A peroxiredoxin-based proteinaceous scaffold for the growth and differentiation of neuronal cells and tumour stem cells in the absence of prodifferentiation agents

Cimini, Annamaria; Ardini, Matteo; Gentile, Roberta; Giansanti, Francesco; Benedetti, Elisabetta; Cristiano, Loredana; Fidoamore, Alessia; Scotti, S.; Panella, Gloria; Angelucci, Francesco; Ippoliti, Rodolfo

doi:10.1002/term.2144

Cited by 4 publications

(8 citation statements)

References 41 publications

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“…The involvement of PRDXs in the initiation and progression of human cancer was reported in many studies [13,15,61] and some of them were reported to be differentially expressed in colorectal cancers. However, in most of the studies, the PRDXs were studied separately and only the mRNA level or protein level were investigated.…”

Section: Discussionmentioning

confidence: 98%

Peroxiredoxins and Immune Infiltrations in Colon Adenocarcinoma: Their Negative Correlations and Clinical Significances, an In Silico Analysis

Zhang

Gao

et al. 2020

J. Cancer

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Background: Peroxiredoxins (PRDXs) were reported to be associated with inflammation response in previous studies. In colon adenocarcinoma (COAD), however, their correlations and clinical significance were unclear. Methods: The RNA-seq data of 452 COAD patients with clinical information was downloaded from The Cancer Genome Atlas (TCGA) and transcripts per million (TPM) normalized. Comparisons of relative expressions of PRDXs between COAD tumor and normal controls were applied. PRDXs dy-regulations in COAD were validated via Oncomine, Human Protein Atlas (HPA) and Gene Expression Omnibus (GEO) repository. Through Tumor Immune Estimation Resource (TIMER), the immune estimation of TCGA-COAD patients was downloaded and the dy-regulated PRDXs were analyzed for their correlations with immune infiltrations in COAD. The TCGA-COAD patients were divided into younger group (age≤65 years) and older group (age>65 years) to investigate the prognostic roles of age, TNM stage, dy-regulated PRDXs and the immune infiltrations in different age groups through Kaplan-Meier survival and Cox regression analyses. Results: Three of the PRDX members showed their expressional differences both at protein and mRNA level. PRDX2 was consistently up-regulated while PRDX6 down-regulated in COAD. PRDX1 was overexpressed (mRNA) while nuclear absent (protein) in the tumor tissues. PRDX1 overexpression and PRDX6 under-expression were also shown in the stem-like colonospheres from colon cancer cells. Via TIMER, PRDX1, PRDX2, and PRDX6 were found to be negatively correlated with the immune infiltrations in COAD. Both in the younger and older patients, TNM stage had prognostic effects on their overall survival (OS) and recurrence-free survival (RFS). CD4 + T cell had independent unfavorable effects on OS of the younger patients while age had similar effects on RFS of the older ones. CD8 + T cell was independently prognostic for RFS in the two groups. Conclusions: Late diagnosis indicated poor prognosis in COAD and dy-regulated PRDXs w might be new markers for its early diagnosis. Age was prognostic and should be considered in the treatments of the older patients. Dy-regulated PRDXs were negatively correlated with immune infiltration levels. CD4 + T cell and CD8 + T cell infiltrations were prognostic in COAD and their potential as immune targets needed further investigation.

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Section: Discussionmentioning

confidence: 98%

Peroxiredoxins and Immune Infiltrations in Colon Adenocarcinoma: Their Negative Correlations and Clinical Significances, an In Silico Analysis

Zhang

Gao

et al. 2020

J. Cancer

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“…The neural-like phenotype and the cell networks are especially highlighted by electron micrographs with the formation of long sprouting neurites on both Cys48Ser (II) and Cys47Ser tube substrates (III). Adapted with permission from ref ( 95 ). Copyright 2016 John Wiley & Sons, Ltd.…”

Section: Peroxiredoxin-based Bionanotechnologymentioning

confidence: 99%

“… 92 Finally, bare tubes of stacked Prx rings have been demonstrated to be efficient biological scaffolds for adhesion and differentiation of stem and tumor-derived cells with no need of differentiating supplements. 95 The use of Prx for bionanotechnology purposes is just initiated and more efforts should be made in the future to completely master its morpheein behavior in order to easily access all the oligomeric structures available for Prx. For example, the interfaces involved in the Prx’s nanocage structure are not determined at the atomic level, even though some indications on how to stabilize this array already exist; the employment of this supramolecular oligomer for practical purposes is, at present, limited, but still very promising if one considers the many applications of ferritin-like or virus-like nanocages in biomedicine and nanotechnology reported so far.…”

Section: Conclusion and Future Perspectivesmentioning

confidence: 99%

“…Namely, human neuroblastoma SH-SY5Y can be seeded and differentiated into neuronal-like phenotypes sprouting neurites and forming a cell network without the addition of N2, as shown by phase contrast microscopy (PCM) and confirmed by expression of neural markers β-tubulin III and NF-200. The differentiation is observed on both Prx-based substrates while being almost absent when seeding the cells over the wild-type proteins forming single rings (Figure b) . To note, very similar effects are observed if using neural cancer stem cells (NCSCs) from human glioblastoma which are prone to adhesion of the neurospheres before spreading and differentiation on both the Prx tubes .…”

Section: Peroxiredoxin-based Bionanotechnologymentioning

confidence: 99%

“…The “sticky” features of the Prx rings have been shown to be useful for assembling metal NP-doped 3D GO materials , and improving the stiffness and biological effects of rGO to induce growth and differentiation of tumor-derived cells as well as to obtain 2D plasmonic nanopores over graphene-coated solid-state membranes . Finally, bare tubes of stacked Prx rings have been demonstrated to be efficient biological scaffolds for adhesion and differentiation of stem and tumor-derived cells with no need of differentiating supplements . The use of Prx for bionanotechnology purposes is just initiated and more efforts should be made in the future to completely master its morpheein behavior in order to easily access all the oligomeric structures available for Prx.…”

Section: Conclusion and Future Perspectivesmentioning

confidence: 99%

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Taking Advantage of the Morpheein Behavior of Peroxiredoxin in Bionanotechnology

et al. 2021

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Morpheeins are proteins that reversibly assemble into different oligomers, whose architectures are governed by conformational changes of the subunits. This property could be utilized in bionanotechnology where the building of nanometric and new high-ordered structures is required. By capitalizing on the adaptability of morpheeins to create patterned structures and exploiting their inborn affinity toward inorganic and living matter, “bottom-up” creation of nanostructures could be achieved using a single protein building block, which may be useful as such or as scaffolds for more complex materials. Peroxiredoxins represent the paradigm of a morpheein that can be applied to bionanotechnology. This review describes the structural and functional transitions that peroxiredoxins undergo to form high-order oligomers, e.g., rings, tubes, particles, and catenanes, and reports on the chemical and genetic engineering approaches to employ them in the generation of responsive nanostructures and nanodevices. The usefulness of the morpheeins’ behavior is emphasized, supporting their use in future applications.

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YAP/TAZ mechano-transduction As the Underlying Mechanism of Neuronal Differentiation Induced By Reduced Graphene Oxide

Catanesi

Panella

Benedetti

et al. 2018

Nanomedicine (Lond.)

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Aim: The aim of this work is the dissection of the molecular pathways underlying the differentiation effect of reduced graphene oxide (GO) materials in the absence of differentiation agents. Materials & methods: Reduced GO is obtained either by drop casting method and heat-treated or biological reduction by the interaction between GO and wtPrxI. Cells were grown on both materials and the differentiation process studied by immunological and morphological detection. Results & conclusion: The results obtained indicate that both reduction methods of GO can determine the modulation of pathway involved in mechano-transduction and differentiation, by affecting YAP/TAZ localization outside the nuclei and increasing neuronal differentiation markers. This suggests that the mechano-transduction pathways are responsible for the differentiation process.

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A peroxiredoxin-based proteinaceous scaffold for the growth and differentiation of neuronal cells and tumour stem cells in the absence of prodifferentiation agents

Cited by 4 publications

References 41 publications

Peroxiredoxins and Immune Infiltrations in Colon Adenocarcinoma: Their Negative Correlations and Clinical Significances, an In Silico Analysis

Peroxiredoxins and Immune Infiltrations in Colon Adenocarcinoma: Their Negative Correlations and Clinical Significances, an In Silico Analysis

Taking Advantage of the Morpheein Behavior of Peroxiredoxin in Bionanotechnology

YAP/TAZ mechano-transduction As the Underlying Mechanism of Neuronal Differentiation Induced By Reduced Graphene Oxide

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