keyword
https://read.qxmd.com/read/21317924/onconase-mediated-nfk%C3%AE-downregulation-in-malignant-pleural-mesothelioma
#21
JOURNAL ARTICLE
C M Goparaju, J D Blasberg, S Volinia, J Palatini, S Ivanov, J S Donington, C Croce, M Carbone, H Yang, H I Pass
Treatment of malignant pleural mesothelioma (MPM) with Ranpirnase (Onconase) results in disruption of protein translation and cell apoptosis. We hypothesize that Onconase exerts an effect via downregulation of nuclear factor kappa B (NFKβ) by specific microRNAs (miRNAs) and that interference of this pathway could have implications for MPM resistance to chemotherapy. Three immortalized MPM cell lines (H2959, H2373 and H2591) were exposed to Onconase at 0-20 μg/ml. Cell counts were measured at 48 and 72 h...
June 16, 2011: Oncogene
https://read.qxmd.com/read/20663928/ranpirnase-frog-rnase-targeted-with-a-humanized-internalizing-anti-trop-2-antibody-has-potent-cytotoxicity-against-diverse-epithelial-cancer-cells
#22
JOURNAL ARTICLE
Chien-Hsing Chang, Pankaj Gupta, Rosana Michel, Meiyu Loo, Yang Wang, Thomas M Cardillo, David M Goldenberg
Ranpirnase (Rap), an amphibian RNase, has been extensively studied both preclinically and clinically as an antitumor agent. Rap can be administered repeatedly to patients without any untoward immune response, with reversible renal toxicity reported to be dose limiting. To enhance its potency and targeted tumor therapy, we describe the generation of a novel IgG-based immunotoxin, designated 2L-Rap(Q)-hRS7, comprising Rap(Q), a mutant Rap with the putative N-glycosylation site removed, and hRS7, an internalizing, humanized antibody against Trop-2, a cell surface glycoprotein overexpressed in variety of epithelial cancers...
August 2010: Molecular Cancer Therapeutics
https://read.qxmd.com/read/20173221/-onconase-a-ribonuclease-with-antitumor-activity
#23
REVIEW
Małgorzata Zwolińska, Piotr Smolewski
Onconase (ranpirnase) is a homologous protein obtained from Rana pipiens frog eggs. The activity of onconase, and particularly its antitumor effect, is strictly connected with ribonuclease(RN-ase) activity. Onconase induces cell death through the decomposition of inner cellular RNA,inhibition of protein synthesis, and inhibition of cell growth and proliferation and it also specifically triggers tumor cell apoptosis. A very important mechanisms of its cytotoxicity is also its antioxidant activity. The results of preclinical trials demonstrated a high activity of onconase against tumor cells, also those resistant to cytostatics...
February 19, 2010: Postȩpy Higieny i Medycyny Doświadczalnej
https://read.qxmd.com/read/19707441/ranpirnase-and-its-potential-for-the-treatment-of-unresectable-malignant-mesothelioma
#24
JOURNAL ARTICLE
Camillo Porta, Chiara Paglino, Luciano Mutti
Ribonucleases are a superfamily of enzymes which operate at the crossroads of transcription and translation, catalyzing the degradation of RNA; they can be cytotoxic because the cleavage of RNA renders indecipherable its information. Ranpirnase is a novel ribonuclease which preferentially degrades tRNA, thus leading to inhibition of protein synthesis and, ultimately, to cytostasis and cytotoxicity. Ranpirnase has demonstrated antitumor activity both in vitro and in vivo in several tumor models. The maximum tolerated dose emerging from phase I studies was 960 g/m(2), with renal toxicity as the main dose-limiting toxicity...
December 2008: Biologics: Targets & Therapy
https://read.qxmd.com/read/19025416/design-and-characterization-of-an-hiv-specific-ribonuclease-zymogen
#25
JOURNAL ARTICLE
Rebecca F Turcotte, Ronald T Raines
Ribonucleases are evoking medical interest because of their intrinsic cytotoxic activity. Most notably, ranpirnase, which is an amphibian ribonuclease, is in advanced clinical trials as a chemotherapeutic agent for the treatment of cancer. Here, we describe a strategy to create a novel antiviral agent based on bovine pancreatic ribonuclease (RNase A), a mammalian homologue of ranpirnase. Specifically, we have linked the N- and C-termini of RNase A with an amino acid sequence that is recognized and cleaved by human immunodeficiency virus (HIV) protease...
November 2008: AIDS Research and Human Retroviruses
https://read.qxmd.com/read/18673289/antibody-targeted-rnase-fusion-proteins-immunornases-for-cancer-therapy
#26
REVIEW
Jürgen Krauss, Michaela A E Arndt, Stefan Dübel, Susanna M Rybak
Ribonucleases (RNases) of the superfamily A exhibit potent antineoplastic activity yet do not mediate appreciable immunogenicity or non-specific toxicity in both animal models and cancer patients. Ranpirnase (Onconase), the first ribonuclease being evaluated as a therapeutic in humans, has progressed to phase III clinical trials in patients with unresectable mesothelioma. Conjugation of RNases to internalizing tumor-targeting monoclonal antibodies was shown to enhance specific cell killing by several orders of magnitude both in vitro and in animal models...
June 2008: Current Pharmaceutical Biotechnology
https://read.qxmd.com/read/18606715/a-novel-combination-ranpirnase-and-rosiglitazone-induce-a-synergistic-apoptotic-effect-by-down-regulating-fra-1-and-survivin-in-cancer-cells
#27
JOURNAL ARTICLE
Maria E Ramos-Nino, Benjamin Littenberg
Accumulating evidence supports the idea that two known phosphatidylinositol 3'-kinase (PI3K) downstream proteins, Fra-1 and Survivin, are potential targets for cancer therapy. Increased expression of Fra-1, a Fos family member of the transcription factor activator protein-1, has been implicated in both the maintenance and the progression of the transformed state of several cancer cells. In addition, high Survivin expression in tumors correlates with more aggressive behavior, lower response to chemotherapeutic drugs, and shortened survival time...
July 2008: Molecular Cancer Therapeutics
https://read.qxmd.com/read/18518759/ranpirnase-as-a-potential-antitumor-ribonuclease-treatment-for-mesothelioma-and-other-malignancies
#28
REVIEW
Amanda K Beck, Harvey I Pass, Michele Carbone, Haining Yang
Ranpirnase, originally isolated from oocytes of the northern leopard frog (Rana pipiens), is a member of the pancreatic RNase A superfamily of ribonucleases. Ranpirnase exerts antiproliferative and cytotoxic effects in vitro and in vivo and has been shown to act synergistically with different cancer therapeutic agents. The cytotoxic and cytostatic effects of ranpirnase are the consequence of tRNA degradation that results in the disruption of protein translation and the induction of programmed cell death (apoptosis)...
June 2008: Future Oncology
https://read.qxmd.com/read/18476793/ranpirnase-onconase-a-cytotoxic-amphibian-ribonuclease-manipulates-tumour-physiological-parameters-as-a-selective-killer-and-a-potential-enhancer-for-chemotherapy-and-radiation-in-cancer-therapy
#29
REVIEW
Intae Lee
BACKGROUND: Ranpirnase, a cytotoxic amphibian ribonuclease, is effective against cancer cells, inducing apoptosis independently of p53 protein. Onconase (the smallest member of the RNase A superfamily) has moved into clinical testing in the US and Europe. OBJECTIVE: The main focuses of this review are to examine the manipulation of tumour physiological parameters by ranpirnase and discuss its molecular, pharmacological and physiological roles in preclinical and clinical trials in terms of benefits and toxicity...
June 2008: Expert Opinion on Biological Therapy
https://read.qxmd.com/read/18215091/ribonucleases-as-novel-chemotherapeutics-the-ranpirnase-example
#30
REVIEW
J Eugene Lee, Ronald T Raines
Ranpirnase, a cytotoxic ribonuclease from the frog Rana pipiens, is the archetype of a novel class of cancer chemotherapeutic agents based on homologs and variants of bovine pancreatic ribonuclease (RNase A). Ranpirnase in combination with doxorubicin is in clinical trials for the treatment of unresectable malignant mesothelioma and other cancers. The putative mechanism for ranpirnase-mediated cytotoxicity involves binding to anionic components of the extracellular membrane, cytosolic internalization, and degradation of transfer RNA leading to apoptosis...
2008: BioDrugs: Clinical Immunotherapeutics, Biopharmaceuticals and Gene Therapy
https://read.qxmd.com/read/18064463/mechanisms-of-enhanced-tumoricidal-efficacy-of-multiple-small-dosages-of-ranpirnase-the-novel-cytotoxic-ribonuclease-on-lung-cancer
#31
JOURNAL ARTICLE
Intae Lee, Kuslima Shogen
PURPOSE: The effect of multiple small dosages of the cytotoxic RNase, ranpirnase (ONCONASE, ONC), on lung cancer was studied. The possible mechanisms for the enhanced tumoricidal efficacy of multiple small dosages of ONC were also investigated. METHODS: Hematoxylin and eosin staining, TUNEL labeling, and caspase-3-antibody labeling were used for in vivo analysis of apoptosis. A growth-delay assay was applied to detect the therapeutic potential of small and multiple dosages of ONC in vivo...
July 2008: Cancer Chemotherapy and Pharmacology
https://read.qxmd.com/read/18019404/the-therapeutic-mechanisms-of-ranpirnase-induced-enhancement-of-radiation-response-on-a549-human-lung-cancer
#32
JOURNAL ARTICLE
Intae Lee, Dae H Kim, Ulas Sunar, Sergey Magnitsky, Kuslima Shogen
AIM: The goal of this study was to investigate the therapeutic potential of combining radiation therapy and cytotoxic RNase, ranpirnase (ONCONASE; ONC), in human lung tumor models in vitro and in vivo. As translational implications, the non-invasive monitoring response to individual therapy with ONC was also investigated to determine the underlying therapeutic mechanisms. MATERIALS AND METHODS: A clonogenic survival assay was used to measure the effect of ONC and radiation on A549 human non-small cell lung carcinoma (NSCLC) cells...
September 2007: In Vivo
https://read.qxmd.com/read/17352247/antitumor-efficacy-of-the-cytotoxic-rnase-ranpirnase-on-a549-human-lung-cancer-xenografts-of-nude-mice
#33
JOURNAL ARTICLE
Intae Lee, Anna Kalota, Alan M Gewirtz, Kuslima Shogen
BACKGROUND: The cytotoxic RNase, ranpirnase (ONCONASE, ONC), may have promising therapeutic implication as an alternative for cisplatin for the treatment of lung cancer, due to inhibition of protein synthesis by t-RNA cleavage. MATERIALS AND METHODS: A549 and NCI-H1975 human NSCLC cell lines were cultured in the presence and absence of ONC. Cytotoxicity was monitored using a clonogenic assay. Using an inverted phase and fluorescence microscope, we studied whether apoptosis was induced by ONC in gefitinib-induced apoptosis-resistant A549 tumor cells...
January 2007: Anticancer Research
https://read.qxmd.com/read/17332922/mild-hyperthermia-predisposes-tumor-cells-to-undergo-apoptosis-upon-treatment-with-onconase
#34
JOURNAL ARTICLE
H Dorota Halicka, Barbara Ardelt, Kuslima Shogen, Zbigniew Darzynkiewicz
Onconase (ONC), (ranpirnase) a cytotoxic ribonuclease isolated from amphibian oocytes and early embryos targeting tumor cells in vitro and in vivo, is currently in a confirmatory Phase IIIb clinical trial for unresectable malignant mesothelioma where it demonstrates antitumor activity with relatively minor overall toxicity to patients. Since hyperthermia has been shown to be synergistic with certain antitumor modalities, the aim of the present study was to explore whether the cytotoxic effects of ONC can be enhanced under conditions of mild hyperthermia...
April 2007: International Journal of Oncology
https://read.qxmd.com/read/17324010/ranpirnase-amphibian-ribonuclease-a-p-30-protein-alfacell
#35
REVIEW
(no author information available yet)
Ranpirnase [Onconase] is an amphibian oocyte/early embryo ribonuclease (RNase) of 105 amino acids in length that is capable of controlling tumour growth by degrading RNA within cancer cells, resulting in inhibition of protein synthesis and arresting mitosis in G(1 )phase. It represents the first successful isolation, purification and characterisation of the oocytic/early embryonic factor that is capable of controlling cell growth activities of the early embryonic tissues. Alfacell Corporation is currently conducting clinical trials of ranpirnase in patients with unresectable malignant mesothelioma and non-small-cell lung cancer...
2007: Drugs in R&D
https://read.qxmd.com/read/16548765/ranpirnase-an-antitumour-ribonuclease-its-potential-role-in-malignant-mesothelioma
#36
REVIEW
Nick Pavlakis, Nicholas J Vogelzang
Ranpirnase (Onconase) is a novel cytotoxic ribonuclease. In clinical development as a single agent in patients with malignant mesothelioma (MM), at 480 microg/m2 intravenously weekly, analysis of survival indicated prolonged periods of stable disease in Phase II trials and a potential survival benefit, compared with doxorubicin, in a small unpublished Phase III trial. In all clinical studies it has generally demonstrated a favourable safety profile except for easily controlled allergic reactions and dose modifications for renal impairment...
April 2006: Expert Opinion on Biological Therapy
https://read.qxmd.com/read/16305992/ribonucleases-as-a-novel-pro-apoptotic-anticancer-strategy-review-of-the-preclinical-and-clinical-data-for-ranpirnase
#37
REVIEW
John Costanzi, David Sidransky, Ami Navon, Howard Goldsweig
Cytotoxic ribonucleases (RNases), such as ranpiranase, represent a novel mechanism-based approach to anticancer therapy. These relatively small proteins selectively attack malignant cells, triggering apoptotic response and inhibiting protein synthesis. Ranpirnase, originally isolated from oocytes of Rana pipiens, is a member of a family of endoribonucleases. The anticancer effects of ranpiranase have been documented in both in vitro and in vivo experimental tumor models. The effects of ranpiranase appear to be selective for cancer cells...
2005: Cancer Investigation
https://read.qxmd.com/read/16109781/effective-therapy-of-human-lymphoma-xenografts-with-a-novel-recombinant-ribonuclease-anti-cd74-humanized-igg4-antibody-immunotoxin
#38
JOURNAL ARTICLE
Chien-Hsing Chang, Puja Sapra, Sailaja S Vanama, Hans J Hansen, Ivan D Horak, David M Goldenberg
Ranpirnase (Rap) is a cytotoxic ribonuclease (RNase) isolated from frog oocytes. Here we describe high antitumor activity of a novel immunotoxin, 2L-Rap-hLL1-gamma4P, composed of 2 Rap molecules, each fused to the N terminus of the light chain of hLL1, an internalizing anti-CD74 humanized antibody. To reduce unwanted side effects, the constant region of hLL1 was changed from gamma1 to gamma4 and further to gamma4P by replacing serine228 to proline to prevent the formation of a half immunoglobulin G (IgG) common for IgG4...
December 15, 2005: Blood
https://read.qxmd.com/read/15950791/overview-on-ongoing-or-planned-clinical-trials-in-europe
#39
REVIEW
Adolfo Favaretto
Malignant pleural mesothelioma (MPM) is a locally invasive malignancy, but only a minority of patients can benefit by surgical resection. Among chemotherapeutic agents only vinorelbine, edatrexate, gemcitabine and raltitrexed have demonstrated response rates >20%. The largest randomised trial in MPM showed an improved median survival with cisplatin and pemetrexed versus cisplatin alone from 9.3 to 12.1 months. For the present overview about 70 requests of information were sent to the major European centres of thoracic oncology...
July 2005: Lung Cancer: Journal of the International Association for the Study of Lung Cancer
https://read.qxmd.com/read/15547713/treatment-of-jurkat-acute-t-lymphocytic-leukemia-cells-by-onconase-ranpirnase-is-accompanied-by-an-altered-nucleocytoplasmic-distribution-and-reduced-expression-of-transcription-factor-nf-kappab
#40
JOURNAL ARTICLE
Shwu Y Tsai, Barbara Ardelt, Tze-Chen Hsieh, Zbigniew Darzynkiewicz, Kuslima Shogen, Joseph M Wu
Onconase (Ranpirnase), a novel ribonuclease isolated from Rana pipiens oocytes, was reported to suppress cancer cell growth in vitro, reduce tumor size in animals, and augment cytotoxicity of several chemotherapeutic agents. Since onconase is currently in phase III clinical trials tested in treatment of mesothelioma, much emphasis has been placed on the mechanism of its anti-tumor activity. Previous studies have shown that onconase-responsive cells become arrested at the G1/S checkpoint of the cell cycle and also undergo apoptosis...
December 2004: International Journal of Oncology
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