Inflammatory Conditions Induce IRES-Dependent Translation of cyp24a1

Rübsamen, Daniela; Kunze, Michael M.; Buderus, Victoria; Brauß, Thilo F.; Bajer, Magdalena M.; Brüne, Bernhard; Schmid, Tobias

doi:10.1371/journal.pone.0085314

Cited by 26 publications

(11 citation statements)

References 38 publications

(51 reference statements)

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“…The presence of CYP24A1 splice variants that may alter enzyme activity have been reported in breast cancer cell lines and tissues (64; 65), and characterization of these variants may help clarify the discrepancies noted above with respect to CYP24A1 expression in breast cancer. The regulation of CYP24A1 by factors other than 1,25D in breast cancer has not been particularly well studied, although inflammation was shown to increase, and miR125b shown to decrease, CYP24A1 in vitro (66; 67). Epigenetic regulation of CYP24A1 by promoter methylation has been reported in lung and prostate cancer (68; 69), but studies in breast cancer are lacking.…”

Section: Role Of Cyp24a1 In Mammary Gland and Breast Cancermentioning

confidence: 99%

Function of the vitamin D endocrine system in mammary gland and breast cancer

Welsh

2017

Molecular and Cellular Endocrinology

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The nuclear receptor for 1α,25-dihydroxycholecalciferol (1,25D), the active form of vitamin D, has anti-tumor actions in many tissues. The vitamin D receptor (VDR) is expressed in normal mammary gland and in many human breast cancers suggesting it may represent an important tumor suppressor gene in this tissue. When activated by 1,25D, VDR modulates multiple cellular pathways including those related to energy metabolism, terminal differentiation and inflammation. There is compelling pre-clinical evidence that alterations in vitamin D status affect breast cancer development and progression, while clinical and epidemiological data are suggestive but not entirely consistent. The demonstration that breast cells express CYP27B1 (which converts the precursor vitamin D metabolite 25D to the active metabolite 1,25D) and CYP24A1 (which degrades both 25D and 1,25D) provides insight into the difficulties inherent in using dietary vitamin D, sun exposure and/or serum biomarkers of vitamin D status to predict disease outcomes. Emerging evidence suggests that the normally tight balance between CYP27B1 and CYP24A1 becomes deregulated during cancer development, leading to abrogation of the tumor suppressive effects triggered by VDR. Research aimed at understanding the mechanisms that govern uptake, storage, metabolism and actions of vitamin D steroids in normal and neoplastic breast tissue remain an urgent priority.

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Section: Role Of Cyp24a1 In Mammary Gland and Breast Cancermentioning

confidence: 99%

Function of the vitamin D endocrine system in mammary gland and breast cancer

Welsh

2017

Molecular and Cellular Endocrinology

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Section: Targeting Ires Elements With Antisense Oligonucleotides and mentioning

confidence: 99%

“…Another interesting recent report has identified an IRES element in the cyp24a1 (1,25-dihydroxyvitamin D3 24-hydroxylase) mRNA, which encodes a protein that inactivates vitamin D3-mediated signaling ( 100 ). This IRES was induced by vitamin D3 and inflammation and involved the PI3K-AKT1 signaling pathway ( 100 ). Cyp24a1 was also found to be induced in breast and colon cancer cells and its enhanced expression may therefore explain the development of tumor resistance to chemotherapies in which D3 is used as an adjuvant agent ( 100 ).…”

Section: Targeting Ires Elements With Antisense Oligonucleotides and mentioning

confidence: 99%

“…This IRES was induced by vitamin D3 and inflammation and involved the PI3K-AKT1 signaling pathway ( 100 ). Cyp24a1 was also found to be induced in breast and colon cancer cells and its enhanced expression may therefore explain the development of tumor resistance to chemotherapies in which D3 is used as an adjuvant agent ( 100 ). Understanding how inflammation causes translational reprogramming in different cancers will be an important step toward targeting IRES-mediated translation for treatment of these diseases.…”

Section: Targeting Ires Elements With Antisense Oligonucleotides and mentioning

confidence: 99%

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Exploring Internal Ribosome Entry Sites as Therapeutic Targets

Komar

Hatzoglou

2015

Front. Oncol.

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Initiation of eukaryotic mRNA translation may proceed via several different routes, each requiring a different subset of factors and relying on different and specific interactions between the mRNA and the ribosome. Two modes predominate: (i) so-called cap-dependent initiation, which requires all canonical initiation factors and is responsible for about 95–97% of all initiation events in eukaryotic cells; and (ii) cap-independent internal initiation, which requires a reduced subset of initiation factors and accounts for up to 5% of the remaining initiation events. Internal initiation relies on the presence of so-called internal ribosome entry site (IRES) elements in the 5′ UTRs of some viral and cellular mRNAs. These elements (often possessing complex secondary and tertiary structures) promote efficient interaction of the mRNA with the 40S ribosome and allow for internal ribosome entry. Internal initiation of translation of specific mRNAs may contribute to development of severe disease and pathological states, such as hepatitis C and cancer. Therefore, this cellular mechanism represents an attractive target for pharmacological modulation. The purpose of this review is to provide insight into current strategies used to target viral and cellular IRESs and discuss the physiological consequences (and potential therapeutic implications) of abrogation/modulation of IRES-mediated translation.

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“…Polysome analysis was performed as described previously (21). Briefly, after incubation with 100 µg/ml cycloheximide for 10 min at 37°C cells were scraped and centrifuged.…”

Section: Polysomal Fractionationmentioning

confidence: 99%

Hydrogen peroxide formation by Nox4 limits malignant transformation

Helfinger

Gall

Henke

et al. 2017

Preprint

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PrecisBy oxidizing AKT and keeping PP2A in the cytosol, the NADPH oxidase Nox4 allows proper DNA damage repair and averts cancer development.not peer-reviewed) is the author/funder. All rights reserved. No reuse allowed without permission.The copyright holder for this preprint (which was . http://dx.doi.org/10.1101/177055 doi: bioRxiv preprint first posted online Aug. 16, 2017; AbstractReactive oxygen species (ROS) can cause cellular damage and are thought to promote cancer-development. Nevertheless, under physiological conditions, all cells constantly produce ROS, either as chemical by-products or for signaling purpose. During differentiation cells induce the NADPH oxidase Nox4, which constitutively produces low amounts of H 2 O 2 . We infer that this constitutive H 2 O 2 is unlikely to be carcinogenic and may rather maintain basal activity of cellular surveillance systems.Utilizing two different murine tumor models we demonstrate that Nox4 prevents malignant transformation and facilitated the recognition of DNA-damage. Upon DNA-damage repair is initiated as consequence of phosphorylation of H2AX (γH2AX). Repair only occurs if nuclear activity of the γH2AX-dephosphorylating phosphatase PP2A is kept sufficiently low, a task fulfilled by Nox4: Nox4 continuously oxidizes AKT, and once oxidized AKT captures PP2A in the cytosol. Absence of Nox4 facilitates nuclear PP2A translocation and dephosphorylation of γH2AX. Simultaneously the proportion of active, phosphorylated AKT is increased. Thus, DNA-damage is not recognized and the increase in AKT activity promotes proliferation. The combination of both events resulted in genomic instability and tumor initiation.With the identification of the first cancer-protective source of reactive oxygen species, Nox4, the paradigm of reactive-oxygen species-induced initiation of malignancies should be revised. (200 words) SignificanceThe stereotype of ROS produced by NADPH oxidases as cause of malignant diseases persists generalized since decades. We demonstrate that the NADPH oxidase Nox4, as constitutive source of ROS, prevents malignant transformation and that its pharmacological not peer-reviewed) is the author/funder. All rights reserved. No reuse allowed without permission.The copyright holder for this preprint (which was . http://dx.doi.org/10.1101/177055 doi: bioRxiv preprint first posted online Aug. 16, 2017; inhibition as currently aspired by several companies will potentially increase the risk of malignant cell transformation and eventually tumor formation.

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Inflammatory Conditions Induce IRES-Dependent Translation of cyp24a1

Cited by 26 publications

References 38 publications

Function of the vitamin D endocrine system in mammary gland and breast cancer

Function of the vitamin D endocrine system in mammary gland and breast cancer

Exploring Internal Ribosome Entry Sites as Therapeutic Targets

Hydrogen peroxide formation by Nox4 limits malignant transformation

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