{"id":1917,"date":"2006-10-23T00:00:00","date_gmt":"2006-10-23T07:00:00","guid":{"rendered":"https:\/\/vermont.salk.edu\/news-release\/targeted-tumor-therapy-when-antagonists-do-the-better-job\/"},"modified":"2006-10-23T00:00:00","modified_gmt":"2006-10-23T07:00:00","slug":"targeted-tumor-therapy-when-antagonists-do-the-better-job","status":"publish","type":"disclosure","link":"https:\/\/www.salk.edu\/zh\/news-release\/targeted-tumor-therapy-when-antagonists-do-the-better-job\/","title":{"rendered":"Targeted tumor therapy: when antagonists do the better job"},"content":{"rendered":"<p>La Jolla, CA  \u2013 Targeted tumor therapy lobs toxic payloads directly into  tumors to destroy cancer cells while leaving normal cells unharmed. In the case  of radiotherapy, these missiles, which should unerringly home in on the target  and make it implode, consist of radioactive bullets guided by small molecules \u2013 known  as agonists \u2013 that recognize and then activate specific receptors over-expressed  on the surface of tumor cells.<\/p>\n<p>But a team including researchers at the Salk Institute for  Biological Studies and collaborators in Switzerland now shows that it may  be better to exploit small molecules that <em>antagonize<\/em> rather than activate receptors. Those findings appear in this week&#8217;s Early  Online Edition of the <em>Proceedings of the National Academy of Sciences.<\/em><\/p>\n<p>&#8220;Our findings mark a paradigm shift,&#8221; says <a href=\"\/zh\/faculty\/rivier.html\/\">Jean Rivier<\/a>, a  professor in the Clayton Foundation Laboratories for Peptide Biology at the  Salk. &#8220;In the past, radiolabeled antagonists were never considered for targeted  cancer therapy since they don&#8217;t trigger the internalization of the  receptor\/ligand complex, which was thought to be the critical step towards  accumulation of the payload. But we found that antagonists have other  properties that may considerably improve the sensitivity of diagnostic  procedures and improve the efficacy of receptor-mediated radiotherapy,&#8221; he  adds.<\/p>\n<p>Radiotherapy, a promising tool in the arsenal against cancer,  delivers lethal molecules directly to a tumor. For example, peptide hormone-producing  tumors, which express receptors for another hormone, somatostatin, are  routinely targeted with radiolabeled somatostatin agonists to diagnose and treat  the tumors. <\/p>\n<p>A normal function of somatostatin, which was isolated in  1973 by Salk researchers, is to block release of growth hormone. However,  synthetic somatostatin receptor agonists have been radiolabeled and used to  treat neuroendocrine tumors. Although these strategies are quite successful, improved  tumor uptake and reduced toxicity to organs like the kidney are still desirable. <\/p>\n<p>Agonists have traditionally been favored in targeted therapy  since they and their activated receptors readily slip inside cells taking the  attached radionuclide with them, destroying them from within. Radiolabeled  antagonists, on the other hand, remain marooned outside the cell and hence,  have never been considered for tumor targeting. <\/p>\n<p>However, the fact that in some cases radiolabeled  antagonists bind to a greater number of receptors than agonists led the  research team to reconsider tumor targeting properties of the long-ignored antagonists.<\/p>\n<p>Rivier&#8217;s lab designed and synthesized several synthetic somatostatin  receptor antagonists, and then senior author Jean Claude Reubi, MD., a  professor at the Institute of Pathology at the University  of Berne in Switzerland and adjunct professor  at Salk, selected the most effective ones based on in vitro assays.<\/p>\n<p>&#8220;Amazingly, we identified, after multiple trials,  errors and refinements, antagonists that had very high binding affinity, were  selective for one receptor subtype only and did not trigger receptor  internalization at all, thus providing the ideal tool to test the validity of the  above postulate,&#8221; says Reubi.<\/p>\n<p>The question of whether this discovery had any practical  application was readily answered in vivo in cancer tumor-bearing mice, when  co-author Helmut R. M\u00e4cke, Ph.D., a professor at the University  Hospital, Department of Radiology in Basel,   Switzerland, loaded  the missiles with radioactive warheads aimed at tumors expressing somatostatin  receptors.<\/p>\n<p>&#8220;One of the most impressive findings is that the amount of  uptake of the antagonist-driven radioligands is particularly high in these  tumors,&#8221; says Rivier. &#8220;As a matter of fact, a 60 percent uptake of all  administered radioactivity has never been achieved before by any somatostatin  receptor agonist, not even the newest ones,&#8221; he adds. <\/p>\n<p>The study revealed that lethal radioactivity remained or  persisted in tumors for up to 72 hours. But what pleased the scientists most  was the high tumor\/kidney uptake ratio. &#8220;This is the critical number for  clinical use. If you want to treat patients, the radiation dose received by  normal tissue, and the kidneys in particular, has to be kept at a minimum,&#8221;  says Rivier. <\/p>\n<p>But why are antagonists more effective than agonists, since antagonists  are reduced to hanging onto the outside of cells? Rivier explains that  agonists, although they internalize, bind to a limited number of receptors, making  them a less efficient target than an antagonist that may be able to bind to a greater  variety of receptor conformations. <\/p>\n<p>&#8220;This finding has paramount consequences for the future  expansion of nuclear medicine,&#8221; says Reubi. M\u00e4cke, who is highly  experienced in in vivo radionuclide targeting, also acknowledges the  significance of using antagonist rather than agonist guidance systems, saying,  &#8220;It is by far the most significant conceptual and pragmatic development of  the past ten years.&#8221;<\/p>\n<p>Also contributing to the work were co-first authors Mihaela  Ginj, Ph.D., and Hanwen Zhang, Ph.D., Damian Wild, MD., and Xuejuan   Wang, MD., all in the M\u00e4cke  laboratory; Beatrice Waser and Renzo Cescato, Ph.D., in the Reubi laboratory; and  Judit Erchegyi, Ph.D., in the Rivier laboratory. <\/p>\n<p>The Salk Institute for Biological Studies in La Jolla, California,  is an independent nonprofit organization dedicated to fundamental discoveries  in the life sciences, the improvement of human health and the training of  future generations of researchers. Jonas Salk, M.D., whose polio vaccine all  but eradicated the crippling disease poliomyelitis in 1955, opened the  Institute in 1965 with a gift of land from the City of San Diego and the financial support of the  March of Dimes.<\/p>","protected":false},"featured_media":0,"template":"","faculty":[110],"disease-research":[],"class_list":["post-1917","disclosure","type-disclosure","status-publish","hentry","faculty-jean-rivier"],"acf":[],"yoast_head":"<!-- This site is optimized with the Yoast SEO plugin v27.3 - https:\/\/yoast.com\/product\/yoast-seo-wordpress\/ -->\n<title>Targeted tumor therapy: when antagonists do the better job - Salk Institute for Biological Studies<\/title>\n<meta name=\"robots\" content=\"index, follow, max-snippet:-1, max-image-preview:large, max-video-preview:-1\" \/>\n<link rel=\"canonical\" href=\"https:\/\/www.salk.edu\/zh\/news-release\/targeted-tumor-therapy-when-antagonists-do-the-better-job\/\" \/>\n<meta property=\"og:locale\" content=\"zh_CN\" \/>\n<meta property=\"og:type\" content=\"article\" \/>\n<meta property=\"og:title\" content=\"Targeted tumor therapy: when antagonists do the better job - Salk Institute for Biological Studies\" \/>\n<meta property=\"og:description\" content=\"La Jolla, CA \u2013 Targeted tumor therapy lobs toxic payloads directly into tumors to destroy cancer cells while leaving normal cells unharmed. 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