60%

Somatic mutations in miRNA genes in lung cancer – potential functional consequences of non-coding sequence variants

Galka-Marciniak

Urbanek-Trzeciak

Nawrocka

et al. 2019

Preprint

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A growing body of evidence indicates that miRNAs may either drive or suppress oncogenesis. However, little is known about somatic mutations in miRNA genes. To determine the frequency and potential consequences of miRNA gene mutations, we analyzed whole exome sequencing datasets of ~500 lung adenocarcinoma (LUAD) and ~500 lung squamous cell carcinoma (LUSC) samples generated in the TCGA. Altogether, we identified >1000 mutations affecting ~500 different miRNA genes and showed that half of all cancers had at least one such mutation. Mutations occurred in most crucial parts of miRNA precursors, including mature miRNA and seed sequences. We showed that seed mutations strongly affected miRNA:target interactions, drastically changing the pool of predicted targets. Mutations may also affect miRNA biogenesis by changing the structure of miRNA precursors, DROSHA and DICER cleavage sites, and regulatory sequence/structure motifs. We identified 10 significantly overmutated hotspot miRNA genes, including the miR-379 gene in LUAD enriched in mutations in the mature miRNA and regulatory sequences. The occurrence of mutations in the hotspot miRNA genes was also shown experimentally. We present a comprehensive analysis of somatic mutations in miRNA genes and show that some of these genes are mutational hotspots, suggesting their potential role in cancer.3

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“…There could be several reasons for this. We have studied previously post-translational modification of PLD2 transcripts and reported how that is under regulation of certain miRs (22,26). For macrophages, we selected miR-138 and miR-887 that are predicted to bind to the 3'UTR of PLD2 (Fig.…”

Section: Mechanism For Pld-mediated Effect Of Rvd5 In Macrophages: (Amentioning

confidence: 99%

“…However, the intracellular mechanism of downstream signaling in macrophages is of interest.Phospholipase D (PLD) is a ubiquitously expressed membrane-associated lipase that hydrolyzes phosphatidylcholine (PC) into free choline and phosphatidic acid (PA) (19)(20)(21). PLD is upregulated in response to various cell stressors, such as hypoxia and nutrient starvation (22,23). Moreover, PLD2 -/mice produced less pro-inflammatory cytokines in a sepsis model (24).…”

mentioning

confidence: 99%

Resolvin D-series regulates Phospholipase D both during inflammation and resolution by modulating phagocyte functions

Ganesan

Henkels

Shah

et al. 2019

Preprint

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A successful acute inflammatory response results in the elimination of infectious agents by neutrophils and monocytes, followed by resolution and repair by tissue-resident and recruited macrophages. D-series resolvins are pro-resolving mediators involved in resolution and tissue repair, their intracellular signaling mechanism(s) are of interest. Here, we report that D-series resolvins activate phospholipase D (PLD), a ubiquitously expressed membrane lipase in modulating phagocyte functions. The mechanism for PLD-mediated actions of RvD5 in polarizing macrophages (M1-M2) was found to be two-pronged: (a) RvD5 inhibits posttranscriptional modifications, by miRs and 3'exonulceases that process PLD2 mRNA, thus increasing PLD2 expression and activity; (b) RvD5 enhances PLD2-S6K signaling and Actin expression required for membrane expansion and efferocytosis. In addition, investigating RvD5's actions in second organ reflow injury, we found that RvD5 did not reduce lung neutrophil myeloperoxidase levels in PLD2 -/mice compared to WT and PLD1 -/mice, pointing to a unique role of PLD2 as the relevant isoform in RvD5-mediated resolution. These results demonstrate that RvD5-PLD2 are attractive targets for therapeutic interventions in vascular inflammation such as I/R injury and cardiovascular diseases. clearance of bacteria (3). Resolvin D5 activates a specific receptor denoted human GPR32 (18). However, the intracellular mechanism of downstream signaling in macrophages is of interest.Phospholipase D (PLD) is a ubiquitously expressed membrane-associated lipase that hydrolyzes phosphatidylcholine (PC) into free choline and phosphatidic acid (PA) (19)(20)(21). PLD is upregulated in response to various cell stressors, such as hypoxia and nutrient starvation (22,23). Moreover, PLD2 -/mice produced less pro-inflammatory cytokines in a sepsis model (24). The product of the PLD reaction, PA, is itself a mitogen and a critical secondary messenger that activates many downstream pathways leading to cell growth and proliferation, vesicle trafficking and cell migration (19)(20)(21). Additionally, PA is conical in shape and carries a negative charge, meaning its accumulation in the membrane results in membrane curvature needed for cell migration (23,(25)(26)(27). Although PLD/PA play a role in macrophage adhesion (25,28), no role of PLD in macrophage polarization has been described as of yet.Phospholipase D (PLD, with the two major mammalian isoforms, PLD1 and PLD2) has a pivotal role in cellular activities such as chemotaxis and phagocytosis (21,(29)(30)(31)(32)(33)(34). Aberrant PLD expression and activity is implicated in inflammation (23,(35)(36)(37)(38) and other cellular functions (21,39). PLD is also actively involved in pro-inflammatory cytokine recruitment, reactive oxygen species (ROS) generation, chemotaxis, and cell invasion (40)(41)(42)(43). In this report, we set out to understand the role of resolvins in inflammation and resolution involving PLD as an intracellular signaling molecule. RESULTS PLD expression and activity in...

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A Repertoire of MicroRNAs Regulates Cancer Cell Starvation by Targeting Phospholipase D in a Feedback Loop That Operates Maximally in Cancer Cells

Cited by 19 publications

References 45 publications

D‐series Resolvins activate Phospholipase D in phagocytes during inflammation and resolution

D‐series Resolvins activate Phospholipase D in phagocytes during inflammation and resolution

Somatic mutations in miRNA genes in lung cancer – potential functional consequences of non-coding sequence variants

Resolvin D-series regulates Phospholipase D both during inflammation and resolution by modulating phagocyte functions

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