Dr. William G. Cance

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  www.rt-image.com/News_Extras/content=8204J05C4856AE8440 - [Cached Version]
  Published on: 2/5/2008    Last Visited: 2/5/2008  

  Overall, approximately three-fourths of patients underwent a partial mastectomy, also known as lumpectomy or breast-conserving surgery, while one-fourth ultimately had a total mastectomy, UF's chairman of surgery William G. Cance, MD, recently reported.

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  www.sciencedaily.com/releases/2007/12/071205122531.htm - [Cached Version]
  Published on: 1/1/2007    Last Visited: 12/7/2007  

  Overall, approximately three-fourths of patients underwent a partial mastectomy, also known as lumpectomy or breast-conserving surgery, while one-fourth ultimately had a total mastectomy, UF's chairman of surgery William G. Cance, M.D., reported Wednesday morning.

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  BIO.COM: Biotechnology Pharmaceutical Therapeutics,... - [Cached Version]
  Published on: 2/1/2006    Last Visited: 2/1/2006  

  "We have found a gene called focal adhesion kinase which is produced at very high levels in human tumors, and our work has shown this makes the tumors more likely to survive as they spread throughout the body and grow," said William G. Cance, M.D., a researcher at the University of Florida Shands Cancer Center and chairman of the department of surgery at UF's College of Medicine."It also makes them more resistant to our attempts to kill them.And we're trying to understand exactly why this gene, which is a small enzyme molecule, is very intimately associated with tumor cell survival."
  
  Focal adhesion kinase, or FAK, is commanding increasing attention and has spawned a flurry of research designed to develop new drug therapies, said Cance, who is known internationally for his genetic investigations of tumor survival.These medicines would prevent FAK from linking with the protein known as vascular endothelial growth factor receptor 3, or VEGFR-3.The protein is tied to the growth of channels in the lymph system that serve as cellular superhighways for cancer spread and is found in breast, colon and thyroid tumors.
  
  Cance and colleagues were the first to pull FAK out of human tumors and to show that human cancers make the molecule in large quantities.In 1996, the team was the first to show that if a tumor is prevented from producing the enzyme it dies.The scientists also have identified some protein receptors FAK binds to; VEGFR-3 is the latest they've discovered and represents a "hot area for developing therapeutics," Cance said.
  
  "We've shown that if you disrupt this interaction - if you block the binding of these two proteins - the tumor cells are more prone to being killed," he said.
  
  UF researchers identified FAK's interaction with VEGFR-3 in cell cultures of human breast cancer.Breast cancers that pump out high volumes of FAK and VEGFR-3 are more aggressive tumors, Cance said.The scientists were able to block FAK from binding with VEGFR-3 by introducing a different protein that stopped cancer cells from dividing and caused them to die but spared normal breast cells.
  
  "FAK is a critical molecule, and in the future different ways of targeting either the enzyme itself or targeting the binding between these various proteins will have a major impact on cancer, I believe," Cance said."We think it's one of the Achilles' heels for tumor cells and you can disrupt it in a number of different ways.For example, we might be able to design drugs that mimic this area of binding and disrupt it in patients."
  
  Because normal cells generate much lower levels of FAK than tumor cells do, treatments could be developed to target FAK and VEGFR-3 at dosages markedly less toxic to healthy tissues yet lethal to cancer.
  
  "We have a therapeutic window," said Cance, the study's senior investigator.
  ...
  "We take our patients, we look at their tumors and we try to find clues to why their tumors grow, why their tumors spread, and we look at the various genes and proteins that make their tumors what they are," Cance said.

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  Details for news - [Cached Version]
  Published on: 7/2/2004    Last Visited: 7/12/2006  

  According to William Cance, professor and chair of the UF department of surgery, the rankings provide a platform for even more success in the future.
  
  "I am delighted to see this level of recognition for the world-class health care provided by the University of Florida physicians and Shands HealthCare," Cance said.

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  Independent Florida Alligator - NEWS - [Cached Version]
  Published on: 7/8/2004    Last Visited: 7/8/2004  

  William Cance, professor and chair of the UF department of surgery, said the rankings are an honor but come as no surprise.
  
  Shands has earned a reputation as one of the nation's best hospitals, and Cance directly attributes this achievement to the hospital's staff.
  
  "We have an active commitment to continue our excellence," said Cance.

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  Inside Florida - Florida High Tech - [Cached Version]
  Published on: 3/1/2006    Last Visited: 6/27/2008  

  William Cance, a researcher at the University of Florida Shands Cancer Center and chairman of the department of surgery at UF's College of Medicine, and his colleagues were the first to remove FAK from human tumors, an achievement that is creating new avenues of research that could lead to improved cancer therapies.

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  Molecular force field helps cancer cells defend... - [Cached Version]
  Published on: 2/11/2006    Last Visited: 8/6/2006  

  "We have found a gene called focal adhesion kinase which is produced at very high levels in human tumors, and our work has shown this makes the tumors more likely to survive as they spread throughout the body and grow," said Dr. William G. Cance, a researcher at the University of Florida Shands Cancer Center and chairman of the department of surgery at UF's College of Medicine."It also makes them more resistant to our attempts to kill them.And we're trying to understand exactly why this gene, which is a small enzyme molecule, is very intimately associated with tumor cell survival."
  
  Focal adhesion kinase, or FAK, is commanding increasing attention and has spawned a flurry of research designed to develop new drug therapies, said Cance, who is known internationally for his genetic investigations of tumor survival.These medicines would prevent FAK from linking with the protein known as vascular endothelial growth factor receptor 3, or VEGFR-3.The protein is tied to the growth of channels in the lymph system that serve as cellular superhighways for cancer spread and is found in breast, colon and thyroid tumors.
  
  Cance and colleagues were the first to pull FAK out of human tumors and to show that human cancers make the molecule in large quantities.In 1996, the team was the first to show that if a tumor is prevented from producing the enzyme it dies.The scientists also have identified some protein receptors FAK binds to; VEGFR- 3 is the latest they've discovered and represents a "hot area for developing therapeutics," Cance said.
  
  "We've shown that if you disrupt this interaction - if you block the binding of these two proteins - the tumor cells are more prone to being killed," he said.
  
  UF researchers identified FAK's interaction with VEGFR-3 in cell cultures of human breast cancer.Breast cancers that pump out high volumes of FAK and VEGFR-3 are more aggressive tumors, Cance said.The scientists were able to block FAK from binding with VEGFR-3 by introducing a different protein that stopped cancer cells from dividing and caused them to die but spared normal breast cells.
  
  "FAK is a critical molecule, and in the future different ways of targeting either the enzyme itself or targeting the binding between these various proteins will have a major impact on cancer, I believe," Cance said."We think it's one of the Achilles' heels for tumor cells and you can disrupt it in a number of different ways.For example, we might be able to design drugs that mimic this area of binding and disrupt it in patients."
  
  Because normal cells generate much lower levels of FAK than tumor cells do, treatments could be developed to target FAK and VEGFR-3 at dosages markedly less toxic to healthy tissues yet lethal to cancer.
  
  "We have a therapeutic window," said Cance, the study's senior investigator.
  ...
  "We take our patients, we look at their tumors and we try to find clues to why their tumors grow, why their tumors spread, and we look at the various genes and proteins that make their tumors what they are," Cance said.

• 
  Molecular force field helps cancer cells defend... - [Cached Version]
  Published on: 2/2/2006    Last Visited: 2/3/2006  

  "We have found a gene called focal adhesion kinase which is produced at very high levels in human tumors, and our work has shown this makes the tumors more likely to survive as they spread throughout the body and grow," said William G. Cance, M.D., a researcher at the University of Florida Shands Cancer Center and chairman of the department of surgery at UF's College of Medicine."It also makes them more resistant to our attempts to kill them.And we're trying to understand exactly why this gene, which is a small enzyme molecule, is very intimately associated with tumor cell survival."
  
  Focal adhesion kinase, or FAK, is commanding increasing attention and has spawned a flurry of research designed to develop new drug therapies, said Cance, who is known internationally for his genetic investigations of tumor survival.These medicines would prevent FAK from linking with the protein known as vascular endothelial growth factor receptor 3, or VEGFR-3.The protein is tied to the growth of channels in the lymph system that serve as cellular superhighways for cancer spread and is found in breast, colon and thyroid tumors.
  
  Cance and colleagues were the first to pull FAK out of human tumors and to show that human cancers make the molecule in large quantities.In 1996, the team was the first to show that if a tumor is prevented from producing the enzyme it dies.The scientists also have identified some protein receptors FAK binds to; VEGFR-3 is the latest they've discovered and represents a "hot area for developing therapeutics," Cance said.
  
  "We've shown that if you disrupt this interaction-if you block the binding of these two proteins-the tumor cells are more prone to being killed," he said.
  
  UF researchers identified FAK's interaction with VEGFR-3 in cell cultures of human breast cancer.Breast cancers that pump out high volumes of FAK and VEGFR-3 are more aggressive tumors, Cance said.The scientists were able to block FAK from binding with VEGFR-3 by introducing a different protein that stopped cancer cells from dividing and caused them to die but spared normal breast cells.
  
  "FAK is a critical molecule, and in the future different ways of targeting either the enzyme itself or targeting the binding between these various proteins will have a major impact on cancer, I believe," Cance said."We think it's one of the Achilles' heels for tumor cells and you can disrupt it in a number of different ways.For example, we might be able to design drugs that mimic this area of binding and disrupt it in patients."
  
  Because normal cells generate much lower levels of FAK than tumor cells do, treatments could be developed to target FAK and VEGFR-3 at dosages markedly less toxic to healthy tissues yet lethal to cancer.
  
  "We have a therapeutic window," said Cance, the study's senior investigator.
  ...
  "We take our patients, we look at their tumors and we try to find clues to why their tumors grow, why their tumors spread, and we look at the various genes and proteins that make their tumors what they are," Cance said.

• 
  ScienceDaily: Molecular Force Field Helps Cancer Cells... - [Cached Version]
  Published on: 2/2/2006    Last Visited: 2/2/2006  

  "We have found a gene called focal adhesion kinase which is produced at very high levels in human tumors, and our work has shown this makes the tumors more likely to survive as they spread throughout the body and grow," said William G. Cance, M.D., a researcher at the University of Florida Shands Cancer Center and chairman of the department of surgery at UF's College of Medicine."It also makes them more resistant to our attempts to kill them.And we're trying to understand exactly why this gene, which is a small enzyme molecule, is very intimately associated with tumor cell survival."
  
  Focal adhesion kinase, or FAK, is commanding increasing attention and has spawned a flurry of research designed to develop new drug therapies, said Cance, who is known internationally for his genetic investigations of tumor survival.These medicines would prevent FAK from linking with the protein known as vascular endothelial growth factor receptor 3, or VEGFR-3.The protein is tied to the growth of channels in the lymph system that serve as cellular superhighways for cancer spread and is found in breast, colon and thyroid tumors.
  
  Cance and colleagues were the first to pull FAK out of human tumors and to show that human cancers make the molecule in large quantities.In 1996, the team was the first to show that if a tumor is prevented from producing the enzyme it dies.The scientists also have identified some protein receptors FAK binds to; VEGFR-3 is the latest they've discovered and represents a "hot area for developing therapeutics," Cance said.
  
  "We've shown that if you disrupt this interaction - if you block the binding of these two proteins - the tumor cells are more prone to being killed," he said.
  
  UF researchers identified FAK's interaction with VEGFR-3 in cell cultures of human breast cancer.Breast cancers that pump out high volumes of FAK and VEGFR-3 are more aggressive tumors, Cance said.The scientists were able to block FAK from binding with VEGFR-3 by introducing a different protein that stopped cancer cells from dividing and caused them to die but spared normal breast cells.
  
  "FAK is a critical molecule, and in the future different ways of targeting either the enzyme itself or targeting the binding between these various proteins will have a major impact on cancer, I believe," Cance said."We think it's one of the Achilles' heels for tumor cells and you can disrupt it in a number of different ways.For example, we might be able to design drugs that mimic this area of binding and disrupt it in patients."
  
  Because normal cells generate much lower levels of FAK than tumor cells do, treatments could be developed to target FAK and VEGFR-3 at dosages markedly less toxic to healthy tissues yet lethal to cancer.
  
  "We have a therapeutic window," said Cance, the study's senior investigator.
  ...
  "We take our patients, we look at their tumors and we try to find clues to why their tumors grow, why their tumors spread, and we look at the various genes and proteins that make their tumors what they are," Cance said.

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  Tenafly Times: Health & Nature Archives November 2005... - [Cached Version]
  Published on: 11/1/2005    Last Visited: 4/28/2006  

  "This is a testimony to Dr. Copeland's lifetime of excellence in surgery," said William Cance, M.D., a UF professor and chairman of the department of surgery.
  ...
  "This is the most distinguished position an American surgeon can ever attain, being recognized as the leader of the umbrella organization for all surgeons in North America," Cance added.

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