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Monoclonal antibodies are the most widely used form of cancer
immunotherapy at this time.
Monoclonal antibody therapy uses antibodies that are made in
the lab rather than by a person's own immune system. This type of
treatment is considered a form of passive immunotherapy. These
treatments do not require the person's immune system to start the fight
against the cancer. Once the antibodies are given, they can then
recruit other parts of the immune system to destroy the cancer cells.
The first monoclonal antibodies were made in the lab by fusing
a myeloma (a type of bone marrow cancer) cell from a mouse with a mouse
B cell that makes a certain antibody. The cell that results from this
fusion is called a hybridoma.
Combining a B cell that can recognize one special antigen and
a long-lived myeloma cell makes the resulting hybridoma cell a
long-lasting, antibody-making factory. Because the antibodies made are
all identical clones made from a single (mono) hybridoma cell, they are
called monoclonal
antibodies (sometimes abbreviated as MoAbs or MAbs).
The first MAbs were made entirely from mouse cells. One
problem with this is that the human immune system will see these
antibodies as foreign (because they're from a different species) and
then will mount a response against them. In the short term, this can
sometimes cause allergic-type reactions. In the long term, it means
that the antibodies may only work the first time they are given; after
that, the body's immune system is primed to destroy them before they
can be helpful.
Over time, researchers have learned how to replace some parts
of these mouse antibody proteins with human parts. Depending on how
much of the MAb is human, these are called chimeric or humanized
antibodies. Some MAbs are now fully human, which means they are likely
to be even safer and may be more effective than older MAbs.
An even newer approach uses fragments of antibodies instead of
whole ones. Smaller pieces may be better able to reach a tumor, which
may make them more effective.
Over the past 10 years or so, the Food and Drug Administration
(FDA) has approved several MAbs to treat certain cancers, as seen in
the table below.
Clinical trials of monoclonal antibody therapy are also being
done on almost every type of cancer. As researchers have found more
antigens that are linked to cancer, they have been able to make
monoclonal antibodies against more and more cancers.
Monoclonal antibodies used to treat cancer
| MAb name
|
Trade
name |
Used to
treat: |
Approved
in: |
| rituximab |
Rituxan®
|
non-Hodgkin lymphoma |
1997 |
| trastuzumab |
Herceptin®
|
breast cancer |
1998 |
| gemtuzumab ozogamicin* |
Mylotarg®
|
acute myelogenous leukemia
(AML) |
2000 |
| alemtuzumab |
Campath®
|
chronic lymphocytic
leukemia (CLL) |
2001 |
| ibritumomab tiuxetan* |
Zevalin®
|
non-Hodgkin lymphoma
|
2002 |
| tositumomab* |
Bexxar®
|
non-Hodgkin lymphoma |
2003 |
| cetuximab |
Erbitux®
|
colorectal cancer
head
& neck cancers |
2004
2006 |
| bevacizumab |
Avastin®
|
colorectal cancer
non-small cell lung cancer
breast cancer
glioblastoma
kidney cancer |
2004
2006
2008
2009
2009 |
| panitumumab |
Vectibix®
|
colorectal cancer |
2006 |
| ofatumumab |
Arzerra®
|
chronic lymphocytic
leukemia (CLL) |
2009 |
*conjugated
monoclonal antibodies
Two types of monoclonal antibodies are used in cancer
treatments:
- Naked
monoclonal antibodies are those without any
drug or radioactive material attached to them.
- Conjugated
monoclonal antibodies are those joined
to a chemotherapy drug, radioactive particle, or a toxin (a substance
that poisons cells).
Naked monoclonal antibodies
Naked MAbs are the most commonly used MAbs at this time.
Although they all work by attaching themselves to specific antigens,
they can be helpful in different ways.
Markers for destruction
Some naked MAbs attach to cancer cells to act as a marker for
the body's immune system to destroy them. Antibodies now in use in this
group include:
Rituximab
(Rituxan): Rituximab is used to treat B-cell
non-Hodgkin lymphoma and some other diseases. It is a monoclonal
antibody against the CD20 antigen, found on B cells. It works, in part,
by labeling cells so that the immune system can attack them.
Ofatumumab (Arzerra): Ofatumumab is another antibody against the CD20
antigen. It is used mainly to treat chronic lymphocytic leukemia when other
treatments are no longer effective.
Alemtuzumab
(Campath): Alemtuzumab is an antibody against the
CD52 antigen, which is found on both B cells and T cells. It is used to
treat some patients with B-cell chronic lymphocytic leukemia.
Activation blockers
Some naked MAbs don't really interact with a person's own
immune system. Their effects come from their ability to attach to the
specific antigens that are working parts of cancer cells or other cells
that help cancer cells grow, and stop them from working. These MAbs are
also referred to as targeted therapies. Examples of FDA-approved MAbs
of this type include:
Trastuzumab
(Herceptin): Trastuzumab is an antibody against
the HER2/neu protein. A large amount of this protein is present on
tumor cells in some cancers. When HER2/neu is activated, it helps these
cells grow. Trastuzumab stops these proteins from becoming active. It
is used to treat breast cancers that have large amounts of this
protein.
Cetuximab
(Erbitux): Cetuximab is an antibody against the EGFR
protein, which is present in large amounts on some tumor cells and
helps them grow and divide. Cetuximab blocks the activation of EGFR. It
is used to treat some advanced colorectal cancers as well as some head
and neck cancers.
Panitumumab
(Vectibix): This MAb also targets the EGFR
antigen. It is used to treat some cases of advanced colorectal cancer.
Bevacizumab
(Avastin): Bevacizumab targets the VEGF protein,
which is normally made by tumor cells to attract new blood vessels to
feed their growth. Bevacizumab attaches to VEGF, which blocks it from
signaling for new blood vessels to form. This MAb is used along with
chemotherapy to treat some colorectal, lung, breast, and kidney cancers,
as welll as glioblastomas (a type of brain tumor).
It is being studied for use against other cancers.
Some of these antibodies have been used for many years. At
first they were used mostly after other treatments had stopped working.
But more studies have been done and continue to be done. Now, these
antibodies are being used earlier in the course of cancer treatment.
Side effects
Monoclonal antibodies are given intravenously (injected into a
vein). Compared with side effects of chemotherapy, the side effects of
naked MAbs are usually fairly mild and are often more like an allergic
reaction. If they do occur, it is most often while the drug is first
being given.
Possible side effects can include:
- fever
- chills
- weakness
- headache
- nausea
- vomiting
- diarrhea
- low blood pressure
- rashes
Some MAbs also have effects that are specific to the antigens
they target. For instance, like most chemotherapy drugs, some can
affect the bone marrow. This can cause lower levels of blood cells,
which can increase the risk of bleeding and infection in some people.
Conjugated monoclonal antibodies
Conjugated MAbs are monoclonal antibodies that are attached to
drugs, toxins, or radioactive substances. The MAbs are used as homing
devices to take these substances directly to the cancer cells. The MAb
circulates in the body until it can find and hook onto the target
antigen. It then delivers the toxic substance where it is needed most.
This lessens the damage to normal cells in other parts of the body.
Conjugated antibodies may pack more of a punch than naked
MAbs, but for this reason they often cause more side effects, too. The
side effects depend on which type of substance they're attached to.
Conjugated MAbs are also sometimes referred to as tagged,
labeled, or
loaded
antibodies. They can be divided into groups
depending on what they are linked to.
- MAbs with radioactive particles attached are
referred to as radiolabeled,
and therapy with this type of antibody is
known as radioimmunotherapy
(RIT).
- MAbs with chemotherapy drugs attached are often
referred to as chemolabeled.
- MAbs attached to toxins are called immunotoxins.
Radiolabeled antibodies
Two radiolabeled antibodies have been approved to treat
cancer.
- Ibritumomab
tiuxetan (Zevalin) delivers
radioactivity directly to cancerous B lymphocytes. It is used to treat
B-cell non-Hodgkin lymphoma that has not responded to standard
treatment.
- Tositumomab
(Bexxar) is used to treat certain types
of non-Hodgkin lymphoma that no longer respond to rituximab (Rituxan)
or chemotherapy.
Aside from being used to treat cancer, radiolabeled antibodies
can also be used along with special cameras to help find areas of
cancer metastasis (spread) in the body. While some radiolabeled
antibodies such as ProstaScint (for prostate cancer) have been approved
by the FDA, their role in helping to detect cancer has been very
limited so far.
Chemolabeled antibodies
These are being studied and are available in the United States
only through clinical trials at this time. None have been approved by
the FDA as of mid-2009.
Immunotoxins
Immunotoxins are made by attaching MAbs to bacterial toxins
such as diphtheria toxin (DT) or pseudomonal exotoxin (PE40), or to
plant toxins such as ricin A or saporin.
Immunotoxins have shown some early promise in shrinking a few
cancers, particularly lymphomas. But some major problems still need to
be solved before this new form of cancer treatment can be used more
widely.
The only immunotoxin approved for treating cancer is
gemtuzumab ozogamicin (Mylotarg). It has a toxin called calicheamicin,
attached to an antibody against the CD33 antigen, which is present on
most leukemia cells. Gemtuzumab is used to treat some people with acute
myelogenous leukemia.
Another immunotoxin, BL22, showed promising results in early
studies against some forms of chronic leukemia, even in patients who no
longer responded to chemotherapy. In early clinical trials, about 2 out
of 3 patients had complete responses to the treatment (no evidence of
cancer) that lasted up to 2 years. A newer, improved version of this
immunotoxin, known as HA22 (CAT-8015), is now being studied.
Clinical trials of other immunotoxins are also being done in
people with certain leukemias, lymphomas, brain tumors, and other
cancers.
Go back
to Immunotherapy.
Last Medical Review: 08/25/2009
Last Revised: 10/27/2009
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