Making the Investigational Oncology Pipeline More Efficient and Effective: Are We Headed in the Right Direction?

LoRusso, Patricia; Anderson, Aparna; Boerner, Scott A.; Averbuch, Steven D.

doi:10.1158/1078-0432.ccr-10-1279

Cited by 36 publications

(25 citation statements)

References 43 publications

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“…La plupart des TMC en développement sont des agents ciblant une ou plusieurs altérations moléculaires qui sont supposées être impliquées dans l'oncogenèse. Une voie de recherche possible pour essayer d'obtenir une réponse rapide à la question de l'efficacité du médica-ment consiste à enrichir la population en patients présentant une anomalie moléculaire spécifique : ainsi les patients ne sont traités qu'en connaissance de la biologie de leur propre cancer, et le but est d'essayer de trouver le bon médicament à un cancer donné [7]. Plusieurs équipes dans le monde, et en particulier en France, sont en train de développer des approches de ce type, et d'essayer de montrer que les phases I/II précoces de dévelop-pement puissent devenir de vérita-bles alternatives thérapeutiques pour des patients ayant un cancer avancé.…”

Section: Essais Précoces Et Preuve Du Conceptunclassified

Agents antiangiogéniques et association de TMC: attention danger

Massard

2012

Oncologie

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Greater knowledge in cancer biology has led to the isolation of molecular targets implicated in cell physiology. New treatments blocking a specific molecular target, in particular compounds blocking kinase activity, which play a key role in the transmission of the proliferation or angiogenesis signal, called molecular targeted therapies (MTTs), have shown benefit for several tumors and now are widely used including oral small molecules and monoclonal antibodies. Nevertheless, MTTs can inhibit major pathways in normal or non cancerous cells leading to unexpected off-target side effects, morbidity, reduced drug doses or even drug cessation. The combination of anti-angiogenic therapies with other MTTs could be challenging because of drug interactions or side effects.Résumé : Une plus grande connaissance de la biologie des cancers a permis d'identifier des cibles thérapeutiques. De nouvelles thérapies qui bloquent des altérations moléculaires impliquées dans les processus oncogé-niques ont été ainsi développées, et qui sont désignées par le terme « thérapies moléculaires ciblées » (TMC), que ce soit des anticorps monoclonaux ou des inhibiteurs de tyrosine-kinase. Cependant, ces TMC ont aussi des effets secondaires qui peuvent entraîner un arrêt du traitement ou des diminutions de doses. La combinaison des antiangiogéniques avec des TMC s'est montrée particulière-ment difficile compte tenu de problèmes de toxicités ou d'interactions médicamenteuses.

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Section: Essais Précoces Et Preuve Du Conceptunclassified

Agents antiangiogéniques et association de TMC: attention danger

Massard

2012

Oncologie

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“…While promising results for the compound emerged from phase I and phase II studies, the drug failed to show any advantage in a pivotal phase III trial with patients with refractory advanced non-small cell lung cancer. Subsequent analysis suggested that the drug might have had some success with a selected sub-population [49,50]. In light of this and other well-known phase III failures, the Task Force recommended that investigators consider stratified, adaptive designs that allow phase II trials to select a population in the course of a trial and continue study of the subpopulation in order to provide more precise indications for phase III trials [51,52].…”

Section: Phase II Trialsmentioning

confidence: 99%

Clinical trials in the age of personalized medicine

Keating

Cambrosio

2011

J Med Pers

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The paper reviews some of the transformations of cancer clinical trial protocols made necessary by the emergence of molecularly targeted agents. These changes include the creation of a new phase of clinical trials (phase 0) and the alteration of the parameters governing the other three phases. The situation remains unstable: repeated attempts to speed up the development of new drugs have not yet led to a consensus on how to best do so. The new targeted agents raise issues that go beyond the purely technical as changing protocols implicate changes in the organization of translational research.

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“…This consensus will not be achieved quickly or easily because these are not no-benefit treatments. Many of the articles in this issue of CCR Focus explore aspects of this problem in great depth (26)(27)(28)(29)(30). Even after health reform, our very heterogeneous and fragmented system will make it difficult to implement such limitations fairly and equitably.…”

Section: Rule Of Rescuementioning

confidence: 99%

Value and Cancer Care: Toward an Equitable Future

Schnipper

Brock

2010

Clinical Cancer Research

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Health care expenses in the United States are increasing inexorably. At the current rate of growth, it is anticipated that 20% of the gross national product will consist of health-related expenditures within the next decade. Cancer is the second leading cause of death in the United States, and it is increasing in prevalence because of the aging of the population and the limited number of successful prevention strategies. As the biological characteristics of cancer come into sharper focus, targeted therapies are being developed that offer the promise of increased clinical benefit with fewer toxicities than are associated with conventional treatment. Although spectacular successes are infrequent with this approach, to date, the majority of targeted therapies are modestly effective at best, and extremely costly. This observation suggests that a broadly acceptable definition of value in a cancer therapeutic agent is not at hand, but is sorely needed from the vantage points of the patient and society. A corollary issue of enormous import is how to equitably distribute the health care dollar in the service of achieving the greatest good for the greatest number. Although cancer is responsible for only 5% of the health care budget, its cost is increasing and it can be viewed as paradigmatic when contemplating the problem of equity in health care. Here, a number of concepts are discussed that focus on this goal and its implications for the cancer patient and society at large.Clin Cancer Res; 16(24); 6004-8. Ó2010 AACR.Health care costs in the United States are increasing at a rate that exceeds overall economic growth. It is estimated that 20% of the gross national product will be allocated to health care in 2020. The burden to the economy as a whole is unambiguous and unsustainable. The burden to individuals affected by disease and their families is sometimes intolerable, leading to medical expenditures that precipitate declarations of personal bankruptcy. Cancer is the second most common cause of death in the United States, as well as an enormous cause of morbidity and psychological pain. Although not the primary driver of increasing US health care costs (cancer constitutes approximately 5% of the nation's health care costs; ref. 1), the costs of contemporary cancer care provide a model for understanding the problems and positing equitable solutions that might be incorporated into US health care. In order to provide a rational and ethical basis for arguing for constructive change, cancer can be viewed paradigmatically. In that context, its impact on society and the individual are explored, and societal considerations are addressed in the service of providing for more equitable allocations of the health care (cancer care) dollar. Principles of ValueThe burden on societyThe absolute number of dollars spent on cancer care during the periods between 1987 and 2001 to 2005 doubled, increasing from $24 billion to $48.1 billion per year. The basis for this doubling is the increased prevalence of the disease, probably as...

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Making the Investigational Oncology Pipeline More Efficient and Effective: Are We Headed in the Right Direction?

Cited by 36 publications

References 43 publications

Agents antiangiogéniques et association de TMC: attention danger

Agents antiangiogéniques et association de TMC: attention danger

Clinical trials in the age of personalized medicine

Value and Cancer Care: Toward an Equitable Future

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