New Tumor-Targeting Agent Images a Wide Range of Cancers
By MedImaging International staff writers Posted on 30 Jun 2014 |
Scientists reported that a new type of tumor-targeting agent can search out and target dozens of solid tumors, even illuminating brain cancer stem cells that do not respond to current treatments.
Moreover, years of animal studies and early human clinical trials show that this tumor-targeting, alkylphosphocholine (APC) molecule can deliver two types of “cargoes” right to cancer cells: a radioactive or fluorescent imaging label, or a radioactive medicine that binds and destroys cancer cells.
The study’s findings were reported in the June 13, 2014, issue of the journal Science Translational Medicine. The APC targeting platform is a synthetic molecule that exploits a weakness common to cancers as diverse as breast, lung, brain, and melanoma. These cancer cells lack the enzymes to metabolize phospholipid ethers, a cell membrane component that is easily cleared by normal cells. When administered in an intravenous solution, APC goes throughout the body—even across the blood-brain barrier—and adhere to the membrane of cancer cells. The cancer cells take up the APC and the imaging or treatment medication riding on the molecular platform, and retain it for days to weeks, resulting in direct cancer cell imaging or treatment.
The APC analogs were able to tag 55 of 57 different cancers. This large study had multiple stages, including testing in cancer cell lines, in rodents and rodents infected with human and rodent cancers, and in human patients with different cancers such as colorectal, breast, lung, and glioblastoma.
“I was a skeptic; it’s almost too good to be true,” said co-lead author Dr. John S. Kuo, associate professor of neurosurgery and director of the comprehensive brain tumor program at the University of Wisconsin (UW) School of Medicine and Public Health (Madison, USA). “It is a very broad cancer-targeting agent in terms of the many different cancers that tested positive. The APC analogs even sometimes revealed other sites of cancer in patients that were small, asymptomatic and previously undetected by physicians.”
Dr. Kuo specializes in the treatment of brain tumors, and also leads the UWCCC CNS Tumors group that are conducting many clinical trials for glioma, a brain cancer that is incurable because current treatments leave behind cancer stem cells that can seed and regrow the cancer. He noted that it was encouraging that the APC analogs also captured cancer stem cells and will also likely target them for additional treatment. “It’s also potentially superior to current imaging methods because the standard clinical MR or PET imaging may give false-positive results due to surgical scars, post-treatment effects, inflammation, or even infection, making it difficult to know if the cancer has truly returned,” he stated.
Dr. Kuo noted that the fluorescent intraoperative APC imaging might help make cancer surgeries more effective and safer; any cancer cells that cannot be safely removed can be targeted afterwards with radioactive APC therapy. In addition, APC imaging might avoid the false-positive findings of current imaging, so cancer patients can stay on effective therapies and likely avoid the risks and costs of “second look” surgeries.
The large multidisciplinary study team was also led by co-lead author Dr. Jamey P. Weichert, associate professor of radiology, who cofounded and serves as chief scientific officer of Cellectar Biosciences, Inc., a Madison-based company developing the APC analog platform for cancer imaging and therapy.
Related Links:
University of Wisconsin School of Medicine and Public Health
Moreover, years of animal studies and early human clinical trials show that this tumor-targeting, alkylphosphocholine (APC) molecule can deliver two types of “cargoes” right to cancer cells: a radioactive or fluorescent imaging label, or a radioactive medicine that binds and destroys cancer cells.
The study’s findings were reported in the June 13, 2014, issue of the journal Science Translational Medicine. The APC targeting platform is a synthetic molecule that exploits a weakness common to cancers as diverse as breast, lung, brain, and melanoma. These cancer cells lack the enzymes to metabolize phospholipid ethers, a cell membrane component that is easily cleared by normal cells. When administered in an intravenous solution, APC goes throughout the body—even across the blood-brain barrier—and adhere to the membrane of cancer cells. The cancer cells take up the APC and the imaging or treatment medication riding on the molecular platform, and retain it for days to weeks, resulting in direct cancer cell imaging or treatment.
The APC analogs were able to tag 55 of 57 different cancers. This large study had multiple stages, including testing in cancer cell lines, in rodents and rodents infected with human and rodent cancers, and in human patients with different cancers such as colorectal, breast, lung, and glioblastoma.
“I was a skeptic; it’s almost too good to be true,” said co-lead author Dr. John S. Kuo, associate professor of neurosurgery and director of the comprehensive brain tumor program at the University of Wisconsin (UW) School of Medicine and Public Health (Madison, USA). “It is a very broad cancer-targeting agent in terms of the many different cancers that tested positive. The APC analogs even sometimes revealed other sites of cancer in patients that were small, asymptomatic and previously undetected by physicians.”
Dr. Kuo specializes in the treatment of brain tumors, and also leads the UWCCC CNS Tumors group that are conducting many clinical trials for glioma, a brain cancer that is incurable because current treatments leave behind cancer stem cells that can seed and regrow the cancer. He noted that it was encouraging that the APC analogs also captured cancer stem cells and will also likely target them for additional treatment. “It’s also potentially superior to current imaging methods because the standard clinical MR or PET imaging may give false-positive results due to surgical scars, post-treatment effects, inflammation, or even infection, making it difficult to know if the cancer has truly returned,” he stated.
Dr. Kuo noted that the fluorescent intraoperative APC imaging might help make cancer surgeries more effective and safer; any cancer cells that cannot be safely removed can be targeted afterwards with radioactive APC therapy. In addition, APC imaging might avoid the false-positive findings of current imaging, so cancer patients can stay on effective therapies and likely avoid the risks and costs of “second look” surgeries.
The large multidisciplinary study team was also led by co-lead author Dr. Jamey P. Weichert, associate professor of radiology, who cofounded and serves as chief scientific officer of Cellectar Biosciences, Inc., a Madison-based company developing the APC analog platform for cancer imaging and therapy.
Related Links:
University of Wisconsin School of Medicine and Public Health
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