By Elizabeth Whittington
Revlimid Reaches
the Finish Line for Myelodysplastic Syndromes
After positive
results in a phase III trial and a recommendation from
the Food and Drug Administration’s Oncology Drugs
Advisory Committee, Revlimid® (lenalidomide)
was approved in late 2005 for certain types of myelodysplastic syndromes (MDS),
a variety of blood disorders that can cause low blood counts, including anemia,
which require frequent blood transfusions.
Revlimid is especially effective
in a quarter of MDS patients who carry a specific chromosome
5 deletion. Taken orally, Revlimid can cause many of
these patients
to no longer need blood transfusions, improving their quality of life. A phase
III trial showed Revlimid, a derivative of Thalomid® (thalidomide), allowed
two thirds of patients to become transfusion-independent for more than a year.
Though no trial has shown a risk of birth defects in patients taking Revlimid,
the drug is currently only available through a restricted distribution program
called RevAssist, which requires doctors and pharmacists to register in order
to prescribe the drug. Women must have regular pregnancy tests, and both men
and women must use contraceptives.
In addition to MDS, Revlimid has also
shown activity in patients with relapsed multiple myeloma. The FDA
is considering the drug for multiple myeloma and is expected to
approve Revlimid for that indication in mid-2006. It is also being
tested in metastatic melanoma and chronic lymphocytic leukemia.
Common side effects of Revlimid include neutropenia, fatigue and
diarrhea.
For more information,
visit www.revlimid.com.
Double Approval
for Sutent
The FDA approved a new oral
drug called Sutent® (sunitinib) in January for
both advanced kidney cancer as well as a rare type of sarcoma of the stomach
called gastrointestinal stromal tumor (GIST). The approval made Sutent the first
drug to be simultaneously approved for two cancers.
Sutent blocks the activity
of multiple enzymes (called tyrosine kinases) that are involved
in transmitting signals from the outside to the inside of the cancer
cell. Sutent can block the development of new blood vessels (called
angiogenesis), essentially starving the tumor of blood and nutrients
(see “Picking Up Momentum for Treating Renal Cell Carcinoma,”).
In phase II trials, Sutent shrank tumors by at least a third in
up to 37 percent of advanced kidney cancer patients.
GIST is a rare tumor that occurs in
the stomach and other parts of the digestive system. Fortunately,
most GIST patients respond to Gleevec® (imatinib), but over
time, some patients become resistant to Gleevec and need an alternative
treatment. When used against Gleevec-resistant GIST, Sutent had
significant activity, prolonging time to tumor progression from
six weeks to 27 weeks when compared with placebo. The most commonly
reported side effects include fatigue, diarrhea and a rash on the
hands and feet.
For more information on
Sutent, go to www.sutent.com.
Monoclonal Antibody
Approval a First for Head & Neck Cancer
Erbitux® (cetuximab) received approval from the
FDA on March 1 for head and neck cancer, a second approval
for the monoclonal antibody, which is already on the
market for treating metastatic colorectal cancer in
combination with Camptosar® (irinotecan). In 2005,
nearly 40,000 Americans were diagnosed with head and
neck cancer, including cancers of the tongue, mouth,
salivary glands, throat and voice box.
In colorectal,
head and neck and other cancers, the number of receptors
for epidermal growth factors is higher on the surface
of cancer cells than normal cells. When
Erbitux binds to the epidermal growth factor receptor on cancer cells, it inhibits
the signal for cancer cell growth. In one of the largest phase III studies ever
conducted in head and neck cancer patients, Erbitux in combination with radiation
prevented the spread of cancer more effectively than radiation alone and improved
median survival by nearly two years.
Other studies show Erbitux is effective in patients whose
cancers don’t respond to platinum-based therapy, such as Paraplatin®
(carboplatin) and Platinol® (cisplatin). The most common side
effect with Erbitux is an acne-like rash.
For more information on
Erbitux, go to www.erbitux.com. |
