Results for 'anti‐cancer drugs'

977 found
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  1.  23
    Jordan Goodman;, Vivien Walsh. The Story of Taxol: Nature and Politics in the Pursuit of an Anti‐Cancer Drug. xiii + 292 pp., illus., bibl., index. Cambridge: Cambridge University Press, 2001. $27.95. [REVIEW]Linda F. Hogle - 2002 - Isis 93 (4):762-763.
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  2.  15
    Jordan Goodman and Vivien Walsh, the story of taxol: Nature and politics in the pursuit of an anti-cancer drug. Cambridge: Cambridge university press, 2001. Pp. XIII+282. £18.95, $27.95. [REVIEW]Carsten Timmermann - 2003 - British Journal for the History of Science 36 (1):87-127.
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  3.  21
    Are tumor cells protected from some anti‐cancer drugs by elevated APC/C activity? (Comment on DOI: 10.1002/bies.201100094). [REVIEW]Duncan J. Clarke - 2011 - Bioessays 33 (12):898-898.
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  4.  23
    Modular transporters for subcellular cell‐specific targeting of anti‐tumor drugs.Alexander S. Sobolev - 2008 - Bioessays 30 (3):278-287.
    A major problem in the treatment of cancer is the specific targeting of anti‐tumor drugs to these abnormal cells. Ideally, such a drug should act over short distances to minimize damage to healthy cells, and target subcellular compartments that have the highest sensitivity to the drug. Photosensitizers, alpha‐emitting radionuclides and many other medicines could be considered as such drugs if they possessed cellular and subcellular specificity. The author describes a novel approach of using modular recombinant transporters to target (...)
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  5.  31
    Informing materials: drugs as tools for exploring cancer mechanisms and pathways.Etienne Vignola-Gagné, Peter Keating & Alberto Cambrosio - 2017 - History and Philosophy of the Life Sciences 39 (2):10.
    This paper builds on previous work that investigated anticancer drugs as ‘informed materials’, i.e., substances that undergo an informational enrichment that situates them in a dense relational web of qualifications and measurements generated by clinical experiments and clinical trials. The paper analyzes the recent transformation of anticancer drugs from ‘informed’ to ‘informing material’. Briefly put: in the post-genomic era, anti-cancer drugs have become instruments for the production of new biological, pathological, and therapeutic insights into the underlying etiology (...)
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  6. Resveratrol and rapamycin: are they anti‐aging drugs?Matt Kaeberlein - 2010 - Bioessays 32 (2):96-99.
  7.  30
    Chromatin Stability as a Target for Cancer Treatment.Katerina V. Gurova - 2019 - Bioessays 41 (1):1800141.
    In this essay, I propose that DNA‐binding anti‐cancer drugs work more via chromatin disruption than DNA damage. Success of long‐awaited drugs targeting cancer‐specific drivers is limited by the heterogeneity of tumors. Therefore, chemotherapy acting via universal targets (e.g., DNA) is still the mainstream treatment for cancer. Nevertheless, the problem with targeting DNA is insufficient efficacy due to high toxicity. I propose that this problem stems from the presumption that DNA damage is critical for the anti‐cancer activity (...)
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  8.  28
    FabAct®: a decision‐making tool for the anticipation of the preparation of anticancer drugs.Brigitte Bonan, Nicolas Martelli, Malik Berhoune, Ludovic-Alexandre Vidal, Evren Sahin & Patrice Prognon - 2010 - Journal of Evaluation in Clinical Practice 16 (6):1129-1135.
  9.  21
    Stress‐induced cellular adaptive strategies: Ancient evolutionarily conserved programs as new anticancer therapeutic targets.Arcadi Cipponi & David M. Thomas - 2014 - Bioessays 36 (6):552-560.
    Despite the remarkable achievements of novel targeted anti‐cancer drugs, most therapies only produce remission for a limited time, resistance to treatment, and relapse, often being the ultimate outcome. Drug resistance is due to highly efficient adaptive strategies utilized by cancer cells. Exogenous and endogenous stress stimuli are known to induce first‐line responses, capable of re‐establishing cellular homeostasis and determining cell fate decisions. Cancer cells may also mount second‐line adaptive strategies, such as the mutator response. Hypermutable subpopulations of cells (...)
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  10.  22
    Inflammation, reproduction, cancer and all that…. The regulation and role of the inducible prostaglandin synthase.Harvey R. Herschman, Weilin Xie & Srinivasa Reddy - 1995 - Bioessays 17 (12):1031-1037.
    Discovery of a second, inducible prostaglandin synthase provides explanations for many previously puzzling observations, but also raises new questions about prostanoid synthesis. A cis‐acting sequence closely related to the cyclic AMP response element has been shown to play a role in both basal and induced prostaglandin synthase 2 gene expression. Aspirin and other currently available non‐steroidal anti‐inflammatory drugs that inhibit prostaglandin synthase activity do not effectively discriminate between the inducible prostaglandin synthase 2 and constitutive prostaglandin synthase 1 enzymes. Identification (...)
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  11. Property, Rights, and the constitution of contemporary Indian Biomedicine: Notes from the gleevec case.Kaushik Sunder Rajan - 2011 - Social Research: An International Quarterly 78 (3):975-998.
    Drawing upon an exemplary case surrounding a patent on the anti-cancer drug Gleevec, I trace how intellectual property regimes drive the re-institutionalization of pharmaceutical development in India today in unsettled and contested ways. I am interested in how this case resolves, in an apparent purification, into technical and constitutional components; how the technical components are entirely unsettled; and how the constitutional components open up questions regarding the relationship between biocapital and issues of constitutionalism, rights, and corporate social responsibility.
     
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  12.  13
    Zebrafish: A new model on the pharmaceutical catwalk.Ulrike Langheinrich - 2003 - Bioessays 25 (9):904-912.
    Zebrafish is recognized as one of the most important vertebrate model organisms; however, its value in pharmacological studies has not been extensively explored and exploited. In this review, I summarize significant findings about the effects of drugs and medicines on important physiological processes in zebrafish. Our experiments have shown that cardiovascular, anti‐angiogenic and anti‐cancer drugs elicit comparable responses in zebrafish embryos to those in mammalian systems. Similar observations have been reported by other laboratories, exposing zebrafish to a (...)
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  13.  13
    DNA topoisomerase dysfunction: A new goal for antitumor chemotherapy.Paul J. Smith - 1990 - Bioessays 12 (4):167-172.
    Topoisomerase enzymes – found in prokaryotes to human cells – control conformational changes in DNA and aid the orderly progression of DNA replication, gene transcription and the separation of daughter chromosomes at cell division. Several classes of anti‐cancer drugs are now recognised as topoisomerase poisons because of their ability to trap topoisomerase molecules on DNA as ‘cleavable complexes’. Understanding how drugs generate such complexes and why they are toxic to actively growing cancer cells is a major challenge (...)
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  14.  35
    The Ras‐ERK pathway: Understanding site‐specific signaling provides hope of new anti‐tumor therapies.Fernando Calvo, Lorena Agudo-Ibáñez & Piero Crespo - 2010 - Bioessays 32 (5):412-421.
    Recent discoveries have suggested the concept that intracellular signals are the sum of multiple, site‐specified subsignals, rather than single, homogeneous entities. In the context of cancer, searching for compounds that selectively block subsignals essential for tumor progression, but not those regulating “house‐keeping” functions, could help in producing drugs with reduced side effects compared to compounds that block signaling completely. The Ras‐ERK pathway has become a paradigm of how space can differentially shape signaling. Today, we know that Ras proteins are (...)
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  15.  10
    Playing only one instrument may be not enough: Limitations and future of the antiangiogenic treatment of cancer.Ana R. Quesada, Miguel Ángel Medina & Emilio Alba - 2007 - Bioessays 29 (11):1159-1168.
    Angiogenesis plays an essential role in tumor growth, invasion and metastasis. After initial pessimism about the usefulness of the antiangiogenic therapeutic approach for cancer, interest has increased in the development of antiangiogenic compounds after the first clinical approval of an antiangiogenic therapy. The anti‐vascular endothelial growth factor (VEGF) antibody bevacizumab has recently been approved for use in combination with chemotherapy for the treatment of metastatic colorectal and non‐small cell lung cancer patients. However, no survival benefit has been demonstrated in anti‐VEGF (...)
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  16.  6
    DNA topoisomerases: Advances in understanding of cellular roles and multi‐protein complexes via structure‐function analysis.Shannon J. McKie, Keir C. Neuman & Anthony Maxwell - 2021 - Bioessays 43 (4):2000286.
    DNA topoisomerases, capable of manipulating DNA topology, are ubiquitous and indispensable for cellular survival due to the numerous roles they play during DNA metabolism. As we review here, current structural approaches have revealed unprecedented insights into the complex DNA‐topoisomerase interaction and strand passage mechanism, helping to advance our understanding of their activities in vivo. This has been complemented by single‐molecule techniques, which have facilitated the detailed dissection of the various topoisomerase reactions. Recent work has also revealed the importance of topoisomerase (...)
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  17.  14
    Are anti‐cancer patents intrinsically immoral?Dave Speijer - 2024 - Bioessays 46 (6):2400081.
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  18.  29
    Expanding roles for AMP‐activated protein kinase in neuronal survival and autophagy.Jeroen Poels, Miloš R. Spasić, Patrick Callaerts & Koenraad K. Norga - 2009 - Bioessays 31 (9):944-952.
    AMP‐activated protein kinase (AMPK) is an evolutionarily conserved cellular switch that activates catabolic pathways and turns off anabolic processes. In this way, AMPK activation can restore the perturbation of cellular energy levels. In physiological situations, AMPK senses energy deficiency (in the form of an increased AMP/ATP ratio), but it is also activated by metabolic insults, such as glucose or oxygen deprivation. Metformin, one of the most widely prescribed anti‐diabetic drugs, exerts its actions by AMPK activation. However, while the functions (...)
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  19.  18
    RGS proteins as targets in the treatment of intestinal inflammation and visceral pain: New insights and future perspectives.Maciej Salaga, Martin Storr, Kirill A. Martemyanov & Jakub Fichna - 2016 - Bioessays 38 (4).
    Regulators of G protein signaling (RGS) proteins provide timely termination of G protein‐coupled receptor (GPCR) responses. Serving as a central control point in GPCR signaling cascades, RGS proteins are promising targets for drug development. In this review, we discuss the involvement of RGS proteins in the pathophysiology of the gastrointestinal inflammation and their potential to become a target for anti‐inflammatory drugs. Specifically, we evaluate the emerging evidence for modulation of selected receptor families: opioid, cannabinoid and serotonin by RGS proteins. (...)
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  20.  56
    Anti‐cancer selection as a source of developmental and evolutionary constraints.Frietson Galis & Johan A. J. Metz - 2003 - Bioessays 25 (11):1035-1039.
    Recently at least two papers1,2have appeared that look at cancer from an evolutionary perspective. That cancer has a negative effect on fitness needs no argument. However, cancer origination is not an isolated process, but the potential for it is linked in diverse ways to other genetically determined developmental events, complicating the way selection acts on it, and through it on the evolution of development. The two papers take a totally different line. Kavanagh argues that anti‐cancer selection has led to (...)
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  21.  27
    Moral ambivalence towards the Cancer Drugs Fund.Ilias Ektor Epanomeritakis - 2019 - Journal of Medical Ethics 45 (9):623-626.
    The UK’s Cancer Drugs Fund was introduced in 2010 following the Conservative Party’s promise to address the fact that numerous efficacious cancer drugs were not available because of their cost ineffectiveness, as deduced by the National Institute of Health and Care Excellence. While, at face value, this policy appears only to promote the UK’s public welfare, a deeper analysis reveals the ethically unjustifiable inconsistencies that the CDF introduces; where is the analogous fund for other equally severe diseases? Have (...)
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  22.  7
    Physicians’ Perspectives on Ethical Issues Regarding Expensive Anti-Cancer Treatments: A Qualitative Study.Charlotte H. C. Bomhof, Maartje Schermer, Stefan Sleijfer & Eline M. Bunnik - 2022 - AJOB Empirical Bioethics 13 (4):275-286.
    Background When anti-cancer treatments have been given market authorization, but are not (yet) reimbursed within a healthcare system, physicians are confronted with ethical dilemmas. Arranging access through other channels, e.g., hospital budgets or out-of-pocket payments by patients, may benefit patients, but leads to unequal access. Until now, little is known about the perspectives of physicians on access to non-reimbursed treatments. This interview study maps the experiences and moral views of Dutch oncologists and hematologists.Methods A diverse sample of oncologists and hematologists (...)
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  23.  19
    Use of bacteria in anti‐cancer therapies.Rachel M. Ryan, Jeffrey Green & Claire E. Lewis - 2006 - Bioessays 28 (1):84-94.
    While a number of valid molecular targets have been discovered for tumours over the past decade, finding an effective way of delivering therapeutic genes specifically to tumours has proved more problematic. A variety of viral and non‐viral delivery vehicles have been developed and applied in anti‐cancer gene therapies. However, these suffer from either inefficient and/or short‐lived gene transfer to target cells, instability in the bloodstream and inadequate tumour targeting. Recently, various types of non‐pathogenic obligate anaerobic and facultative anaerobic bacteria (...)
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  24.  39
    The two faces of FBW7 in cancer drug resistance.Zhiwei Wang, Hidefumi Fukushima, Daming Gao, Hiroyuki Inuzuka, Lixin Wan, Alan W. Lau, Pengda Liu & Wenyi Wei - 2011 - Bioessays 33 (11):851-859.
    Chemotherapy is an important therapeutic approach for cancer treatment. However, drug resistance is an obstacle that often impairs the successful use of chemotherapies. Therefore, overcoming drug resistance would lead to better therapeutic outcomes for cancer patients. Recently, studies by our own and other groups have demonstrated that there is an intimate correlation between the loss of the F‐box and WD repeat domain‐containing 7 (FBW7) tumor suppressor and the incurring drug resistance. While loss of FBW7 sensitizes cancer cells to certain (...), FBW7‐/‐ cells are more resistant to other types of chemotherapies. FBW7 exerts its tumor suppressor function by promoting the degradation of various oncoproteins that regulate many cellular processes, including cell cycle progression, cellular metabolism, differentiation, and apoptosis. Since loss of the FBW7 tumor suppressor is linked to drug resistance, FBW7 may represent a novel therapeutic target to increase drug sensitivity of cancer cells to conventional chemotherapeutics. This paper thus focuses on the new functional aspects of FBW7 in drug resistance. (shrink)
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  25.  13
    Off-label use of bevacizumab in the treatment of retinal disease: ethical implications.Landon James Rohowetz - 2019 - Journal of Medical Ethics 45 (10):668-672.
    Anti-vascular endothelial growth factor therapy has revolutionised the treatment of a variety of ophthalmic conditions and has become the first-line therapy for a range of retinal diseases. Bevacizumab, a VEGF inhibitor first approved for the treatment of colorectal cancer, has been shown to be nearly or virtually as effective and safe as other anti-VEGF therapies in the treatment of certain retinal diseases but is not approved or registered by the Food and Drug Administration or European Medicines Agency. While other anti-VEGF (...)
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  26.  3
    Affordable Access to Cancer Drugs and Other Lifesaving Medicines in the United States.Evaristus Chiedu Obi - 2018 - Ethics in Biology, Engineering and Medicine 9 (1):99-115.
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  27.  13
    Reframing cancer: challenging the discourse on cancer and cancer drugs—a Norwegian perspective: Reframing Cancer.Roger Strand, Caroline Engen & Mille Sofie Stenmarck - 2021 - BMC Medical Ethics 22 (1):1-10.
    BackgroundAs the range of therapeutic options in the field of oncology increases, so too does the strain on health care budgets. The imbalance between what is medically possible and financially feasible is frequently rendered as an issue of tragic choices, giving rise to public controversies around health care rationing.Main bodyWe analyse the Norwegian media discourse on expensive cancer drugs and identify four underlying premises: (1) Cancer drugs are de facto expensive, and one does not and should not question (...)
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  28.  24
    Is there a morally right price for anti-retroviral drugs in the developing world?Ross Brennan & Paul Baines - 2005 - Business Ethics: A European Review 15 (1):29-43.
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  29. Nonsteroidal anti-inflammatory drugs: adverse effects on the central nervous system.Adam F. Cohen - 1969 - In P. Vinken & G. Bruyn (eds.), Handbook of Clinical Neurology. North Holland. pp. 2--415.
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  30.  11
    Inhibition of tumor angiogenesis as a strategy to circumvent acquired resistance to anti‐cancer therapeutic agents.Robert S. Kerbel - 1991 - Bioessays 13 (1):31-36.
    Cancers have a formidable capacity to develop resistance to a large and diverse array of chemical, biologic, and physical anti‐neoplastic agents. This can be largely traced to the instability of the tumor cell genome, and the resultant ability of tumor cell populations to generate phenotypic variants rapidly. It is therefore argued that anti‐cancer strategies should be directed at eliminating those genetically stable normal diploid cells that are required for the progressive growth of tumors. Micro‐vascular endothelial cells comprising the tumor (...)
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  31.  8
    DNA topoisomerase II mutations and resistance to anti‐tumor drugs.Yegor S. Vassetzky, Gian-Carlo Alghisi & Susan M. Gasser - 1995 - Bioessays 17 (9):767-774.
    Mutations in DNA topoisomerase II are often correlated with drug‐resistance in tumor cell lines. Studies of topoisomerase II‐mediated drug‐resistance in various model systems, as well as the sequencing of such mutations from drug‐resistant tumors, have shed light on the functional domains of topoisomerase II, on how it interacts with inhibitors, and on the different mechanisms by which cells avoid the toxic effects of many clinically important anti‐tumor drugs.
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  32.  22
    BET‐ting on Nrf2: How Nrf2 Signaling can Influence the Therapeutic Activities of BET Protein Inhibitors.Nirmalya Chatterjee & Dirk Bohmann - 2018 - Bioessays 40 (5):1800007.
    BET proteins such as Brd3 and Brd4 are chromatin‐associated factors, which control gene expression programs that promote inflammation and cancer. The Nrf2 transcription factor is a master regulator of genes that protect the organism against xenobiotic attack and oxidative stress. Nrf2 has demonstrated anti‐inflammatory activity and can support cancer cell malignancy. This review describes the discovery, mechanism and biomedical implications of the regulatory interplay between Nrf2 and BET proteins. Both Nrf2 and BET proteins are established drug targets. Small molecules that (...)
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  33.  3
    Unintended Consequences of Coverage Laws Targeting Cancer Drugs.Maximilian Salcher-Konrad & Huseyin Naci - 2020 - Journal of Law, Medicine and Ethics 48 (3):552-554.
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  34.  17
    Ras regulatory interactions: Novel targets for anti‐cancer intervention?George C. Prendergast & Jackson B. Gibbs - 1994 - Bioessays 16 (3):187-191.
    Advances in the understanding of Ras oncoprotein function suggest novel points for anti‐tumor intervention. First, upstream‐acting guanine nucleotide exchange factors and SH2/SH3 domain‐containing adaptor proteins that link Ras with growth factor receptor tyrosine kinases have recently been characterized. Second, work on downstream‐acting Ras effector functions including the Ras GTPase‐activating protein (p120GAP) and the Raf kinase has revealed direct biochemical interactions that are functionally required for oncogenic Ras signalling. We summarize progress in these areas and discuss the potential for novel applications (...)
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  35.  36
    Cardiovascular disease and non‐steroidal anti‐inflammatory drug prescribing in the midst of evolving guidelines.Timothy T. Pham, Michael J. Miller, Donald L. Harrison, Ann E. Lloyd, Kimberly M. Crosby & Jeremy L. Johnson - 2013 - Journal of Evaluation in Clinical Practice 19 (6):1026-1034.
  36.  31
    Individual patient data meta‐analysis of randomized anti‐epileptic drug monotherapy trials.Paula R. Williamson, Anthony G. Marson, Catrin Tudur, Jane L. Hutton & David Chadwick - 2000 - Journal of Evaluation in Clinical Practice 6 (2):205-214.
  37.  25
    The application of pharmacoeconomic modelling to estimate a value‐based price for new cancer drugs.George Dranitsaris, Ilse Truter, Martie S. Lubbe, Wayne Cottrell, Biljana Spirovski & Jonathan Edwards - 2012 - Journal of Evaluation in Clinical Practice 18 (2):343-351.
  38.  40
    Evaluation of chloroquine as a potent anti‐malarial drug: issues of public health policy and healthcare delivery in post‐war Liberia.Moses B. F. Massaquoi & Stephen B. Kennedy - 2003 - Journal of Evaluation in Clinical Practice 9 (1):83-87.
    Chloroquine-resistant plasmodium falciparum malaria is a serious public health threat that is spreading rapidly across Sub-Saharan Africa. It affects over three quarters (80%) of malarial endemic countries. Of the estimated 300-500 million cases of malaria reported annually, the vast majority of malarial-related morbidities occur among young children in Africa, especially those concentrated in the remote rural areas with inadequate access to appropriate health care services. In Liberia, in vivo studies conducted between 1993 and 2000 observed varying degrees of plasmodium falciparum (...)
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  39.  42
    Is there a morally right price for anti-retroviral drugs in the developing world?Ross Brennan & Paul Baines - 2005 - Business Ethics, the Environment and Responsibility 15 (1):29–43.
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  40.  14
    Why the Outcome of Anti‐Tumor Immune Responses is Heterogeneous: A Novel Idea in the Context of Immunological Heterogeneity in Cancers.Jing H. Wang - 2020 - Bioessays 42 (10):2000024.
    The question as to why some hosts can eradicate their tumors while others succumb to tumor‐progression remains unanswered. Here, a provocative concept is proposed that intrinsic differences in the T cell receptor (TCR) repertoire of individuals may influence the outcome of anti‐tumor immunity by affecting the frequency and/or variety of tumor‐reactive CD8 and/or CD4 tumor‐infiltrating lymphocytes. This idea implicates that the TCR repertoire in a given patient might not provide sufficiently different TCR clones that can recognize tumor antigens, namely, “a (...)
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  41.  9
    Case Studies in Bioethics: Regulating an Anti-Aging Drug.Sidney Callahan & James F. Childress - 1978 - Hastings Center Report 8 (3):19.
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  42.  67
    “Do We Really Need Hepatitis B on the Second Day of Life?” Vaccination Mandates and Shifting Representations of Hepatitis B.Elena Conis - 2011 - Journal of Medical Humanities 32 (2):155-166.
    In the decade following hepatitis B vaccine’s 1981 approval, U.S. health officials issued evolving guidelines on who should receive the vaccine: first, gay men, injection drug users, and healthcare workers; later, hepatitis B-positive women’s children; and later still, all newborns. States laws that mandated the vaccine for all children were quietly accepted in the 1990s; in the 2000s, however, popular anti-vaccine sentiment targeted the shot as an emblem of immunization policy excesses. Shifting attitudes toward the vaccine in this period were (...)
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  43.  36
    Corpus Interruptus: Biotech Drugs, Insurance Providers and the Treatment of Breast Cancer.Jane E. Schultz - 2007 - Journal of Bioethical Inquiry 4 (2):93-102.
    In researching the biomedically-engineered drug Neulasta, a breast cancer patient becomes aware of the extent to which knowledge about the development and marketing of drugs influences her decisions with regard to treatment. Time spent on understanding the commercial interests of insurers and pharmaceutical companies initially thwarts but ultimately aids the healing process. This first-person narrative calls for physicians to recognize that the alignment of commercial interests transgresses the patient’s humanity.
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  44.  35
    Corpus interruptus: Biotech drugs, insurance providers and the treatment of breast cancer. [REVIEW]Jane E. Schultz - 2007 - Journal of Bioethical Inquiry 4 (2):103-103.
    In researching the biomedically-engineered drug Neulasta (filgrastim), a breast cancer patient becomes aware of the extent to which knowledge about the development and marketing of drugs influences her decisions with regard to treatment. Time spent on understanding the commercial interests of insurers and pharmaceutical companies initially thwarts but ultimately aids the healing process. This first-person narrative calls for physicians to recognize that the alignment of commercial interests transgresses the patient’s humanity.
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  45.  7
    Transmissible cancers in mammals and bivalves: How many examples are there?Antoine M. Dujon, Georgina Bramwell, Benjamin Roche, Frédéric Thomas & Beata Ujvari - 2021 - Bioessays 43 (3):2000222.
    Transmissible cancers are elusive and understudied parasitic life forms caused by malignant clonal cells (nine lineages are known so far). They emerge by completing sequential steps that include breaking cell cooperation, evade anti‐cancer defences and shedding cells to infect new hosts. Transmissible cancers impair host fitness, and their importance as selective force is likely largely underestimated. It is, therefore, crucial to determine how common they might be in the wild. Here, we draw a parallel between the steps required for (...)
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  46.  12
    Affordable Access to Cancer and Other Lifesaving Drugs in the United States.Evaristus Obi - forthcoming - Ethics in Biology, Engineering and Medicine: An International Journal.
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  47.  24
    Targeting tumor suppressor genes for cancer therapy.Yunhua Liu, Xiaoxiao Hu, Cecil Han, Liana Wang, Xinna Zhang, Xiaoming He & Xiongbin Lu - 2015 - Bioessays 37 (12):1277-1286.
    Cancer drugs are broadly classified into two categories: cytotoxic chemotherapies and targeted therapies that specifically modulate the activity of one or more proteins involved in cancer. Major advances have been achieved in targeted cancer therapies in the past few decades, which is ascribed to the increasing understanding of molecular mechanisms for cancer initiation and progression. Consequently, monoclonal antibodies and small molecules have been developed to interfere with a specific molecular oncogenic target. Targeting gain‐of‐function mutations, in general, has been productive. (...)
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  48.  6
    Do Personality Traits Matter? Exploring Anti-drug Behavioral Patterns in a Computer-Assisted Situated Learning Environment.Tien-Chi Huang & Yu-Jie Chen - 2022 - Frontiers in Psychology 13.
    Drug abuse has been and continues to be, a common social issue worldwide, yet the efficiency of widely adopted sweeping speech for anti-drug campaigns has proven inefficient. To provide students with a safe and efficient learning situation related to drug refusal skills, we used a novel approach rooted in a serious learning game and concept map during a brief extracurricular period to help students understand drugs and their negative effects. The proposed game-based situational learning system allowed all students to (...)
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  49.  28
    Adopting an Anti-Racist Model of COVID-19 Drug Allocation and Prioritization.Akilah A. Jefferson - 2020 - American Journal of Bioethics 20 (9):33-36.
    Volume 20, Issue 9, September 2020, Page 33-36.
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  50.  91
    Taking Drugs Very Seriously.J. A. Corlett - 2013 - Journal of Medicine and Philosophy 38 (2):235-248.
    Neither anti-illegal drug proponents nor their detractors have wholly plausible arguments for their positions, because neither takes responsibility for drug use sufficiently seriously. Instead, only a policy that places users’ responsibility at the forefront of the problem is acceptable, one that is sufficiently respectful of actual or potential nonusers’ rights not to be wrongfully harmed, directly or indirectly, by drug use, or coerced to support it in any way.
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