Treating Cancer with Immunotherapy and Targeted Therapy by David A. Olle
Author:David A. Olle
Language: eng
Format: epub
ISBN: 9781683924500
Publisher: Mercury Learning and Information
Published: 2020-10-15T00:00:00+00:00
60. How are targeted therapies developed?
Once a candidate target has been identified, the next step is to develop a therapy that affects the target in a way that interferes with its ability to promote cancer cell growth or survival. For example, a targeted therapy could reduce the activity of the target or prevent it from binding to a receptor that it normally activates, among other possible mechanisms.
There are two main types of targeted therapy:
⢠Small-molecule compounds are typically developed for targets that are located inside the cell because such agents can enter cells relatively easily.
⢠Monoclonal antibodies are relatively large and generally cannot enter cells, so they are used only for targets that are outside cells or on the cell surface.
Candidate small molecules are usually identified in what are known as âhigh-throughput screens,â in which the effects of thousands of test compounds on a specific target protein are examined. Compounds that affect the target (sometimes called âlead compoundsâ) are then chemically modified to produce numerous closely related versions of the lead compound. These related compounds are then tested to determine which are most effective and have the fewest effects on nontarget molecules.
Monoclonal antibodies are developed by injecting animals (usually mice) with purified target proteins, causing the animals to make many different types of antibodies against the target. These antibodies are then tested to find the ones that bind best to the target without binding to non-target proteins.
Before monoclonal antibodies are used in humans, they are âhumanizedâ by replacing as much of the mouse antibody molecule as possible with corresponding portions of human antibodies. Humanizing is necessary to prevent the human immune system from recognizing the monoclonal antibody as âforeignâ and destroying it before it has a chance to bind to its target protein. Humanization is not an issue for small-molecule compounds, because they are not typically recognized by the body as foreign.
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