Rhein Inhibits AlkB Repair Enzymes and Sensitizes Cells to Methylated DNA Damage

Li, Qi; Huang, Yue; Liu, Xichun; Gan, Jianhua; Chen, Hao; Yang, Cai‐Guang

doi:10.1074/jbc.m115.711895

Cited by 69 publications

(61 citation statements)

References 62 publications

(63 reference statements)

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“…Rhein, a natural product, is the first identified FTO inhibitor and competes with m6A-containing RNA for binding to the catalytic domain of FTO [97]. However, rhein is not an FTO-specific inhibitor, and it has been reported that rhein can also inhibit other ALKB family demethylases [98]. Meclofenamic acid (MA) is another FTO inhibitor and shows high selectivity in inhibiting FTO over ALKBH5 [99].…”

Section: Diagnosis and Therapeutic Potentialmentioning

confidence: 99%

The emerging roles of N6-methyladenosine (m6A) deregulation in liver carcinogenesis

2020

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Liver cancer is a common cancer worldwide. Although the etiological factors of liver carcinogenesis are well defined, the underlying molecular mechanisms remain largely elusive. Epigenetic deregulations, such as aberrant DNA methylation and histone modifications, play a critical role in liver carcinogenesis. Analogous to DNA and core histone proteins, reversible chemical modifications on mRNA have recently been recognized as important regulatory mechanisms to control gene expression. N6-methyladenosine (m6A) is the most prevalent internal mRNA modification in mammalian cells. m6A modification is important for controlling many cellular and biological processes. Deregulation of m6A modification has been recently implicated in human carcinogenesis, including liver cancer. In this review, we summarize the recent findings on m6A regulation and its biological impacts in normal and cancer cells. We will focus on the deregulation of m6A modification and m6A regulators in liver diseases and liver cancers. We will highlight the clinical relevance of m6A deregulation in liver cancer. We will also discuss the potential of exploiting m6A modification for cancer diagnosis and therapeutics.

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Section: Diagnosis and Therapeutic Potentialmentioning

confidence: 99%

The emerging roles of N6-methyladenosine (m6A) deregulation in liver carcinogenesis

2020

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“…It is of note that rhein and MA do not specifically inhibit FTO over other enzymes. For example, rhein also binds to 2OG-binding site of AlkB, a dioxygenase from Escherichia coli , and inhibits its activity [101] . As an anti-inflammatory drug, MA binds to the catalytic center of aldo–keto reductase 1C3 (AKR1C3) protein, which catalyzes the reduction of carbonyl groups on both steroids and prostaglandins in humans [102] .…”

Section: Alkbh5 and Fto Are Termed M 6 A Erasersmentioning

confidence: 99%

Structural Insights into N 6-Methyladenosine (m6A) Modification in the Transcriptome

Huang

Yin

2018

Genomics, Proteomics &Amp; Bioinformatics

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More than 100 types of chemical modifications in RNA have been well documented. Recently, several modifications, such as N6-methyladenosine (m6A), have been detected in mRNA, opening the window into the realm of epitranscriptomics. The m6A modification is the most abundant modification in mRNA and non-coding RNA (ncRNA). At the molecular level, m6A affects almost all aspects of mRNA metabolism, including splicing, translation, and stability, as well as microRNA (miRNA) maturation, playing essential roles in a range of cellular processes. The m6A modification is regulated by three classes of proteins generally referred to as the “writer” (adenosine methyltransferase), “eraser” (m6A demethylating enzyme), and “reader” (m6A-binding protein). The m6A modification is reversibly installed and removed by writers and erasers, respectively. Readers, which are members of the YT521-B homology (YTH) family proteins, selectively bind to RNA and affect its fate in an m6A-dependent manner. In this review, we summarize the structures of the functional proteins that modulate the m6A modification, and provide our insights into the m6A-mediated gene regulation.

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“…In a study of brain tumor samples taken from patients treated with alkylating drugs such as temozolomide (TMZ), all samples contained elevated levels of ALKBH2 mRNA over those from patients receiving radiotherapy . TMZ resistance in several glioblastoma cell lines as well as cisplatin resistance in H1299 lung cancer cells was suppressed by siRNA‐mediated knockdown of ALKBH2, and reduced ALKBH2 activity improves sensitivity to alkylating drugs . These findings have stimulated recent efforts to find inhibitors of ALKBH2 …”

Section: Figurementioning

confidence: 99%

Fluorescence Probes for ALKBH2 Allow the Measurement of DNA Alkylation Repair and Drug Resistance Responses

Wilson

Beharry

Srivastava³

et al. 2018

Angewandte Chemie

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The DNA repair enzyme ALKBH2 is implicated in both tumorigenesis as well as resistance to chemotherapy in certain cancers. It is currently under study as a potential diagnostic marker and has been proposed as a therapeutic target. To date, however, there exist no direct methods for measuring the repair activity of ALKBH2 in vitro or in biological samples. Herein, we report a highly specific, fluorogenic probe design based on an oligonucleotide scaffold that reports directly on ALKBH2 activity both in vitro and in cell lysates. Importantly, the probe enables the monitoring of cellular regulation of ALKBH2 activity in response to treatment with the chemotherapy drug temozolomide through a simple fluorescence assay, which has only previously been observed through indirect means such as qPCR and western blots. Furthermore, the probe provides a viable high‐throughput assay for drug discovery.

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Rhein Inhibits AlkB Repair Enzymes and Sensitizes Cells to Methylated DNA Damage

Cited by 69 publications

References 62 publications

The emerging roles of N6-methyladenosine (m6A) deregulation in liver carcinogenesis

The emerging roles of N6-methyladenosine (m6A) deregulation in liver carcinogenesis

Structural Insights into N 6-Methyladenosine (m6A) Modification in the Transcriptome

Fluorescence Probes for ALKBH2 Allow the Measurement of DNA Alkylation Repair and Drug Resistance Responses

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