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In 1960, Dr. Van R. Potter and Dr. Henry Pitot (at McCardle
Laboratory in Madison, Wisconsin), Dr. Tetsuo Ono (then at McCardle
Laboratory and now at the Japanese Foundation for Cancer Research
in Tokyo, Japan) and Dr. Harold P. Morris (then at the National
Cancer Institute and now at Howard University, Washington, D. C. )
decided that an experimental cancer model would be an invaluable
tool to examine neoplastic changes in cells. Since they were study
ing the various highly specific metabolic processes which are
unique to liver tissues, they determined that a transplantable
liver cancer model would be the ideal system to work with. This
system would provide for comparison of normal liver tissue of the
non-tumor bear ing animal, the tumor bearing animal's (host) liver
and the liver cancer. Dr. Morris undertook a series of rat studies
employing several chemicals known to cause liver cancer. Soon the
first Morris hepatomas (#3683, 3924A, 5123) were being studied by
several labs. During the next 18 years, Dr. Morris developed and
transplanted numerous strains of hepatomas of which no two were
identical. These tumors ranged from the very slowly-growing, highly
differentiated cancer tissues, e. g., 96l8A which is a diploid
tumor containing gly cogen and a "nearly normal" complement of
enzymes, to a large group of rapidly-growing, poorly differentiated
cancer tissues, e. g."
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Trucks Go! (Hardcover)
Harold Morris
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