Miz-1 regulates translation of
            <i>Trp53</i>
            via ribosomal protein L22 in cells undergoing V(D)J recombination

Rashkovan, Marissa; Vadnais, Charles; Ross, Julie; Gigoux, Mathieu; Suh, Woong‐Kyung; Gu, Wei; Kosan, Christian; Möröy, Tarik

doi:10.1073/pnas.1412107111

Cited by 31 publications

(33 citation statements)

References 49 publications

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“…We next asked how Rpl22 loss was influencing p53 synthesis. Rpl22 is an RNA binding protein that has been reported to directly regulate p53 synthesis through direct binding to p53 mRNA (33). Rpl22 binds RNA targets through recognition of a stem loop structure with a G-C-U at the neck of the stem (34).…”

Section: Resultsmentioning

confidence: 99%

Rpl22 Loss Selectively Impairs αβ T Cell Development by Dysregulating Endoplasmic Reticulum Stress Signaling

Solanki

Stadanlick

Zhang

et al. 2016

The Journal of Immunology

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While ribosomal proteins (RP) are thought to primarily facilitate biogenesis of the ribosome and its ability to synthesize protein, emerging evidence suggests that individual RP can perform critical regulatory functions that control developmental processes. We showed previously that despite the ubiquitous expression of the RP, Rpl22, germline ablation of Rpl22 in mice causes a selective, p53-dependent block in the development of αβ, but not γδ, T cell progenitors. Nevertheless, the basis by which Rpl22 loss selectively induces p53 in αβ T cell progenitors remained unclear. We show here that Rpl22 regulates the development of αβ T cells by restraining endoplasmic reticulum (ER) stress responses. In the absence of Rpl22, ER stress is exacerbated in αβ, but not γδ, T cell progenitors. The exacerbated ER stress in Rpl22-deficient αβ T lineage progenitors is responsible for selective induction of p53 and their arrest, as pharmacological induction of stress is sufficient to induce p53 and replicate the selective block of αβ T cells, and attenuation of ER stress signaling by knockdown of PERK, an ER stress sensor, blunts p53 induction and rescues development of Rpl22-deficient αβ T cell progenitors. Rpl22-deficiency appears to exacerbate ER stress by interfering with the ability of ER stress signals to block new protein synthesis. Our finding that Rpl22-deficiency exacerbates ER stress responses and induces p53 in αβ T cell progenitors provides insight into how a ubiquitously expressed RP can perform regulatory functions that are selectively required by some cell lineages but not others.

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Section: Resultsmentioning

confidence: 99%

Rpl22 Loss Selectively Impairs αβ T Cell Development by Dysregulating Endoplasmic Reticulum Stress Signaling

Solanki

Stadanlick

Zhang

et al. 2016

The Journal of Immunology

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Section: + 2+mentioning

confidence: 60%

“…Although it is known that the guanine nucleotide binding protein/GTPase Rho suppresses p53-mediated apoptosis downstream of the pre-TCR [ 127 ], the signaling steps that link the pre-TCR to inhibition of p53 are not fully elucidated. Recent evidence shows that the transcription factor Miz-1 induces the expression of the gene encoding ribosomal protein L22 (RPL22), a negative regulator of p53 translation [ 208 ], which is consistent with the role of Miz-1 and RPL22 as prosurvival molecules that antagonize p53 during the β-selection checkpoint of thymocytes [ 209 -211 ].Besides the regulators discussed in previous sections, there are some pre-TCR induced proteins that regulate thymocyte function, but whose connection with signaling components of the pre-TCR complex is poorly characterized. For instance, cyclin D3 is upregulated after β-selection to promote cell-cycle entry, and thymocytes lacking it show defective expansion and are more susceptible to oncogenic transformation [ 212 ].…”

mentioning

confidence: 60%

Transcription factors and target genes of pre-TCR signaling

López-Rodrı́guez

Aramburu

Berga-Bolaños

2015

Cell. Mol. Life Sci.

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Almost 30 years ago pioneering work by the laboratories of Harald von Boehmer and Susumo Tonegawa provided the first indications that developing thymocytes could assemble a functional TCRβ chain-containing receptor complex, the pre-TCR, before TCRα expression. The discovery and study of the pre-TCR complex revealed paradigms of signaling pathways in control of cell survival and proliferation, and culminated in the recognition of the multifunctional nature of this receptor. As a receptor integrated in a dynamic developmental process, the pre-TCR must be viewed not only in the light of the biological outcomes it promotes, but also in context with those molecular processes that drive its expression in thymocytes. This review article focuses on transcription factors and target genes activated by the pre-TCR to drive its different outcomes. KeywordsThymocyte development Pre-TCR expression Pre-TCR signaling Transcription factor Gene expression NF-κB NFATc NFAT5 ETS1 E2A/HEB proteins Bcl2A1 p53 Intrinsic apoptotic pathway We apologize to those authors whose work was not cited due to space limitations or our oversight. The thymus as the place for T cell development: short overview of thymocyte developmentThe thymus is the organ that supports the differentiation and selection of T cells. The thymic stroma promotes T cell development by producing growth factors and ligands for receptors expressed in thymocytes. During mouse embryogenesis, the thymic rudiment differentiates into the cortical and medullary thymic epithelial cell subsets (cTECs and mTECs), the major constituents of thymic stroma [ 1 ]. Only a small subset of hematopoietic precursors with T-lineage potential is able to enter the thymus [ 2 -4 ]. Early lymphoid progenitors (ELPs) enter the thymus at the cortico-medullary junction [ 5 ] and begin their development into T cells through several phenotypically distinct and sequential stages, known as double-negative (DN), double-positive (DP) and singlepositive (SP) based on the surface expression of the co-receptors CD4 and CD8. DN cells are further divided into four consecutive stages on the basis of CD44 and CD25 expression: DN1 (CD44 CD25 ), DN2 (CD44 CD25 ), DN3 (CD44 CD25 ) and DN4 (CD44 CD25 ) cells [ 6 ].Initial thymocyte development from DN1 to DN3 is promoted by molecules produced by cTECs, mainly interleukin-7 (IL-7) and Notch ligands [ 7 , 8 ]. ELPs that home into the thymus retain the expression of the surface receptor c-kit [ 9 ], indeed a small subset of early thymocyte progenitors (EPs) defined within DN1 prothymocytes still has high expression of c-kit [ 10 ]. DN thymocytes move to the subcapsular region of the thymic cortex and express the pre-T-cell receptor (pre-TCR) complex [ 11 , 12 ]. The pre-TCR is a unique molecular complex with an invariant pre-TCRα (pTα) chain associated with a recombined TCRβ chain and the signaling 1,3,* molecules CD3γ, CD3δ, CD3ε and CD3ζ, which also form part of the mature TCR [ 12 , 13 ]. The pre-TCR, along with the DeltaNotch interaction [ 14 ], initiates t...

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“…Delays of 0, 10, 30, 90, 120, 150, 250, 350, 450, 550, 650, 800, and 1000 ms and of 0, 10,30,50,70,90,110,130,150,170,190,210, and 250 ms were used to obtain T 1 and T 2 , respectively.…”

Section: Preparation Of the Miz1-4 And Miz1-4mentioning

confidence: 99%

Structural Insights into c-Myc-interacting Zinc Finger Protein-1 (Miz-1) Delineate Domains Required for DNA Scanning and Sequence-specific Binding

Bédard¹,

Roy²,

Montagne³

et al. 2017

Journal of Biological Chemistry

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Edited by Norma Allewellc-Myc-interacting zinc finger protein-1 (Miz-1) is a polyCys2His2 zinc finger (ZF) transcriptional regulator of many cell cycle genes. A Miz-1 DNA sequence consensus has recently been identified and has also unveiled Miz-1 functions in other cellular processes, underscoring its importance in the cell. Miz-1 contains 13 ZFs, but it is unknown why Miz-1 has so many ZFs and whether they recognize and bind DNA sequences in a typical fashion. Here, we used NMR to deduce the role of Miz-1 ZFs 1-4 in detecting the Miz-1 consensus sequence and preventing nonspecific DNA binding. In the construct containing the first 4 ZFs, we observed that ZFs 3 and 4 form an unusual compact and stable structure that restricts their motions. Disruption of this compact structure by an electrostatically mismatched A86K mutation profoundly affected the DNA binding properties of the WT construct. On the one hand, Miz1-4 WT was found to bind the Miz-1 DNA consensus sequence weakly and through ZFs 1-3 only. On the other hand, the four ZFs in the structurally destabilized Miz1-4 A86K mutant bound to the DNA consensus with a 30-fold increase in affinity (100 nM). The formation of such a thermodynamically stable but nonspecific complex is expected to slow down the rate of DNA scanning by Miz-1 during the search for its consensus sequence. Interestingly, we found that the motif stabilizing the compact structure between ZFs 3 and 4 is conserved and enriched in other long poly-ZF proteins. As discussed in detail, our findings support a general role of compact inter-ZF structures in minimizing the formation of off-target DNA complexes.Miz-1 (c-Myc-interacting zinc finger protein-1) is an 88-kDa protein that contains a BTB (Broad complex, Tramtrack, and Bric-a-brac)-POZ (poxvirus and zinc finger) (POZ) 3 domain at its N terminus followed by 13 ZFs. It was first identified as a direct interactor of the oncogenic protein c-Myc by yeast twohybrid screening (1). Miz-1 is an activator of cell cycle regulator genes, such as the cyclin-dependent kinase inhibitors p15CIP1 (p21), and p57 KIP2 (p57) (2-5). Miz-1 activates the transcription of those genes by recruiting different co-activators, such as the histone acetyltransferase p300 and the nucleophosmin (3, 6). Moreover, it was shown that in response to TGF-␤, Miz-1 forms a complex with the Smad 2/3/4 proteins to activate the expression of p15. This interaction was shown to involve a region located within the first four ZFs of Miz-1 and the MH1 domain of Smad 3 (7). Whereas the role of Miz-1 in cell cycle regulation is well established, recent studies have underlined its implication in other cell cycle-independent processes, such as autophagy, endocytosis, vesicular trafficking, inflammation and DNA repair (8 -11). Moreover, some cytoplasmic functions of Miz-1, such as its implication in the regulation of the Wnt pathway, are emerging, revealing the multifunctional nature of this transcription factor (12).c-Myc can directly bind Miz-1 and repress the expression of p15, p21, and p57, ...

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Miz-1 regulates translation of Trp53 via ribosomal protein L22 in cells undergoing V(D)J recombination

Cited by 31 publications

References 49 publications

Rpl22 Loss Selectively Impairs αβ T Cell Development by Dysregulating Endoplasmic Reticulum Stress Signaling

Rpl22 Loss Selectively Impairs αβ T Cell Development by Dysregulating Endoplasmic Reticulum Stress Signaling

Transcription factors and target genes of pre-TCR signaling

Structural Insights into c-Myc-interacting Zinc Finger Protein-1 (Miz-1) Delineate Domains Required for DNA Scanning and Sequence-specific Binding

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