“ Thus, in the drug development process, biomarkers can be useful tools from the discovery stage, where they are used to investigate pathophysiologic mechanisms related to either diagnosis or prognosis of a. disease, through the later stages of clinical development. Biomarkers can be used in preclinical studies to confirm in vivo activity as well as to investigate dose-response relationships. During early clinical development Inhibitors,research,lifescience,medical programs (phase 1 and 2a), biomarkers are used to evaluate activity and to develop pharmacokinetic-pharmacodynamic relationships. In phase 3 and 4 studies, biomarkers
are useful tools for stratifying study populations. selleck chemicals Tipifarnib surrogate outcomes are biomarkers that fit. the following definition: “a. biomarker that is intended to substitute for a clinical end point. A surrogate end point is expected to predict Inhibitors,research,lifescience,medical clinical benefit, (or harm or lack of benefit or harm) based on epidemiologic, therapeutic, pathophysiologic, or other scientific evidence.”1 This definition of a surrogate outcome illustrates the key difference versus the role of the
biomarker. A biomarker can be used as a. surrogate outcome if it can reasonably predict a. clinical benefit. Thus, although a surrogate outcome is by definition a biomarker, in fact, a very small minority of biomarkers meet, the standard of a. surrogate outcome. Before 1991, regulatory agencies Inhibitors,research,lifescience,medical such as the FDA used surrogate Inhibitors,research,lifescience,medical treatment outcomes in limited settings, mainly in the cardiovascular area. For example, antihypertensive drugs have been approved for marketing based on their effectiveness in lowering blood pressure, and cholesterol-lowering agents have been approved based on their ability to decrease serum cholesterol, not on the direct evidence that they decrease mortality from cardiovascular diseases. In 1991 , during the acquired immune deficiency syndrome (AIDS) epidemic, surrogate outcomes Inhibitors,research,lifescience,medical were utilized for the first, time as a viable path toward regulatory approval. Indeed, an
important, milestone was Cilengitide the use of CD4 cell count as a. surrogate marker, thenthereby because of its predictive value for outcome. This led to the approval of didanosine for the treatment of HIV. In 1992, the FDA formulated a new regulatory process, often referred to as “accelerated approval,” under which marketing approval can be provided for interventions that have been shown to have compelling effects on a validated surrogate treatment, outcome. At, the present, time, there are well-defined procedures in the FDA in which such approvals are routinely examined3; for example, some anticancer treatments have been approved under the accelerated approval regulations.3 In these cases, drugs tested in patients refractory to available treatments are approved on the basis of their effects on tumor size, as assessed by imaging.