Abstract
MNT, a transcription factor of the MXD family, is an important modulator of the oncoprotein MYC. Both MNT and MYC are basic-helix–loop–helix proteins that heterodimerize with MAX in a mutually exclusive manner, and bind to E-boxes within regulatory regions of their target genes. While MYC generally activates transcription, MNT represses it. However, the molecular interactions involving MNT as a transcriptional regulator beyond the binding to MAX remain unexplored. Here we demonstrate a novel MAX-independent protein interaction between MNT and REL, the oncogenic member of the NF-κB family. REL participates in important biological processes and it is altered in a variety of tumors. REL is a transcription factor that remains inactive in the cytoplasm in an inhibitory complex with IκB and translocates to the nucleus when the NF-κB pathway is activated. In the present manuscript, we show that MNT knockdown triggers REL translocation into the nucleus and thus the activation of the NF-κB pathway. Meanwhile, MNT overexpression results in the repression of IκBα, a bona fide REL target. Both MNT and REL bind to the IκBα gene on the first exon, suggesting its regulation as an MNT–REL complex. Altogether our data indicate that MNT acts as a repressor of the NF-κB pathway by two mechanisms: (1) retention of REL in the cytoplasm by MNT interaction, and (2) MNT-driven repression of REL-target genes through an MNT–REL complex. These results widen our knowledge about MNT biological roles and reveal a novel connection between the MYC/MXD and NF-κB pathways, two of the most prominent pathways in cancer.
Highlights
MNT is a protein from the MYC/MAX/MXD/MLX network of transcription factors, which has a pivotal role in controlling cell proliferation, differentiation, metabolism, and oncogenic transformation
The results showed that the MNT–REL complex localizes in the cytoplasm in normal conditions and in the nucleus upon activation of the NF-κB pathway by TNFα (Fig. 3f)
MNT and REL interact in some mouse, rat, and human cell lines, and this complex can be found in both cytoplasm and nucleus
Summary
MNT is a protein from the MYC/MAX/MXD/MLX network of transcription factors, which has a pivotal role in controlling cell proliferation, differentiation, metabolism, and oncogenic transformation. MNT is a basichelix–loop–helix leucine zipper (bHLHLZ) protein that regulates transcription as heterodimers with MAX1,2 or MLX3 and as homodimers[4]. MNT connects the MYC-MAX and MLX-Mondo branches of the network[5]. MNT normally represses gene transcription by binding to. E-boxes and interacting with SIN3 proteins that, in turn, recruit histone deacetylase complexes to its target genes[1,6]. Among the MXD proteins, MNT is the biggest as well as the most ubiquitously expressed and conserved member[7,8]. Whereas Mxd1−/−, Mxi1−/−, and Mxd3−/− mice survive, mice knockout for Mnt die soon after birth[9,10,11,12]
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