33 research outputs found

    Updates on old and weary haematopoiesis

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    Source at https://doi.org/10.3390/ijms19092567. Blood formation, or haematopoiesis, originates from haematopoietic stem cells (HSCs), whose functions and maintenance are regulated in both cell- and cell non-autonomous ways. The surroundings of HSCs in the bone marrow create a specific niche or microenvironment where HSCs nest that allows them to retain their unique characteristics and respond rapidly to external stimuli. Ageing is accompanied by reduced regenerative capacity of the organism affecting all systems, due to the progressive decline of stem cell functions. This includes blood and HSCs, which contributes to age-related haematological disorders, anaemia, and immunosenescence, among others. Furthermore, chronological ageing is characterised by myeloid and platelet HSC skewing, inflammageing, and expanded clonal haematopoiesis, which may be the result of the accumulation of preleukaemic lesions in HSCs. Intriguingly, haematological malignancies such as acute myeloid leukaemia have a high incidence among elderly patients, yet not all individuals with clonal haematopoiesis develop leukaemias. Here, we discuss recent work on these aspects, the ir potential underlying molecular mechanisms, and the first cues linking age-related changes in the HSC niche to poor HSC maintenance. Future work is needed for a better understanding of haematopoiesis during ageing. This field may open new avenues for HSC rejuvenation and therapeutic strategies in the elderl

    Dysregulation of transcription factor activity during formation of cancer-associated fibroblasts

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    The reciprocal interactions between cancer cells and the quiescent fibroblasts leading to the activation of cancer-associated fibroblasts (CAFs) serve an important role in cancer progression. Here, we investigated the activation of transcription factors (TFs) in prostate fibroblasts (WPMY cell line) co-cultured with normal prostate or tumorous cells (RWPE1 and RWPE2 cell lines, respectively). After indirect co-cultures, we performed mRNA-seq and predicted TF activity using mRNA expression profiles with the Systems EPigenomics Inference of Regulatory Activity (SEPIRA) package and the GTEx and mRNA-seq data of 483 cultured fibroblasts. The initial differential expression analysis between time points and experimental conditions showed that co-culture with normal epithelial cells mainly promotes an inflammatory response in fibroblasts, whereas with the cancerous epithelial, it stimulates transformation by changing the expression of the genes associated with microfilaments. TF activity analysis revealed only one positively regulated TF in the RWPE1 co-culture alone, while we observed dysregulation of 45 TFs (7 decreased activity and 38 increased activity) uniquely in co-culture with RWPE2. Pathway analysis showed that these 45 dysregulated TFs in fibroblasts co-cultured with RWPE2 cells may be associated with the RUNX1 and PTEN pathways. Moreover, we showed that observed dysregulation could be associated with FER1L4 expression. We conclude that phenotypic changes in fibroblast responses to co-culturing with cancer epithelium result from orchestrated dysregulation of signaling pathways that favor their transformation and motility rather than proinflammatory status. This dysregulation can be observed both at the TF and transcriptome levels

    Ścieżka chorego na POChP w Polsce: stan obecny i pożądany kierunek zmian. Perspektywa specjalistów pulmonologów

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    Wstęp: Przewlekła obturacyjna choroba płuc (POChP) to jedna z najczęstszych chorób przewlekłych, która stanowi poważne obciążenie dla pacjentów i jest istotnym problemem społecznym. W Polsce POChP jest niedoceniana, zbyt późno diagnozowana, chorzy na POChP nie są optymalnie leczeni. W celu opisania ścieżki chorego na POChP w Polsce, zdefiniowania problemów pojawiających się na etapie rozpoznawania i leczenia choroby oraz zaproponowania możliwych rozwiązań zorganizowano spotkanie doradcze specjalistów chorób płuc. Materiał i metody: Wirtualne spotkanie doradcze odbyło się w lipcu 2021. Wzięło w nim udział 12 ekspertów w dziedzinie chorób płuc reprezentujących ośrodki z całego kraju i posiadających doświadczenie w opiece nad chorymi na POChP. Na podstawie wypowiedzi ekspertów przygotowano raport końcowy przedstawiony w tej publikacji. Zawiera on opinie pogrupowane jako: zidentyfikowane nieprawidłowości i propozycje rozwiązań. Wyniki: Podczas spotkania doradczego omówiono aktualną sytuację związaną z rozpoznawaniem i leczeniem POChP. Główne problemy to: późne rozpoznanie choroby (niewiedza pacjentów, późne kierowanie przez lekarzy POZ), ograniczona dostępność badania spirometrycznego i specjalistów, brak właściwego przepływu informacji między lekarzem POZ a pulmonologiem, brak informacji o przebytych zaostrzeniach, brak aktualnych polskich standardów leczenia POChP. Podsumowanie: W dyskusji zaproponowano szereg rozwiązań (w tym tzw. systemowych), które w opinii ekspertów mogłyby poprawić obecną sytuację: zwiększenie wiedzy społeczeństwa o POChP, poprawa i standaryzacja komunikacji lekarz POZ-pulmonolog oraz edukacja kadr medycznych (wszystkich szczebli opieki nad chorymi) na temat profilaktyki i terapii POChP

    Effects triggered by platinum nanoparticles on primary keratinocytes

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    The platinum (Pt)-group elements (PGEs) represent a new kind of environmental pollutant and a new hazard for human health. Since their introduction as vehicle-exhaust catalysts, their emissions into the environment have grown considerably compared with their low natural concentration in the earth crust. PGE emissions from vehicle catalysts can be also in the form of nanometer-sized particles (Pt nanoparticles [PtNPs]). These elements, both in their metallic form or as ions solubilized in biological media, are now recognized as potent allergens and sensitizers. Human skin is always exposed to toxic particles; therefore, in the present study we addressed the question of whether polyvinylpyrrolidone-coated PtNPs may have any negative effects on skin cells, including predominantly epidermal keratinocytes. In this study, PtNPs of two sizes were used: 5.8 nm and 57 nm, in concentrations of 6.25, 12.5, and 25 μg/mL. Both types of NPs were protected with polyvinylpyrrolidone. Primary keratinocytes were treated for 24 and 48 hours, then cytotoxicity, genotoxicity, morphology, metabolic activity, and changes in the activation of signaling pathways were investigated in PtNP-treated cells. We found that PtNPs trigger toxic effects on primary keratinocytes, decreasing cell metabolism, but these changes have no effects on cell viability or migration. Moreover, smaller NPs exhibited more deleterious effect on DNA stability than the big ones. Analyzing activation of caspases, we found changes in activity of caspase 9 and caspase 3/7 triggered mainly by smaller NPs. Changes were not so significant in the case of larger nanoparticles. Importantly, we found that PtNPs have antibacterial properties, as is the case with silver NPs (AgNPs). In comparison to our previous study regarding the effects of AgNPs on cell biology, we found that PtNPs do not exhibit such deleterious effects on primary keratinocytes as AgNPs and that they also can be used as potential antibacterial agents, especially in the treatment of Escherichia coli, representing a group of Gram-negative species

    Endogenous IL-1 receptor antagonist restricts healthy and malignant myeloproliferation.

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    Here we explored the role of interleukin-1β (IL-1β) repressor cytokine, IL-1 receptor antagonist (IL-1rn), in both healthy and abnormal hematopoiesis. Low IL-1RN is frequent in acute myeloid leukemia (AML) patients and represents a prognostic marker of reduced survival. Treatments with IL-1RN and the IL-1β monoclonal antibody canakinumab reduce the expansion of leukemic cells, including CD34+ progenitors, in AML xenografts. In vivo deletion of IL-1rn induces hematopoietic stem cell (HSC) differentiation into the myeloid lineage and hampers B cell development via transcriptional activation of myeloid differentiation pathways dependent on NFκB. Low IL-1rn is present in an experimental model of pre-leukemic myelopoiesis, and IL-1rn deletion promotes myeloproliferation, which relies on the bone marrow hematopoietic and stromal compartments. Conversely, IL-1rn protects against pre-leukemic myelopoiesis. Our data reveal that HSC differentiation is controlled by balanced IL-1β/IL-1rn levels under steady-state, and that loss of repression of IL-1β signaling may underlie pre-leukemic lesion and AML progression.We thank K. Tasken, J. Saarela and the NCMM at the University of Oslo (UiO), S. Kanse (UiO) and B. Smedsrød (UiT), for access to facilities. We acknowledge Center for Medical Genetics and Molecular Medicine, Haukeland University Hospital (Bergen, Norway) and R. Hovland for karyotyping, FISH, translocation and DNA analyses of AML and MDS patients included in this study, and Department of Pathology, Oslo University Hospital (Oslo, Norway) and S. Spetalen for deep sequencing. L.M. Gonzalez, L.T. Eliassen, X. Zhang, M. Ristic and other members of L. Arranz group, O.P. Rekvig, R. Doohan, L.D. Håland, M.I. Olsen, A. Urbanucci, J. Landskron, K.B. Larsen, R.A. Lyså and UiT Advanced Microscopy Core Facility, UiO and UiT Comparative Medicine Units, for assistance. P. Garcia and S. Mendez-Ferrer for providing NRASG12D and Nes-gfp mice, respectively. P. Garcia and L. Kurian for careful reading of the manuscript. E. Tenstad (Science Shaped) for artwork in schematics. We would also like to thank the AML and MDS patients, and healthy volunteers, who donated biological samples. Our work is supported by a joint meeting grant of the Northern Norway Regional Health Authority, the University Hospital of Northern Norway (UNN) and UiT (Strategisk-HN06-14), Young Research Talent grants from the Research Council of Norway, (Stem Cell Program, 247596; FRIPRO Program, 250901), and grants from the Norwegian Cancer Society (6765150), the Northern Norway Regional Health Authority (HNF1338-17), and the Aakre-Stiftelsen Foundation (2016/9050) to L.A. Vav-Cre NRASG12D experiments were supported by NIH grant R01CA152108 to J.Z.S

    Endogenous IL-1 receptor antagonist restricts healthy and malignant myeloproliferation

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    Here we explored the role of interleukin-1β (IL-1β) repressor cytokine, IL-1 receptor antagonist (IL-1rn), in both healthy and abnormal hematopoiesis. Low IL-1RN is frequent in acute myeloid leukemia (AML) patients and represents a prognostic marker of reduced survival. Treatments with IL-1RN and the IL-1β monoclonal antibody canakinumab reduce the expansion of leukemic cells, including CD34+ progenitors, in AML xenografts. In vivo deletion of IL-1rn induces hematopoietic stem cell (HSC) differentiation into the myeloid lineage and hampers B cell development via transcriptional activation of myeloid differentiation pathways dependent on NFκB. Low IL-1rn is present in an experimental model of pre-leukemic myelopoiesis, and IL-1rn deletion promotes myeloproliferation, which relies on the bone marrow hematopoietic and stromal compartments. Conversely, IL-1rn protects against pre-leukemic myelopoiesis. Our data reveal that HSC differentiation is controlled by balanced IL-1β/IL-1rn levels under steady-state, and that loss of repression of IL-1β signaling may underlie pre-leukemic lesion and AML progression

    Państwo, gospodarka, społeczeństwo w integrującej się Europie TOM 1

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    Ze wstępu: "III Międzynarodowa Konferencja Naukowa, jaką w pierwszych dniach czerwca 2003 roku zorganizowała Krakowska Szkoła Wyższa, poświęcona była uczczeniu wyjątkowego jubileuszu 500-lecia urodzin jej patrona - Andrzeja Frycza Modrzewskiego. Jednak to nie myśl polityczna tego wielkiego Polaka i reformatora stała się wiodącym tematem konferencji. W centrum zainteresowań znalazły się zagadnienia 0 wiele bardziej aktualne, dotyczące bowiem integracji europejskiej. Problematyka tym bardziej żywotna, gdyż dotykająca bieżącego życia politycznego - zwłaszcza w kontekście referendum akcesyjnego, które odbyło się w równy tydzień po konferencji. Tak więc jej uczestnicy mieli doskonałą okazję do podjęcia interesujących rozważań związanych z perspektywą rozwoju państwa, gospodarki i społeczeństwa w warunkach integracji europejskiej."(...
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