Your search keyword '"Alicja Dziadosz"' showing total 7 results

1. Identification of novel interferon responsive protein partners of human leukocyte antigen A (HLA-A) using cross-linking mass spectrometry (CLMS) approach

Author

Ashita Singh, Monikaben Padariya, Jakub Faktor, Sachin Kote, Sara Mikac, Alicja Dziadosz, Tak W. Lam, Jack Brydon, Martin A. Wear, Kathryn L. Ball, Ted Hupp, Alicja Sznarkowska, Borek Vojtesek, and Umesh Kalathiya

Subjects

Medicine, Science

Abstract

Abstract The interferon signalling system elicits a robust cytokine response against a wide range of environmental pathogenic and internal pathological signals, leading to induction of a subset of interferon-induced proteins. We applied DSS (disuccinimidyl suberate) mediated cross-linking mass spectrometry (CLMS) to capture novel protein–protein interactions within the realm of interferon induced proteins. In addition to the expected interferon-induced proteins, we identified novel inter- and intra-molecular cross-linked adducts for the canonical interferon induced proteins, such as MX1, USP18, OAS3, and STAT1. We focused on orthogonal validation of a cohort of novel interferon-induced protein networks formed by the HLA-A protein (H2BFS-HLA-A-HMGA1) using co-immunoprecipitation assay, and further investigated them by molecular dynamics simulation. Conformational dynamics of the simulated protein complexes revealed several interaction sites that mirrored the interactions identified in the CLMS findings. Together, we showcase a proof-of-principle CLMS study to identify novel interferon-induced signaling complexes and anticipate broader use of CLMS to identify novel protein interaction dynamics within the tumour microenvironment.

Published

2022

2. Recapitulating Solid Stress on Tumor on a Chip for Nanomedicine Diffusive Transport Prediction

Author

Alberto Martín-Asensio, Sergio Dávila, Jean Cacheux, Agnieszka Lindstaedt, Alicja Dziadosz, Darius Witt, Macarena Calero, Igor Balaz, and Isabel Rodríguez

Subjects

microfluidics, nanomedicine, organ-on-a-chip, solid tumors, tumor-on-a-chip, Biotechnology, TP248.13-248.65, Medical technology, R855-855.5

Abstract

The characteristic mechanical forces at play within tumors include the abnormal solid and fluid stresses. These, together with the increased extracellular matrix (ECM) stiffness, are the major transport barriers affecting the nanomedicine delivery to solid tumors. Due to the elevated pressure within the tumor microenvironment, the transport of nanomedicines through the interstitial space is limited to diffusion. While this particular scenario is central for nanomedicine delivery to solid tumors, it has not been modeled in vitro before. To this end, herein, a tumor‐on‐a‐chip microfluidic device is developed that is capable of recapitulating the solid stress scenario in tumors. This is achieved by integrating a pneumatic actuation to apply compression to the enclosed hydrogel ECM filling medium. Transport studies of model nanoparticles (NPs) across this medium are performed to determine their diffusion. For these NPs, it is demonstrated that their transport is drastically reduced by 65% due to the compression of the ECM gel matrix, reducing its pore size, with only an applied pressure of ≈4 Pa. The results obtained show that the actuated tumor‐on‐a‐chip device can be used to evaluate the diffusive penetration capability of nanomedicines within a mechanical‐constrained microenvironment such that of tumors.

Published

2023

3. Identification of a Stable, Non-Canonically Regulated Nrf2 Form in Lung Cancer Cells

Author

Sara Mikac, Michał Rychłowski, Alicja Dziadosz, Alicja Szabelska-Beresewicz, Robin Fahraeus, Theodore Hupp, and Alicja Sznarkowska

Subjects

Nrf2 detection, Nrf2 antibodies, Nrf2 migration in SDS-PAGE, Therapeutics. Pharmacology, RM1-950

Abstract

Nrf2 (nuclear factor erythroid 2 (NF-E2)-related factor 2) transcription factor is recognized for its pro-survival and cell protective role upon exposure to oxidative, chemical, or metabolic stresses. Nrf2 controls a number of cellular processes such as proliferation, differentiation, apoptosis, autophagy, lipid synthesis, and metabolism and glucose metabolism and is a target of activation in chronic diseases like diabetes, neurodegenerative, and inflammatory diseases. The dark side of Nrf2 is revealed when its regulation is imbalanced (e.g., via oncogene activation or mutations) and under such conditions constitutively active Nrf2 promotes cancerogenesis, metastasis, and radio- and chemoresistance. When there is no stress, Nrf2 is instantly degraded via Keap1-Cullin 3 (Cul3) pathway but despite this, cells exhibit a basal activation of Nrf2 target genes. It is yet not clear how Nrf2 maintains the expression of its targets under homeostatic conditions. Here, we found a stable 105 kDa Nrf2 form that is resistant to Keap1-Cul3-mediated degradation and translocates to the nucleus of lung cancer cells. RNA-Seq analysis indicate that it might originate from the exon 2 or exon 3-truncated transcripts. This stable 105 kDa Nrf2 form might help explain the constitutive activity of Nrf2 under normal cellular conditions.

Published

2021

4. Major Histocompatibility Complex class I heavy chains localize in both cytoplasmic and nuclear compartment

Author

Maria Gómez-Herranz, Alicja Dziadosz, Sara Mikac, Michał Rychłowski, Robin Fahraeus, Natalia Marek-Trzonkowska, Elżbieta Chruściel, Zuzanna Urban-Wójciuk, Ines Papak, Łukasz Arcimowicz, Tomasz Marjanski, Witold Rzyman, and Alicja Sznarkowska

Abstract

The Major Histocompatibility Complex class I (MHC-I) molecules present antigenic peptides (AP) to CD8+T cells for self versus non-self recognition. Loading of AP on MHC-I takes place in the endoplasmic reticulum (ER), upon shuttling of cytoplasmic AP substrates to the ER. Understanding of this process has been influenced by the view that MHC-I antigens are produced from the proteasomal degradation of cellular proteins. Recent observations on the intronic and untranslated region-derived peptides as well as on the non-AUG translation products presented on the MHC-I open the possibility that antigenic peptides can derive from pre-spliced mRNAs translated in the nuclear compartment. In this brief report, we show that a fraction of human MHC-I molecules (human leukocyte antigens type A, HLA-A) is present in the nuclei of cells, in the proximity of histone H2B. With this finding, we hope to initiate a new direction of research on the nuclear role of MHC-I and ask whether the loading of antigens can take place in the nuclear compartment.

Published

2022

5. Identification of the N-terminally truncated Nrf2 isoform with different regulation and indications of novel functions of Nrf2

Author

Sara Mikac, Alicja Dziadosz, Monikaben Padariya, Umesh Kalathiya, Robin Fahraeus, Natalia Marek-Trzonkowska, Elżbieta Chruściel, Zuzanna Urban-Wójciuk, Ines Papak, Łukasz Arcimowicz, Tomasz Marjanski, Witold Rzyman, and Alicja Sznarkowska

Subjects

Physiology (medical), Biochemistry

Published

2023

6. Keap1-resistant ΔN-Nrf2 isoform does not translocate to the nucleus upon electrophilic stress

Author

Sara Mikac, Alicja Dziadosz, Monikaben Padariya, Umesh Kalathiya, Robin Fahraeus, Natalia Marek-Trzonkowska, Elzbieta Chrusciel, Zuzanna Urban-Wojciuk, Ines Papak, Lukasz Arcimowicz, Tomasz Marjanski, Witold Rzyman, and Alicja Sznarkowska

Abstract

The Nrf2 pathway is an essential defense pathway in a cell. It responds to oxidative and electrophilic stress via derepression of Nrf2 from Keap1-Cul3-mediated degradation, accumulation of Nrf2 in the nucleus and transcriptional activation of a number of detoxifying and cell protective Nrf2 target genes. Here we report that normal and cancer cells also express the N-terminally truncated Nrf2 isoform (ΔN-Nrf2), which originates from an alternative promoter. Co-immunoprecipitation together with molecular dynamics simulation showed that the binding between ΔN-Nrf2 and Keap1 is impaired, resulting in the much higher stability of this form. ΔN-Nrf2 is retained in the cytoplasm in response to electrophilic stress, indicating that it does not regulate transcription under the same stress stimuli as the full-length Nrf2. Altogether this data suggests that Nrf2 has other functions in cells than transcriptional activation of genes, which most probably rely on the protein-protein interactions in the cytoplasm. The regulation between these functions takes place on the level of transcription.Significance StatementThis work signifies the importance of alternative transcription in assigning the function to the produced protein. Nrf2 transcripts produced from the second promoter of the Nrf2 gene give rise to the N-terminally truncated Nrf2 form (ΔN-Nrf2), which is retained in the cytoplasm upon stress, thus it has a different role in cells than transcriptional regulation. ΔN-Nrf2 is resistant to the Keap1-Cul3 degradation pathway and is highly expressed in all tested cell types. This work points to the new, cytoplasmic role of Nrf2 in cells, determined at the level of transcription.

Published

2022

7. Identification of a Stable, Non-Canonically Regulated Nrf2 Form in Lung Cancer Cells

Author

Ted R. Hupp, Alicja Sznarkowska, Alicja Szabelska-Beresewicz, Robin Fåhraeus, Sara Mikac, Michał Rychłowski, and Alicja Dziadosz

Subjects

0301 basic medicine, Nrf2 migration in SDS-PAGE, Physiology, Clinical Biochemistry, Cell, RM1-950, Biochemistry, digestive system, environment and public health, Article, 03 medical and health sciences, Exon, 0302 clinical medicine, medicine, Nrf2 detection, Molecular Biology, Transcription factor, Gene, Cancer och onkologi, Chemistry, Autophagy, Lipid metabolism, Cell Biology, Nrf2 antibodies, respiratory system, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Apoptosis, 030220 oncology & carcinogenesis, Cancer and Oncology, Therapeutics. Pharmacology, Homeostasis

Abstract

Nrf2 (nuclear factor erythroid 2 (NF-E2)-related factor 2) transcription factor is recognized for its pro-survival and cell protective role upon exposure to oxidative, chemical, or metabolic stresses. Nrf2 controls a number of cellular processes such as proliferation, differentiation, apoptosis, autophagy, lipid synthesis, and metabolism and glucose metabolism and is a target of activation in chronic diseases like diabetes, neurodegenerative, and inflammatory diseases. The dark side of Nrf2 is revealed when its regulation is imbalanced (e.g., via oncogene activation or mutations) and under such conditions constitutively active Nrf2 promotes cancerogenesis, metastasis, and radio- and chemoresistance. When there is no stress, Nrf2 is instantly degraded via Keap1-Cullin 3 (Cul3) pathway but despite this, cells exhibit a basal activation of Nrf2 target genes. It is yet not clear how Nrf2 maintains the expression of its targets under homeostatic conditions. Here, we found a stable 105 kDa Nrf2 form that is resistant to Keap1-Cul3-mediated degradation and translocates to the nucleus of lung cancer cells. RNA-Seq analysis indicate that it might originate from the exon 2 or exon 3-truncated transcripts. This stable 105 kDa Nrf2 form might help explain the constitutive activity of Nrf2 under normal cellular conditions.

Published

2021