Temat: cancer cells - Katalog OPAC zbiorów

Skocz do pozycji: 1.

Tytuł:: Use of cell therapy as a means of targeting chemotherapy to inoperable pancreatic cancer
Autorzy:: Günzburg, Walter
Salmons, Brian
Powiązania:: https://bibliotekanauki.pl/articles/1041363.pdf
Data publikacji:: 2005
Wydawca:: Polskie Towarzystwo Biochemiczne
Tematy:: cytochrome P450
chemotherapy
genetically modified cells
cell therapy
encapsulated cells
pancreatic cancer
Opis:: Although approved for the treatment of pancreatic cancer, the chemotherapeutic agent ifosfamide is not an effective therapy for this type of tumour. Ifosfamide must be activated by cytochrome P450 (P450) enzymes in the liver, initially to a short lived intermediate and then to toxic metabolites that are subsequently distributed by the circulatory system. Particularly for pancreatic cancer, this liver-mediated conversion results in relatively high systemic toxicities and poor therapeutic concentrations at the liver-distant site of the tumour. Activation of ifosfamide at the site of the tumour may allow lower doses to be used, while increasing the therapeutic index due to the resultant active concentrations generated locally. A cell-based therapy has been conceived where encapsulated, 293-derived cells genetically modified to overexpress a cytochrome P450 enzyme, are implanted near solid tumours. The cells are encapsulated in polymers of cellulose sulphate in order to provide a means of immunoprotection in vivo as well as to physically constrain them to the vicinity of the tumour. A major advantage of this strategy is that it allows one standard cell line to be applied to all patients and this approach can be extended to the treatment of other tumour types. After proof of principle studies in animal models, a phase I/II clinical trial was initiated in patients with stage III/IV nonresectable pancreatic cancer. Encapsulated cells were angiographically placed into the tumour vasculature of 14 patients and followed by systemic low dose ifosfamide treatment. Angiographic delivery of encapsulated cells proved feasible in all but one patient, and was well tolerated with no capsule or ifosfamide treatment-related adverse events. Four of the treated patients showed tumour regressions after capsule delivery and ifosfamide treatment in computer-tomography scans. The other 10 patients showed no further tumour growth (i.e. stable disease) during 20 weeks observation period. The median life expectancy of the patient collective was extended two fold as compared to age and status matched historical controls, with a 3-fold improvement in one year survival being attained. Evidence for a clinical benefit of the treatment was also obtained on the basis of standard parameters for quality of life. This approach has been evaluated by the European Medicines Evaluation Agency (EMEA) and orphan drug status has been granted. A pivotal clinical trial is now being planned with the help of the EMEA. Taken together, the data from this clinical trial suggest that encapsulated cytochrome P450-expressing cells combined with chemotherapy may be useful for the local treatment of a number of solid tumours and support the performance of further clinical studies of this new treatment.
Źródło:: Acta Biochimica Polonica; 2005, 52, 3; 601-607
0001-527X
Pojawia się w:: Acta Biochimica Polonica
Dostawca treści:: Biblioteka Nauki

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Skocz do pozycji: 2.

Tytuł:: Tumors and the danger model.
Autorzy:: Kowalczyk, Dariusz
Powiązania:: https://bibliotekanauki.pl/articles/1043752.pdf
Data publikacji:: 2002
Wydawca:: Polskie Towarzystwo Biochemiczne
Tematy:: cancer
danger signal
dendritic cells
Opis:: This article reviews the evidence for the danger model in the context of immune response to tumors and the insufficiency of the immune system to eliminate tumor growth. Despite their potential immunogenicity tumors do not induce significant immune responses which could destroy malignant cells. According to the danger model, the immune surveillance system fails to detect tumor antigens because transformed cells do not send any danger signals which could activate dendritic cells and initiate an immune response. Instead, tumor cells or antigen presenting cells turn off the responding T cells and induce tolerance. The studies reviewed herein based on model tumor antigens, recombinant viral vectors and detection of tumor specific T cells by MHC/peptide tetramers underscore the critical role of tumor antigen presentation and the context in which it occurs. They indicate that antigen presentation only by activated but not by cancer or resting dendritic cells is necessary for the induction of immune responses to tumor antigens. It becomes apparent that the inability of dendritic cells to become activated provides a biological niche for tumor escape from immune destruction and seems to be a principal mechanism for the failure of tumor immune surveillance.
Źródło:: Acta Biochimica Polonica; 2002, 49, 2; 295-302
0001-527X
Pojawia się w:: Acta Biochimica Polonica
Dostawca treści:: Biblioteka Nauki

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Skocz do pozycji: 3.

Tytuł:: Trastuzumab Efficacy Quantified by Fluorine-19 Magnetic Resonance Imaging
Autorzy:: Bartusik-Aebisher, Dorota
Aebisher, David
Czmil, Mrs Anna
Mazur, Damian
Powiązania:: https://bibliotekanauki.pl/articles/895489.pdf
Data publikacji:: 2020-06-29
Wydawca:: Polskie Towarzystwo Farmaceutyczne
Tematy:: trastuzumab
magnetic resonance imaging
breast cancer cells
three-dimensional cell culture
Trastuzumab conjugates
Opis:: The purpose of this study was to conjugate Trastuzumab with fluorine-bearing PAMAM dendrimer to compare activities in three-dimensional (3D) cultured breast cancer cells with parent Trastuzumab. An in vitro study was performed to determine cellular responses to fluorinated Trastuzumab conjugates by Magnetic Resonance Imaging (MRI). Breast cancer cells were cultured in 3D geometry. Proton (1H) MRI and Fluorine-19 (19F) MRI were used for visualization of cellular locations within a Hollow Fiber Bioreactor (HFBR) device and to monitor the cellular response to treatment. The results of this study confirm that cell growth is significantly decreased following treatment with Trastuzumab conjugates. The use of fluorinated Trastuzumab conjugates decreases breast cancer cell growth in 3D cultures and allows for tracking of drug delivery to cancer cells via 19F.
Źródło:: Acta Poloniae Pharmaceutica - Drug Research; 2020, 77, 3; 495-503
0001-6837
2353-5288
Pojawia się w:: Acta Poloniae Pharmaceutica - Drug Research
Dostawca treści:: Biblioteka Nauki

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Skocz do pozycji: 4.

Tytuł:: The influence of Viburnum opulus polyphenolic compounds on metabolic activity and migration of HeLa and MCF cells
Autorzy:: Zakłos-Szyda, Małgorzata
Pawlik, Nina
Powiązania:: https://bibliotekanauki.pl/articles/105848.pdf
Data publikacji:: 2019
Wydawca:: Centrum Badań i Innowacji Pro-Akademia
Tematy:: Viburnum opulus
polyphenols
cancer cells migration
mitochondrial potential
antioxidant effect
polifenole
migracja komórek rakowych
potencjał mitochondrialny
działanie przeciwutleniające
Opis:: In recent years, research of antitumor activity of natural compounds isolated from plant material has increased. Polyphenols have gained significant attention due to their proapoptotic abilities and their involvement in migration and inhibition of metastasis processes. The anticancer effects of polyphenolic extracts of Viburnum opulus fruit against human breast (MCF-7) and cervical (HeLa) cancer cell lines have been confirmed in this study. It was demonstrated that the tested preparations (methanol – M and acetone – A from pomace, juice – J and juice after extraction to the solid phase SPE – PF) show cytotoxic activity and regulate the migration process of cancer cells. The degree of inhibition of cell migration was measured at two times - 24 h and 48 h after addition of the tested preparations. The highest toxicity towards both cell lines was demonstrated by the polyphenol fraction obtained after juice purification SPE (IC50 values at concentration of 63,541 and 19,380 μg/mL for HeLa and MCF cell lines, respectively). At the same time, the same preparation inhibited cell migration the most (nearly 70% compared to controls at both times at the concertation of 15 and 30 μg/mL). All preparations showed the antioxidant ability, but the Viburnum opulus juice (200 and 350 μg/mL) and the preparation after its purification (15 and 30 μg/mL) have larger ability to inhibit the intracellular oxidative stress (30-40%) than preparation obtained from pomace (nearly by 20% at concentration of 20 and 50 μg/mL of M and A). Despite the antioxidative capacity of the preparations, they simultaneously decreased cellular mitochondrial potential. The results obtained indicate the high potential of components of Viburnum opulus polyphenolic compounds can be used in the production of innovative dietary supplements or pharmacological preparations for people with an increased risk or inclination towards developing breast or cervical cancer.
Źródło:: Acta Innovations; 2019, 31; 33-42
2300-5599
Pojawia się w:: Acta Innovations
Dostawca treści:: Biblioteka Nauki

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Skocz do pozycji: 5.

Tytuł:: The influence of acupuncture TENS currents on the proliferation of cancer cells tested in vitro
Wpływ prądu TENS akupunkturowego na proliferację komórek nowotworowych w badaniach in vitro
Autorzy:: Pełczyńska, Marzena
Milczarek, Magdalena
Maciejewska, Magdalena
Wietrzyk, Joanna
Powiązania:: https://bibliotekanauki.pl/articles/1790857.pdf
Data publikacji:: 2019-12-02
Wydawca:: Akademia Wychowania Fizycznego im. Bronisława Czecha w Krakowie
Tematy:: proliferation of cancer cells
in vitro assay
electrotherapy
physiotherapy
cancer
rehabilitation
proliferacja komórek nowotworowych
badania in vivo
elektroterapia
fizjoterapia
rehabilitacja
Opis:: Introduction: Transcutaneous Electrical Nerve Stimulation (TENS) is a very popular, non-pharmacological antianalgetic method. Nonetheless, knowledge on using this method is very limited in the treatment of patients with cancer anamnesis. Unfortunately, there are not many results of research referring to the application of this method. It is much more difficult to exclude the possibility of proneoplastic activity regarding these methods than to confirm this action. Aim: The aim of the study was to evaluate the influence of TENS currents on the proliferation of cancer cells tested in vitro. Materials and methods: The following human cell lines were used - A549, ES-2, HT29, MCF-7. The cells were plated 24 h before treatment. Then, the cells were exposed to AL-TENS currents (0.1 mA, 1.0 mA and 10 mA), t imp. 200μs; f 2 Hz, constant; duration: 20 min. The in vitro cytotoxic effects were examined after 96 h in SRB assay. In the other experiment, there were three expositions – 24, 48 and 72 hours from the beginning of the experiment. Results: In this assay, the acceleration of cancer cell proliferation after single or triple-dose expositions to AL-TENS currents was not observed. Conclusions: The AL-TENS current after repeated doses did not accelerate proliferation of cancer cells in in vitro conditions.
Wstęp: Przezskórna elektrostymulacja nerwów (TENS) jest szeroko stosowaną niefarmakologiczną metodą leczenia przeciwbólowego. Jednak wiedza na temat wpływu tej metody na proces nowotworowy jest fragmentaryczna. Dlatego też zastosowanie jej w leczeniu pacjentów po przebytej chorobie nowotworowej jest bardzo ograniczone. Niestety, w literaturze nie ma wielu wyników badań odnoszących się bezpośrednio do takich metod. Tym bardziej, że znacznie trudniej jest wykluczyć pronowotworową aktywność tych metod, niż ją potwierdzić. Cel pracy: Celem badań było sprawdzenie hipotezy o pobudzającym wpływie prądu TENS na proliferację komórek nowotworowych w warunkach in vitro. Materiał i metody: Badania przeprowadzono w oparciu o 96 godzinny test SRB proliferacji in vitro dla komórek linii nowotworowych: A549 (rak płuc); ES-2 (rak jajnika); HT29 (rak jelita grubego); MCF-7 (rak piersi). Komórki zostały poddane działaniu prądu TENS akupunkturowego o parametrach: 0,1 mA, 1 mA i 10 mA na dołek, czas impulsu 200μs, symetryczny, częstotliwość 2 Hz, stała, czas ekspozycji 20 min, w pojedynczej dawce po 24 godzinach lub w serii trzech ekspozycji po 24, 48 i 72 godzinach od początku eksperymentu. Wyniki: W wyniku przeprowadzonych badań uzyskano niewielkie zmiany proliferacji w badanych komórkach. Żadna ze zmian nie była statystycznie istotna, w szczególności nie obserwowano istotnego statystycznie przyspieszenia proliferacji. Wnioski: Ani pojedyncza ekspozycja na prąd TENS akupunkturowy, ani seria trzykrotnej ekspozycji nie powoduje istotnego przyspieszenia proliferacji komórek nowotworowych.
Źródło:: Medical Rehabilitation; 2019, 23(4); 42-46
1427-9622
1896-3250
Pojawia się w:: Medical Rehabilitation
Dostawca treści:: Biblioteka Nauki

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Skocz do pozycji: 6.

Tytuł:: The expression of CD44, CD90 and CD133 in response to cisplatin in hepatocellular cancer cells
Autorzy:: Donmez Cakıl, Yaprak
Gunes Ozunal, Zeynep
Gokceoglu Kayalı, Damla
Gulhan Aktas, Ranan
Powiązania:: https://bibliotekanauki.pl/articles/2040155.pdf
Data publikacji:: 2021-03-30
Wydawca:: Uniwersytet Rzeszowski. Wydawnictwo Uniwersytetu Rzeszowskiego
Tematy:: cancer
cisplatin
hepatocellular
stem cells
Opis:: Introduction. Cancer is a leading cause of mortality. Hepatocellular cancer is one of the malignancies associated with poor outcome and resistance to pharmacotherapy. Cancer stem cells (CSCs) contribute to resistance to therapy and hence lead to the treatment failure of tumors. Aim. This study aims to explore the expression of CSCs in response to cisplatin treatment in HepG2 hepatocellular cancer cell line. Material and methods. Cell proliferation test, CCK-8, was used to evaluate the cell proliferation following cisplatin treatment for 72 hours. The expressions of CSC markers CD44, CD90, and CD133 were assessed by flow cytometric analysis. Results. The results showed a dose-dependent decrease in cell proliferation and increased expression of CSC markers CD44 and CD90 in response to cisplatin. Conclusion. Understanding the roles of CSC markers may point to new targets and therapeutic strategies to predict and overcome cisplatin resistance.
Źródło:: European Journal of Clinical and Experimental Medicine; 2021, 1; 18-22
2544-2406
2544-1361
Pojawia się w:: European Journal of Clinical and Experimental Medicine
Dostawca treści:: Biblioteka Nauki

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Skocz do pozycji: 7.

Tytuł:: The effect of Topotecan on oxidative stress in MCF-7 human breast cancer cell line
Autorzy:: Timur, Mujgan
Akbas, S
Ozben, Tomris
Powiązania:: https://bibliotekanauki.pl/articles/1041340.pdf
Data publikacji:: 2005
Wydawca:: Polskie Towarzystwo Biochemiczne
Tematy:: MCF-7 cells
Topotecan
antioxidants
breast cancer
oxidative stress
Opis:: Purpose. Topotecan, a semisynthetic water-soluble derivative of camptothecin exerts its cytotoxic effect by inhibiting topoisomerase I and causes double-strand DNA breaks which inhibit DNA function and ultimately lead to cell death. In previous studies it was shown that camptothecin causes ROS formation. The aim of this study was to investigate if Topotecan like camptotecin causes oxidative stress in MCF-7 human breast cancer cell line. Determining the oxidant effect of Topotecan may elucidate a possible alternative mechanism for its cytotoxicity. Experimental design. MCF-7 cells were cultured and exposed to Topotecan for 24 h at 37°C. The viability of the cells (% of control) was measured using the colorimetric 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyl tetrazolium bromide (MTT) assay. Lipid peroxidation (TBARS), protein oxidation (carbonyl content), sulfhydryl, glutathione (GSH) levels, superoxide dismutase (SOD), catalase (CAT) and glutathione peroxidase (GPx) activities were determined in MCF-7 cells with and without Topotecan incubation. Results. We found the IC50 concentration of Topotecan as 0.218 µM in MCF-7 cells. This concentration of Topotecan was used in the incubations of the cells. Our data indicated increased oxidative status, as revealed by increased lipid peroxidation and protein oxidation, and decreased GSH and sulfhydryl levels in MCF-7 cells exposed to Topotecan compared to control cells. In contrast, there was a slight increase in SOD and a significant increase in GPx and catalase activity in MCF-7 cells incubated with Topotecan compared to the control. Conclusions. These results support our hypothesis that Topotecan increases oxidative stress in MCF-7 cells.
Źródło:: Acta Biochimica Polonica; 2005, 52, 4; 897-902
0001-527X
Pojawia się w:: Acta Biochimica Polonica
Dostawca treści:: Biblioteka Nauki

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Skocz do pozycji: 8.

Tytuł:: Surface-modified SPION systems for cancer therapy
Autorzy:: Karewicz, Anna
Karnas, Karolina
Dulińska-Litewka, Joanna
Kapusta, Czesław
Lekka, Małgorzata
Powiązania:: https://bibliotekanauki.pl/articles/1844916.pdf
Data publikacji:: 2020
Wydawca:: Akademia Górniczo-Hutnicza im. Stanisława Staszica w Krakowie. Polskie Towarzystwo Biominerałów
Tematy:: SPION systems
cancer therapy
tumor cells
system SPION
terapia
komórki rakowe
Źródło:: Engineering of Biomaterials; 2020, 23, 158 spec. iss.; 13
1429-7248
Pojawia się w:: Engineering of Biomaterials
Dostawca treści:: Biblioteka Nauki

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Skocz do pozycji: 9.

Tytuł:: Sulforaphane-mediated induction of a phase 2 detoxifying enzyme NAD(P)H:quinone reductase and apoptosis in human lymphoblastoid cells.
Autorzy:: Misiewicz, Irena
Skupińska, Katarzyna
Kowalska, Elżbieta
Lubiński, Jan
Kasprzycka-Guttman, Teresa
Powiązania:: https://bibliotekanauki.pl/articles/1041549.pdf
Data publikacji:: 2004
Wydawca:: Polskie Towarzystwo Biochemiczne
Tematy:: cancer chemoprevention
sulforaphane
lymphoblastoid cells
Opis:: The effect of sulforaphane on human lymphoblastoid cells originating from a patient of a high cancer risk was studied. Sulforaphane (SFN) is a naturally occurring substance of chemopreventive activity. In our study, changes in cell growth, induction of apoptosis and phase 2 enzymes as well as glutathione level were examined. Apoptosis was tested by confocal microscopy at three stages: change in mitochondrial membrane potential, caspase activation and phosphatidylserine externalization. We show that SFN increases the activity of the detoxification system: it increases quinone reductase activity at low concentration (0.5-1 μM) and raises glutathione level in a dose-dependent manner. At higher doses (2.5-10 μM) sulforaphane is a cell growth modulator, as it caused cell growth cessation (IC50 = 3.875 μM), and apoptosis inducer. The results obtained suggest that sulforaphane acts as a chemopreventive agent in human lymphoblastoid cells.
Źródło:: Acta Biochimica Polonica; 2004, 51, 3; 711-721
0001-527X
Pojawia się w:: Acta Biochimica Polonica
Dostawca treści:: Biblioteka Nauki

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Skocz do pozycji: 10.

Tytuł:: Strategie odżywcze komórek nowotworowych – przegląd wybranych typów nowotworów z uwzględnieniem zmian w poziomie i wzorze ekspresji transporterów glukozy
Nutritional strategies of tumor cells – review of selected cancer types involving changes of expression level and pattern of glucose
Autorzy:: Gajek, K.
Wiatrak, B.
Ślęzak, A.
Ussowicz, M.
Powiązania:: https://bibliotekanauki.pl/articles/261959.pdf
Data publikacji:: 2017
Wydawca:: Politechnika Wrocławska. Wydział Podstawowych Problemów Techniki. Katedra Inżynierii Biomedycznej
Tematy:: GLUT1
SGLT1
hipoksja
komórki nowotworowe
transport glukozy
hypoxia
cancer cells
glucose transport
Opis:: Zaburzona równowaga pomiędzy proliferacją a dojrzewaniem i różnicowaniem komórek nowotworowych powoduje szybki wzrost guza, prowadząc do zwiększenia zapotrzebowania na składniki odżywcze, m.in. glukozę i tlen. Pierwszą odpowiedzią komórek nowotworowych na niewystarczającą ilość składników odżywczych jest zmiana metabolizmu na beztlenowy (efekt Warburga). Glukoza niezbędna do przeprowadzenia tego procesu dostarczana jest za pomocą transporterów – najczęściej białek GLUT1 i SGLT1. Zmiana poziomu i wzoru ekspresji transporterów glukozy w komórkach nowotworowych w porównaniu z komórkami odpowiednich tkanek prawidłowych świadczy o adaptacji, do której doszło w obrębie guza. Dotychczasowe badania pozwoliły ustalić, w których rodzajach nowotworów dochodzi do zmian w ekspresji białek GLUT1 i SGLT1 oraz pokazały, że zmiany te mogą mieć bezpośredni związek z zaawansowaniem choroby i rokowaniem dla pacjentów. Niniejsza praca ma charakter przeglądowy i stanowi zestawienie zmian w poziomie ekspresji transporterów glukozy w niektórych typach nowotworów. Określenie poziomu ekspresji tych białek w komórkach nowotworowych może mieć kluczowe znaczenie dla spersonalizowanej terapii przeciwnowotworowej.
Due to imbalance between proliferation, differentiation and maturation, cancer cells grow rapidly and require elevated levels of oxygen and glucose. The main strategy of cancer cells is to prevent starvation is the anaerobic adaptation of cellular metabolism known as the Warburg’s effect. Increased glucose uptake is maintained by alterating the level and the pattern of glucose transporters expression, mainly GLUT1 and SGLT1. In many cancer types, these proteins are present despite their absence in healthy tissue. Previous researches revealed cancer types in which GLUT1 and SGLT1 expression are altered. There is a strong direct correlation between their expression pattern, cancer stage and prognosis for the patient. This review provides an overview of changes in the level of glucose transporters expression in some cancer types. Determination of glucose transporters expression levels in cancer cells could be crucial for personalized cancer treatment.
Źródło:: Acta Bio-Optica et Informatica Medica. Inżynieria Biomedyczna; 2017, 23, 2; 133-146
1234-5563
Pojawia się w:: Acta Bio-Optica et Informatica Medica. Inżynieria Biomedyczna
Dostawca treści:: Biblioteka Nauki

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Skocz do pozycji: 11.

Tytuł:: Simvastatin modulates β-catenin/MDR1 expression on spheres derived from CF41.Mg canine mammary carcinoma cells
Autorzy:: Cruz, P.
Reyes, F.
Torres, C.G.
Powiązania:: https://bibliotekanauki.pl/articles/2087784.pdf
Data publikacji:: 2018
Wydawca:: Polska Akademia Nauk. Czytelnia Czasopism PAN
Tematy:: β-catenin
MDR1
simvastatin
canine mammary carcinoma cells
cancer stem cells
Źródło:: Polish Journal of Veterinary Sciences; 2018, 21, 1; 95-99
1505-1773
Pojawia się w:: Polish Journal of Veterinary Sciences
Dostawca treści:: Biblioteka Nauki

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Skocz do pozycji: 12.

Tytuł:: Salinomycyna – przełom w leczeniu raka jajnika?
Salinomycin – a breakthrough in the treatment of ovarian cancer?
Autorzy:: Huczyński, Adam
Markowska, Janina
Ramlau, Rodryg
Sajdak, Stefan
Szubert, Sebastian
Stencel, Katarzyna
Powiązania:: https://bibliotekanauki.pl/articles/1030100.pdf
Data publikacji:: 2016
Wydawca:: Medical Communications
Tematy:: cancer stem cells
ovarian cancer
salinomycin
komórki macierzyste raka
rak jajnika
salinomycyna
Opis:: It is believed that cancer stem cells are the primary cause of cancer chemotherapy resistance, metastasis and relapse. The cancer stem cells form a small population of cells present in the tumor (accounting for less than 2% of the tumor mass) and have properties which enable them to survive chemo- and radiotherapy. These cells have the ability to self-renew, do not undergo apoptosis, display overexpression of the ALDH1A1 enzyme and ABC genes which encode transport proteins, and furthermore make use of various signaling pathways (Wnt, Notch, Hedgehog). Cancer stem cells may be identified and isolated from the tumor based on the characteristic biomarkers (CD44+, CD133+, CD117+, BMi1, Oct-4, nestin). It has been demonstrated that salinomycin, an antibiotic obtained from Streptomyces albus, eliminates cancer stem cells, which are resistant to treatment with cytostatics. Salinomycin causes apoptosis of these cells through a number of mechanisms, including the disruption of the Na+/K+ ion balance in biological membranes, inhibition of the Wnt pathway and resistance to transporters, increase in the activity of caspases, activation of the MAPKp38 pathway and inhibition of the nuclear transcription factor NF-κB. Salinomycin has an effect on many types of cancer. It may turn out to be a breakthrough in the therapy of chemotherapy-resistant cancers.
Uważa się, że główną przyczyną chemiooporności, przerzutów i nawrotów raka jajnika są komórki macierzyste raka. Jest to obecna w guzie mała populacja komórek (stanowiąca mniej niż 2% jego masy), których właściwości pozwalają im przetrwać chemio- i radioterapię. Komórki te mają zdolność do samoodnowy, nie podlegają apoptozie, wykazują nadekspresję genów ABC kodujących białka transportowe, enzymu ALDH1A1 i korzystają z różnych szlaków sygnałowania (Wnt, Notch, Hedgehog). Komórki macierzyste raka można zidentyfikować oraz izolować z guza na podstawie charakterystycznych biomarkerów (CD44+, CD133+, CD117+, BMi1, Oct-4, nestyna). Wykazano, że salinomycyna, antybiotyk uzyskany ze Streptomyces albus, eliminuje komórki macierzyste raka, które są oporne na leczenie cytostatykami. Salinomycyna powoduje apoptozę tych komórek poprzez wiele mechanizmów, w tym poprzez zakłócenie jonowego bilansu Na+/K+ w błonach biologicznych, hamowanie szlaku Wnt i oporności na działanie transporterów, wzrost aktywności kaspaz, aktywację szlaku MAPKp38 oraz hamowanie jądrowego czynnika transkrypcyjnego NF-κB. Salinomycyna jest aktywna w wielu rodzajach nowotworów. Może okazać się przełomem w terapii nowotworów chemioopornych.
Źródło:: Current Gynecologic Oncology; 2016, 14, 3; 156-161
2451-0750
Pojawia się w:: Current Gynecologic Oncology
Dostawca treści:: Biblioteka Nauki

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Skocz do pozycji: 13.

Tytuł:: Relationship of c-myc and erbB oncogene family gene aberrations and other selected factors to ex vivo chemosensitivity of ovarian cancer in the modified ATP-chemosensitivity assay.
Autorzy:: Vogt, Ulf
Falkiewicz, Bogdan
Bielawski, Krzysztof
Bosse, Ulrich
Schlotter, Claus
Powiązania:: https://bibliotekanauki.pl/articles/1044426.pdf
Data publikacji:: 2000
Wydawca:: Polskie Towarzystwo Biochemiczne
Tematy:: cultured tumor cells
antitumor drug screening assays
oncogenes
ovarian cancer
antineoplastic agents
Opis:: A pilot study on relationships of selected molecular factors [erbB-1, erbB-2, erbB-3, and c-myc oncogene average gene copy numbers (AGCN); steroid receptors and pS2 gene expression; tumor cells' DNA values] to the ex vivo chemosensitivity of ovarian cancer in a modified adenosine triphosphate cell viability chemosensitivity assay (ATP-CVA), was performed. Despite the relatively small number of patients, numerous correlations among the factors tested were found. Nevertheless, only c-myc gene dosage positively affected ex vivo chemosensitivity of tumors tested.
Źródło:: Acta Biochimica Polonica; 2000, 47, 1; 157-164
0001-527X
Pojawia się w:: Acta Biochimica Polonica
Dostawca treści:: Biblioteka Nauki

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Skocz do pozycji: 14.

Tytuł:: Reactive oxygen species in BCR-ABL1-expressing cells - relevance to chronic myeloid leukemia
Autorzy:: Antoszewska-Smith, Joanna
Pawlowska, Elzbieta
Blasiak, Janusz
Powiązania:: https://bibliotekanauki.pl/articles/1038675.pdf
Data publikacji:: 2017
Wydawca:: Polskie Towarzystwo Biochemiczne
Tematy:: chronic myeloid leukemia
reactive oxygen species
DNA damage
DNA repair
cancer stem cells
imatinib resistance
Opis:: Chronic myeloid leukemia (CML) results from the t(9;22) reciprocal chromosomal translocation producing the BCR-ABL1 gene, conferring growth and proliferation advantages in the CML cells. CML progresses from chronic, often syndrome-free, to blast phase, fatal if not treated. Although the involvement of BCR-ABL1 in some signaling pathways is considered as the cause of CML, the mechanisms resulting in its progression are not completely known. However, BCR-ABL1 stimulates the production of reactive oxygen species (ROS), which levels increase with CML progression and induce BCR-ABL1 self-mutagenesis. Introducing imatinib and other tyrosine kinase inhibitors (TKIs) to CML therapy radically improved its outcome, but TKIs-resistance became an emerging problem. TKI resistance can be associated with even higher ROS production than in TKI-sensitive cells. Therefore, ROS-induced self-mutagenesis of BCR-ABL1 can be crucial for CML progression and TKI resistance and in this way should be taken into account in therapeutic strategies. As a continuous production of ROS by BCR-ABL1 would lead to its self-destruction and death of CML cells, there must be mechanisms controlling this phenomenon. These can be dependent on DNA repair, which is modulated by BCR-ABL1 and can be different in CML stem and progenitor cells. Altogether, the mechanisms of the involvement of BCR-ABL1 in ROS signaling can be engaged in CML progression and TKI-resistance and warrant further study.
Źródło:: Acta Biochimica Polonica; 2017, 64, 1; 1-10
0001-527X
Pojawia się w:: Acta Biochimica Polonica
Dostawca treści:: Biblioteka Nauki

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Skocz do pozycji: 15.

Tytuł:: Numerical experiments with model equations of cancer invasion of tissue
Autorzy:: Kolev, M.
Zubik-Kowal, B.
Powiązania:: https://bibliotekanauki.pl/articles/206179.pdf
Data publikacji:: 2011
Wydawca:: Polska Akademia Nauk. Instytut Badań Systemowych PAN
Tematy:: in vivo tumorigenicity
cancer cells
proliferation
chemotaxis
haptotaxis
extracellular matrix
tumour invasion
mathematical model
animal models
approximations
Opis:: In this paper we investigate a mathematical model of cancer invasion of tissue, which incorporates haptotaxis, chemotaxis, proliferation and degradation rates for cancer cells and the extracellular matrix, kinetics of urokinase receptor, and urokinase plasminogen activator cycle. We solve the model using spectrally accurate approximations and compare its numerical solutions with laboratory data. The spectral accuracy allows to use low-dimensional matrices and vectors, which speeds up the computations of the numerical solutions and thus to estimate the parameter values for the model equations. Our numerical results demonstrate correlations between numerical data computed from the mathematical model and in vivo tumour growth rates from prostate cell lines.
Źródło:: Control and Cybernetics; 2011, 40, 3; 779-791
0324-8569
Pojawia się w:: Control and Cybernetics
Dostawca treści:: Biblioteka Nauki

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