Intact NYN/PIN-Like Domain is Crucial for the Degradation of Inflammation-Related Transcripts by ZC3H12D

Wawro, Mateusz; Kochan, Jakub; Krzanik, Sylwia; Jura, Jolanta; Kasza, Aneta

doi:10.1002/jcb.25665

Cited by 29 publications

(40 citation statements)

References 27 publications

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“…When comparing combined TMZ + OKN treatment to TMZ alone ( Figure 5 B ), interesting downregulated genes are IGR1 (associated with shorter disease-free survival in patients whose tumors are ER positive and HER2 positive [56] ; IGF1R signaling pathway is very relevant in drug resistance [57] ), XIST (increased level associated with shorter survival and poorer prognosis [58] ), and PRKDC (prognostic biomarker for chemoresistance in breast cancer patients [59] ). Interesting upregulated genes include ZC3H12A (crucial negative regulator of inflammation [60] ) and RN7SK (potential antiproliferative and tumor-suppressive function [61] ).…”

Section: Discussionmentioning

confidence: 99%

OKN-007 Increases temozolomide (TMZ) Sensitivity and Suppresses TMZ-Resistant Glioblastoma (GBM) Tumor Growth

Towner

Smith

Saunders

et al. 2019

Translational Oncology

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Treatment of glioblastoma (GBM) remains a challenge using conventional chemotherapy, such as temozolomide (TMZ), and is often ineffective as a result of drug resistance. We have assessed a novel nitrone-based agent, OKN-007, and found it to be effective in decreasing tumor volumes and increasing survival in orthotopic GBM xenografts by decreasing cell proliferation and angiogenesis and increasing apoptosis. In this study, we assessed combining OKN-007 with TMZ in vivo in a human G55 GBM orthotopic xenograft model and in vitro in TMZ-resistant and TMZ-sensitive human GBM cell lines. For the in vivo studies, magnetic resonance imaging was used to assess tumor growth and vascular alterations. Percent animal survival was also determined. For the in vitro studies, cell growth, IC50 values, RNA-seq, RT-PCR, and ELISA were used to assess growth inhibition, possible mechanism-of actions (MOAs) associated with combined OKN-007 + TMZ versus TMZ alone, and gene and protein expression levels, respectively. Microarray analysis of OKN-007–treated rat F98 glioma tumors was also carried out to determine possible MOAs of OKN-007 in glioma-bearing animals either treated or not treated with OKN-007. OKN-007 seems to elicit its effect on GBM tumors via inhibition of tumorigenic TGF-β1, which affects the extracellular matrix. When combined with TMZ, OKN-007 significantly increases percent survival, decreases tumor volumes, and normalizes tumor blood vasculature in vivo compared to untreated tumors and seems to affect TMZ-resistant GBM cells possibly via IDO-1, SUMO2, and PFN1 in vitro. Combined OKN-007 + TMZ may be a potentially potent treatment strategy for GBM patients.

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Section: Discussionmentioning

confidence: 99%

OKN-007 Increases temozolomide (TMZ) Sensitivity and Suppresses TMZ-Resistant Glioblastoma (GBM) Tumor Growth

Towner

Smith

Saunders

et al. 2019

Translational Oncology

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“…Interesting is also the phenomenon of the regulation of Regnase-1 level by other members of the ZC3H12 family. All proteins from this family (including Regnase-1 itself) are able to degrade Regnase-1 transcript (Iwasaki et al 2011;Wawro et al 2016Wawro et al , 2017M Wawro, A Solecka, W Sowinska, et al, unpubl.). In the present study, we have shown that ZC3H12B interacts with Regnase-1 3 ′ UTR although we could not confirm its direct interaction with Regnase-1 mRNA using RIP.…”

Section: Discussionmentioning

confidence: 99%

“…Briefly, the V5-TC tag was excised with KpnI and NotI and the STreptagII-Flag tag was inserted by ligation of two phosphorylated and reannealed oligos (StrepFlagM2s: CCACCATGGCAAGCTGGAGCCACCCGCAGT TCGAAAAGGGTGCAGACTACAAAGACGATGACGACAAGCTT GC; StrepFlagM2s: GGCCGCAAGCTTGTCGTCATCGTCTTTG TAGTCTGCACCCTTTTCGAACTGCGGGTGGCTCCAGCTTGCC AT GGTGGGTAC spSBtet-GP was a gift from Eric Kowarz (Addgene plasmid #60495) (Kowarz et al 2015). The luciferase constructs (pmirGLO_IL-6-3 ′ UTR, pmirGLO_IL-6-3 ′ UTRΔCE, pmirGLO_ZC3H12A-3 ′ UTR, pmirGLO_VEGFA-3 ′ UTR, and pmir-GLO_IER3-3 ′ UTR) were described previously (Kochan et al 2016;Wawro et al 2016Wawro et al , 2017. The sequences of all used constructs were verified by Sanger sequencing (Genomed) and the expression of the recombinant proteins was confirmed by western blotting analysis.…”

Section: Plasmid Constructionmentioning

confidence: 99%

“…Our knowledge of the biological roles played by other members of the ZC3H12 family is very limited, although it appears that these members are also involved in inflammatory processes. ZC3H12D (MCPIP4) participates in the degradation of proinflammatory mRNAs, such as the mRNAs of IL-2, IL-6, IL-10, TNF, IER3, and Regnase-1 (Zhang et al 2015;Wawro et al 2017). Similar to Regnase-1, the overexpression of ZC3H12D attenuates global protein ubiquitination and leads to the inhibition of the TLR2and TLR4-induced activation of JNK, ERK, and NF-κB signaling and TLR4-induced inflammatory gene expression in macrophages (Huang et al 2012).…”

Section: Introductionmentioning

confidence: 99%

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ZC3H12B/MCPIP2, a new active member of the ZC3H12 family

Wawro

Kochan

et al. 2019

RNA

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ZC3H12B is the most enigmatic member of the ZC3H12 protein family. The founding member of this family, Regnase-1/ MCPIP1/ZC3H12A, is a well-known modulator of inflammation and is involved in the degradation of inflammatory mRNAs. In this study, for the first time, we characterized the properties of the ZC3H12B protein. We show that the biological role of ZC3H12B depends on an intact NYN/PIN RNase domain. Using RNA immunoprecipitation, experiments utilizing actinomycin D and ELISA, we show that ZC3H12B binds interleukin-6 (IL-6) mRNA in vivo, regulates its turnover, and results in reduced production of IL-6 protein upon stimulation with IL-1β. We verified that regulation of IL-6 mRNA stability occurs via interaction of ZC3H12B with the stem-loop structure present in the IL-6 3 ′ ′ ′ ′ ′ UTR. The IL-6 transcript is not the only target of ZC3H12B. ZC3H12B also interacts with other known substrates of Regnase-1 and ZC3H12D, such as the 3 ′ ′ ′ ′ ′ UTRs of IER3 and Regnase-1, and binds IER3 mRNA in vivo. Using immunofluorescence, we examined the localization of ZC3H12B within the cell. ZC3H12B forms small, granule-like structures in the cytoplasm that are characteristic of proteins involved in mRNA turnover. The overexpression of ZC3H12B inhibits proliferation by stalling the cell cycle in the G2 phase. This effect of ZC3H12B is also NYN/PIN dependent. The analysis of the ZC3H12B mRNA level reveals its highest expression in the human brain and the neuroblastoma cell line SH-SY5Y, although the factors regulating its expression remain elusive. Down-regulation of ZC3H12B in SH-SY5Y cells by specific shRNAs results in up-regulation of ZC3H12B-target mRNAs.

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“…Zc3h12d is upregulated upon endotoxin exposure, and its knockdown leads to a strong increase in the levels of IL‐1β, IL‐6, and TNF‐α, as well as other transcripts encoding additional inflammatory factors . Degradation of these mRNAs depends on the intact RNase domain of Zc3h12d . Although Zc3h12a and Zc3h12d appear to target common transcripts and seem to interact by co‐immunoprecipitation, they act independently in degrading IL‐6 mRNA .…”

Section: Biological Roles Of Regnase‐1‐related Proteinsmentioning

confidence: 99%

ZC3H12A/MCPIP1/Regnase‐1‐related endonucleases: An evolutionary perspective on molecular mechanisms and biological functions

Habacher

Ciosk

2017

BioEssays

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The mammalian Zc3h12a/MCPIP1/Regnase-1, an extensively studied regulator of inflammatory response, is the founding member of a ribonuclease family, which includes proteins related by the presence of the so-called Zc3h12a-like NYN domain. Recently, several related proteins have been described in Caenorhabditis elegans, allowing comparative evaluation of molecular functions and biological roles of these ribonucleases. We discuss the structural features of these proteins, which endow some members with ribonuclease (RNase) activity while others with auxiliary or RNA-independent functions. We also consider their RNA specificity and highlight a common role for these proteins in cellular defense, which is remarkable considering the evolutionary distance and fundamental differences in cellular defense mechanisms between mammals and nematodes.

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Intact NYN/PIN-Like Domain is Crucial for the Degradation of Inflammation-Related Transcripts by ZC3H12D

Cited by 29 publications

References 27 publications

OKN-007 Increases temozolomide (TMZ) Sensitivity and Suppresses TMZ-Resistant Glioblastoma (GBM) Tumor Growth

OKN-007 Increases temozolomide (TMZ) Sensitivity and Suppresses TMZ-Resistant Glioblastoma (GBM) Tumor Growth

ZC3H12B/MCPIP2, a new active member of the ZC3H12 family

ZC3H12A/MCPIP1/Regnase‐1‐related endonucleases: An evolutionary perspective on molecular mechanisms and biological functions

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